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CD1d2在胸腺细胞上的表达不足以使CD1d1缺陷小鼠中的自然杀伤T细胞发育。

Expression of CD1d2 on thymocytes is not sufficient for the development of NK T cells in CD1d1-deficient mice.

作者信息

Chen Y H, Wang B, Chun T, Zhao L, Cardell S, Behar S M, Brenner M B, Wang C R

机构信息

Gwen Knapp Center for Lupus and Immunology Research, Committee on Immunology, Department of Pathology, University of Chicago, IL 60637, USA.

出版信息

J Immunol. 1999 Apr 15;162(8):4560-6.

Abstract

CD1 is an MHC class I-like molecule that has been conserved throughout mammalian evolution. Unlike MHC class I molecules, CD1 can present unique nonprotein antigens to T cells. The murine CD1 locus contains two highly homologous genes, CD1d1 and CD1d2. CD1d1 is essential for the development of a major subset of NK T cells that promptly secrete IL-4 following activation. However, the function of CD1d2 has not yet been demonstrated. In the present study, we examined the expression of CD1d2 in CD1d1-deficient (CD1d1 degrees) mice with the anti-CD1 Ab 3H3. Unlike CD1d1, which is expressed by all lymphocytes, CD1d2 can be detected only on the surface of thymocytes. To determine whether CD1d2 can select a unique subset of NK T cells, we compared the remnant population of NK T cells in CD1d1 degrees and CD1d1, CD1d2-double deficient (CD1d1 degrees CD1d2 degrees) mice. No significant difference in the number of NK T cells and cytokine secretion capacity can be detected between CD1d1 degrees and CD1d1 degrees CD1d2 degrees mice, indicating that CD1d2 cannot substitute for CD1d1 in NK T cell development. The inability of CD1d2 to select NK T cells is not due to the structural constraints of CD1d2 since CD1d2-transfected cells can be recognized by both NK T cell hybridomas and freshly isolated NK T cells. Given the structural similarities, it is possible that the low levels of surface expression and limited tissue distribution of CD1d2 may prevent it from functioning in the selection and expansion of NK T cells.

摘要

CD1是一种类似于MHC I类的分子,在整个哺乳动物进化过程中一直保守存在。与MHC I类分子不同,CD1能够将独特的非蛋白质抗原呈递给T细胞。小鼠CD1基因座包含两个高度同源的基因,即CD1d1和CD1d2。CD1d1对于一类主要的NK T细胞亚群的发育至关重要,这类NK T细胞在激活后会迅速分泌IL-4。然而,CD1d2的功能尚未得到证实。在本研究中,我们用抗CD1抗体3H3检测了CD1d1缺陷(CD1d1°)小鼠中CD1d2的表达。与所有淋巴细胞都表达的CD1d1不同,CD1d2仅能在胸腺细胞表面检测到。为了确定CD1d2是否能选择出独特的NK T细胞亚群,我们比较了CD1d1°小鼠和CD1d1、CD1d2双缺陷(CD1d1°CD1d2°)小鼠中NK T细胞的剩余群体。在CD1d1°小鼠和CD1d1°CD1d2°小鼠之间,未检测到NK T细胞数量和细胞因子分泌能力的显著差异,这表明在NK T细胞发育过程中,CD1d2不能替代CD1d1。CD1d2无法选择NK T细胞并非由于其结构限制,因为转染了CD1d2的细胞能够被NK T细胞杂交瘤和新鲜分离的NK T细胞识别。鉴于结构上的相似性,CD1d2表面表达水平低且组织分布有限,可能使其无法在NK T细胞的选择和扩增中发挥作用。

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