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Liver diseases in patients
with HIV infection
Aung Zayar Paing
Introduction
—  Abnormal liver function tests can be seen frequently
in HIV patients. (prevalence as high as 30%)
—  Liver disease is the second commonest cause of
mortality in HIV patients.
—  Hepatitis virus coinfections represent the most
significant cause of liver disease in HIV patients.
—  Some other conditions also play their role to cause
liver injury in HIV patients.
Lancet 2011; 377: 1198–1209
AIDS Rev. 2013; 15:25-31
Lancet 2011; 377: 1198–1209
Different causes of hepatitis in
HIV infected patients
HAIVN M2-08-Hepatic Toxicity in Patients Taking ARVs-EN
HAIVN M2-08-Hepatic Toxicity in Patients Taking ARVs-EN
Hepatitis Coinfections
AIDS Rev. 2013; 15:25-31
HBV coinfection
—  ARVs like Tenofovir (TDF), Lamivudine (3TC) and
Emtricitabine (FTC) are active against HIV as well
as HBV.
—  WHO guideline 2013 recommends to start ART for
HIV-HBV coinfected patients with evidence of
severe chronic liver disease.
—  US DHHS guideline advises to start ART for all
patients who need anti-HBV treatment.
Hepatic flare up after HAART in
HBV coinfected patients
—  Some patients with HIV-HBV coinfection experience
hepatic flare up having high ALT levels.
—  Like IRIS associated with OIs, high antigen burden
(high HBV DNA level) (ID 2009:199, Crane et al.
http://jid.oxfordjournals.org/)
ALT and HBV DNA values in HF and non-HF subjects over 1st 12 weeks
after HAART initiation.
x-axis: Weeks after HAART initiation. y-axis 1: HBV DNA log 10 c/ml. y-
axis 2: ALT IU/L.
Avihingsanon et al. AIDS Research and Therapy 2012 9:6 doi:10.1186/1742-6405-9-6
HCV coinfection
—  Nearly 1/3 of HCV patients progress to cirrhosis at
a median time of less than 20 years.
—  Compared to HCV monoinfected patients, HIV-
HCV coinfected patients have 3 times greater risk of
progression to cirrhosis or decompensated liver
disease.
—  Peginterferon + Ribavirin is the mainstay treatment.
—  Interferon sparing regimens are possible for some
genotypes recently after the introduction of new
directly active antiviral (DAA) Sofosbuvir.
AASLDGuideline
Drug interaction and toxicities
—  AZT + RBV - increased risk of anemia
—  ddI + RBV – life threatening ddI-associated
mitochondrial toxicity including hepatomegaly/
steatosis, pancreatitis, and lactic acidosis
—  ABC - decreased response to PegIFN/RBV ???
—  Other DAAs, Boceprevir and telaprevir interacts
significantly with EFV.
Hepatitis E virus infection
in HIV patients
—  Some studies showed that HIV infected patients
have increased susceptibility to hepatitis E virus
infection.
—  Acute HEV infection can mimic drug induced liver
injury.
—  HIV patients have risk of chronic HEV infection.
(HEV RNA in serum or stools for 6 months or more)
—  Myanmar is one of the countries with high
prevalence of HEV infection.
Source:TheLancet2012;379:2477-2488(DOI:10.1016/
S0140-6736(11)61849-7)
Source and route of HEV1–4 infection
HEV1 and HEV2 are waterborne only, with possible human-to-human
transmission, including vertical transmission.
Hepatotoxicity of drugs
HAIVN M2-08-Hepatic Toxicity in Patients Taking ARVs-EN
HAIVN M2-08-Hepatic Toxicity in Patients Taking ARVs-EN
Martin Fisher’s presentation: ICVH 2013
JournalofHepatology2011vol.54|773–794
Martin Fisher’s presentation: ICVH 2013
Hyperbilirubinemia due to
some PIs
Liver metabolism of bilirubin and
potential mechanisms of interference
of atazanavir (ATV) and indinavir
(IDV). Uridine diphosphate
glucuronosyltransferase 1A1 is the
liver enzyme that conjugates the
bilirubin. The insertion of an extra
dinucleotide (TA) on the promoter
gene of the UGT1A1 results in a
decreased enzyme activity. Atazanavir
and IDV inhibit the UGT1A1, which in
turn result in hyperbilirubinemia.
http://www.nature.com/tpj/journal/v6/n4/fig_tab/6500374f6.html
ACTG grading system for
hepatotoxicity
Grade 1 Grade 2 Grade 3 Grade 4
ALT* ≤ 2.5 x ULN 2.6 – 5.0 x ULN 5.1-10.0 x ULN 10.0 x ULN
If	
  Grade	
  1	
  or	
  2	
  hepatotoxicity	
  occurs	
  during	
  NVP	
  lead-­‐in	
  dose,	
  lead-­‐in	
  dose	
  can	
  extend	
  	
