Ratto-Kim S, Sitz K V, Garner R P, Kim J H, Davis C, Aronson N, Ruiz N, Tencer K, Redfield R R, Birx D L
Henry M. Jackson Foundation, Rockville, MD 20850, USA.
J Infect Dis. 1999 Feb;179(2):337-44. doi: 10.1086/314587.
This longitudinal study was designed to evaluate cellular immunity in early-stage, asymptomatic human immunodeficiency virus (HIV)-1-infected persons (CD4 cell count,>400/mm3; median, 625/mm3) who were immunized with either recombinant (r) gp160 or placebo every 2 months for 5 years. Proliferative responses were assessed against rgp160, rp24, and a panel of recall antigens and mitogens. Despite good reactivity to recall antigens, at baseline approximately 33% had proliferative responses to gp160, and approximately 42% showed p24 gag responses. There was no statistical difference between vaccine and placebo groups for antigens or mitogens. After 1 year, approximately 73% of the subjects in the vaccine arm had new or boosted responses to gp160, versus approximately 18% in the placebo arm. Statistical significance was maintained throughout the study. Recurrent vaccination with recombinant gp160 was proven to be persistently immunogenic, increasing significantly the ability of HIV-1-infected persons to mount new proliferative responses to the vaccine.
这项纵向研究旨在评估早期无症状人类免疫缺陷病毒(HIV)-1感染者(CD4细胞计数>400/mm³;中位数为625/mm³)的细胞免疫情况,这些感染者每2个月接受一次重组(r)gp160或安慰剂免疫,共持续5年。评估了针对rgp160、rp24以及一组回忆抗原和丝裂原的增殖反应。尽管对回忆抗原有良好反应,但在基线时约33%的人对gp160有增殖反应,约42%的人表现出p24 gag反应。疫苗组和安慰剂组在抗原或丝裂原方面无统计学差异。1年后,疫苗组约73%的受试者对gp160有新的或增强的反应,而安慰剂组约为18%。整个研究过程中均保持统计学显著性。已证明用重组gp160反复接种具有持续免疫原性,显著提高了HIV-1感染者对疫苗产生新的增殖反应的能力。
