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二硫键参与维持刚果锥虫循环后期形态交叉反应决定簇的隐蔽性。

Disulfide bond involvement in the maintenance of the cryptic nature of the cross-reacting determinant of metacyclic forms of Trypanosoma congolense.

作者信息

Fish W R, Muriuki C W, Muthiani A M, Grab D J, Lonsdale-Eccles J D

机构信息

International Laboratory for Research on Animal Diseases, Nairobi, Kenya.

出版信息

Biochemistry. 1989 Jun 27;28(13):5415-21. doi: 10.1021/bi00439a015.

DOI:10.1021/bi00439a015
PMID:2476173
Abstract

The variable surface glycoprotein (VSG) of African trypanosomes possesses a 1,2-dimyristoylglycosylphosphatidylinositol at the carboxy terminus. Cleavage of the 1,2-dimyristoylglycerol (1,2-DMG) moiety from the VSG reportedly results in a higher apparent molecular mass and an increased binding of antibodies against the "cross-reacting determinant" (CRD), a cryptic epitope present on most VSGs. Using metacyclic forms of Trypanosoma congolense, we show that the processes involved are more complex than heretofore presumed and that the removal of the 1,2-DMG moiety may not be necessary for binding of anti-CRD antibodies (RxCRD). Among other findings, we observe the following: (1) in sonicated samples of trypanosomes metabolically labeled with [3H]myristate, the binding of RxCRD on Western blots is coincident with bands containing labeled (membrane form) VSGs; (2) disulfide reduction of trypanosome sonicates suffices to promote RxCRD binding in the presence or absence of inhibitors of a glycosylphosphatidylinositol-specific phospholipase C; (3) trypanosomes directly solubilized in detergents show quantitative and qualitative differences in RxCRD binding which depend upon the detergent used and the order of addition of disulfide reducing agents. We conclude that the binding of RxCRD to T. congolense metacyclic VSGs depends upon the degree of unfolding of the molecule and is clearly a complex, multistep process in which structural changes and disulfide reduction play pivotal roles.

摘要

非洲锥虫的可变表面糖蛋白(VSG)在羧基末端含有一个1,2 - 二肉豆蔻酰基糖基磷脂酰肌醇。据报道,从VSG上切割下1,2 - 二肉豆蔻酰甘油(1,2 - DMG)部分会导致更高的表观分子量,并增加针对“交叉反应决定簇”(CRD)的抗体结合,CRD是大多数VSG上存在的一个隐蔽表位。利用刚果锥虫的循环后期形式,我们发现所涉及的过程比迄今推测的更为复杂,并且去除1,2 - DMG部分对于抗CRD抗体(RxCRD)的结合可能不是必需的。在其他发现中,我们观察到以下几点:(1)在用[³H]肉豆蔻酸进行代谢标记的锥虫超声处理样品中,Western印迹上RxCRD的结合与含有标记的(膜形式)VSG的条带一致;(2)锥虫超声处理物的二硫键还原足以在存在或不存在糖基磷脂酰肌醇特异性磷脂酶C抑制剂的情况下促进RxCRD结合;(3)直接用去污剂溶解的锥虫在RxCRD结合上表现出定量和定性的差异,这取决于所用的去污剂和二硫键还原剂的添加顺序。我们得出结论,RxCRD与刚果锥虫循环后期VSG的结合取决于分子的展开程度,并且显然是一个复杂的多步骤过程,其中结构变化和二硫键还原起着关键作用。

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