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低剂量阴茎 SIVmac251 暴露于感染腺病毒 5 型（Ad5）的恒河猴，然后用复制缺陷型 Ad5 为基础的 SIV gag/pol/nef 疫苗免疫，再现了类似 HIV-1 疫苗的 IIb 期临床试验的结果。

Low-dose penile SIVmac251 exposure of rhesus macaques infected with adenovirus type 5 (Ad5) and then immunized with a replication-defective Ad5-based SIV gag/pol/nef vaccine recapitulates the results of the phase IIb step trial of a similar HIV-1 vaccine.

机构信息

Center for Comparative Medicine, University of California, Davis, California, USA.

出版信息

J Virol. 2012 Feb;86(4):2239-50. doi: 10.1128/JVI.06175-11. Epub 2011 Dec 7.

DOI:10.1128/JVI.06175-11

PMID:22156519

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3302390/

Abstract

The Step Trial showed that the MRKAd5 HIV-1 subtype B Gag/Pol/Nef vaccine did not protect men from HIV infection or reduce setpoint plasma viral RNA (vRNA) levels but, unexpectedly, it did modestly enhance susceptibility to HIV infection in adenovirus type 5 (Ad5)-seropositive, uncircumcised men. As part of the process to understand the results of the Step Trial, we designed a study to determine whether rhesus macaques chronically infected with a host-range mutant Ad5 (Ad5hr) and then immunized with a replication defective Ad5 SIVmac239 Gag/Pol/Nef vaccine were more resistant or susceptible to SIV infection than unimmunized rhesus macaques challenged with a series of escalating dose penile exposures to SIVmac 251. The Ad5 SIV vaccine induced CD8(+) T cell responses in 70% of the monkeys, which is similar to the proportion of humans that responded to the vaccine in the Step Trial. However, the vaccine did not protect vaccinated animals from penile SIV challenge. At the lowest SIV exposure dose (10(3) 50% tissue culture infective doses), 2 of 9 Ad5-seropositive animals immunized with the Ad5 SIV vaccine became infected compared to 0 of 34 animals infected in the other animal groups (naive animals, Ad5-seropositive animals immunized with the empty Ad5 vector, Ad5-seronegative animals immunized with the Ad5 SIV vaccine, and Ad5-seronegative animals immunized with the empty Ad5 vector). Penile exposure to more concentrated virus inocula produced similar rates of infection in all animal groups. Although setpoint viral loads were unaffected in Step vaccinees, the Ad5 SIV-immunized animals had significantly lower acute-phase plasma vRNA levels compared to unimmunized animals. Thus, the results of the nonhuman primate (NHP) study described here recapitulate the lack of protection against HIV acquisition seen in the Step Trial and suggest a greater risk of infection in the Ad5-seropositive animals immunized with the Ad5 SIV vaccine. Further studies are necessary to confirm the enhancement of virus acquisition and to discern associated mechanisms.

摘要

步骤试验表明，MRKAd5 HIV-1 亚型 B gag/pol/nef 疫苗不能保护男性免受 HIV 感染或降低病毒载量（vRNA）水平，但出乎意料的是，它确实适度增加了对腺病毒 5 型（Ad5）血清阳性、未割包皮男性的 HIV 感染易感性。作为理解步骤试验结果的过程的一部分，我们设计了一项研究，以确定是否慢性感染宿主范围突变型 Ad5（Ad5hr）的恒河猴，然后用复制缺陷型 Ad5 SIVmac239 gag/pol/nef 疫苗免疫，与用一系列递增剂量的阴茎暴露于 SIVmac251 挑战的未免疫恒河猴相比，对 SIV 感染更有抵抗力或易感性。Ad5 SIV 疫苗诱导了 70%的猴子的 CD8+T 细胞反应，这与步骤试验中对疫苗有反应的人类比例相似。然而，疫苗并不能保护接种疫苗的动物免受阴茎 SIV 挑战。在最低的 SIV 暴露剂量（10350%组织培养感染剂量）下，9 只 Ad5 血清阳性动物中，有 2 只接种 Ad5 SIV 疫苗的动物感染，而在其他动物组中，有 0 只动物感染（未感染动物、接种空 Ad5 载体的 Ad5 血清阳性动物、接种 Ad5 SIV 疫苗的 Ad5 血清阴性动物和接种空 Ad5 载体的 Ad5 血清阴性动物）。阴茎暴露于更浓缩的病毒接种物产生了所有动物组相似的感染率。虽然接种疫苗的个体的病毒载量没有变化，但接种 Ad5 SIV 的动物的急性期血浆 vRNA 水平明显低于未接种的动物。因此，这里描述的非人类灵长类动物（NHP）研究结果再现了步骤试验中观察到的对 HIV 获得的缺乏保护作用，并表明接种 Ad5 SIV 疫苗的 Ad5 血清阳性动物感染的风险更大。需要进一步的研究来确认对病毒获得的增强作用，并辨别相关机制。

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低剂量阴茎 SIVmac251 暴露于感染腺病毒 5 型（Ad5）的恒河猴，然后用复制缺陷型 Ad5 为基础的 SIV gag/pol/nef 疫苗免疫，再现了类似 HIV-1 疫苗的 IIb 期临床试验的结果。

Low-dose penile SIVmac251 exposure of rhesus macaques infected with adenovirus type 5 (Ad5) and then immunized with a replication-defective Ad5-based SIV gag/pol/nef vaccine recapitulates the results of the phase IIb step trial of a similar HIV-1 vaccine.

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