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曼氏血吸虫钙调神经磷酸酶亚基的分子克隆及其在排泄系统中的免疫定位

Molecular cloning of Schistosoma mansoni calcineurin subunits and immunolocalization to the excretory system.

作者信息

Mecozzi B, Rossi A, Lazzaretti P, Kady M, Kaiser S, Valle C, Cioli D, Klinkert M Q

机构信息

Institute of Cell Biology, Consiglio Nazionale delle Ricerche, Rome, Italy.

出版信息

Mol Biochem Parasitol. 2000 Oct;110(2):333-43. doi: 10.1016/s0166-6851(00)00287-5.

Abstract

In order to explain the schistosomicidal effect of cyclosporin A, the hypothesis was advanced that the drug, complexed with cyclophilin, inhibits the phosphatase activity of parasite calcineurin (CN), with mechanisms similar to those operating in its immunosuppressive action. As a preparatory step to the testing of this hypothesis, we report the molecular cloning of both CN subunits in Schistosoma mansoni. The catalytic (A) subunit has a predicted sequence of 607 amino acids and shows substantial similarity to other cloned CNs, except for the carboxy-terminal end that is highly divergent. The regulatory (B) subunit consists of 169 amino acids that are 86% identical to those of the human counterpart and, from its anomalous electrophoretic mobility, it appears to be myristoylated. The results of Southern blotting experiments are compatible with the existence of multiple genes for CNA and a single gene for CNB. Western blots showed that both subunits are present at all stages of the parasite life cycle and can be detected both in the soluble and in the membrane fraction. Immunofluorescence confocal microscopy revealed a striking concentration of the anti-CNA reactivity in 6-8 discrete spots in the schistosomula and in distinct spots along the body of the adult parasite, corresponding to the expected localization of flame cells. Both patterns were confirmed by a perfect co-localization of the anti-CNA signal with that of a previously characterized anti-flame cell monoclonal antibody. The preferential confinement of schistosome CN to the protonephridial system suggests that the enzyme in the parasite may fulfil similar functions to those performed in mammalian kidneys.

摘要

为了解释环孢素A的杀血吸虫作用,有人提出假说,认为该药物与亲环蛋白结合后,会抑制寄生虫钙调神经磷酸酶(CN)的磷酸酶活性,其作用机制与其免疫抑制作用相似。作为检验这一假说的前期准备步骤,我们报告了曼氏血吸虫中两种CN亚基的分子克隆情况。催化性(A)亚基预测有607个氨基酸序列,与其他已克隆的CN有很大相似性,但羧基末端差异很大。调节性(B)亚基由169个氨基酸组成,与人类对应亚基的氨基酸序列有86%的同一性,且从其异常的电泳迁移率来看,它似乎被肉豆蔻酰化了。Southern印迹实验结果与存在多个CNA基因和单个CNB基因的情况相符。Western印迹显示,这两种亚基在寄生虫生命周期的所有阶段都存在,并且在可溶性部分和膜部分都能检测到。免疫荧光共聚焦显微镜显示,抗CNA反应性在童虫的6 - 8个离散斑点以及成虫虫体的不同斑点中显著聚集,这与焰细胞的预期定位相对应。通过抗CNA信号与先前鉴定的抗焰细胞单克隆抗体的信号完美共定位,证实了这两种模式。血吸虫CN优先局限于原肾系统,这表明寄生虫中的这种酶可能具有与哺乳动物肾脏中所执行的功能类似的功能。

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