June 12, 2013

Aggressive Liver Cancer Tracked to Genetic Driver

By Charles Bankhead, Staff Writer, MedPage Today

Published: June 12, 2013

Reviewed by Robert Jasmer, MD; Associate Clinical Professor of Medicine, University of California, San Francisco

Action Points

  • An oncofetal gene normally silenced in the adult liver contributes to hepatocellular carcinoma through several cellular pathways.
  • Note that the findings confirmed the oncofetal gene SALL4 as a biomarker for an aggressive subtype of HCC that has a poor prognosis and suggest that SALL4 may be a potential therapeutic target in liver tumors harboring the mutated gene

An oncofetal gene normally silenced in the adult liver contributes to hepatocellular carcinoma (HCC) through several cellular pathways, investigators reported.

SALL4-positive tumor specimens overexpressed genes involved in proliferation and metastasis. Blocking the gene's protein released an inhibited tumor suppressor that prevented tumor formation in preclinical models of HCC.

The findings confirmed SALL4 as a biomarker for an aggressive subtype of HCC that has a poor prognosis and established SALL4 as a potential therapeutic target in liver tumors harboring the mutated gene, Daniel G. Tenen, MD, of the Cancer Science Institute of Singapore, and co-authors reported online in the New England Journal of Medicine.

"The absence of SALL4 expression in the healthy adult liver enhances the potential of SALL4 as a treatment target in hepatocellular carcinoma," the authors concluded.

SALL4 has a major role in the maintenance of pluripotency and self-renewal of embryonic stem cells. In preclinical models, SALL4 expression declines gradually during development and is silenced in adulthood. SALL4 has been observed in leukemia and in several types of solid tumors, including HCC.

The observation of expression of SALL4 in the murine fetal liver but not the adult liver led to the hypothesis that SALL4 plays a role in the poor-prognosis, progenitor-like subtype of HCC in adult humans.

To test their hypothesis, Tenen and colleagues compared SALL4 expression in surgically resected HCC specimens of 179 patients and archived specimens from matched patients without HCC. The investigators found that 55.6% of the HCC specimens were SALL4 positive and that the HCC specimens had a significantly higher number of SALL4-expressing cells as compared with the control liver specimens (P<0.001).

By gene-expression microarray analysis, the authors found upregulation of SALL4 in several different groups of HCC specimens. They also detected significantly different (P<0.001) levels of SALL4 expression in 228 matched HCC and non-HCC liver specimens obtained from a different institution.

The investigators analyzed SALL4 expression across 10 HCC cell lines, using polymerase chain-reaction assay techniques. The studies showed consistent expression of SALL4 but at varying levels among the different cell lines. Analysis of two nontransformed liver cell lines showed no SALL4 expression.

To examine the clinical relevance of SALL4 reactivation in HCC, Tenen and colleagues performed clinicopathologic analyses of two independent HCC specimen sets. They found that higher SALL4 expression was associated with worse prognosis, including worse survival, in both sets of specimens (P=0.02 to P=0.002). SALL4-positive HCCs had a gene-expression profile associated with poorly differentiated, aggressive tumors that have a poor prognosis.

Additional studies showed that SALL4 expression had no association with baseline liver function or with the presence or absence of lymph node metastasis.

The authors assessed the importance of SALL4 to HCC by performing SALL4-knock down studies. The resulting loss of function was associated with decreased cell viability, increased apoptosis, and decreased tumorigenicity in HCC cells.

Results of the loss-of-function studies suggested that SALL4 is a potential therapeutic target in HCC. They tested a recently described peptide that blocks interaction between SALL4 and a histone deacetylase-containing nucleosome remodeling and HDAC (NuRD) complex, an interaction necessary for SALL4 to function as a transcription repressor.

The studies showed that the SALL4 peptide decreased viability of SALL4-positive HCC cells by induction of PTEN and that the effect was reversed by a PTEN inhibitor.

"The discovery of a role for SALL4 in hepatocellular carcinoma, its association with prognosis, and the antitumor effects of a newly identified peptide blocker targeting it have potential therapeutic significances," the authors said. "Testing for the presence of SALL4 at diagnosis may be helpful not only for determining the prognosis but also for identifying patients who are likely to have a response to treatment."

The study contributed important new information to the origin and potential treatment of aggressive HCC, according to the authors of an accompanying editorial. However, some questions remain.

"Although these data are convincing, it is not known whether targeting of SALL4 alone would have sufficient antitumor activity or whether inhibition of the associated transcriptomic programs is required to prevent recurrent disease," said Jens U. Marquardt, MD, of the National Cancer Institute, and Snorri S. Thorgeirsson, MD, PhD, of Johannes Gutenberg University in Mainz, Germany.

"Another open question is whether responses to SALL4 inhibition in stemness-associated tumors vary according to the patient's ethnic origin and the cause of hepatocellular carcinoma. This variability has been repeatedly observed in other targeted therapies. Also, the present data do not resolve whether tumors that overexpress SALL4 are derived from reprogrammed hepatocytes or rare stem cells."

An urgent need exists for clinical translation of the findings to guide individualized therapy for HCC and to improve the poor outcome associated with the disease, they added.

The study was supported by the Singapore National Medical Research Council, the Singapore Ministry of Education and the National Research Foundation, and the National Institutes of Health.

Tenen reported no relevant disclosures. One or more co-authors disclosed relationships with sanofi-aventis and Merck.

Primary source: New England Journal of Medicine
Source reference:
Yong KJ, et al "Oncofetal gene SALL4 in aggressive hepatocellular carcinoma" N Engl J Med 2013; DOI: 10.1056/NEJMoa1300297.

Additional source: New England Journal of Medicine
Source reference:
Marquardt JU, Thorgeirsson SS "SALL4 in 'stemness'-driven hepatocarcinogenesis" N Engl J Med 2013; DOI: 10.1056/NEJMe1303026.

Source

B-Cell Lymphomas in HIV/HCV-Coinfected Patients

Published in Journal Watch HIV/AIDS Clinical Care June 10, 2013

The histology of lymphomas in this population differs from that seen in HIV-monoinfected patients, suggesting a novel mechanism of lymphomagenesis.

HIV-monoinfected patients have an increased risk for B-cell non-Hodgkin lymphoma (NHL) — most commonly, high-grade malignancies such as diffuse large B-cell lymphoma (DLBCL) and Burkitt lymphoma. Several studies have suggested that hepatitis C virus (HCV)-monoinfected patients may also have an increased risk for NHL. To understand whether HCV coinfection influences the types of lymphomas seen in HIV-infected patients, investigators in France examined a series of tumors found in HIV/HCV-coinfected and HIV-monoinfected patients.

Forty-one HIV-monoinfected patients and 6 HIV/HCV-coinfected patients with NHL were enrolled in a prospective study between 2007 and 2009. At the time of NHL diagnosis, HIV RNA was undetectable in 4 of the 6 coinfected patients and 16 of the 41 HIV-monoinfected patients; the median CD4 count was 449 and 292 cells/mm3, respectively. In the HIV/HCV-coinfected group, 5 of the 6 cases had features of lymphoplasmacytic lymphoma (LPL) or marginal zone lymphoma (MZL; e.g., mucosal-associated lymphoid tissue lymphoma). In the HIV-monoinfected group, the most common subtype was DLBCL; only 1 case had features of MZL/LPL.

The course of one coinfected patient was notable. After the diagnosis of splenic MZL, he received antiretroviral therapy, with suppression of his HIV RNA but no hematologic response. Subsequent anti-HCV therapy (pegylated interferon and ribavirin) resulted in a dramatic decrease in clonal B cells in his blood coinciding with a drop in HCV RNA level.

Comment: Lymphoma has been associated with several infectious agents, including human herpes virus-8, human T-lymphotropic virus type 1, Epstein-Barr virus, HIV, and Helicobacter pylori. Now, this study suggests that hepatitis C virus coinfection might be linked to particular types of non-Hodgkin lymphoma in HIV-infected patients. The hematologic response to anti-HCV therapy seen in the current study is reminiscent of a previous report describing regression of splenic lymphoma in HCV-monoinfected patients after interferon therapy (N Engl J Med 2002; 347:89) and suggests that, as with Helicobacter-associated lymphoma, chronic antigenic stimulation may contribute to lymphomagenesis.

Rajesh T. Gandhi, MD

Citation(s):

Terrier B et al. Characteristics of B-cell lymphomas in HIV/HCV-coinfected patients during the combined antiretroviral therapy era: An ANRS CO16 LYMPHOVIR cohort study. J Acquir Immune Defic Syndr 2013 Jun 1; 63:249. (http://dx.doi.org/10.1097/QAI.0b013e31828a77f0)

Medline abstract (Free)

Source

Both Simeprevir and Sofosbuvir Likely Approved by 2014 —Clinical/Ethical/Pharmacoeconomic Dilemmas Loom

hcv

Paul Sax • June 11th, 2013

As expected, simeprevir, and now also sofosbuvir, are being given “priority review” by the FDA.

With the 6-month rule under the Prescription Drug User Fee Act — usually just said as “pah-DOOF-ah” — that means there’s a good chance we’ll have both of these anti-HCV drugs some time in late 2013.

Which also means HCV treaters will soon face a major dilemma regarding management of HCV genotype 1.

For those not following this field closely, here’s the deal:

  • If approved, both simeprevir and sofosbuvir will be indicated for treatment of HCV genotype 1, but only in combination with pegylated interferon/ribavirin. (Sofosbuvir approval is also expected for genotype 2/3, just with ribavirin.)
  • Both will be one pill once daily. Simple!
  • Both will cost a lot. Reminder, a course of telaprevir is $50,000, and these two new drugs are better.
  • The interim results of the COSMOS study, presented at CROI this year, showed a >90% cure rate in 80 prior null responders (no cirrhosis) who received simeprevir and sofosbuvir together for 12 or 24 weeks, with and without ribavirin. There was no interferon in this study.  (The full slide set of the presentation is on NATAP.)

