Human erythroid spectrin alpha subunit and its SH3 domain are sensitive to acidic Plasmodium falciparum proteolytic activity.

S L Le Bonniec, C Fournier, C Deregnaucourt, P Grellier, D Dhermy, M C Lecomte, J Schrevel
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Abstract

Many proteases play a crucial role in the Plasmodium intraerythrocytic life cycle. Spectrin depletion, one of the major events involved in parasite release from the red blood cell, results from proteolytic activities associated with the presence of the intracellular parasite. Here, we describe a new acidic proteolytic activity from Plasmodium falciparum, whose target is the alpha-subunit of human spectrin. Immunoblotting experiments with antibodies specific for the tryptic peptides of the alpha-chain and in vitro proteolysis tests on recombinant peptides from different regions of the spectrin alpha subunit demonstrated that cleavage sites for the parasite proteolytic activity were localized within the SH3 motif of the alpha-chain sequence. Remarkably, this Plasmodium protease activity on spectrin SH3 substrate was unable to cleave the SH3 from fodrin, a non-erythroid spectrin.

人红细胞谱蛋白α亚基及其SH3结构域对酸性恶性疟原虫蛋白水解活性敏感。
许多蛋白酶在疟原虫的红细胞内生命周期中起着至关重要的作用。Spectrin耗竭是红细胞中寄生虫释放的主要事件之一,是与细胞内寄生虫存在相关的蛋白水解活动的结果。在这里,我们描述了恶性疟原虫的一种新的酸性蛋白水解活性,其目标是人光谱蛋白的α亚基。α -链色氨酸特异性抗体免疫印迹实验和α -亚基不同区域重组肽的体外蛋白水解实验表明,疟原虫蛋白水解活性的裂解位点位于α -链序列的SH3基序内。值得注意的是,疟原虫蛋白酶在spectrin SH3底物上的活性不能将SH3从fodrin(一种非红系spectrin)中分离出来。
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