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T淋巴细胞对非H-2同种抗原的继发性体外反应——在异种血清中诱导的自身H-2限制性反应——不依赖于初次刺激的非H-2同种抗原。

Secondary in vitro responses of T lymphocytes to non-H-2 alloantigens self-H-2-restricted responses induced in heterologous serum are not dependent on primary-stimulating non-H-2 alloantigens.

作者信息

Peck A B, Andersson L C, Wigzell H

出版信息

J Exp Med. 1977 Apr 1;145(4):802-18. doi: 10.1084/jem.145.4.802.

Abstract

The role of non-H-2 alloantigens, specifically Mls locus products, in secondary in vitro T-cell-mediated cytotoxicity has been studied. Splenic T lymphocytes, activated against Mls locus alloantigens in primary-mixed cultures and isolated by velocity sedimentation gradient separation techniques, were used as responding populations in secondary mixed leukocyte cultures (MLCs) and cell-mediated lympholysis (CML). Such T-cell clones could be shown to exhibit either "self"-H-2-restricted or anti-Mls locus-specific reactivity, with this dichotomy of reactivity depending only on the primary culture conditions. Mls locus-activated T lymphocytes generated in cultures supplemented with homologous serum exhibited specific memory responses in MLC, yet remained incapable of effecting target cell destruction against Mls locus antigens or against "self"-H-2-structures in CML. In contrast, activated T-cell clones generated in the presence of heterologous serum displayed H-2-restricted reactivity in both secondary MLC and CML. H-2-restricted MLC activation was controlled by products of the H-2 serologically defined regions. Although heterologous serum was a necessary (and sufficient) entity for development of H-2-restricted responses, evidence argues against the possibility that heterologous serum acts via modification of cell surface components.

摘要

已对非H-2同种抗原,特别是Mls基因座产物在体外继发性T细胞介导的细胞毒性中的作用进行了研究。在原代混合培养物中针对Mls基因座同种抗原活化并通过速度沉降梯度分离技术分离的脾T淋巴细胞,用作继发性混合淋巴细胞培养物(MLC)和细胞介导的淋巴细胞溶解(CML)中的反应群体。此类T细胞克隆可显示出“自身”H-2限制性或抗Mls基因座特异性反应性,这种反应性的二分法仅取决于原代培养条件。在补充同源血清的培养物中产生的Mls基因座活化的T淋巴细胞在MLC中表现出特异性记忆反应,但在CML中仍无法对Mls基因座抗原或“自身”H-2结构进行靶细胞破坏。相比之下,在异源血清存在下产生的活化T细胞克隆在继发性MLC和CML中均表现出H-2限制性反应性。H-2限制性MLC活化受H-2血清学定义区域的产物控制。尽管异源血清是产生H-2限制性反应所必需(且充分)的因素,但有证据表明异源血清并非通过修饰细胞表面成分起作用。

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