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间日疟原虫的基因组测序确定了大陆隔离以及与乙胺嘧啶敏感性降低相关的突变。

Genome sequencing of Plasmodium malariae identifies continental segregation and mutations associated with reduced pyrimethamine susceptibility.

作者信息

Ibrahim Amy, Mohring Franziska, Manko Emilia, van Schalkwyk Donelly A, Phelan Jody E, Nolder Debbie, Borrmann Steffen, Adegnika Ayola A, Di Santi Silvia Maria, Alam Mohammad Shafiul, Mondal Dinesh, Nosten Francois, Sutherland Colin J, Moon Robert W, Clark Taane G, Campino Susana

机构信息

Faculty of Infectious & Tropical Diseases, London School of Hygiene & Tropical Medicine, London, UK.

Public Health England Malaria Reference Laboratory, London School of Hygiene & Tropical Medicine, London, UK.

出版信息

Nat Commun. 2024 Dec 30;15(1):10779. doi: 10.1038/s41467-024-55102-3.

Abstract

Plasmodium malariae parasites are widely observed across the tropics and sub-tropics. This slow-growing species, known to maintain chronic asymptomatic infections, has been associated with reduced antimalarial susceptibility. We analyse 251 P. malariae genomes from 28 countries, and leveraging 131,601 high-quality SNPs, demonstrate segregation of African and Asian isolates. Signals of recent evolutionary selection were identified in genes encoding putative surface proteins (pmmsp1) and putative erythrocyte invasion proteins (pmdpap3, pmrbp2, pmnif4). Amino acid substitutions were identified in orthologs of genes associated with antimalarial susceptibility including 2 amino acid substitutions in pmdhfr aligning with pyrimethamine resistance mutations in P. falciparum. Additionally, we characterise pmdhfr mutation F57L and demonstrate its involvement in reduced susceptibility to pyrimethamine in an in vitro parasite assay. We validate CRISPR-Cas9 mediated ortholog replacement in P. knowlesi parasites to determine the function of pmdhfr mutations and demonstrate that circulating pmdhfr genotypes are less susceptible to pyrimethamine.

摘要

间日疟原虫在热带和亚热带地区广泛存在。这种生长缓慢的物种会引发慢性无症状感染,并且与抗疟药物敏感性降低有关。我们分析了来自28个国家的251个间日疟原虫基因组,并利用131,601个高质量单核苷酸多态性(SNP),证明了非洲和亚洲分离株的分离情况。在编码假定表面蛋白(pmmsp1)和假定红细胞入侵蛋白(pmdpap3、pmrbp2、pmnif4)的基因中发现了近期进化选择的信号。在与抗疟药物敏感性相关的基因直系同源物中发现了氨基酸替换,包括pmdhfr中的2个氨基酸替换,这些替换与恶性疟原虫中的乙胺嘧啶抗性突变一致。此外,我们对pmdhfr突变F57L进行了表征,并在体外寄生虫试验中证明了其与对乙胺嘧啶敏感性降低有关。我们验证了CRISPR-Cas9介导的诺氏疟原虫直系同源物替换,以确定pmdhfr突变的功能,并证明循环中的pmdhfr基因型对乙胺嘧啶的敏感性较低。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fa61/11685946/ba61ccc1cd5e/41467_2024_55102_Fig1_HTML.jpg

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