首页> 外文期刊>Peptides: An International Journal >Conserved high activity binding peptides from the Plasmodium falciparum Pf34 rhoptry protein inhibit merozoites in vitro invasion of red blood cells.
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Conserved high activity binding peptides from the Plasmodium falciparum Pf34 rhoptry protein inhibit merozoites in vitro invasion of red blood cells.

机译:来自恶性疟原虫Pf34 rhoptry蛋白的保守的高活性结合肽在体外抑制裂殖子入侵红细胞。

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摘要

Rhoptries are specialized secretory organelles found in all members of the genus Plasmodium whose proteins have been considered as promising vaccine candidates due to their involvement in cell invasion and the formation of the parasitophorous vacuole (PV). The Plasmodium falciparum Pf34 protein was recently identified as a rhoptry-neck protein located in detergent-resistant microdomains (DRMs) that is expressed in mature intraerythrocytic parasite stages, but its biological function is still unknown. Receptor-ligand assays carried out in this study found that peptides 36,051 ((101)DKKFSESLKAHMDHLKILNN(120)Y), 36,053 ((141)KKYIIKEIQNNKYLNKEKKS(160)), 36,055 ((181)WLESVNNIEEKSNILKNIKS(200)Y) and 36,056 ((201)QLLNNIASLNHTLSEEIKNI(220)Y), located in the central portion of Pf34, were found to establish protease-sensitive interactions of high affinity and specificity with receptors on the surface of red blood cell (RBCs). In vitro assays showed that Pf34 high activity binding peptides (HABPs) inhibit invasion of RBCs by P. falciparum merozoites, therefore suggesting that Pf34 could act as an adhesin during invasion and supporting the inclusion of Pf34 HABPs in further studies to develop antimalarial control methods.
机译:斜纹夜蛾是在疟原虫属的所有成员中发现的专门的分泌细胞器,由于它们参与细胞侵袭和寄生虫空泡(PV)的形成,其蛋白质被认为是有希望的候选疫苗。最近,恶性疟原虫Pf34蛋白被鉴定为位于成熟抗红细胞内寄生虫阶段表达的去污剂抗性微域(DRM)中的rhoptry-neck蛋白,但其生物学功能仍然未知。在这项研究中进行的受体配体分析发现,肽36,051((101)DKKFSESLKAHMDHLKILNN(120)Y),36053((141)KKYIIKEIQNNKYLNKEKKSKS(160)),36,055((181)WLESVNNIEEKSNILKNIKS(200)Y)和36,056(( 201)QLLNNIASLNHTLSEEIKNI(220)Y)位于Pf34的中心部分,可与红细胞(RBC)表面的受体建立高亲和力和特异性的蛋白酶敏感性相互作用。体外试验表明,Pf34高活性结合肽(HABPs)抑制恶性疟原虫裂殖子对RBC的侵袭,因此表明Pf34可以在侵袭过程中充当粘附素,并支持在进一步研究中开发Pf34 HABPs以开发抗疟疾控制方法。

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