So if these two drugs are both approved as expected, one could easily make the case that the best treatment for HCV genotype 1 — in terms of efficacy, safety, tolerability, pretty much everything except drug-drug interactions and cost — will be the COSMOS regimen of simeprevir and sofosbuvir, with or without ribavirin. And emphatically without interferon.

And that, my dear friends, is off-label use.

So let’s get inside the head of the various players in this potential drama to imagine what they’ll be thinking.

It’s January, 2014, and a patient previously treated with interferon/ribavirin for 48 weeks who relapsed is coming in to review his new treatment options. Here are some potential thought balloons:

Patient: I just want what works best. Sure would be nice to avoid all those nasty interferon side effects I had the last time I was treated.
Provider: I’d like to prescribe simeprevir plus sofosbuvir to avoid all those nasty interferon side effects the last time he was treated. I have some uncertainty about whether to include ribavirin, and whether to treat for 12 or 24 weeks.
Provider’s RN/PA/NP/PharmD who manages all HCV treatment:  Sure will be nice to avoid all those nasty interferon side effects that happened the last time he was treated.
Patient’s insurance company: Both simeprevir and sofosbuvir?  Two DAAs? You gotta be kidding me — we’re not paying since the regimen is not FDA-approved. Here’s a toll-free number for you to call and argue the case, but the estimated hold time is longer (by a factor of 10) than trying to call an airline to get a flight changed during a blizzard.
Phamaceutical company: We invested a gazillion dollars to bring these drugs to market. Plus, if you consider the net societal savings by curing HCV and avoiding cirrhosis, liver failure, hepatocellular carcinoma, liver transplants, secondary transmission etc, the price is justified.
Activists:  The best treatment should be available for all!
Academic MD expert who has been asked to comment, but isn’t actually seeing this patient (or any patient) today because he/she is writing grants and papers, or traveling:  The sample size of the COSMOS study is too small to influence clinical practice.

Of course, this will all settle out once there are multiple non-interferon HCV treatment options out there.

Source

Mental Health Screening in HIV: Guideline and Commentary

Francine Cournos, MD

Jun 12, 2013

Mental Health Screening in HIV: Expert Commentary

Nothing is more frightening to many healthcare providers than being faced with patients who are exhibiting abnormal behavior. People who are obviously mentally impaired are often strongly discriminated against in medical care settings and often receive very poor healthcare, even when they have life-threatening medical emergencies.

Knowing how to assess people who present with abnormal mental states is a critical component of essential medical care. The Mental Health Screening Quick Reference Guide from the New York State Department of Health (NYS DOH) AIDS Institute can help clinicians in assessing the mental health status of HIV-infected patients.

The conditions that we label mental illnesses are on a continuum with physical illnesses, and this may be particularly important to consider in people with advanced HIV infection. For example, a change in mental status, especially when it is sudden and associated with confusion and a fluctuating level of consciousness, is highly suggestive of delirium. Delirium is a medical emergency with numerous causes, including liver failure, kidney failure, opportunistic infections, space-occupying lesions of the central nervous system, hypoxia, metabolic disturbances, a high fever of any cause, and HIV itself.

Therefore, the first step in assessing a patient's abnormal mental state is to evaluate the patient for serious medical conditions. This is true even if the patient has a known psychiatric history, because severely ill psychiatric patients often also present with serious untreated medical conditions. Note that evaluating agitated patients may require assistance from other hospital staff -- it is always important to ensure your own safety as well as that of the patient.

Also at the boundary of mental illness and medical illness is the large number of alcohol- and drug-related conditions. Alcohol withdrawal is a common cause of abnormal behavior and can result in death from seizures and hyperpyrexia if left untreated.

Another type of medical and psychiatric emergency is the patient who presents with or is imminently at risk for a suicide attempt. Those who have made attempts may need urgent medical treatment, and all require immediate supervision to prevent further harm. An effective screening and triage approach is essential to managing these patients.

Ultimately, however, the most common mental disorders seen in people with HIV infection are mood disorders; anxiety disorders, including post-traumatic stress disorder (PTSD); and alcohol or other substance use disorders. Indeed, key populations most at risk for HIV infection often have high rates of mental illness, even before becoming HIV infected. For example, men who have sex with men typically have higher rates of substance use, mood, and anxiety disorders compared with the general population, whereas sex workers, especially those who work outdoors, have high rates of substance use disorders and PTSD.

Biological, psychological, and psychosocial factors can influence the ways in which mental disorders can be caused by or exacerbated by HIV infection. Major depression is of particular importance and is best conceptualized as a medical comorbidity of HIV infection. The symptoms of depression are as much physical as they are mental, and some patients report few or no psychological disturbances but instead present with severe fatigue accompanied by numerous physical symptoms.

Emerging evidence suggests a bidirectional relationship between depression and inflammation, whereby one disorder makes the other more likely. This may help explain why approximately one third of patients with HIV infection suffer from major depression, and why major depression is associated with increased morbidity and mortality from HIV infection. In addition, because major depression is associated with failure to access and adhere to HIV care and treatment, it is clearly worthy of treatment in its own right in people with HIV, independent of its broader effects.

Finally, the direct effect of HIV on the brain can cause cognitive impairment. Although tools can be used to screen for HIV-associated dementia, much more common forms of milder or asymptomatic cognitive impairment can be more difficult to assess. A collaborative approach between primary care and mental health providers is critical to ensuring that full evaluations and neuropsychological testing are performed as needed.

Mental Health Screening in HIV

Editor's Note: This guideline was prepared by the New York State Department of Health (NYS DOH) AIDS Institute HIV Clinical Guidelines Program and was originally published in graphical format as Mental Health Screening: A Quick Reference Guide for HIV Primary Care Clinicians. A text-based version was developed by NYS DOH and has been published here.

Overview

People with HIV are more likely to experience mental health symptoms than are those in the general population.[1] Depression, anxiety, PTSD, and cognitive impairment are among the most common disorders. Risk for suicide or violence may be present. Any sudden change in cognitive function, consciousness, or behavior should prompt immediate assessment for delirium caused by an acute medical complication.

The Mental Health Screening Quick Reference Guide may be used in the primary care setting to perform routine mental health assessment for HIV-infected patients.

All HIV-infected patients should receive baseline and ongoing assessment of the followinga:

  • Mental health disorders:

    • Depression (every visit)

    • Anxiety (at least annually)

    • PTSD (at least annually)

  • Cognitive function (at least annually)

  • Sleep habits and appetite (every visit)

  • Psychosocial status (at least annually)

  • Suicidal/violent ideation (every visit)

  • Alcohol and substance use (at least annually) b

aFor most patients, mental health screening requires approximately 10-20 minutes.
bAt-risk drug and alcohol users should be screened more frequently to identify escalation of present levels of use or harmful consequences from use.

The complexity of mental health diagnosis and treatment in the setting of HIV often requires a collaborative approach between primary care and mental health providers (ie, psychiatrists, psychologists, clinical social workers, and psychiatric nurse practitioners).

Assessments and Screenings

Assessment for Depression, Anxiety, and PTSD

A brief screening tool, such as the Patient Health Questionnaire (PHQ-2), may be used for routine depression screening. Annual mental health screening for depression, anxiety, and PTSD can be performed with the Substance Abuse/Mental Illness Symptoms Screener (SAMISS) questionnaire,[2] which is a comprehensive mental health screening tool that has been validated in HIV-infected patients. A positive screen from these tools should prompt further evaluation by a member of the healthcare team and, if necessary, referral to a mental health provider.

For the PHQ-2 and other screening tools, see Mental Health Screening Tools. For questions from the SAMISS questionnaire that can be used for annual assessment, see the Mental Health Screening Quick Reference Guide.

Assessment of Cognitive Function

Early motor and cognitive slowing may be detected with the International HIV Dementia Scale, which can be administered by nonneurologists and has been validated in HIV-infected patients.[3] To access the International HIV Dementia Scale, refer to Mental Health Screening Tools.

Assessment of Sleep and Appetite

Sleep and appetite are important elements of a mental health assessment. Insomnia occurs frequently in HIV-infected patients and during all stages of HIV disease,[4] and weight loss is a strong predictor of HIV disease progression.[5] Resources for sleep and appetite include:

Substance Use Screening

A positive screen from any one of the following tools indicates the need for additional evaluation for substance use disorders:

  • Single Alcohol Screening Question;

  • The Two-Item Conjoint Screen (TICS); or

  • CAGE-AID (CAGE-Adapted to Include Drugs).

For these and other available tools, see the Substance Use Screening Quick Reference Guide. For additional information on substance use screening, see Screening and Ongoing Assessment for Substance Use.

Screening for and Management of Acute Suicidal or Violent Ideation or Behavior

The following algorithm can be used in the HIV primary care setting to screen for the risk for acute suicidal or violent ideation or behavior.

805386--figure-1

Algorithm for screening for the risk for acute suicidal or violent ideation or behavior.

Considerations for Mental Health Referral

Successful mental health referral involves communication between medical and mental health providers, as well as patient education. Referral to a mental health provider is warranted when a patient presents with:

  • Risk for violence to self or others;

  • Psychosis, including delusions, hallucinations, flight of ideas, and disordered thinking;

  • Poor response or relapse of psychiatric symptoms while receiving medication/treatment; or

  • Active substance abuse or relapse to substance use with mental health disorder.*

*Refer to a program for dually diagnosed patients.

Additional Considerations

HIV-Related Triggers of Mental Distress

Clinicians should be aware of triggers that can cause mental distress, such as:

Learning of HIV status and disclosure to sex partners, family, and friends;

Physical illness, diagnosis of a sexually transmitted disease, introduction of antiretroviral medications, or AIDS diagnosis;

Hospitalization (particularly first hospitalization);

Life changes (eg, death of a significant other, end of relationship, job loss); or

Necessity of making end-of-life permanency-planning decisions.

