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蛋白酶和蛋白聚糖在肥大细胞及其他造血细胞颗粒中的包装。小鼠肥大细胞蛋白酶7上的一组组氨酸簇调节其与肝素丝甘蛋白聚糖的结合。

Packaging of proteases and proteoglycans in the granules of mast cells and other hematopoietic cells. A cluster of histidines on mouse mast cell protease 7 regulates its binding to heparin serglycin proteoglycans.

作者信息

Matsumoto R, Sali A, Ghildyal N, Karplus M, Stevens R L

机构信息

Department of Medicine, Harvard Medical School, Brigham and Women's Hospital, Boston, Massachusetts 02115, USA.

出版信息

J Biol Chem. 1995 Aug 18;270(33):19524-31. doi: 10.1074/jbc.270.33.19524.

DOI:10.1074/jbc.270.33.19524
PMID:7642636
Abstract

Mouse mast cell protease 7 (mMCP-7) is a tryptase stored in the secretory granules of mast cells. At the granule pH of 5.5, mMCP-7 is fully active and is bound to heparin-containing serglycin proteoglycans. to understand the interaction of mMCP-7 with heparin inside and outside the mast cell, this trytase was first studied by comparative protein modeling. The "pro" form of mMCP-7 was then expressed in insect cells and studied by site-directed mutagenesis. Although mMCP-7 lacks known linear sequences of amino acis that interact with heparin, the three-dimensional model of mMCP-7 revealed an area on the surface of the folded protein away from the substrate-binding site that exhibits a strong positive electrostatic potential at the acidic pH of the granule. In agreement with this calculation, recombinant pro-mMCP-7 bound to a heparin-affinity column at pH 5.5 and readily dissociated from the column at pH > 6.5. Site-directed mutagenesis confirmed the prediction that the conversion of His residues 8,68, and 70 in the positively charged region into Glu prevents the binding of pro-mMCP-7 to heparin. Because the binding requires positively charged His residues, native mMCP-7 is able to dissociate from the protease/proteoglycan macromolecular complex when the complex is exocytosed from bone marrow-derived mast cells into a neutral pH environment. Many hematopoietic effector cells store positively charged proteins in granules that contain serglycin proteoglycans. The heparin/mMCP-7 interaction, which depends on the tertiary structure of the tryptase, may be representative of a general control mechanism by which hematopoietic cells maximize storage of properly folded, enzymatically active proteins in their granules.

摘要

小鼠肥大细胞蛋白酶7(mMCP - 7)是一种储存在肥大细胞分泌颗粒中的类胰蛋白酶。在颗粒pH值为5.5时,mMCP - 7具有完全活性,并与含肝素的丝甘氨酸蛋白聚糖结合。为了解mMCP - 7在肥大细胞内外与肝素的相互作用,首先通过比较蛋白质建模对这种类胰蛋白酶进行了研究。然后在昆虫细胞中表达了mMCP - 7的“前体”形式,并通过定点诱变进行研究。尽管mMCP - 7缺乏与肝素相互作用的已知氨基酸线性序列,但mMCP - 7的三维模型显示,在折叠蛋白表面远离底物结合位点的区域,在颗粒的酸性pH值下呈现出强正静电势。与该计算结果一致,重组前体mMCP - 7在pH 5.5时与肝素亲和柱结合,并在pH > 6.5时容易从柱上解离。定点诱变证实了以下预测:将带正电荷区域中的组氨酸残基8、68和70转换为谷氨酸会阻止前体mMCP - 7与肝素结合。由于这种结合需要带正电荷的组氨酸残基,当该复合物从骨髓来源的肥大细胞胞吐到中性pH环境中时,天然mMCP - 7能够从蛋白酶/蛋白聚糖大分子复合物中解离。许多造血效应细胞在含有丝甘氨酸蛋白聚糖的颗粒中储存带正电荷的蛋白质。肝素/mMCP - 7的相互作用取决于类胰蛋白酶的三级结构,可能代表了一种普遍的控制机制,通过该机制造血细胞在其颗粒中最大限度地储存正确折叠、具有酶活性的蛋白质。

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