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Session 91 Poster Abstracts
Vaccine Trials in Human Subjects
Friday, 1:30 - 3:30 pm
Hall A


511    
Predictors of Successful Response to Hepatitis A Vaccine in HIV-infected Persons
E Overton1, Diana R Nurutdinova*1, S Sungkanuparph1, R Groger1, W Seyfried1, and W Powderly2
1Washington Univ Sch of Med, St Louis, MO, USA and 2Univ Coll, Dublin, Ireland

Background:  Hepatitis A infection remains a health risk for HIV-infected persons. While the inactivated hepatitis A virus (HAV) vaccine affords protection to immunocompetent persons > 95% of the time, rates of developing protective antibody in HIV+ persons range from 9 to 94%. The effect of HIV viremia on HAV vaccine response has not previously been reported.

Methods:  In this retrospective cohort study of a 906-patient HIV clinic, HIV-infected patients who had received HAV vaccine were identified. Medical records were reviewed for demographics, number of vaccine doses, CD4+ T-cell nadir and count at time of vaccination, HIV viral load at time of vaccination, and antiretroviral therapy at time of vaccination. For continuous and dichotomous variables, t-test and χ2 were used, respectively. Univariate and multivariate analysis by logistic regression were used to determine factors which predicted a successful immune response (reactive HAV antibody) after HAV vaccination.

Results:  Of the 906 patients, 189 (21%) had evidence of prior HAV infection and 347 (38%) had received at least 1 dose of HAV vaccine; 235 had IgG antibody data before and after vaccination. Of these, 112 (48%) developed a reactive antibody response after vaccination. Only HIV viral load < 1000 copies/mL was predictive of successful antibody response. The median HIV viral load in the responders was < 400 copies/mL and the median viral load in non-responders was 1846 copies/mL. The table below shows the differences between the vaccinees who developed a reactive HAV antibody (responders) and those who did not:

 

 

Responders

Non-responders

p Value

 

n = 112

n = 123

 

African American

78 (70%)

80 (65%)

0.23

Female

38 (34%)

36 (24%)

0.39

Median age (range)

39 (19 to 62)

37 (18 to 71)

0.97

CD4 nadir (range)

234 (0 to 1150)

212 (0 to 994)

0.07

Received 2 injections

75 (32%)

76 (32%)

0.58

CD4 at Vax#1 (range)

438 (5 to 1701)

397 (0 to 1224)

0.08

Viral load < 1000 copies/mL at Vax#1

73 (65%)

56 (46%)

<0.001

 

Conclusions:  Suppression of HIV replication at time of HAV vaccination is associated with an increased likelihood of developing a protective antibody response in HIV-infected persons. Neither nadir CD4+ T-cell count nor the value at time of vaccination predicted antibody response. These results suggest the significance of control of viral replication at time of HAV vaccination. The low rate of HAV vaccination response (48%) suggests the importance of developing new approaches to vaccination in HIV-infected persons.

Keywords: Hepatitis A Vaccine; HIV; Antibody response