Elements of a Psychosocial Assessment

The following assessment may help determine the need for additional support:

Stability of housing,* employment, and government assistance, and level of education

Support network and safety:

   ✓ Does the patient have contact with family and friends? Are they aware of the patient's HIV status?

   ✓ Does the patient have a partner? Is the patient afraid of his/her partner or someone else close?

Legal issues, including end-of-life arrangements

*Contact information, housing, and support network should be closely monitored for patients with unstable living situations.

Prescribing Considerations

Use of full prescribing information, knowledge of drug/drug interactions, and patient education are important components of effective psychopharmacologic treatment. Consultation with a psychiatrist experienced in HIV treatment may be warranted.

References

  1. Bing EG, Burnam MA, Longshore D, et al. Psychiatric disorders and drug use among human immunodeficiency virus-infected adults in the United States. Arch Gen Psychiatry. 2001;58:721-728. Abstract

  2. Pence BW, Gaynes BN, Whetten K, Eron JJ Jr, Ryder RW, Miller WC. Validation of a brief screening instrument for substance abuse and mental illness in HIV-positive patients. J Acquir Immune Defic Syndr. 2005;40:434-444. Abstract

  3. Sacktor NC, Wong M, Nakasujja N, et al. The International HIV Dementia Scale: a new rapid screening test for HIV dementia. AIDS. 2005;19:1367-1374. Abstract

  4. Reid S, Dwyer J. Insomnia in HIV infection: a systematic review of prevalence, correlates, and management. Psychosom Med. 2005;67:260-269. Abstract

  5. Colecraft E. HIV/AIDS: nutritional implications and impact on human development. Proc Nutr Soc. 2008;67:109-113. Abstract

Source

Staying Informed: Anticipating New Regimens with Direct Acting Antivirals for Hepatitis C

United States Department of Veterans Affairs

for Health Care Providers

The approval of two hepatitis C virus (HCV) protease inhibitors by the U. S. Food and Drug Administration in 2011--boceprevir and telaprevir--marked the start of a new chapter in hepatitis C treatment. These were the first new drugs approved in 10 years for hepatitis C treatment. With boceprevir and telaprevir, triple combination therapy for patients with genotype 1 HCV infection has become available, combining peginterferon and ribavirin with either of these two agents. This represents a huge advance in hepatitis C treatment, with improved sustained viral response (SVR) rates among patients who had never been treated before as well as among patients who had relapsed after treatment or did not fully respond to standard treatment.

But the story of hepatitis C treatment will not end here. Several new drugs are being developed for all strains of HCV, not just genotype 1. At this writing, no other new drugs are yet FDA approved or available for use, but several new agents may be approved in the next few years, making new treatment regimens available for patients.

All of these new drugs are called "DAAs"--direct acting antivirals. There are four major different HCV DAA classes:

  1. HCV NS3/4 Protease Inhibitors
  2. Nucleos(t)ide HCV NS5B Polymerase Inhibitors
  3. Non-nucleos(t)ide HCV NS5B Polymerase Inhibitors
  4. HCV NS5A Inhibitors

DAAs Under Development

HCV NS3/4 Protease Inhibitors Nucleos(t)ide HCV NS5B Polymerase Inhibitors Non-nucleos(t)ide HCV NS5B Polymerase Inhibitors HCV NS5A Inhibitors
Telaprevir Sofosbuvir BI-207127 Daclatasvir
Boceprevir Mericitabine VX-222 Ledipasvir (GS-5885)
Danoprevir ABT-333 ABT-267
Simeprevir BMS-791325
ABT-450 (with ritonavir) Tegobuvir
Faldaprevir GS-9669
Asunaprevir
GS-9451

While boceprevir and telaprevir currently can only be used in combination with peginterferon and ribavirin, studies are currently exploring other new drug regimens using DAAs with and without interferon.

  • Interferon-containing treatment: combining one of the new DAAs with peginterferon plus ribavirin.
  • Interferon-free treatment: combining DAAs with each other and/or with ribavirin, for regimens which do not use interferon at all and are "interferon-free."

It is far too early to know which new drug combinations, if any, will receive FDA approval or when. But it is important to be aware that Phase 2 and Phase 3 current trials are showing increased SVR rates, shortened durations of treatment, and acceptable adverse event profiles, creating intriguing possibilities for patients who have not been candidates for hepatitis C treatment because of the toxicities caused by interferon. However, it is also important to know that these results have been obtained in carefully selected clinical trial populations and that effectiveness in the real-world is unlikely to be as high. In addition, the relatively small numbers of patients treated in these trials mean that these new drugs may show unexpected side effects.

Knowing that newer HCV treatment regimens with better efficacy and safety may be available in the next few years, you will likely consider for each of your HCV patients the question of whether it is best to treat them now with or whether to defer treatment and wait for more DAAs to become available.

Reasons to treat a patient now:

  • Treatment earlier in the course of HCV infection is associated with higher SVR rates, an important consideration since SVR is associated with a greatly decreased risk of progression to advanced liver disease and death.
  • Current SVR rates with triple therapy for genotype 1 patients are better than ever.
  • The patient already has advanced fibrosis (stage 3 or 4) and deferring treatment could allow further disease progression and decompensation towards decompensation.
  • There is no guarantee that drugs under development will be available in a reasonable period of time, nor that their efficacy and toxicity will be as favorable as in early studies.

Reasons to defer treatment until future drugs become available:

  • Current regimens have are highly complex and impose significant pill burdens and other logistic issues on patients.
  • Future regimens may have a significantly better benefit-risk profile than currently available therapies.
  • A high rate of adverse events with current therapies.
  • Some patients who may have contraindications to interferon may be candidates for an interferon-free regimen with potentially less toxicity.

Regardless of whether providers and patients decide to initiate treatment now or defer anti-viral therapy, the following principles are critical:

  • All patients with HCV should be evaluated for candidacy for anti-viral treatment, including those with a history of depression, substance use disorders, alcohol use disorders, or other psychiatric comorbidities.
  • Patients with psychiatric comorbidities that represent contraindications to anti-viral treatment should be offered effective, evidence-based treatments for such comorbid conditions.
  • Patients who are not immediate candidates for anti-viral treatment should be periodically re-evaluated to determine whether they may benefit from such treatment.

Rena K. Fox, MD

May 30, 2013

Source

Treat now or wait?

United States Department of Veterans Affairs

for Veterans and the Public

Frequently Asked Questions

Q: With new hepatitis C drugs likely to come on the market, should I get treated now or wait?

Choosing when to start on treatment is a decision that only you and your provider can make. Hepatitis C treatment currently involves a combination of two or three drugs: pegylated interferon, ribavirin and sometimes telaprevir or boceprevir. These combinations can cause unpleasant side effects, including fatigue, depression, nausea, anemia, and rash. And the treatment doesn't always get rid of the virus.

However, new drug regimens are under study, which may be easier to take, may have fewer side effects, may need shorter duration of treatment, and may have much higher chances of getting rid of the virus.

So how do you decide if and when to get treated?

In general, the current treatments should be used for patients whose hepatitis C is more advanced. These patients shouldn't wait for new drugs if they can safely tolerate the treatment.

If you have mild liver damage, which is progressing at a very slow rate, waiting for new drugs to be developed might be a better choice. Even if you have had the virus for several years, or have a high viral load, there usually isn't a need to get treated right away if there isn't much liver damage.

There are other reasons why your provider may decide not to start you on treatment:

  • You may have serious liver damage and complications of liver disease and may be too ill to tolerate the currently available medications.
  • You may not have a strong likelihood of responding to the current medications because of your genotype, viral load, or other medical problems.
  • You may have other medical or psychiatric problems, such as chronic lung disease, heart failure, or severe depression, which could be worsened by taking medications for your hepatitis C.
  • You may be trying to conceive children or not be using regular birth control methods, and the ribavirin would be harmful to a fetus.
  • You may be drinking alcohol heavily or using drugs, which would interfere with the hepatitis C therapy.
  • You may have other issues or priorities in your life (such as preparing for an upcoming move, taking care of young children at home, or having travel commitments with your work) that would make the treatment, the side effects, and the necessary follow-up too difficult to manage at the current time.

Under these circumstances, the better option is "watchful waiting." Watchful waiting means that your health care provider carefully monitors the progression of your hepatitis C, keeping treatment with currently available medications in mind as an option.

Watchful waiting means close follow up and observation while not on treatment:

  • You MAY have liver enzyme blood tests done once or twice a year
  • You MAY consider having a liver biopsy every 3 to 5 years
  • You do NOT need to have the hepatitis C "viral load" rechecked or repeated
  • You SHOULD be going to regular doctor appointments
  • You SHOULD be following your doctor's lifestyle recommendations, such as avoiding alcohol, getting to or keeping a normal body weight, and treating other conditions such as diabetes and high cholesterol, so you will limit any further damage to your liver

Rena K. Fox, MD

June 04, 2013

Source

Daily Pill Cuts HIV Risk in IV Drug Users

160380253

By Michael Smith, North American Correspondent, MedPage Today

Published: June 12, 2013

Reviewed by Robert Jasmer, MD; Associate Clinical Professor of Medicine, University of California, San Francisco

Action Points

  • Tenofovir (Viread) once a day can prevent HIV transmission among injection drug users.
  • Note that the study suggests that pre-exposure prophylaxis should be considered as an additional prevention method, along with such things as needle exchanges, promotion of safer sex and injecting practices, and counseling

(Viread) once a day can prevent HIV transmission among injection drug users, researchers reported.

In a randomized, phase III trial, daily tenofovir reduced the risk of HIV by nearly half, compared with placebo, in a cohort of injection drugs users in Bangkok, according to Michael Martin, MD, of the CDC, and colleagues.

The study is the latest to show that so-called pre-exposure prophylaxis (PrEP) can protect people at high risk for HIV from infection, Martin and colleagues reported online in The Lancet.

Previous research has shown that tenofovir PrEP -- either alone or in combination with emtricitabine (Emtriva) -- can reduce the risk of infection in men who have sex with men, in heterosexual men and women, and in heterosexual couples where one partner has HIV and the other does not.

