Antiretroviral
Regimens with Lamivudine (Epivir) Produce Good CD4 Cell Recovery and HIV Suppression
with Fewer Liver Flares in HIV-HBV Coinfected Patients
 | HIV-HBV
coinfected patients in South Africa who received antiretroviral regimens containing
lamivudine (3TC; Epivir) -- which is dually active against both viruses -- achieved
good CD4 cell gains and HIV suppression and had fewer flare-ups of liver inflammation,
according to a poster presented at the Fifth International AIDS Society Conference
on HIV Pathogenesis, Treatment, and Prevention last week in Cape Town, South Africa. |
By
Liz Highleyman Hepatitis
B virus (HBV) coinfection is common among HIV
positive people in areas where hepatitis B is endemic, but how best to manage
coinfected patients -- especially in resource-limited settings -- has not been
extensively studied. Prince
Manzini from the South African Military Health Service and colleagues with the
Phidisa II Study Group looked at the impact of treatment with lamivudine-containing
combination antiretroviral therapy
(ART) in HIV-HBV coinfected individuals. Phidisa
II was a randomized clinical trial comparing 4 combination ART regimens, 2 containing
lamivudine and 2 without. The study included 1771 South Africans with symptomatic
HIV disease or a CD4 count below 200 cells/mL. Patients with a positive hepatitis
B surface antigen (HBsAg) test prior to randomization were identified as coinfected.
A total
of 106 patients (6%) were HIV-HBV coinfected.
This group was significantly more likely to be male, had lower platelet counts
and serum albumin, and had higher ALT levels than HIV
monoinfected patients. Baseline characteristics were well balanced, however,
between the 57 participants receiving lamivudine-containing regimens and the 49
patients on non-lamivudine ART. Over
a median follow-up period of about 2 years, the researchers compared CD4 cell
recovery and HIV RNA suppression between patients receiving lamivudine-containing
and non-lamivudine regimens. Episodes
of hepatic flare -- liver inflammation indicated by serious ALT elevation -- were
also assessed. Flares were defined as ALT > 135 IU/mL in patients with a normal
baseline level or an increase of more than 1000 IU/mL in patients who started
with an elevated level. They also used a more stringent definition, ALT > 225
IU/mL in patients with a normal baseline level or an increase of more than 3.5
x baseline level if initially high (equivalent to grade 3 hepatotoxicity.) Results "HIV-HBV
coinfected individuals were more likely to have higher ALT and lower albumin and
platelet counts at baseline, possible indicators of more severe underlying liver
disease," the investigators concluded. "However, as described previously
by the others, there was no suggestion that the presence of HIV-HBV coinfection
impaired either the immunological or virological response to combination ART,
irrespective of the use or not of [lamivudine]. "Reductions
in overall serum transaminase levels relative to baseline were observed in HIV-HBV
coinfected subjects receiving both [lamivudine-containing ART] and [non-lamivudine
ART]," they continued. "Hepatic flare was substantially more common
in coinfected patients compared t those with HIV monoinfection." "The
pathogenesis of hepatic flare in patients with HIV-HBV coinfection is often multifactorial
and additional work to examine measures of HBV replication and serological changes
during follow-up in this trial is ongoing and should provide valuable additional
information," they added. South
African Military Health Service, Pretoria, South Africa. 7/31/09 Reference
P
Manzini and others (Phidisa II Study Group). Impact
of lamivudine (3TC)-containing combination antiretroviral therapy (cART) in South
African patients co-infected with HIV and hepatitis B virus (HBV); a randomised,
controlled trial (Phidisa II). 5th International AIDS Society Conference on
HIV Pathogenesis, Treatment, and Prevention (IAS 2009). July 19-22, 2009. Cape
Town, South Africa. Abstract
WePeB231.
| 
6 months: 105 vs 84 cells/mm3;
