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环孢素和FK506在人胸腺细胞中的分子作用模式。

Molecular mode of action of cyclosporin and FK506 in human thymocytes.

作者信息

Reem G H

机构信息

Department of Pharmacology, New York University Medical Center, New York 10016.

出版信息

J Autoimmun. 1992 Apr;5 Suppl A:159-65. doi: 10.1016/0896-8411(92)90030-t.

Abstract

The molecular mode of action of cyclosporin, three of its non-immunosuppressive analogs, N-methyl-l-alanyl cyclosporin, acetyl cyclosporin and cyclosporin S3, and of FK506 was studied in primary cultures of human thymocytes. Nuclear factors derived from thymocytes activated with phorbol myristate acetate and concanavalin A were tested for their ability to bind to a synthetic radiolabelled probe corresponding to the NF-AT region (-285 to -255) of the IL-2 gene. Binding was observed, and it was inhibited by CsA (100 ng/ml), while the analogs at ten-fold higher concentrations (1000 ng/ml) were only partially inhibitory. CsA in combination with FK506 inhibited binding of nuclear factors at the NF-AT site, and acted in concert.

摘要

在人胸腺细胞原代培养物中研究了环孢素、其三种非免疫抑制类似物(N-甲基-L-丙氨酰环孢素、乙酰环孢素和环孢素S3)以及FK506的分子作用模式。检测了由佛波酯肉豆蔻酸酯和伴刀豆球蛋白A激活的胸腺细胞衍生的核因子与对应于IL-2基因NF-AT区域(-285至-255)的合成放射性标记探针结合的能力。观察到有结合现象,且其被环孢素A(100 ng/ml)抑制,而浓度高十倍(1000 ng/ml)的类似物仅具有部分抑制作用。环孢素A与FK506联合使用可抑制核因子在NF-AT位点的结合,且二者协同发挥作用。

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