中和敏感的R5嗜性猿猴-人类免疫缺陷病毒SHIV-2873Nip,其携带从一名近期感染HIV C亚型的婴儿分离出的env基因。
Neutralization-sensitive R5-tropic simian-human immunodeficiency virus SHIV-2873Nip, which carries env isolated from an infant with a recent HIV clade C infection.
作者信息
Siddappa Nagadenahalli B, Song Ruijiang, Kramer Victor G, Chenine Agnès-Laurence, Velu Vijayakumar, Ong Helena, Rasmussen Robert A, Grisson Ricky D, Wood Charles, Zhang Hong, Kankasa Chipeppo, Amara Rama Rao, Else James G, Novembre Francis J, Montefiori David C, Ruprecht Ruth M
机构信息
Dana-Farber Cancer Institute, Boston, MA 02115, USA.
出版信息
J Virol. 2009 Feb;83(3):1422-32. doi: 10.1128/JVI.02066-08. Epub 2008 Nov 19.
Human immunodeficiency virus clade C (HIV-C) accounts for >56% of all HIV infections worldwide. To investigate vaccine safety and efficacy in nonhuman primates, a pathogenic, R5-tropic, neutralization-sensitive simian-human immunodeficiency virus (SHIV) carrying HIV-C env would be desirable. We have constructed SHIV-2873Ni, an R5-tropic SHIV carrying a primary pediatric HIV-C env gene isolated from a 2-month-old Zambian infant, who died within 1 year of birth. SHIV-2873Ni was constructed using SHIV-1157ipd3N4 (R. J. Song, A. L. Chenine, R. A. Rasmussen, C. R. Ruprecht, S. Mirshahidi, R. D. Grisson, W. Xu, J. B. Whitney, L. M. Goins, H. Ong, P. L. Li, E. Shai-Kobiler, T. Wang, C. M. McCann, H. Zhang, C. Wood, C. Kankasa, W. E. Secor, H. M. McClure, E. Strobert, J. G. Else, and R. M. Ruprecht. J. Virol. 80:8729-8738, 2006) as the backbone, since the latter contains additional NF-kappaB sites in the long terminal repeats to enhance viral replicative capacity. The parental virus, SHIV-2873Ni, was serially passaged through five rhesus monkeys (RMs); SHIV-2873Nip, the resulting passaged virus, was reisolated from the fourth recipient about 1 year postinoculation. SHIV-2873Nip was replication competent in RM peripheral blood mononuclear cells of all random donors tested and was exclusively R5 tropic, and its env gene clustered with HIV-C by phylogenetic analysis; its moderate [corrected] sensitivity to neutralization led to classification as a tier 2 [corrected] virus. Indian-origin RMs were inoculated by different mucosal routes, resulting in high peak viral RNA loads. Signs of virus-induced disease include depletion of gut CD4(+) T lymphocytes, loss of memory T cells in blood, and thrombocytopenia that resulted in fatal cerebral hemorrhage. SHIV-2873Nip is a highly replication-competent, mucosally transmissible, pathogenic R5-tropic virus that will be useful to study viral pathogenesis and to assess the efficacy of immunogens targeting HIV-C Env.
人类免疫缺陷病毒C亚型(HIV-C)占全球所有HIV感染的56%以上。为了研究在非人灵长类动物中的疫苗安全性和有效性,需要一种携带HIV-C包膜基因的致病性、R5嗜性、中和敏感的猿猴-人类免疫缺陷病毒(SHIV)。我们构建了SHIV-2873Ni,这是一种R5嗜性的SHIV,携带从一名2个月大的赞比亚婴儿分离出的原发性儿科HIV-C包膜基因,该婴儿在出生后1年内死亡。SHIV-2873Ni是使用SHIV-1157ipd3N4(R.J.宋、A.L.切宁、R.A.拉斯穆森、C.R.鲁普雷希特、S.米尔沙希迪、R.D.格里森、W.徐、J.B.惠特尼、L.M.戈因斯、H.翁、P.L.李、E.沙伊-科比勒、T.王、C.M.麦肯、H.张、C.伍德、C.坎卡萨、W.E.西科尔、H.M.麦克卢尔、E.斯特罗伯特、J.G.埃尔塞和R.M.鲁普雷希特。《病毒学杂志》80:8729 - 8738,2006)作为骨架构建的,因为后者在长末端重复序列中含有额外的核因子κB位点以增强病毒复制能力。亲代病毒SHIV-2873Ni在5只恒河猴(RM)中连续传代;传代后得到的病毒SHIV-2873Nip在接种后约1年从第四只受体中重新分离出来。SHIV-2873Nip在所有测试的随机供体的RM外周血单个核细胞中具有复制能力,并且完全是R5嗜性的,通过系统发育分析其包膜基因与HIV-C聚类;其对中和的中等[校正后]敏感性导致其被归类为2级[校正后]病毒。印度起源的RM通过不同的黏膜途径接种,导致病毒RNA载量出现高峰。病毒诱导疾病的迹象包括肠道CD4(+)T淋巴细胞耗竭、血液中记忆T细胞丧失以及血小板减少症,后者导致致命的脑出血。SHIV-2873Nip是一种具有高度复制能力、可经黏膜传播的致病性R5嗜性病毒,将有助于研究病毒发病机制并评估针对HIV-C Env的免疫原的疗效。
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