Center for Biomedical Research, Population Council, New York, New York, United States of America.
PLoS One. 2009 Nov 30;4(11):e8060. doi: 10.1371/journal.pone.0008060.
Herpes simplex virus type-2 (HSV-2) infection enhances the transmission and acquisition of human immunodeficiency virus (HIV). This occurs in symptomatic and asymptomatic stages of HSV-2 infection, suggesting that obvious herpetic lesions are not required to increase HIV spread. An animal model to investigate the underlying causes of the synergistic action of the two viruses and where preventative strategies can be tested under such complex physiological conditions is currently unavailable.
METHODOLOGY/PRINCIPAL FINDINGS: We set out to establish a rhesus macaque model in which HSV-2 infection increases the susceptibility to vaginal infection with a model immunodeficiency virus (simian-human immunodeficiency virus, SHIV-RT), and to more stringently test promising microbicides. HSV-2 exposure significantly increased the frequency of vaginal SHIV-RT infection (n = 6). Although cervical lesions were detected in only approximately 10% of the animals, long term HSV-2 DNA shedding was detected (in 50% of animals followed for 2 years). Vaginal HSV-2 exposure elicited local cytokine/chemokine (n = 12) and systemic low-level HSV-2-specific adaptive responses in all animals (n = 8), involving CD4(+) and CD8(+) HSV-specific T cells (n = 5). Local cytokine/chemokine responses were lower in co-infected animals, while simian immunodeficiency virus (SIV)-specific adaptive responses were comparable in naïve and HSV-2-infected animals (n = 6). Despite the increased frequency of SHIV-RT infection, a new generation microbicide gel, comprised of Carraguard(R) and a non-nucleoside reverse transcriptase inhibitor MIV-150 (PC-817), blocked vaginal SHIV-RT infection in HSV-2-exposed animals (n = 8), just as in naïve animals.
CONCLUSIONS/SIGNIFICANCE: We established a unique HSV-2 macaque model that will likely facilitate research to define how HSV-2 increases HIV transmission, and enable more rigorous evaluation of candidate anti-viral approaches in vivo.
单纯疱疹病毒 2 型(HSV-2)感染会增强人类免疫缺陷病毒(HIV)的传播和感染。这种情况发生在 HSV-2 感染的有症状和无症状阶段,这表明增加 HIV 传播并不需要明显的疱疹病变。目前还没有一种动物模型可以研究这两种病毒协同作用的根本原因,也无法在如此复杂的生理条件下测试潜在的预防策略。
方法/主要发现:我们着手建立一个恒河猴模型,在该模型中,HSV-2 感染会增加阴道感染模型免疫缺陷病毒(猿猴-人免疫缺陷病毒,SHIV-RT)的易感性,并更严格地测试有前途的杀微生物剂。HSV-2 暴露显著增加了阴道 SHIV-RT 感染的频率(n=6)。尽管只有大约 10%的动物检测到宫颈病变,但检测到长期 HSV-2 DNA 脱落(在随访 2 年的 50%动物中)。阴道 HSV-2 暴露会引起所有动物(n=8)局部细胞因子/趋化因子(n=12)和全身低水平的 HSV-2 特异性适应性反应,涉及 CD4(+)和 CD8(+) HSV 特异性 T 细胞(n=5)。在合并感染的动物中,局部细胞因子/趋化因子反应较低,而在未感染和 HSV-2 感染的动物中,SIV 特异性适应性反应相当(n=6)。尽管 SHIV-RT 感染的频率增加,但新一代杀微生物凝胶 Carraguard(R)和非核苷类逆转录酶抑制剂 MIV-150(PC-817)阻断了 HSV-2 暴露动物的阴道 SHIV-RT 感染(n=8),就像在未感染动物中一样。
结论/意义:我们建立了一种独特的 HSV-2 猴模型,这可能有助于研究 HSV-2 如何增加 HIV 传播,并使体内更严格地评估候选抗病毒方法。
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