"This study completes the picture of PrEP efficacy for all major HIV risk groups," Martin said in a statement. "We now know that pre-exposure prophylaxis can be a potentially vital option for HIV prevention in people at very high risk for infection, whether through sexual transmission or injecting drug use."

But an outside expert cautioned that the study does not show clearly that PrEP prevents HIV transmission caused by sharing needles.

There's "no biological marker" that can distinguish between HIV acquired through sex and HIV transmitted by needles, noted Salim Abdool Karim, MBChB, PhD, of the University of KwaZulu-Natal in Durban, South Africa.

It's likely that at least some of the observed efficacy was due to reduced sexual transmission, he argued in an accompanying commentary piece.

Nonetheless, Karim concluded, "the overall result is that daily tenofovir does reduce HIV transmission in injecting drug users" and PrEP should be considered as an additional prevention method, along with such things as needle exchanges, promotion of safer sex and injecting practices, and counseling.

The researchers enrolled 2,413 volunteers -- ages 20 through 60, HIV-negative, and reporting injecting drugs within the previous 12 months -- from 17 drug-treatment clinics in Bangkok.

Study participants were randomly assigned on a one-to-one basis to either tenofovir or placebo and followed for an average of 4 years. They were offered condoms and methadone treatment and got monthly HIV testing, combined with risk-reduction and adherence counseling and blood safety tests every 3 months.

Two participants had HIV at enrollment (both in the placebo group) and 50 became infected during follow-up.

Of those, 17 were in the tenofovir arm, for an incidence of 0.35 per 100 person-years, and 33 were in the placebo group, for an incidence of 0.68 per 100 person-years.

Those rates yielded a 48.9% reduction in HIV incidence among those taking the drug, which was significant at P=0.01.

The drug was safe and well tolerated, the researchers reported, with only two significant differences in adverse events: 8% of those getting tenofovir reported nausea and or vomiting, compared with 5% in the placebo arm, which was significant at P=0.002.

And 53% of tenofovir volunteers had grade 1 or 2 elevations in alanine aminotransferase, compared with 49% of those getting placebo, which was significant at P=0.003.

As in previous PrEP trials, adherence was an important factor in efficacy, Martin and colleagues noted.

For instance, in a case-control substudy among participants in the tenofovir arm, the risk of HIV infection was reduced 70% for those in whom tenofovir was found, compared with participants without detectable tenofovir in their blood, the researchers reported.

"These results underscore the importance of helping people using pre-exposure prophylaxis achieve effective levels of adherence," Martin said.

The study had support from the CDC and the Bangkok Metropolitan Administration. One author reported financial links with Gilead. but all other authors, including Martin, said they had no conflicts, according to the journal.

Abdool Karim was the co-principal investigator of the CAPRISA 004 tenofovir gel trial, and is a co-inventor on two pending patents of tenofovir gel against HSV-1 and HSV-2 with scientists from Gilead Sciences, according to the journal.

Primary source: The Lancet
Source reference:
Choopanya K, et al "Antiretroviral prophylaxis for HIV infection in injecting drug users in Bangkok, Thailand (the Bangkok Tenofovir Study): a randomised, double-blind, placebo-controlled phase 3 trial" Lancet 2013; DOI: 10.1016/S0140-6736(13)61127-7.

Additional source: The Lancet
Source reference:
Abdool Karim SS "HIV pre-exposure prophylaxis in injecting drug users" Lancet 2013; DOI: 10.1016/S0140-6736(13)61140-X.

Source

CDC: Unsafe injections a growing problem

JUN 12, 2013

By: Christine Blank

Unsafe injections remain a problem in the United States and throughout the world, according to a recent Centers for Disease Control and Prevention’s (CDC) Morbidity and Mortality Weekly Report

While injection safety had been a public health issue mainly in low-income and middle-income country settings, overall incidents have increased substantially in recent years. Since 2001, at least 49 outbreaks have occurred because of contamination of injectable medical products, according to the CDC. Globally, the burden of disease from unsafe injections in 2000 included approximately 20 million new hepatitis B virus infections, 2 million new hepatitis C infections, and 250,000 new HIV infections.

The CDC believes proposed engineering solutions may help prevent syringe reuse in the future. Proposals include the redesign of syringes to change color after use or the incorporation of tamper-evident packaging.

In addition, CDC and its partners in the Safe Injection Practices Coalition have developed the One & Only campaign. “The ultimate goal of the campaign is to prevent outbreaks, infections, and the need for patient notification,” the CDC stated. “Recognizing that education is necessary but not always sufficient, policies and mechanisms must be in place to support and ensure that injection safety and infection control procedures are followed [and] to mandate corrective action,” the agency added.

As part of increased patient involvement in medical decision-making, The One & Only campaign encourages patients to ask their healthcare provider about bloodborne pathogen safety.

The CDC has implemented the 4 “Es” to help prevent unsafe injection practices. They include epidemiologic surveillance, reporting, monitoring, and investigation of outbreaks potentially related to unsafe injections; educational initiatives to promote understanding and use of safe injection and basic infection control practices; enforcement and oversight by federal and state authorities; and engineering of devices, equipment, and processes to reduce or eliminate disease transmission risks.

Source

Cirrhotic ascites review: Pathophysiology, diagnosis and management

World J Hepatol. 2013 May 27; 5(5): 251-263.

Published online 2013 May 27. doi: 10.4254/wjh.v5.i5.251.

©2013 Baishideng Publishing Group Co., Limited. All rights reserved.

Christopher M Moore and David H Van Thiel.

Christopher M Moore, David H Van Thiel, Section of Hepatology, Department of Medicine, Rush University Medical Center, Chicago, IL 60612, United States

Author contributions: Moore CM contributed to conception, drafting and revision, and final approval of this article; Van Thiel DH contributed to the conception, drafting and revision, and final approval of this article.

Correspondence to: Christopher M Moore, MD, Section of Hepatology, Department of Medicine, Rush University Medical Center, 1725 W Harrison St, Chicago, IL 60612, United States. christopher_moore@rush.edu

Telephone: +1-312-9425861 Fax: +1-312-5633945

Received February 16, 2013; Revised April 13, 2013; Accepted April 18, 2013;

Abstract

Ascites is a pathologic accumulation of peritoneal fluidcommonly observed in decompensated cirrhotic states.Its causes are multi-factorial, but principally involve significant volume and hormonal dysregulation in the setting of portal hypertension. The diagnosis of ascites is considered in cirrhotic patients given a constellation of clinical and laboratory findings, and ultimately confirmed, with insight into etiology, by imaging and paracentesis procedures. Treatment for ascites is multi-modal including dietary sodium restriction, pharmacologic therapies, diagnostic and therapeutic paracentesis, and in certain cases transjugular intra-hepatic portosystemic shunt. Ascites is associated with numerous complications including spontaneous bacterial peritonitis, hepato-hydrothorax and hepatorenal syndrome. Given the complex nature of ascites and associatedcomplications, it is not surprising that it heralds increased morbidity and mortality in cirrhotic patients and increased cost-utilization upon the health-care system. This review will detail the pathophysiology of cirrhotic ascites, common complications derived from it, and pertinent treatment modalities.

Keywords: Ascites, Cirrhosis, Hepato-hydrothorax, Hepatorenal syndrome, Spontaneous bacterial peritonitis

Core tip: Ascites is an accumulation of fluid most commonly found in cirrhosis with portal hypertension. Ascites can cause or is associated with a number of complications including spontaneous bacterial peritonitis, hepato-hydrothorax and hepatorenal syndrome. Ascites itself, and these associated complications are a significant cause of morbidity and mortality in cirrhotic patients. The management of ascites is complex, utilizing an array of medications and interventional therapies to maintain appropriate total body volume, prevent multi-organ dysfunction, and manage against increased risk for associated infections.

INTRODUCTION

Ascites is a very common manifestation of decompensated cirrhosis and represents a pathologic accumulation of fluid within the peritoneal cavity[1-3]. The term “ascites” is derived from the Greek term “askos” in reference to its similar appearance to a winebag or sac. This seems rather appropriate, both in description of presentation and as an allusion to a main cause of cirrhosis. The term “ascitic fluid” is also utilized in the literature however it is in a way redundant. The clinical presentation of ascites has been described since antiquity, reasonably inferred from passages in the Egyptian medical text, the Ebers Papyrus c. 1550 BCE[4].

Cirrhotic ascitic fluid accumulation results from a number of factors broadly defined in terms of hormonal and cytokine dysregulation and related volume overload in the setting of portal hypertension[1]. The manifestation of ascites is an important landmark in the progression of cirrhosis: (1) it is the most common cause for hospital admissions and thus contingent costs; (2) it portends increased 1-year mortality; and (3) functions as a risk-stratification marker for orthotopic liver transplantation (OLT)[1,5-7]. This review will characterize the pathophysiology of cirrhotic ascitic fluid formation, the complications surrounding ascites, and basic medical management of these processes.

PATHOPHYSIOLOGY

For the purposes of this discussion, the focus will be on cirrhotic ascites, in the setting of portal hypertension, which comprises approximately 85% of all cases[1,2,5].Other causes of ascites (non-cirrhotic)can be broadly defined as pre- or post-hepatic in origin. Pre-hepatic causes might include: portal vein thrombosis, lymphoma, abdominal lymphatic injury or obstruction, bowel perforation, renal failure, pancreatitis, peritoneal tuberculosis, or a malignancy with peritoneal implants. Post-hepatic causes include congestive heart failure usually associated with pulmonary hypertension, constrictive pericarditis, the Budd-Chiari syndrome, and stricture/web formation in the inferior vena cava (IVC)[1,5]. This latter category, regarding IVC stricture/web formation, is likely to manifest rather slowly overtime as obstruction to critical flow progresses.

