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Synthetic peptides from conserved regions of the Plasmodium falciparum early transcribed membrane and ring exported proteins bind specifically to red blood cell proteins.

机译:恶性疟原虫早期转录的膜和环状输出蛋白保守区的合成肽与红细胞蛋白特异性结合。

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Severe malaria pathology is directly associated with cytoadherence of infected red blood cells (iRBCs) to healthy RBCs and/or endothelial cells occurring during the intraerythrocytic development of Plasmodium falciparum. We synthesized, as 20-mer long peptides, the members of the ring exported (REX) protein family encoded in chromosome 9, as well as the early transcribed membrane proteins (E-TRAMP) 10.2 and 4, to identify specific RBC binding regions in these proteins. Twelve binding peptides were identified (designated as HABPs): three were identified in REX1, two in REX2, one in REX3, two in REX4 and four in E-TRAMP 10.2. The majority of these HABPs was conserved among different P. falciparum strains, according to sequence analysis. No HABPs were found in E-TRAMP 4. Bindings of HABPs were saturable and sensitive to the enzymatic treatment of RBCs and HABPs had different structural features, according to circular dichroism studies. Our results suggest that the REX and E-TRAMP families participate in relevant interactions with RBC membrane proteins, which highlight these proteins as potential targets for the development of fully effective immunoprophylactic methods.
机译:严重的疟疾病理与感染性红细胞(iRBC)与恶性疟原虫红细胞内发育期间发生的健康RBC和/或内皮细胞的细胞粘附直接相关。我们合成了长20肽的长链,编码了9号染色体上编码的环输出(REX)蛋白家族成员,以及早期转录的膜蛋白(E-TRAMP)10.2和4,以识别RBC结合区域中的特定RBC这些蛋白质。鉴定了十二种结合肽(称为HABP):在REX1中鉴定了三个,在REX2中鉴定了两个,在REX3中鉴定了一个,在REX4中鉴定了两个,在E-TRAMP 10.2中鉴定了四个。这些HABP中的大多数在不同的iP中是保守的。根据序列分析确定了恶性疟原虫菌株。在E-TRAMP 4中未发现HABP。根据圆二色性研究,HABP的结合是饱和的且对RBC的酶处理敏感,并且HABP具有不同的结构特征。我们的结果表明,REX和E-TRAMP家族参与了与RBC膜蛋白的相关相互作用,从而突出了这些蛋白作为开发完全有效的免疫预防方法的潜在目标。

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