  
next	
  2	
  weeks	
  (maximum).	
  
If	
  ALT	
  sFll	
  raised	
  and	
  <	
  grade	
  2	
  stop	
  NVP	
  and	
  start	
  EFV.	
  
Other conditions
Alcoholic hepatitis
—  Alcoholism is common in HIV patients and
alcoholic hepatitis sometimes complicate HIV
treatment.
—  Abrupt stopping of alcohol in chronic drinker is
dangerous and the patient may suffer from alcohol
withdrawal. (mild to sever manifestation like
Delirium Tremens)
Signs and symptoms
CCO HIV inPractice
—  AST/ALT ratio - usually > 1
—  GGT - may be increased (low sensitivity/specificity
for alcohol abuse
—  Bilirubin may be increased
—  INR - raised
—  PT - prolonged
Nonalcoholic Fatty Liver Disease
(NAFLD)
—  NAFLD is the condition caused by accumulation of
Triglycerides in hepatocytes associated with obesity,
diabetes mellitus and hyperlipidemia.
—  Non-alcoholic steatohepatitis is the progressive
form of NAFLD.
—  40-70% HIV-HCV coinfected patients are found to
have hepatic steatosis.
—  The risk is higher in patients taking ddI or d4T
—  AST/ALT ration is usually < 1
http://dx.doi.org/10.1155/2013/493413
Thank you

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Liver Diseases in Patients with HIV infections

