People co-infected with HIV and HCV, mostly with hepatitis C
virus (HCV) genotype 3, responded about as well as HIV-negative people to interferon-based
therapy after taking into account other factors associated with poor treatment response,
according to an Italian study presented at the 53rd Interscience Conference on Antimicrobial Agents and Chemotherapy (ICAAC)
this month in Denver. Advanced liver fibrosis was common in the co-infected
group, supporting the need for early treatment.
An estimated one-third of HIV-positive people are
co-infected with HCV, with higher rates in countries where the HIV epidemic is
largely driven by injecting drug use. Over years or decades, chronic hepatitis C
can lead to serious liver disease, including advanced fibrosis, cirrhosis and
hepatocellular carcinoma. HIV/HCV co-infected people tend to experience faster
liver disease progression and do not respond as well to interferon as people
with HCV alone.
Paola Nasta from Spedali Civili di Brescia and
colleagues compared treatment outcomes amongst HIV/HCV co-infected and HCV
mono-infected people with HCV genotype 2 or 3 treated at their hospital between
2005 and 2010. Genotypes 2 and 3 have traditionally been classified as
'easier-to-treat' in comparison with 'harder-to-treat' genotypes 1 and 4.
Glossary
- erythropoietin
-
A natural hormone made in the kidneys to stimulate the production of red blood cells by the bone marrow.
- neutropenia
A shortage of neutrophils, a type of white blood
cell that fights bacterial infections.
This
retrospective analysis included 113 HIV/HCV co-infected and 627 HCV mono-infected
adults not previously treated for hepatitis C. About 85% of the co-infected
participants and two-thirds of the mono-infected participants were men and the mean age
was 45 years. All the HIV-positive participants were on antiretroviral
therapy with undetectable HIV viral load and the mean CD4 cell count was 455
cells/mm3.
Most of the
co-infected participants (95%) had HCV genotype 3, whereas the mono-infected
patients were more evenly divided between genotypes 2 and 3 (45 and 55%,
respectively). Nearly one-quarter of co-infected patients, but only 5% in the
mono-infected group, had advanced fibrosis/cirrhosis (stage F4) at baseline.
The co-infected group was less likely to have high baseline HCV RNA (33 vs
51%) but more likely to have a low platelet count (mean 163,200 vs 208,400/mcl).
Two-thirds of
participants were treated with pegylated interferon alfa-2a (Pegasys) and one-third with pegylated
interferon alfa-2b (PegIntron) along
with weight-based ribavirin (15mg/kg/day). All co-infected people were treated
for 48 weeks. HCV mono-infected patients could stop at 24 weeks if they had
absent-to-moderate fibrosis, low baseline HCV viral load or rapid virological
response at week 4. Both groups stopped due to futility if HCV RNA was still
detectable after 12 weeks of therapy.
Anaemia and
neutropenia can be treatment-limiting side-effects of ribavirin and interferon.
Patients with cirrhosis were eligible to use erythropoietin (EPO) to stimulate
red blood cell production. If haemoglobin remained low despite EPO, they could
reduce their ribavirin dose. All HIV-positive participants could use granulocyte
colony-stimulating factor (GCSF) to promote white blood cell growth, but
HIV-negative people could do so only if they had cirrhosis. Those with
persistent white blood cell deficiency could lower their interferon dose.
The overall sustained
virological response (SVR) rate after completion of treatment was 69%, but it was
significantly lower in the HIV/HCV co-infected group (58%) compared with the
HCV mono-infected group (67%). HIV-negative individuals were 50% more likely to
respond to treatment (odds ratio 1.5).
Co-infected and
mono-infected participants were equally likely to be virological non-responders
(15 vs 16%). But co-infected people were slightly more likely to experience
post-treatment relapse even though they were treated for longer (50 vs 45%, not a
significant difference). A similar proportion in both groups discontinued
treatment early for any reason (35 vs 40%).
There were not enough HIV-positive people with HCV
genotype 2 to analyse the genotypes separately, but looking at all participants
together, the SVR rate for genotype 2 was significantly higher than for
genotype 3 (72 vs 61%, respectively). This might have contributed to the lower
response rate in the co-infected group compared with the mono-infected group,
which had a more even genotype distribution.
Co-infected
people were more likely to lower their ribavirin dose (26 vs 18%), though much
less likely to prematurely stop interferon (9 vs 68%). A similar proportion of
patients in both groups developed anaemia (12 vs 10%) but fewer co-infected
people used EPO (2 vs 16%). The co-infected group was significantly more
likely to have neutropenia (42 vs 12%) and to use GCSF (41 vs 4%).
Factors
significantly associated with sustained response were advanced fibrosis –
reducing the likelihood of SVR by 60% – high baseline HCV viral load,
ribavirin dose reduction and early interruption of pegylated interferon.
After adjusting
for these and other factors influencing treatment response, having HIV itself was
not an independent predictor of worse treatment response.
"HCV mono- and HIV/HCV co-infected patients seem
to have a similar rate of SVR in our clinical setting," the researchers
concluded. They suggested this might be due to HIV-positive people receiving a
longer duration of treatment or being more likely to use GCSF to maintain
higher drug doses.
Because
HIV/HCV co-infected people have a higher rate of advanced fibrosis, and because
this is one of the most important variables related to poor treatment outcomes,
the researchers recommended that co-infected people with HCV genotypes
2 or 3 should receive early treatment.