Putative circumsporozoite protein (CSP) of Plasmodium vivax is considerably distinct from the well-known CSP and plays a role in the protein ubiquitination pathway.

Q3 Biochemistry, Genetics and Molecular Biology Gene: X Pub Date : 2019-11-12 eCollection Date: 2019-12-01 DOI:10.1016/j.gene.2019.100024

Manoswini Dash, Veena Pande, Abhinav Sinha

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Abstract

Amidst technical challenges which limit successful culture and genetic manipulation of P. vivax parasites, we used a computational approach to identify a critical target with evolutionary significance. The putative circumsporozoite protein on chromosome 13 of P. vivax (PvpuCSP)is distinct from the well-known vaccine candidate PfCSP. The aim of this study was to understand the role of PvpuCSP and its relatedness to the well-known CSP. The study revealed PvpuCSP as a membrane bound E3 ubiquitin ligase involved in ubiquitination. It has a species-specific tetra-peptide unit which is differentially repeated in various P. vivax strains. The PvpuCSP is different from CSP in terms of stage-specific expression and function. Since E3 ubiquitin ligases are known antimalarial drug targets targeting the proteasome pathway, PvpuCSP, with evolutionary connotation and a key role in orchestrating protein degradation in P. vivax, can be explored as a potential drug target.

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间日疟原虫的假定环孢子虫蛋白（CSP）与众所周知的 CSP 有很大不同，它在蛋白质泛素化途径中发挥作用。

技术上的挑战限制了对间鞭毛虫寄生虫的成功培养和基因操作，在这种情况下，我们利用计算方法确定了一个具有进化意义的关键靶标。间日疟原虫第13号染色体上的假定环孢子虫蛋白（PvpuCSP）与众所周知的候选疫苗PfCSP不同。本研究的目的是了解 PvpuCSP 的作用及其与众所周知的 CSP 的关系。研究发现，PvpuCSP 是一种膜结合 E3 泛素连接酶，参与泛素化。它有一个物种特异性的四肽单元，在不同的间日疟原虫菌株中有不同的重复。PvpuCSP 在特异性表达和功能方面与 CSP 不同。由于 E3 泛素连接酶是针对蛋白酶体途径的已知抗疟疾药物靶标，PvpuCSP 具有进化内涵，在协调间日疟原虫蛋白质降解方面发挥着关键作用，因此可作为潜在的药物靶标进行研究。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Gene: X Biochemistry, Genetics and Molecular Biology-Genetics

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