Malignant ascites, which is found in 10% of cases, can occur as a result of any neoplastic disease having peritoneal metastasis, but is more common with breast, bronchus, ovary, gastric, pancreatic or colon cancer. Up to 20% of cases of malignant ascites have a tumor of unknown origin. Most cases of malignant ascites have a high protein content[8-10]. Because there are multiple potential causes of ascites other than liver disease and/or portal hypertensive origin, non-hepatic disease processes should be ruled out through clinical history and by utilizing specific laboratory testing and imaging. As an example, in the setting of chronic pancreatitis with associated pseudocyst and internal fistulae formation, significant fluid can directly enter into the peritoneal cavity and manifest as abdominal distension with pain. In particular an elevated ascitic fluid amylase level, found on diagnostic paracentesis, is strongly diagnostic for this category. The physician might be especially sensitive to this diagnosis in a patient with a significant history of alcohol use, chronic pancreatitis and steatorrhea. Notably, the serum-ascites albumin gradient (SAAG) is a useful tool for segregating ascites-associated disease processes due to portal hypertension, such as cirrhosis, from the many other non-portal hypertensive causes of ascites[11]. A SAAG value ≥ 1.1 g/dL strongly supports (97% sensitivity) a diagnosis of portal hypertension as causal[11].

Despite its well known presentation, the pathogenesis of ascites remains incompletely understood and continues to evolve. A hybrid theory currently prevails, having arisen out of the “overflow” and “underfill” theories of the past generation[1,2,5]. A brief sketch of these views suggests the following: (1) continuous injury to the liver as a combination of both exogenous factors, e.g., chronic alcohol or viral or non-alcoholic steatohepatitis (NASH) injury; (2) in the setting of an appropriate genetic disposition; and (3) continued micro-processes of inflammation, necrosis and collagen deposition/regeneration, all conspiring to transform the liver from a low-resistance to a high-resistance system, e.g., a spectrum of fibrosis with vascular smooth muscle dysfunction[11]. These continued processes can lead, in aggregate, to increased pressure in the portal vein, i.e., portal hypertension. The portal vein is normally approximately 8 cm in length and usually < 13 mm in diameter. It is formed by the union of the splenic and superior mesenteric vein systems; the inferior mesenteric vein enters one of these vessels, or at their junction, quite variably. Portal hypertension is defined as being 6 mmHg or greater as measured by the wedged hepatic vein gradient, and in particular, ascites formation usually occurs at 8 mmHg or greater. For completeness, it is noted that further clinical decompensation in the form variceal formation (10 mmHg), increased risk of variceal bleeding (12 mmHg) and risk for recurrent variceal bleeding (20 mmHg), correlate nicely with these increasing portal pressures[12-16]. This clinical sequence portends significant morbidity and mortality and can be interlaced with relatedfurther complications of hepatic encephalopathy (HE), spontaneous bacterial peritonitis (SBP), hepato-hydrothorax (HHT) and hepatorenal syndrome (HRS)[12].

Thus in the setting of portal hypertension, backflow and stasis of vasodilatory substances, e.g., nitric oxide, begin to accumulate[17]. This causes, amongst other results splanchnic vasodilation with resultant hypoperfusion (although even when globally euvolemic or hypervolemic) of the renal system. Appropriately in this sense, therenin-angiotensin-aldosterone system (RAAS) is activated leading to aggressive fluid retention[18-20]. In brief, renin is secreted from the renal juxtaglomerular apparatus (JGA) around the proximal nephrons in response to changes in vascular pressures, changes in serum sodium, and from activation of the sympathetic nervous system[17]. It in turn will convert angiotensinogen (made in the liver) to angiotensin I which is further converted to angiotensin II by angiotensin converting enzyme (ACE) in the lungs[17-19]. Angiotensin II has multiple important functions that drive fluid acquisition and retention, including stimulation of the thirst drive, release of aldosterone from the zona glomerulosa of the adrenal cortex, and secretion of vasopressin from the posterior pituitary[17-19]. This excess retained blood volume is thought to leak-out (filtered in a sense) directly from both the liver surface, and the mesenteric vessels. This latter mechanism is due to increased hydrostatics and vascular wall permeability, and concurrently decreased oncotic (osmotic) fluid retention in the form of absolute or relative hypoalbuminemia. These three parameters, as described in the classical Starling equation, overwhelm the reabsorptive capacity of the peritoneal surface and lymphatic system[17-19].

Normally, the peritoneal cavity is decompressed and has a pressure of 5-10 mmHg, containing approximately 25-50 mL of serous fluid. This fluid normally provides a low resistance film over which bowel can move past each other and further hydrates the serosal surfaces maintaining pliability and integrity. The maximum absorption of fluid out of the peritoneum is approximately 850 mL/d in optimal settings. This property of absorption (selective filtration) provides the theory under which peritoneal dialysis operates[21,22]. It can be observed that alterations in the properties of the lymphatic system or the peritoneal surface area, either by inflammatory, infectious or fibrotic/mechanical processes can alter optimal re-absorption. Thus, continued dysregulation of these parameters can lead to profound ascitic fluid retention.

CLINICAL PRESENTATION

Ascites represents a very common manifestation of decompensated cirrhosis and thus on presentation[1,12] if cirrhosis has not already been defined for the patient, risk factors for its usual precursors, namely alcoholic use, viral hepatitis and NASH should be explored[1,12]. The clinical presentation of ascites is variable: it can occur slowly as observed in common and classical liver diseases, or suddenly as in new mechanical obstruction to the major vessels. For instance, hepatic or portal vein thrombosis, compression of the IVC due to trauma with a hematoma or infection, or acute hepatic failure. In the setting of thrombosis, causes for a hypercoaguable state should be sought: infectious, inflammatory, malignancy or hematologic genetic dispositions.Ascites can be painless, and if it is associated with abdominal pain may simply represent discomfort from mechanical distension, or super-imposed infection as in SBP, or even hepatocellular carcinoma[12,23]. Thus, while ascites represents a natural progression of cirrhosis, its appearance should prompt a careful investigation for other causes and complications as well[12].

An increase in abdominal girth can be due to a few generic processes. An increase in the width of the abdominal wall itself, i.e., an enlarging panniculus; or it can represent the accumulation of solid, gas or liquid within the intestines or peritoneal space. Solid causes can represent retained and accumulating stool in constipation, or a malignant mass such ovarian cancer. Gaseous distension can also be observed in those with constipation or small intestinal bacterial overgrowth. Liquid retention, when focused, can represent a cystic object or loculated ascites. When the liquid is distributed uniformly, one certainly considers non-complicated ascites from liver or other sources (vida supra). The most common clinical complaints associated with liver related-ascites are an increase in abdominal girth, abdominal fullness, discomfort or ache, shortness of breath, early satiation and a sense of reduced mobility[12,22,24]. These symptoms are sensibly scaled to the actual amount of volume. Ascites can be of three severities: grade I, wherein it is diagnosed by abdominal ultrasound, which requires approximately 100 mL of fluid within the peritoneum (recall that normal volume is approximately 25-50 mL); grade II, implying at least 1000 mL of peritoneal fluid, which can be detected with physical examination through the classic exam findings of sagging flanks, shifting dullness, fluid-wave, and the more laborious and rarely utilized Puddle’s sign;grade III, manifested as a grossly distended abdomen, implying liters of ascitic fluid. This final grade can elicit a severe form of discomfort, and may be described as a tense ascites[1,12,22,24].

PARACENTESIS AND LABORATORY TESTING

Proper evaluation of ascites rests upon direct assessment through paracentesis: to characterize the fluid origin, and whether it is sterile, infectious and/or malignant. Unfortunately, there has been much lore related to the contra-indications and complications of this procedure. As with any procedure, coagulation status is a reasonable concern, and indeed in cirrhotics with ascites their coagulation status is altered but it is not at all obvious in which direction (pro- or anti-coagulant)[25]. Certainly there is a deficiency in the production and/or activity of coagulation compounds as would be indicated by the altered international normalized ratio (INR), but this parameter does not measure all coagulation factors, e.g., protein C - a procoagulant. The idea that these patients are “auto-anticoagulated” is not true, and they can in fact be at real risk for thrombo-embolic disease[26]. Considering this problematic background, one must look at the empiric data, and although limited, suggests that paracentesis has been well-tolerated in patients with platelet counts below 20000 cells/mm3 and an INR as high as 8.7[27-29]. Complications of wall hematoma requiring transfusion and infection are remote. A reasonable absolute contra-indication would be in disseminated intravascular coagulation[12]. The evidence for requisite transfusions of blood products, by non-hepatology procedural services, to meet the arbitrary limits of an INR < 1.5 or platelets > 50000 cells/mm3 is unfounded, wasteful in resources and time, and itself incurs risks of transfusion reactions.

A diagnostic paracentesis, as opposed to a therapeutic paracentesis (vida infra), requires approximately 30-50 mL, and is mandatory in all cases of new onset ascites or ascites occurring in an individual with a change in clinical status to include fever, abdominal pain, new onset or worsening HE and any sign or symptom of infection generally. Paracentesis may be revealing for SBP even in hospital admissions not thought related to hepatic disease, e.g., a presentation of weakness with painless ascites[24,28]. Ascitic fluid analysis in all cases should include cell counts and differential, albumin and total protein, and ascitic fluid culture aliquoted at the bedside[28]. Other studies depending upon the clinical situation or appearance of the ascitic fluid can include lactate dehydogenase (LDH), cytology, amylase, glucose, total protein (TP), and triglycerides[12].

