IMMUNOGENICITY, SAFETY AND TOLERABILITY OF VARYING DOSES AND REGIMENSOF INACTIVATED HEPATITIS-A VIRUS-VACCINE IN NAVAJO CHILDREN

The Navajo are known to be at high risk for hepatitis A virus (HAV) in fection. This study investigated the safety and immunogenicity of an i nvestigational, alum-adjuvanted, formalin-inactivated HAV vaccine (VAQ TA (R)) developed by Merck Research Laboratories in Navajo children. O ne hundred two of 212 children, ages 4 to 12 years, were HAV-seronegat ive (<10 mIU/ml by an enhanced sensitivity modification of the HAVAB ( R); Abbott). Ninety of these children received the HAV vaccine. Study participants were given vaccines containing various viral protein conc entrations: Group A (n = 18), 6 units; Group B (n = 36), 13 units; and Group C (n = 36), 25 units HAV protein (1 unit approximate to 1 ng vi ral protein antigen). Three-dose (0, 8, 24 weeks) and two-dose (0, 24 weeks) regimens were compared in subgroups within B and C. The vaccine was well-tolerated and there were no serious adverse reactions; no va ccinee developed hepatitis A. After 1 dose 82 to 100% of children sero converted (greater than or equal to 10 mIU/ml, modified HAVAB (R); Abb ott) and 100% seroconverted after 2 doses. After 1 dose the geometric mean titer for antibody was: Group A, 22 mIU/ml; Group B, 18 mIU/ml; a nd Group C, 38 mIU/ml. After 3 doses geometric mean titers increased t o 10106 mIU/ml in Group A, 7258 mIU/ml in Group B and 11856 mIU/ml in Group C. Further field studies are indicated to evaluate its use in hi gh risk populations, such as the Navajo.