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Low Multiplicity of HIV-1 Infection and No Vaccine Enhancement in VAX003 Injection Drug Users

机译:VAX003注射吸毒者中HIV-1感染的多重性低且未增强疫苗

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Background.?We performed human immunodeficiency virus type 1 (HIV-1) transmitted/founder (T/F) virus analysis of the VAX003 vaccine efficacy trial participants to characterize the transmission bottleneck and test for vaccine-associated reduction or enhancement of infection in this injection drug user (IDU) cohort. Methods.?We performed single genome sequencing of plasma vRNA from 50 subjects sampled in early HIV infection. Sequences were analyzed phylogenetically, T/F viruses enumerated, and a sieve analysis performed. Results.?Eight of 19 (42%) placebo recipients were productively infected by more than 1 virus (range 1–5, median 1, mean 1.7). This frequency of multiple virus transmission was greater than reported for heterosexual cohorts (19%, P = .03) but not statistically different from vaccine recipients (22.6%, P .05), where the range was 1–3, median 1, and mean 1.3 (P .05 for all comparisons). An atypical sieve effect was detected in Env V2 but was not associated with reduction or enhancement of virus acquisition. Conclusions.?The number of T/F viruses in IDUs was surprising low, with 95% of individuals infected by only 1–3 viruses. This finding suggests that a successful vaccine or other prevention modality generally needs to protect against only one or a few viruses regardless of risk behavior. T/F analysis identified an atypical genetic sieve in the V2 region of Envelope and found no evidence for vaccine-mediated enhancement in VAX003.
机译:背景:我们对VAX003疫苗功效试验参与者进行了人类免疫缺陷病毒1型(HIV-1)传播/建立者(T / F)病毒分析,以鉴定传播瓶颈,并在此方法中测试与疫苗相关的感染减少或增强注射吸毒者(IDU)队列。方法:我们对来自早期HIV感染的50名受试者的血浆vRNA进行了单基因组测序。系统发育分析序列,列举T / F病毒,并进行筛分分析。结果。有19名(42%)安慰剂接受者被一种以上的病毒有效感染(范围1-5,中位数1,平均1.7)。多重病毒传播的频率高于异性队列报道的频率(19%,P = .03),但与疫苗接种者(22.6%,P> .05)的差异无统计学意义,后者的范围为1-3,中位数为1,均值为1.3(所有比较均P> 0.05)。在Env V2中检测到非典型的筛查效果,但与减少或增强病毒获取无关。结论:IDU中的T / F病毒数量惊人地低,有95%的个体仅感染1-3种病毒。这一发现表明,无论风险行为如何,成功的疫苗或其他预防手段通常仅需要防御一种或几种病毒。 T / F分析在Envelope的V2区域发现了一个非典型的遗传筛,没有发现疫苗介导的VAX003增强的证据。

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