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TP5在单核细胞中触发涉及丝裂原活化蛋白激酶的信号转导。

TP5 triggers signal transduction involving mitogen activated protein kinases in monocytes.

作者信息

Gonser S, Crompton N E, Weber P J, Beck-Sickinger A G, Folkers G

机构信息

Department of Pharmacy, ETH Zürich, Switzerland.

出版信息

J Recept Signal Transduct Res. 1999 Jan-Jul;19(1-4):155-66. doi: 10.3109/10799899909036642.

Abstract

The pentapetide thymopentin (TP5) corresponding to the aminoacids RKDVY represents the residues 32-36 of thymopoietin (TP), which was originally isolated from bovine thymus. Both were observed to induce T-cell differentiation and maturation. Recently however it was shown, that TP represents the N-terminal 49 aa of the human thymopoietin (TMPO) isoforms TMPO alpha, beta and gamma, which are localized in the nucleus. TP5 was investigated in a variety of diseases and showed efficacy by improving the immune balance, whereby different cells increased in cell number or activity. Findings which support the assumption of multifunctional efficacy and a description of TP and TP5 modulating T cells lack any interpretation on molecular level. In the present study we investigated the binding of TP5 on white blood cells. We identified monocytes and neutrophils as TP5-binding cells by displacing fluorescein-labelled TP5 with an excess of unlabelled TP5 in competition assays. Binding of TP5 on cell surface proteins resulted in cellular signalling and we report here that TP5 triggers signal transduction involving mitogen activated protein kinases p42/p44 (MAPKs) in monocytes.

摘要

与氨基酸RKDVY对应的五肽胸腺五肽(TP5)代表胸腺生成素(TP)的32 - 36位残基,TP最初是从牛胸腺中分离出来的。两者均被观察到可诱导T细胞分化和成熟。然而最近研究表明,TP代表人类胸腺生成素(TMPO)亚型TMPOα、β和γ的N端49个氨基酸,这些亚型定位于细胞核。TP5已在多种疾病中进行了研究,并通过改善免疫平衡显示出疗效,不同细胞的数量或活性增加。支持TP和TP5具有多功能疗效以及调节T细胞的假设的研究结果,在分子水平上缺乏任何解释。在本研究中,我们研究了TP5与白细胞的结合。在竞争试验中,我们通过用过量的未标记TP5取代荧光素标记的TP5,确定单核细胞和中性粒细胞为TP5结合细胞。TP5与细胞表面蛋白的结合导致细胞信号传导,我们在此报告TP5触发单核细胞中涉及丝裂原活化蛋白激酶p42/p44(MAPKs)的信号转导。

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