Langhoff E, McElrath J, Bos H J, Pruett J, Granelli-Piperno A, Cohn Z A, Steinman R M
Laboratory of Cellular Physiology and Immunology, Rockefeller University, New York, New York 10021.
J Clin Invest. 1989 Nov;84(5):1637-43. doi: 10.1172/JCI114341.
We have addressed the capacity of HIV-1 infection to alter the growth of primary CD4+ T cells, but at the clonal level. Single T cells were expanded in the presence of PHA, IL-2, and small numbers of accessory dendritic cells. We report two new findings. First, T cells from seropositive individuals, even those with AIDS and markedly reduced CD4+ counts, exhibit a normal cloning efficiency, and proliferative capacity. This result is in contrast to two prior reports of a low cloning efficiency in CD4+ T cells from HIV-1-infected patients. Second, when we added high doses of exogenous HIV-1 to T cell clones from control subjects, we observed infection but not cytotoxicity or loss of CD4+ cells, following addition of virus stocks at days 0, 3, and/or 7 of clonal growth. The same HIV-1 isolates markedly reduced CD4+ T cells in bulk mononuclear cultures. When tested at day 11, HIV-1 mRNA was expressed in some cells of exogenously infected clones by in situ hybridization; when tested at day 18, several clones could transactivate a TAT-sensitive cell line. These findings suggest that the loss of CD4+ T cells in infected individuals is not the inevitable result of the activation of latent infection, or spread of a productive infection, during clonal growth.
我们已经探讨了HIV-1感染在克隆水平上改变原代CD4+ T细胞生长的能力。单个T细胞在PHA、IL-2和少量辅助树突状细胞存在的情况下进行扩增。我们报告了两项新发现。首先,血清反应阳性个体的T细胞,即使是那些患有艾滋病且CD4+计数明显降低的个体,其克隆效率和增殖能力均正常。这一结果与之前两篇关于HIV-1感染患者CD4+ T细胞克隆效率低下的报道形成对比。其次,当我们向来自对照受试者的T细胞克隆中添加高剂量外源性HIV-1时,在克隆生长的第0天、第3天和/或第7天添加病毒原液后,我们观察到了感染,但未观察到细胞毒性或CD4+细胞的损失。相同的HIV-1分离株在大量单核细胞培养物中显著减少了CD4+ T细胞。在第11天进行检测时,通过原位杂交在外源性感染克隆的一些细胞中检测到了HIV-1 mRNA;在第18天进行检测时,几个克隆能够激活对TAT敏感的细胞系。这些发现表明,感染个体中CD4+ T细胞的损失并非克隆生长过程中潜伏感染激活或有生产性感染传播的必然结果。
