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α 型对 β 型:我们是否即将揭开自然杀伤 T 细胞内源性配体之谜?

Alpha versus beta: are we on the way to resolve the mystery as to which is the endogenous ligand for natural killer T cells?

机构信息

Department of Medicine, Hebrew University - Hadassah Medical Center, Jerusalem, Israel.

出版信息

Clin Exp Immunol. 2009 Dec;158(3):300-7. doi: 10.1111/j.1365-2249.2009.04030.x. Epub 2009 Sep 30.

Abstract

Natural killer T (NKT) lymphocytes are a unique subset of cells that play a role in regulating the immune system. For the past decade, studies have focused upon attempts to define these cells and to determine the ligand(s) that are required for their development and peripheral activation. Many research groups have focused upon determining the mechanisms for activating or inhibiting NKT cells in an attempt to control immune-mediated disorders as well as infectious and malignant conditions by using different ligand structures. Alpha-anomeric glycolipids and phospholipids derived from mammalian, bacterial, protozoan and plant species have been suggested as potential ligands for these lymphocytes. Some of these ligands were structured in forms that can bind to CD1d molecules. The lack of alpha-anomeric glycosphingolipids in mammals and the modest effect of these ligands in human studies, along with recent data from animal models and humans on the NKT-dependent immunomodulatory effect of beta-glycosphingolipids, suggest that the beta-anomeric ligands have the potential to be the endogenous NKT ligand.

摘要

自然杀伤 T(NKT)淋巴细胞是一类独特的细胞亚群,在调节免疫系统中发挥作用。在过去的十年中,研究集中于定义这些细胞以及确定其发育和外周激活所需的配体。许多研究小组专注于确定激活或抑制 NKT 细胞的机制,试图通过使用不同的配体结构来控制免疫介导的疾病以及感染和恶性疾病。来自哺乳动物、细菌、原生动物和植物物种的α-差向异构糖脂和磷脂已被提议作为这些淋巴细胞的潜在配体。其中一些配体的结构可以与 CD1d 分子结合。哺乳动物中缺乏α-差向异构糖脂以及这些配体在人类研究中的适度作用,以及动物模型和人类关于β-糖脂的 NKT 依赖性免疫调节作用的最新数据表明,β-差向异构配体有可能成为内源性 NKT 配体。

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