Endocytosis constitute the infectious route of HIV-1 entry in human and rabbit monocytes lacking the CD4 receptor.

Microbiologica Pub Date : 1991-04-01
G Filice, P M Cereda, P Orsolini, L Soldini, E Razzini, D Campisi, R Gulminetti
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Abstract

To obtain "functionally" CD4 negative human monocytes (0-5 CD4 +/1 x 10(6)/cells), 50 ng/5.10(5) cells of OKT4A were added daily after a pre-incubation with OKT4A (100 ng/5.10(5) cells. In our experimental conditions the blocking the CD4 receptor of human monocytes with OKT4A monoclonal antibody did not prevent HIV-1 infection, although the level of virus replication appeared lower than that in cultures without OKT4A. "Naturally"CD4 negative rabbit monocytes infected with HIV-1 also released a detectable level of virus after 12-15 up 28-30 days. In "naturally" CD4 negative rabbit monocytes and "functionally" CD4 negative human monocytes, the virus particles entering via phagocytosis are not infectious because multiple well defined virions were observed in phagocytic vacuoles and the envelopes of these particles did not appear to interact with the vacuolar membrane. The infectious particles were represented by endocytic vesicles containing only the core of HIV after fusion between the viral envelope and endocytic membrane. Fusion between the viral envelope and plasma membrane on the cellular surface was never observed, in spite of examining greater than 1000 virions bound the surface of human and rabbit macrophage monocytes. The absence of cytopathic effect in the rabbit and human CD4 negative monocytes infected with HIV-1, and conversely the presence of specific sequences of HIV in the genomic DNA may indicate that the macrophages-monocytes serve as an important reservoir for the persistence of HIV in infected hosts, similar to the other related Lentiviruses. Our virological data have also demonstrated that virus infection can be transmitted from rabbit and human infected monocytes to uninfected H9 cells. This preliminary study may offer important evidence for the development and testing of vaccines and compounds that inhibit HIV penetration of susceptible cells.

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在缺乏CD4受体的人和家兔单核细胞中,内吞作用是HIV-1进入的感染途径。
为了获得“功能性”CD4阴性人单核细胞(0-5 CD4 +/1 × 10(6)/细胞),与OKT4A (100 ng/5.10(5)细胞预孵育后,每天添加50 ng/5.10(5)个OKT4A细胞。在我们的实验条件下,用OKT4A单克隆抗体阻断人单核细胞的CD4受体并不能阻止HIV-1感染,尽管病毒复制水平比不含OKT4A的培养低。感染HIV-1的“自然”CD4阴性兔单核细胞也在12-15天至28-30天后释放出可检测水平的病毒。在“自然”CD4阴性的兔单核细胞和“功能性”CD4阴性的人单核细胞中,通过吞噬进入的病毒颗粒没有传染性,因为在吞噬空泡中观察到多个定义明确的病毒粒子,这些颗粒的包膜似乎没有与空泡膜相互作用。在病毒包膜与内吞膜融合后,感染颗粒以仅含有HIV核心的内吞囊泡为代表。尽管检测了人类和兔子巨噬细胞单核细胞表面超过1000个病毒粒子,但从未观察到细胞表面病毒包膜和质膜的融合。在感染HIV-1的兔和人CD4阴性单核细胞中没有细胞病变效应,相反,在基因组DNA中存在特定的HIV序列,这可能表明巨噬细胞单核细胞与其他相关的慢病毒一样,是HIV在感染宿主中持续存在的重要储存库。我们的病毒学数据还表明,病毒感染可以从兔和人感染的单核细胞传播到未感染的H9细胞。这项初步研究可能为开发和测试抑制艾滋病毒渗透易感细胞的疫苗和化合物提供重要证据。
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