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作 者:加路[1] 郑煜煌[1] 陈霞[1] 何艳[1] 周华英[1] 谌资[1]
机构地区:[1]中南大学湘雅二医院感染科、艾滋病研究室,长沙410011
出 处:《中南大学学报(医学版)》2011年第11期1037-1045,1020,共9页Journal of Central South University :Medical Science
基 金:suported by National Science and Technolgy lmportant Item of China(2008ZX10001-008,2008ZX10005-003,2009ZX10005-015)
摘 要:高效抗反转录病毒疗法可以有效地减少HIV的复制,但却不能完全恢复CD4+T细胞的数量。即使病毒血清学指标得到良好控制的病人,CD4+T细胞数也很难达到正常水平。目前研究表明:γ链细胞因子在始动、维持及调节免疫稳态和炎症反应中发挥重要作用。γ链细胞因子具有多重功能,如在健康及疾病中作为调节和效应分子发挥作用,因此,该家族因子、受体及其信号转导通路可成为治疗性干预的潜在靶点。γ链细胞因子IL-2,IL-7,IL-15和IL-21是T细胞稳态的重要调节者,因此成为升高T细胞水平和功能及增强AIDS免疫受累患者疫苗诱发病毒特异性T细胞应答等免疫治疗中的主要可选靶点之一。Although highly active antiretroviral therapy(HAART) can effectively reduce the HIV replication,complete recovery of CD4+ T cells does not always occur,even among patients with high virological control.Current researches on γ-chain cytokines have understood the biology and their crucial roles in initiating,maintaining,and regulating the immunologic homeostasis and the inflammatory processes.Due to the multiple functions such as the regulatory and effector cellular function in healthy and disease state,these molecules,their receptors,and their signal transduction pathways are promising candidates for therapeutic interference.The common γ-chain cytokines IL-2,IL-7,IL-15,and IL-21 are primary regulators of T cell homeostasis and thus have been considered prime immunotherapeutic candidates,both for increasing T cell levels/function and augmenting vaccine-elicited viral-specific T cell responses in immunocompromised AIDS patients.The objective of this review is to update the role of the common γ-chain cytokines IL-2,IL-7,IL-15,and IL-21 in HIV AIDS pathogenesis.
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