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一种对人I型和IV型胶原具有特异性的克氏锥虫分泌型80 kDa蛋白酶。

A Trypanosoma cruzi-secreted 80 kDa proteinase with specificity for human collagen types I and IV.

作者信息

Santana J M, Grellier P, Schrével J, Teixeira A R

机构信息

Laboratório Multidisciplinar de Pesquisa em Doença de Chagas, Departamentos de Biologia Celular e de Patologia, Universidade de Brasília, CP 04536, 70919-970, Brasília, DF, Brazil.

出版信息

Biochem J. 1997 Jul 1;325 ( Pt 1)(Pt 1):129-37. doi: 10.1042/bj3250129.

Abstract

Specific interactions between parasites and extracellular matrix components are an important mechanism in the dissemination of Chagas' disease. Binding of the extracellular matrix proteins to Trypanosoma cruzi receptors has been described as a significant step in this phenomenon. In this study, a specific proteinase activity was identified in cell-free extracts of amastigote, trypomastigote and epimastigote forms of T. cruzi using the collagenase fluorogenic substrate N-Suc-Gly-Pro-Leu-Gly-Pro-7-amido-4-methylcoumarin. Isolation of this activity was achieved by a four-step FPLC procedure. Optimal enzyme activity was found to occur at pH 8.0 and was associated with a single T. cruzi 80 kDa protein (Tc 80 proteinase) on SDS/PAGE under reducing conditions. An internal peptide sequence of Tc 80 proteinase was obtained (AGDNYTPPE), and no similarity was found to previously described proteinases of T. cruzi. This enzyme activity is strongly inhibited by HgCl2, tosyl-lysylchloromethane ('TLCK') p-chloromercuribenzoate and benzyloxycarbonyl-Phe-Ala-diazomethane. The purified enzyme was able to hydrolyse purified human [14C]collagen types I and IV at neutral pH, but not 14C-labelled BSA, rat laminin, rabbit IgG or small proteins such as insulin or cytochrome c. In addition, Tc 80 proteinase activity was found to be secreted by T. cruzi forms infective to mammalian cells. Furthermore we demonstrated that purified Tc 80 proteinase mediates native collagen type I hydrolysis in rat mesentery. This feature is compared with that of Clostridium histolyticum collagenase. These findings suggest that Tc 80 proteinase may facilitate T. cruzi host-cell infection by degrading the collagens of the extracellular matrix and could represent a good target for Chagas' disease chemotherapy.

摘要

寄生虫与细胞外基质成分之间的特异性相互作用是恰加斯病传播的重要机制。细胞外基质蛋白与克氏锥虫受体的结合被认为是这一现象中的重要步骤。在本研究中,使用胶原酶荧光底物N - Suc - Gly - Pro - Leu - Gly - Pro - 7 - 氨基 - 4 - 甲基香豆素,在克氏锥虫无鞭毛体、上鞭毛体和锥鞭毛体形式的无细胞提取物中鉴定出一种特异性蛋白酶活性。通过四步快速蛋白质液相色谱(FPLC)程序实现了该活性的分离。发现在还原条件下的SDS / PAGE上,最佳酶活性在pH 8.0时出现,并与单一的克氏锥虫80 kDa蛋白(Tc 80蛋白酶)相关。获得了Tc 80蛋白酶的内部肽序列(AGDNYTPPE),并且未发现与先前描述的克氏锥虫蛋白酶有相似性。该酶活性受到HgCl2、甲苯磺酰 - 赖氨酰氯甲烷(“TLCK”)、对氯汞苯甲酸酯和苄氧羰基 - Phe - Ala - 重氮甲烷的强烈抑制。纯化的酶能够在中性pH下水解纯化的人I型和IV型[14C]胶原,但不能水解14C标记的牛血清白蛋白、大鼠层粘连蛋白、兔IgG或诸如胰岛素或细胞色素c等小蛋白质。此外,发现Tc 80蛋白酶活性由对哺乳动物细胞有感染性的克氏锥虫形式分泌。此外,我们证明纯化的Tc 80蛋白酶介导大鼠肠系膜中天然I型胶原的水解。将该特征与溶组织梭菌胶原酶的特征进行了比较。这些发现表明,Tc 80蛋白酶可能通过降解细胞外基质的胶原促进克氏锥虫感染宿主细胞,并且可能是恰加斯病化疗的良好靶点。

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