In regards gross appearance, ascitic fluid that is non-neutrocytic nor infected should be clear to yellow and transparent. In normal ascitic fluid the neutrophil count should be < 250 cells/mm3, wherein the neutrophils are usually presented as a percentage of the total white blood cell (WBC) count. A common misinterpretation is to read this percentage as the absolute number of neutrophils, potentially missing a diagnosis of SBP. An elevated WBC count itself is certainly indicative of inflammation, and usually, but not definitively of infection, e.g., SBP[12,28]. Other molecules such as lactoferrin have been evaluated for utility as sensitive ascitic biomarkers of infection but have yet to yield cost-effective results[30,31]. In the setting of peritoneal dialysis patients, lower thresholds for peritoneal infection have been described[32], e.g., > 50 neutrophils/mm3. In cases of “bloody taps”, a correction factor of subtracting 1 neutrophil for every 250 red blood cells (RBCs) should be implemented when defining the type of ascites. If a milky appearance is observed it could suggest a high triglyceride count (chylous ascites from injured lymphatic ducts) of > 100-200 mg/dL[33]. An elevated ascitic fluid amylase level would be very suggestive for pancreatic ascites, e.g., in the setting of a patient with chronic pancreatitis with pseudocysts, and a history of alcohol abuse.

A basic analysis of ascitic fluid albumin can be instructive when compared to serum albumin as the SAAG (where ≥ 1.1 g/dL defines a high albumin gradient) suggests portal-hypertension origin with 97% sensitivity[11]. Accuracy is decreased if the serum and ascitic fluid albumin are not drawn at the same time, or if the serum albumin is < 1.1 g/dL[12]. Note that one cannot infer that portal hypertension is from cirrhosis, although this may be a common cause, but other causes pre- and post-hepatic (vida supra) can also present in this fashion as well[12]. For instance cardiac ascites, a post-hepatic cause, with a SAAG ≥ 1.1 g/dL and an ascitic TP > 2.5 mg/dL, is a reasonable conclusion in the appropriate patient who has a history of heart failure, elevated brain natriuretic peptide, and a dilated IVC[34].

INFECTIOUS ASCITIC FLUID TREATMENT

The interface between the bowel, the intestinal microbiota, and the ascitic fluid is a dynamic one[35,36]. There is a constant translocation of bacteria across the bowel wall; the wall integrity is variable in part due to host genetics, nutritional status and local bacterial interactions. There is usually clearance of these invading bacteria by the immune system after surveillance and capture by neutrophils and macrophages with assisted opsonic molecules, e.g., immunoglobulins or complement[37,38]. The generation of SBP thus likely is a manifestation of (1) bacterial type and burden; (2) gut integrity; (3) volume status; and (4) local and global immune function[37-39]. The symptoms of SBP can range from fevers and abdominal pain to a more subtle change in mental status, e.g., HE, to being totally asymptomatic[12].

Infectious ascitic fluid is analyzed conceptually and practically through cell count/differential and fluid culture and is configured into four categories, the most important being SBP, defined as a neutrophil count > 250 cells/mm3 and a positive mono-microbial ascitic culture[12,40]. If the cell count is < 250 cells/mm3 and there is a positive ascitic culture this is defined as non-neutrocytic bacterascites (NNBA), whereas a negative ascitic culture with > 250 cells/mm3 is culture-negative neutrocytic ascites (CNNA). A neutrophil count > 250 cells/mm3 in the setting of a positive polymicrobial ascitic culture suggests, usually in the setting of bowel perforation, a secondary bacterial peritonitis. This diagnosis is supported by ascitic TP > 1 g/dL, glucose < 50 mg/dL and LDH > 225 U/L, the so-called Runyon’s criteria[41]. In practice, with a positive neutrophil count, while culture results are pending, a provisional diagnosis of SBP will be granted and antimicrobial treatment initiated (vida infra). Given appropriate clinical indications NNBA and CNNA are treated in similar fashion to SBP. Secondary bowel peritonitis, beyond the utilization of antibiotics to include anaerobic coverage, will necessitate imaging and intervention for presumed bowel leak and/or perforation.

Standard treatment for SBP involves immediate implementation of third-generation cephalosporin such as iv ceftriaxone 1-2 g daily for five days, although oral fluoroquinolones have been utilized with success as well[42,43]. Repeat paracentesis is not needed unless there is clinical indication of failing treatment. Given the risks of renal dysfunction, specifically HRS (vida infra), in the setting of alterations in effective circulating volume, iv albumin has been utilized to maintain oncotic tone and renal perfusion. Initial studies demonstrated a benefit when iv albumin was dosed as 1.5 g/kg on day 1 and 1.0 g/kg on day 3, yielding renal protection and improved mortality[44]. Sub-analysis of these patients, further prompted by the large cost of iv albumin, suggested that patients with SBP and blood urea nitrogen (BUN) > 30 mg/dL and total bilirubin (TB) > 4 mg/mL would best benefit[45]. Ideally, one would seek for prevention of SBP as opposed to reactive treatment, and in this regard three groups have shown to benefit from antibiotic prophylaxis. In those (1) with prior SBP, oral norfloxacin 400 mg daily or equivalent indefinitely; (2) patients in the setting of gastrointestinal hemorrhage, to receive iv ceftriaxone 1 g daily × 7 d or equivalent; and (3) hospitalized patients with ascitic TP < 1.5 g/dL and serum Na < 130 mmol/L or BUN > 25 mg/dL or serum creatinine (Cr) > 1.2 mg/dL; otherwise TP < 1.5 g/dL with Child-Turcotte-Pugh (CTP) score > 9 and TB > 3 mg/dL, to receive oral ciprofloxacin 500 mg daily or oral trimethoprim-sulfamethoxazole double-strength daily[46-52].

NON-INFECTIOUS ASCITIC FLUID TREATMENT

Insofar as ascites represents a component of ongoing cirrhotic decompensation, reversible behaviors contributing to the primary process, e.g., alcoholic intake in a patient with alcoholic-induced cirrhosis, or diabetes and hyper-lipidemia in NASH patients, should be controlled[53]. Additionally, external therapy support groups and family involvement may prove crucial in helping the patient maintain sobriety and therapeutic compliance. A diet consisting of 2000 mg/d or less of salt (equivalent to 88 mmol/d of Na) is advocated given the physiologic limits of serum Na processing and secretion through the urine[53-56]. Serum Na governs volume status generally, and thus fluid restriction is not required and is likely not practical. Overloaded states with hyponatremia, even to levels between 110-120 mmol/L are common and well tolerated when approached slowly. Adherence to such a restricted Na diet can be evaluated by measuring 24-h urinary Na, wherein at least 78 mmol/d should be excreted (with water following Na) and resultant weight loss. More practically, a spot urine Na to potassium (K) ratio > 1 in the setting of weight gain also suggests dietary non-adherence[24]. Given the prognosis of ascites as common manifestation of decompensated cirrhosis, and the increased risk for mortality, these patients should be evaluated for OLT, the expedience of which is gauged approximately by their model for end-stage liver disease (MELD) score (vida infra)[1,6,12]. Although not absolute, a sobriety period, in the case of alcoholic cirrhosis, of approximately 6 mo is required of these patients as a predictor of compliance. Furthermore, certain medications, such as non-steroidal anti-inflammatory drugs (NSAIDs), ACE inhibitors (ACEIs), and antibiotics such as aminoglycosides, should be avoided in patients with cirrhotic ascites. NSAIDs inhibit prostaglandins (which function to dilate afferent arterioles) whereas ACEIs inhibit ACEs (which activate angiotensin II, which functions to constrict efferent arterioles). In either case regulation of glomerular perfusion is diminished, increasing potential for renal injury. Antibiotics such as aminoglycosides can be directly nephrotoxic.

Beyond dietary and behavioral measures, or those who cannot tolerate such restrictions, diuretic therapy provides another method for ascitic fluid control[57,58]. The standard combination includes spironolactone, an aldosterone antagonist, which down-regulates Na channels from the apical surface of the principal cells of the renal cortical collecting ducts; and, furosemide a Na-K-2 chloride (Cl) symport inhibitor in the ascending limb of the loop of Henle of the kidney. Spironolactone has a half-life of approximately 24 h, whereas furosemide has a half-life of approximately 1.5 h. They are utilized in a ratio of 100 mg of spironolactone to 40 mg of furosemide, which in theory provides for robust natriuresis with subsequent flow of water, while maintainingnormokalemia[24,56]. Spironolactone is initiated at 100 mg/d and increased every 5-7 d (in 100 mg steps) to a maximum of 400 mg/d, as needed for response. Furosemide is initiated at a dose of 40 mg/d to be increased at 40 mg/d until a maximum of 160 mg/d is achieved[24].

Patients should undergo frequent clinical and biochemical monitoring particularly during the first month of diuretic treatment. The maximum recommended weight loss during diuretic therapy for ascites should be 0.5 kg/d in patients without edema and 1 kg/d in patients with edema. These diuretics have proven to be an excellent method for slow fluid removal and commensurate weight loss. The goal of long-term treatment is to maintain the patient free of ascites with the lowest dose of diuretics. There are no absolute levels in regards to the degree of renal impairment or hyponatremia for which diuretics should not be initiated. However progressive renal injury with a Cr rise to > 1.5 mg/dL and hyponatremia < 120 mmol/L, respectively are sensible parameters which should elicit caution and tapering or cessation of diuretics. In patients with chronic kidney disease (CKD) or transient alterations in renal function, which are common in these patients, likely higher doses of diuretics will be required. The physician should be weary for diuretic-induced pre-renal acute kidney injury (AKI) or the HRS (vida infra). In this setting, there are likely to be frequent episodes for hyperkalemia given the usage of the spironolactone[24]. Additionally, intractable muscle cramps may develop, and thus precipitate a reduction of diuretics[58]. Alternative drugs to spironolactone, usually given the side-effects of gynecomastia and/or sexual dysfunction, or those allergic to the sulfa moiety, may be given amiloride. Amiloride is a direct inhibitor of the apical Na channel in the principal cells of the renal cortical collecting duct[59]. Furosemide can be exchanged for bumetanide, a similar acting diuretic, in those not responding to high doses. It is approximately × 40 more potent than furosemide with a similar side-effect profile[60,61].

