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在体内浸润H-2不相容心脏同种异体移植物的T淋巴细胞中,很大一部分表达编码细胞毒性细胞特异性丝氨酸蛋白酶的基因,但不表达MEL-14定义的淋巴结归巢受体。

A high proportion of T lymphocytes that infiltrate H-2-incompatible heart allografts in vivo express genes encoding cytotoxic cell-specific serine proteases, but do not express the MEL-14-defined lymph node homing receptor.

作者信息

Mueller C, Gershenfeld H K, Lobe C G, Okada C Y, Bleackley R C, Weissman I L

机构信息

Department of Pathology, Stanford University Medical Center, California 94305.

出版信息

J Exp Med. 1988 Mar 1;167(3):1124-36. doi: 10.1084/jem.167.3.1124.

Abstract

The role of cytotoxic cells in in vivo immune functions such as allograft rejection is unknown. To begin to assess the function of cytolytic cells in vivo we have begun with cytolytic cell-specific functional molecules: we have isolated and characterized cytolytic cell-specific cDNA clones from cytolytic T cell clones, both encoding distinct serine esterases. The HF gene encodes a trypsin-like enzyme while the C11 gene encodes an enzyme with likely specificity for acidic residues. Here we demonstrate, using in situ hybridization with RNA probe, that both genes are expressed selectively in a subset of T lymphocytes that have infiltrated cardiac allografts. The phenotype of these cells is consistent with the most frequent phenotype of active CTL raised in vitro: they are predominantly CD4-, CD8+, MEL-14- T cell blasts. Thus the expression of these genes, each of which encodes serine esterase found in killer cell granules in vitro, is a valid marker for these cells in vivo as well. The kinetics of their accumulation is consistent with, but not proof of, a putative role in allograft rejection. It is likely that HF and C11 gene expression will be of diagnostic value.

摘要

细胞毒性细胞在诸如同种异体移植排斥等体内免疫功能中的作用尚不清楚。为了开始评估体内溶细胞性细胞的功能,我们从溶细胞性细胞特异性功能分子入手:我们从溶细胞性T细胞克隆中分离并鉴定了溶细胞性细胞特异性cDNA克隆,两者均编码不同的丝氨酸酯酶。HF基因编码一种类胰蛋白酶,而C11基因编码一种可能对酸性残基具有特异性的酶。在此,我们使用RNA探针原位杂交证明,这两个基因均在浸润心脏同种异体移植物的一部分T淋巴细胞中选择性表达。这些细胞的表型与体外培养的活性CTL最常见的表型一致:它们主要是CD4-、CD8+、MEL-14-T细胞母细胞。因此,这些基因的表达,每个基因在体外均编码杀伤细胞颗粒中发现的丝氨酸酯酶,在体内也是这些细胞的有效标志物。它们积累的动力学与同种异体移植排斥中的假定作用一致,但并非证据。HF和C11基因表达可能具有诊断价值。

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