  • 1. Liver diseases in patients with HIV infection Aung Zayar Paing
  • 2. Introduction —  Abnormal liver function tests can be seen frequently in HIV patients. (prevalence as high as 30%) —  Liver disease is the second commonest cause of mortality in HIV patients. —  Hepatitis virus coinfections represent the most significant cause of liver disease in HIV patients. —  Some other conditions also play their role to cause liver injury in HIV patients.
  • 3. Lancet 2011; 377: 1198–1209
  • 4. AIDS Rev. 2013; 15:25-31
  • 5. Lancet 2011; 377: 1198–1209
  • 6. Different causes of hepatitis in HIV infected patients
  • 7. HAIVN M2-08-Hepatic Toxicity in Patients Taking ARVs-EN
  • 8. HAIVN M2-08-Hepatic Toxicity in Patients Taking ARVs-EN
  • 10. AIDS Rev. 2013; 15:25-31
  • 11. HBV coinfection —  ARVs like Tenofovir (TDF), Lamivudine (3TC) and Emtricitabine (FTC) are active against HIV as well as HBV. —  WHO guideline 2013 recommends to start ART for HIV-HBV coinfected patients with evidence of severe chronic liver disease. —  US DHHS guideline advises to start ART for all patients who need anti-HBV treatment.
  • 12. Hepatic flare up after HAART in HBV coinfected patients —  Some patients with HIV-HBV coinfection experience hepatic flare up having high ALT levels. —  Like IRIS associated with OIs, high antigen burden (high HBV DNA level) (ID 2009:199, Crane et al. http://jid.oxfordjournals.org/)
  • 13. ALT and HBV DNA values in HF and non-HF subjects over 1st 12 weeks after HAART initiation. x-axis: Weeks after HAART initiation. y-axis 1: HBV DNA log 10 c/ml. y- axis 2: ALT IU/L. Avihingsanon et al. AIDS Research and Therapy 2012 9:6 doi:10.1186/1742-6405-9-6
  • 14. HCV coinfection —  Nearly 1/3 of HCV patients progress to cirrhosis at a median time of less than 20 years. —  Compared to HCV monoinfected patients, HIV- HCV coinfected patients have 3 times greater risk of progression to cirrhosis or decompensated liver disease. —  Peginterferon + Ribavirin is the mainstay treatment. —  Interferon sparing regimens are possible for some genotypes recently after the introduction of new directly active antiviral (DAA) Sofosbuvir.
  • 16. Drug interaction and toxicities —  AZT + RBV - increased risk of anemia —  ddI + RBV – life threatening ddI-associated mitochondrial toxicity including hepatomegaly/ steatosis, pancreatitis, and lactic acidosis —  ABC - decreased response to PegIFN/RBV ??? —  Other DAAs, Boceprevir and telaprevir interacts significantly with EFV.
  • 17. Hepatitis E virus infection in HIV patients —  Some studies showed that HIV infected patients have increased susceptibility to hepatitis E virus infection. —  Acute HEV infection can mimic drug induced liver injury. —  HIV patients have risk of chronic HEV infection. (HEV RNA in serum or stools for 6 months or more) —  Myanmar is one of the countries with high prevalence of HEV infection.
  • 18. Source:TheLancet2012;379:2477-2488(DOI:10.1016/ S0140-6736(11)61849-7) Source and route of HEV1–4 infection HEV1 and HEV2 are waterborne only, with possible human-to-human transmission, including vertical transmission.
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  • 22. HAIVN M2-08-Hepatic Toxicity in Patients Taking ARVs-EN
  • 23. HAIVN M2-08-Hepatic Toxicity in Patients Taking ARVs-EN
  • 27. Hyperbilirubinemia due to some PIs Liver metabolism of bilirubin and potential mechanisms of interference of atazanavir (ATV) and indinavir (IDV). Uridine diphosphate glucuronosyltransferase 1A1 is the liver enzyme that conjugates the bilirubin. The insertion of an extra dinucleotide (TA) on the promoter gene of the UGT1A1 results in a decreased enzyme activity. Atazanavir and IDV inhibit the UGT1A1, which in turn result in hyperbilirubinemia. http://www.nature.com/tpj/journal/v6/n4/fig_tab/6500374f6.html
  • 28. ACTG grading system for hepatotoxicity Grade 1 Grade 2 Grade 3 Grade 4 ALT* ≤ 2.5 x ULN 2.6 – 5.0 x ULN 5.1-10.0 x ULN 10.0 x ULN If  Grade  1  or  2  hepatotoxicity  occurs  during  NVP  lead-­‐in  dose,  lead-­‐in  dose  can  extend     next  2  weeks  (maximum).   If  ALT  sFll  raised  and  <  grade  2  stop  NVP  and  start  EFV.  
  • 30. Alcoholic hepatitis —  Alcoholism is common in HIV patients and alcoholic hepatitis sometimes complicate HIV treatment. —  Abrupt stopping of alcohol in chronic drinker is dangerous and the patient may suffer from alcohol withdrawal. (mild to sever manifestation like Delirium Tremens)
  • 31. Signs and symptoms CCO HIV inPractice
  • 32. —  AST/ALT ratio - usually > 1 —  GGT - may be increased (low sensitivity/specificity for alcohol abuse —  Bilirubin may be increased —  INR - raised —  PT - prolonged
  • 33. Nonalcoholic Fatty Liver Disease (NAFLD) —  NAFLD is the condition caused by accumulation of Triglycerides in hepatocytes associated with obesity, diabetes mellitus and hyperlipidemia. —  Non-alcoholic steatohepatitis is the progressive form of NAFLD. —  40-70% HIV-HCV coinfected patients are found to have hepatic steatosis. —  The risk is higher in patients taking ddI or d4T —  AST/ALT ration is usually < 1