More recently, a novel class of compounds has been generated to exploit the pathway of vasopressin[62]. Vasopressin is a naturally occurring compound built in the hypothalamus and stored in the posterior pituitary which is then secreted in response to alterations in blood volume and high serum osmolarity. In such settings it will bind the vasopressin-2 (V2) receptor on the basolateral surface of the principal cells of the renal cortical collecting ducts and through intra-cellular signaling promote the insertion of aquaporin 2 channels in the apical surface to allow for free water entry[62]. This process naturally concentrates urine while expanding total body volume.

In particular one compound, tolvaptan, has been approved for use in volume dysregulated states such as cirrhosis, congestive heart failure and syndrome of inappropriate anti-diuretic hormone[63]. By blocking vasopressin from binding the V2 receptor, a massive aquaresis takes place with correction of the volume state and normalization of serum Na concentration. In patients with a serum Na < 135 mmol/L, tolvaptan is dosed at 15 mg/d in an inpatient setting, and can be up-titrated by 15 mg/d to a maximum of 60 mg/d[63]. Significant improvement in serum Na concentration with tolvaptan, compared to placebo, was observed within 8 h of usage. Given the significant aquaresis, (1) patients should not be hypovolemic; (2) they should have adequate thirst mechanism and access to fluids; and (3) should have their electrolytes monitored closely to prevent overly rapid correction, which in acute settings can lead to osmotic demyelination syndrome[64-66].

AUGMENTED MEDICAL MANAGEMENT OF ASCITES

While diuretics provide excellent maintenance of volume status in decompensated cirrhotics, rapid treatment for ascites, especially tense ascites (grade III), is best through a therapeutic large-volume paracentesis (LVP)[12,24,67]. LVP can be performed all at once, wherein a catheter is temporarily placed and removed, or with an indwelling peritoneal drain for up to three days to slowly remove ascitic fluid over that time. Notably, the peritoneal drain method of LVP is not associated with increased frequency of SBP[68]. An initial LVP whether in an outpatient or inpatient setting, should be sent for ascitic fluid cell count/differential and cell culture to assess for SBP. Up to 15% of LVP may be associated with paracentesis induced circulatory dysfunction (PICD), which is characterized by an activation of the RAAS due to true or perceived volume dysregulation: (1) arterial underfilling and unloading of high-pressure baroreceptors; (2) stimulation of non-osmotic hypersecretion of vasopressin; (3) free water retention and dilutional hyponatremia; and (4) associated renal dysfunction[69]. Given these concerns, iv albumin replacement (8.5 g/kg for each liter of ascitic fluid removed) is indicated in cases where more than 5 L of ascitic fluid is removed[70-72]. Albumin, the most abundant circulating protein in the plasma, is endowed with an array of non-oncotic effects as well, including functioning as an anti-oxidant, anti-inflammatory and positive inotrope[73].

Despite such success, given the risks inherent in the use of iv albumin, as a blood product and its cost, other modalities have been attempted. Terlipressin, with a half-life of 6 h, is a vasopressin analog with selectivity for the V1 receptors on vascular smooth muscle cells, which induces vasoconstriction. In theory the maintenance of vascular tone through terlipressin should reduce, at least in part, some factors that generate PICD[74]. A notable study suggested that in cirrhotic patients with tense ascites who were assigned to receive standard iv albumin replacement or terlipressin (total 3 mg iv) after therapeutic paracentesis, both were effective in reducing manifestations of PICD. There were no significant differences in arterial blood volume (as measured by plasma renin and aldosterone levels) nor in renal impairment or hyponatremia between either group[75].

Following the LVP, patients should receive the minimum dose of diuretics necessary to prevent re-accumulation of the ascites. A small population of ascites patients may be defined as having refractory ascites: ascites which cannot be adequately controlled through dietary, pharmacologic or LVP modalities[74]. Furthermore, a subgroup of patients maybe intolerant to augmented medical management given symptomatic or biochemical side-effects, and thus classified as diuretic-intractable ascites[74,76,77]. Or, a sub-group of patients may retain significant ascites despite optimized and maximal therapy and thus are classified as diuretic-resistant ascites. These groups of patients may require serial LVP, in some cases up to twice per month, which can be time-consuming, costly and increase the risk for iatrogenic infections. There have been smaller studies examining the role of other pharmacologic modalities in refractory ascites, such as midodrine, an alpha-1 agonist upon arterial and venous vessels, inducing increased vascular tone. Midodrine has been shown to be as effective as iv albumin in preventing PICD in such patients with refractory ascites, with minimal side-effects and high cost-efficiency[78]. Compare this to terlipressin, which showed similar outcomes in such patients (vida supra)[75]. Note however that in the latter case, terlipressin must be given through intravenous, and it is currently not available in the United States. Interestingly, non-selective beta-blockers, which have shown benefit in cirrhotic patients in preventing variceal hemorrhage, are associated with increased mortality, 4 × higher compared to those not on beta-blockers, when observed specifically in those patients with refractory ascites[79]. It is postulated that these beta-blockers may be inhibiting compensatory cardiac output (via a negative inotropic effect) and thus pre-disposing to PICD. Further is the interesting finding that in these patients the CTP score, which includes an ascites parameter, is better at predicting mortality than the MELD score. These results require further validation, but may indicate that in the fraction of patients with refractory ascites, beta-blockers should be contra-indicated.

The prognosis of patients with refractory ascites is very poor, and if eligible, should be referred for OLT and/or transjugular intra-hepatic portosystemic shunt (TIPS) as bridge to OLT[80-85]. TIPS is a procedure that has been evolving since the 1980s[86] and relies on the principle of establishing direct continuity (low-resistance) from a large portal branch to a hepatic vein by way of a shunting stent. This stent bypasses the cirrhotic (high-resistance) parenchymal tissue which had generated the portal hypertension and resultant ascites[83]. Recall the portal hypertension develops in the setting of a HWPG of 6 mmHg or greater, and that at 8 mmHg ascites develops, and at 10-12 mmHg varices develop with increased risk of hemorrhage. TIPS is a quite common procedure and not technically demanding with current radiologic techniques. Procedural complications such as failed TIPS deployment and endotipsitis are rare. Concern for TIPS stent thrombosis post-procedurally is minimal in the era of covered stents[83,87,88]. Its strongest indications are in those with refractory ascites and/or recurrent variceal hemorrhage[83]. Overall TIPS has shown benefit in the decreased requirement for diuretics, improved quality of life, and likely a trend towards improved mortality when compared to repetitive paracentesis in patients with refractory ascites[82-85,87-92]. In the MELD era, a score of 14 or less suggests a good candidate for TIPS procedure, a score of 24 or greater, suggests that OLT is more beneficial, and a score in-between requires individual consideration of a risk/benefit analysis to the patient[83,93].

Whether TIPS is ultimately cost-effective, in which most of the cost is up-front at the time of procedure, compared to LVP, where cost is aggregated over time, is still an open question and likely institution dependant. Total TIPS cost have gone down given the decreased requirement for revision in the era of covered stents. Given the physiologic mechanism by which TIPS operates, certain concerns naturally arise: TIPS is contra-indicated in patients with (1) significant right heart failure or pulmonary hypertension as it will place rapid unduevolume burden upon these organs; (2) patients with recurrent HE, as it will not allow for as much detoxification and regulation of the culprit amines; (3) polycystic liver disease or a liver containing malignancy or abscess; (4) active infection; and (5) severe renal disease, given rapid alterations in vascular volume distribution[83,94,95].

There is a small group of patients with refractory ascites, who for a variety of reasons cannot undergo TIPS or OLT, and for whom serial paracentesis has resulted in too much distress or protein losses. In many cases these represent patients who also have peritoneal malignant implants[96-99]. For these scenarios, a peritoneal-venous shunt (PVS) was envisioned, conserving and directing fluid and protein from the peritoneum into the superior vena cava (SVC). There are two types, the LaVeen and the Denver, both one-way valve stents, which empty into the SVC based upon different opening pressures[96]. Contra-indications include loculated ascites, coagulation disorders, and advanced cardiac or renal failure; hemorrhagic ascites and high ascetic TP can cause drain occlusion. Interestingly, in malignant ascites, limited studies have not demonstrated increased systemic metastasis facilitated by stent transfer into the circulatory system. Overall these shunts have not prolonged survival in these patient populations, nor those with HRS[97]. Shunt patency is poor, with < 20% at 2 years. Furthermore SBP and/or sepsis require PVS removal[97]. In general, PVS should be considered as sub-optimal therapy, after standard therapies of diuretics, LVP and TIPS have failed or are contra-indicated[12,83,97].

PULMONARY COMPLICATIONS

HHT is an accumulation of ascitic fluid within the pleural space that occurs in approximately 10% of cirrhotics. In about 85% of these patients it is right-sided, and in others it can be bilateral or even left-sided alone[100]. The etiology is thought to be from the combination of both hemostatic pressure from the ascites pushing through diaphragmatic defects or rents in combination with the “pull” of the negative intra-thoracic pressure[101]. In some cases this combination can effectively drain the peritoneal cavity such that one may have HHT in the absence of a distended abdomen. Normally the pleural space is a potential one, wherein pleural fluid volume is approximately < 25 mL per lung, providing a low frictional interface between the parietal and visceral pleurae. The normal pleural fluid is generated from the parietal pleura, and to a lesser extent the visceral pleura, and reabsorbed by pleural lymphatics. In the setting chronic disease, lymphatic absorption can increase to > 20 × normal baseline rates[102].

