在人类免疫缺陷病毒1型原发性感染期间,通常会出现多种V1/V2包膜变体。
Multiple V1/V2 env variants are frequently present during primary infection with human immunodeficiency virus type 1.
作者信息
Ritola Kimberly, Pilcher Christopher D, Fiscus Susan A, Hoffman Noah G, Nelson Julie A E, Kitrinos Kathryn M, Hicks Charles B, Eron Joseph J, Swanstrom Ronald
机构信息
University of North Carolina at Chapel Hill, 22-062 Lineberger Cancer Center, CB 7295, Chapel Hill, NC 27599-7295, USA.
出版信息
J Virol. 2004 Oct;78(20):11208-18. doi: 10.1128/JVI.78.20.11208-11218.2004.
Human immunodeficiency virus type 1 (HIV-1) exists as a complex population of multiple genotypic variants in persons with chronic infection. However, acute HIV-1 infection via sexual transmission is a low-probability event in which there is thought to be low genetic complexity in the initial inoculum. In order to assess the viral complexity present during primary HIV-1 infection, the V1/V2 and V3 variable regions of the env gene were examined by using a heteroduplex tracking assay (HTA) capable of resolving these genotypic variants. Blood plasma samples from 26 primary HIV-1-infected subjects were analyzed for their level of diversity. Half of the subjects had more than one V1/V2 viral variant during primary infection, indicating the frequent transmission of multiple variants. This observation is inconsistent with the idea of infrequent transmission based on a small transmitting inoculum of cell-free virus. In chronically infected subjects, the complexity of the viral populations was even greater in both the V1/V2 and the V3 regions than in acutely infected subjects, indicating that in spite of the presence of multiple variants in acute infection, the virus does pass through a genetic bottleneck during transmission. We also examined how well the infecting virus penetrated different anatomical compartments by using the HTA. Viral variants detected in blood plasma were compared to those detected in seminal plasma and/or cerebral spinal fluid of six individuals. The virus in each of these compartments was to a large extent identical to virus in blood plasma, a finding consistent with rapid penetration of the infecting variant(s). The low-probability transmission of multiple variants could be the result of transient periods of hyperinfectiousness or hypersusceptibility. Alternatively, the inefficient transfer of a multiply infected cell could account for both the low probability of transmission and the transfer of multiple variants.
1型人类免疫缺陷病毒(HIV-1)在慢性感染患者体内以多种基因型变体的复杂群体形式存在。然而,通过性传播的急性HIV-1感染是一个低概率事件,据认为初始接种物中的基因复杂性较低。为了评估原发性HIV-1感染期间存在的病毒复杂性,利用能够解析这些基因型变体的异源双链追踪分析(HTA)对env基因的V1/V2和V3可变区进行了检测。对26名原发性HIV-1感染受试者的血浆样本进行了多样性水平分析。一半的受试者在原发性感染期间有不止一种V1/V2病毒变体,这表明多种变体频繁传播。这一观察结果与基于少量无细胞病毒传播接种物的罕见传播观点不一致。在慢性感染受试者中,V1/V2和V3区域的病毒群体复杂性甚至比急性感染受试者更大,这表明尽管急性感染中存在多种变体,但病毒在传播过程中确实会经历基因瓶颈。我们还利用HTA研究了感染病毒穿透不同解剖学部位的情况。将血浆中检测到的病毒变体与6名个体的精液和/或脑脊液中检测到的变体进行了比较。这些部位中的每一个部位的病毒在很大程度上与血浆中的病毒相同,这一发现与感染变体的快速穿透一致。多种变体的低概率传播可能是短暂的高感染性或高易感性时期的结果。或者,多重感染细胞的低效转移可能解释了传播的低概率和多种变体的转移。
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