CD40 activation: lessons for HIV immunotherapy from malignancies?

Journal of HIV therapy Pub Date : 2005-09-01
Rifca Le Dieu, John Gribben
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Abstract

In HIV, the immune defects seen are due not only to a decrease in T-cell numbers, but also to qualitative impairment in T-cell function as well as decreased antigen-presenting cell (APC) function. These defects in cell-mediated immunity lead to increased level of infection, contributing to inability to clear the HIV virus, and an increased incidence of tumours. One of the major defects in HIV appears to be the failure of CD4 T cells to provide CD 154 (CD40 ligand)-mediated help, which is required for APC function. In lymphomas, activation through CD40 leads to increased APC activity and induction of immune responses against tumours. Such an effect may also be useful in HIV to increase response against the virus and improve immune surveillance of tumours.

CD40活化:恶性肿瘤HIV免疫治疗的经验教训?
在HIV中,所见的免疫缺陷不仅是由于t细胞数量的减少,而且是由于t细胞功能的定性损伤以及抗原提呈细胞(APC)功能的降低。细胞介导免疫中的这些缺陷导致感染水平升高,导致无法清除艾滋病毒,并增加肿瘤的发生率。HIV的主要缺陷之一似乎是CD4 T细胞无法提供cd154 (CD40配体)介导的帮助,这是APC功能所必需的。在淋巴瘤中,通过CD40激活导致APC活性增加并诱导针对肿瘤的免疫反应。这种效应也可能对艾滋病毒有用,以增加对病毒的反应并改善对肿瘤的免疫监测。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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