Cirrhotic patients who develop a significant amount HHT (approximately after 1 L) tend to have symptoms of shortness of breath and cough. The accumulation of this fluid can lead to hypoexemia, atelectasis, pneumonia and empyema[99,101]. Initial evaluation can include a lateral and posteroanterior chest X-ray, which will show blunting at approximately 50 and 200 mL, respectively. A CT scan of the chest can also be considered to assess for other causes of these symptoms and signs. Initial management should involve a thoracentesis for both diagnostic and therapeutic purposes[99,101]. Similar to a paracentesis, the most useful testing will be to examine the fluid for cell count/differential, cell culture, albumin and TP, with results that should be similar to classical pleural effusions defined as a transudate rather than exudate by Light’s criteria[103]. Infected pleural fluid, i.e., spontaneous bacterial empyema (SBE), should always be of concern, and it has been identified in cases where the ascites did not have SBP and in even cases without any ascites[104]. SBE is diagnosed by a positive culture (usually Escheria, Streptococcus or Enterococcus) or a neutrophil count of > 250 cell/mm3. Standard treatment includes a third-generation cephalosporin or equivalent antibiotic[104]. Chest tubes should not be attempted given the high risk of procedural complications, e.g., abdominal penetration, bleeding, and infection. There is also justified concern for the chronic loss of pleural fluid protein and serum electrolyte abnormalities[105].

Beyond the initial evaluation with thoracentesis, standard measures of dietary restriction and diuretic therapy should be continued[83]. In cases of persistent HHT that have failed these therapies, TIPS has been attempted under the same principles for treatment of refractory ascites in select patients[106,107]. Another procedure is pleurodesis, a process in which an agent such as tetracycline or talc are introduced into the pleural space after which a robust inflammatory reaction occurs that results in visceral to parietal pleural wall fusion[108]. Unfortunately, in most cirrhotic patients, the flow of ascitic fluid entry across the diaphragm and into the pleural space is so high that there is rarely enough time for the pleurae to maintain good approximation for durable fusion. It should only be considered in those patients who have failed first line therapies, and are ineligible for TIPS or OLT[83].

RENAL COMPLICATIONS

Renal injury, encompassing a spectrum from acute to chronic causes, is very common in decompensated cirrhotic patients given the significant alterations in volume and hormonal regulation, vascular tone, immune function and related infections, and the utilization of numerous medications and contrast-assisted procedures[109-111]. Classically AKI is segregated into pre-renal, renal and post-renal causes, and with severe or sustained insult this can lead CKD with the possible utilization of renal replacement therapy (RRT) in either case. For instance, pre-renal causes might include hypovolemia or renal artery thrombosis; renal (intrinsic) causes might include toxicity from infection, malignancy or medications and iv contrast; post-renal causes might include ureteral stone obstruction or extrinsic ureteral compression by a pelvic malignancy[109,111-114].

The HRS should be considered in all cirrhotic patients who develop pure AKI or AKI within a CKD setting[111,115]. HRS, as with any AKI, should be considered when a rise in serum Cr × 1.5 baseline and decrease in urine output are observed in the setting of cirrhosis, and confounding causes for pre-renal, renal and post-renal mechanisms have been reasonably excluded[109,115]. HRS occurs in approximately 30% of patients with SBP treated with antibiotics and is associated with a poor survival[12]. The exact etiology of HRS is unknown, but does involve (1) RAAS dysregulation with avid fluid retention (vida supra); (2) splanchnic vessel dilation and a local vaso-constrictive effect at the level of the nephron driven by renin, angiotensin II and other vasoconstrictors; and (3) altered cardiac function[115]. The renal JGA continually perceives an effectively low circulating volume and thus continuously activates these volume retaining and vasoconstrive mechanisms.

The HRS is classified into two distinct subtypes: type 1 HRS is characterized by a rapid and progressive impairment in renal function (increase in serum Cr to ≥ 2.5 mg/dL or a reduction in the Cr clearance (CrCl) to < 20 mL/min in less than two weeks; type 2 HRS is characterized by a slowly progressive impairment of renal function manifested by an increase in serum Cr to ≥ 1.5 mg/dL or a CrCl to < 40 mL/min[111,115]. Survival in these patients is rather poor, with 50% mortality at less than one month for type 1 HRS and 50% mortality at 6 mo for type 2 HRS[74,116]. Given the complex intrinsic nature of the HRS, it is not surprising that it is defined by negation, i.e., by that which it is not. The criteria for HRS have been evolving and currently include following criteria: (1) rise in serum Cr to > 1.5 mg/dL; (2) the absence of hypovolemic shock (defined by the withdrawl of diuretics and the failure of serum Cr to fall below 1.5 mg/dL in the setting of at least 1 L of saline or standard albumin fluid bolus); (3) the absence of nephrotoxic medications or recent iv contrast; and (4) the absence of intrinsic renal disease as assessed by renal ultrasound and proteinuria < 0.5 g/d and microhematuria < 50 RBCs/high powered field[12,74,111,115,116]. Note that sepsis is not part of the exclusion criteria; HRS is commonly precipitated by SBP in many instances, hence the rationale of antibiotic treatments (vida supra).

As the diagnosis of HRS can herald significant morbidity and mortality in cirrhotic patients OLT should be considered as definitive therapy, if they are eligible. Diuretics should be discontinued, and high grade ascites should be reduced with paracentesis as large peritoneal pressures can compress renal arteries (abdominal compartment syndrome), further worsening the renal insult[74]. Meanwhile, medical therapies may be considered as a temporizing measure, and work towards maintaining effective arterial perfusion of the kidneys. Terlipressin, an analog of vasopressin, has been much researched in the HRS, either in comparison to placebo, or in combination with iv albumin versus placebo, or in comparison to noradrenaline (norepinephrine), a classical vasoactive alpha adrenergic agonist[116-119]. Studies have supported the benefit of terlipressin in reversing HRS when given for at least 14 d, and which typically yield low relapse rates[116,117]. Further, although more limited, there has been data demonstrating reversal of HRS with noradrenaline similar to terlipressin[119]. Notably, in a few studies when terlipressin was administered with iv albumin there was reversal of HRS and improvement in mortality[120], although its value in septic patients is unknown. Terlipressin is usually dosed at 1 mg/6 h, and can be increased to 2 mg/6 h if no improvement in serum Cr is observed.

Similarly, midodrine, a vasoactive alpha adrenergic agonist with a half-life of approximately 4 h, has also demonstrated HRS benefit, and can be dosed at 10 mg three times per day (tid) and increased to 15 mg tid. Complementarily, octreotide (an inhibitor of splanchnic vasodilators, with a half-life of 1.7 h) is dosed at 100 mcg subcutaneously tid and up to 200 mg tid can be utilized. A therapeutic cocktail of these vasoactive agents, e.g., midodrine or terlipressin, and octreotide, with the utilization of iv albumin dosed at up to 40 g per day in divided doses have demonstrated benefit in HRS[121-124]. It is preferable to use highly concentrated albumin, e.g., 25% vs 5% albumin, given the reduced volume of solution and decreased third-spacing burden upon the patient. Successful treatment will manifest as a decrease in serum Cr, ideally by at least 1 mg/dL and an increase in urine output. If the serum Cr decreases to ≤ 1.5 mg/dL, diuretics can be restarted at half the prior dosing with subsequent careful monitoring of volume status and serum Cr. Certainly, as with other forms of AKI, these patients should be carefully monitored: vital signs, mental status, urine output, electrolyte abnormalities, and overall for uremic signs, which would require emergent use of RRT such as hemodialysis[125].

Serum Cr is utilized as a practical, albeit imperfect marker, for renal function in the clinical setting. By extension, renal function has itself become a proxy for systemic health, and the importance of this fact is reflected in the integration of the serum Cr into the MELD score[126,127]. The MELD score is comprised of the serum TB, serum Cr and INR, yielding an integer score from 6 to 40 which predicts 90-d mortality in non-transplanted cirrhotic patients[128]. The MELD score has been more successful than prior risk stratification methods in prognosticating mortality and equitably distributing organs for appropriately eligible patients[129-131]. However, in its elegant simplicity, it unsurprisingly does not capture the total biology of cirrhosis. Thus certain modifications have been appended, in the form of exception points, notably to those who are on RRT or with low-staged hepatocellular carcinoma, amongst others[132].

As stated, OLT represents the definitive therapy for HRS types 1 and 2, and that while it may “cure” the HRS, it will still leave behind the residual CKD in many patients. Furthermore, as a result of the surgery itself (with significant volume shifts), and afterwards by the lifetime use of potentially nephrotoxic immunosuppressants and baseline co-morbidities, renal function can be expected to decline further, even necessitating RRT in some instances. Such consequences themselves herald significant morbidity and mortality for these transplanted patients. Given these concerns, simultaneous liver-kidney transplant (SLKT) has become prevalent in the MELD era with the following facts noted: (1) inconsistent eligibility criteria for SLKT that varies by transplant center; (2) there has not been consistent benefit to morbidity and mortality for these patients, as had been hoped; and (3) eligible kidneys are removed out of the pool for solitary kidney transplant recipients[132,133]. These problems represent an area of active research, with more formal guidance in development[133].

CONCLUSION

Ascites is a pathologic accumulation of fluid within the peritoneal cavity that is most commonly found incirrhotic patients, and its presence heralds significant morbidity and mortality[1,6,10]. The generation of cirrhotic ascites is multi-factorial, but is found in the setting of portal hypertension, and in essence is driven by global abnormalities in hormonal/cytokine regulation and effective vascular status, in a feed-forward cycle[17-19]. Ascites is problematic on many levels: directly, by causing symptoms of abdominal discomfort and early satiation[12]; and indirectly, by facilitating significant complications of infections and multi-organ dysfunction such as SBP, HHT and HRS[12,38,41,99,115]. The identification of ascites, once suspected, is easily determined through physical exam and imaging[23]. Diagnostic paracentesis is an integral procedure in determining the etiology of ascites and further delineating any associated infection or malignancy[24,28]. Ascites can be managed successfully by aggressive salt restriction and utilization of a diuretic regimen in most patients, however in some instances LVP or even TIPS may be required[54,56,67,83]. Given the complexity and prognosis associated with ascites, a multi-disciplinary approach is required, with work-up for OLT initiated in eligible patients[133]. The biomedical advances in understanding and treating ascites and its complications have been impressive, but nevertheless much work remains in optimizing patient care and patient outcomes.

Footnotes

P- Reviewers Pai CG, Singh V S- Editor Gou SX L- Editor A E- Editor Li JY

References

Source