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T淋巴细胞系对髓鞘碱性蛋白肽段的特异性

Specificity of T lymphocyte lines for peptides of myelin basic protein.

作者信息

Vandenbark A A, Offner H, Reshef T, Fritz R, Chou C H, Cohen I R

出版信息

J Immunol. 1985 Jul;135(1):229-33.

PMID:2582033
Abstract

T lymphocyte lines specific for myelin basic protein (BP) can mediate experimental autoimmune encephalomyelitis (EAE), or can protect against the active induction of the disease. To investigate the antigenic fine specificity of guinea pig (GP) BP-specific T cell lines raised from different rat strains, and to determine whether functionally different T lymphocyte lines and clones recognized the same or different regions of the BP molecule, the proliferation responses of line cells were assessed after stimulation with purified peptides of GP-BP. Lewis rat T cell lines and clones selected for responses to whole GP-BP responded selectively to the 68-88 amino acid sequence of GP-BP, but not to the 1-37, 43-67, or 89-169 sequences. The region of GP-BP recognized by Lewis T cells was additionally defined to include the 75-80 amino acid sequence, because a T cell clone responded equally to GP and rat BP which differed by only one amino acid at position 79, but did not respond to human or bovine BP, which had a Gly-His insertion in this region. T lymphocyte lines derived from the F344 and PVG (Weizmann) rat strains shared the same selective response to peptide 68-88, but lines from BN rats responded to an epitope(s) outside of the 68-88 sequence. The functional capacity of the various T cell lines to mediate experimental autoimmune encephalomyelitis (EAE) or to induce resistance against EAE was independent of their specificity for the different GP-BP peptides; lines specific for epitope(s) within or excluded from the 68-88 sequence could be encephalitogenic depending on their strain of origin, and various lines specific for the 68-88 peptide could induce both disease and protection, disease only, or neither activity.

摘要

对髓鞘碱性蛋白(BP)具有特异性的T淋巴细胞系可介导实验性自身免疫性脑脊髓炎(EAE),或可预防该疾病的主动诱导。为了研究从不同大鼠品系培养的豚鼠(GP)BP特异性T细胞系的抗原精细特异性,并确定功能不同的T淋巴细胞系和克隆是否识别BP分子的相同或不同区域,在用GP-BP的纯化肽刺激后评估系细胞的增殖反应。选择对整个GP-BP有反应的Lewis大鼠T细胞系和克隆对GP-BP的68-88氨基酸序列有选择性反应,但对1-37、43-67或89-169序列无反应。Lewis T细胞识别的GP-BP区域还被定义为包括75-80氨基酸序列,因为一个T细胞克隆对GP和大鼠BP的反应相同,它们在第79位仅相差一个氨基酸,但对人或牛BP无反应,人或牛BP在该区域有一个甘氨酸-组氨酸插入。来自F344和PVG(魏茨曼)大鼠品系的T淋巴细胞系对肽68-88具有相同的选择性反应,但来自BN大鼠的系对68-88序列以外的表位有反应。各种T细胞系介导实验性自身免疫性脑脊髓炎(EAE)或诱导对EAE的抗性的功能能力与其对不同GP-BP肽的特异性无关;对68-88序列内或外的表位具有特异性的系根据其来源品系可能具有致脑炎作用,并且对68-88肽具有特异性的各种系可诱导疾病和保护、仅疾病或无活性。

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