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建立疟原虫肝期感染的异位人肝模型。

Development of an ectopic huLiver model for Plasmodium liver stage infection.

机构信息

Department of Immunology and Microbiology, University of Colorado School of Medicine, Aurora, Colorado, United States of America.

Department of Drug Discovery, Experimental Therapeutics Branch, Walter Reed Army Institute of Research, Silver Spring, Maryland, United States of America.

出版信息

PLoS One. 2023 Mar 16;18(3):e0279144. doi: 10.1371/journal.pone.0279144. eCollection 2023.

Abstract

Early Plasmodium falciparum and P. vivax infection requires parasite replication within host hepatocytes, referred to as liver stage (LS). However, limited understanding of infection dynamics in human LS exists due to species-specificity challenges. Reported here is a reproducible, easy-to-manipulate, and moderate-cost in vivo model to study human Plasmodium LS in mice; the ectopic huLiver model. Ectopic huLiver tumors were generated through subcutaneous injection of the HC-04 cell line and shown to be infectible by both freshly dissected sporozoites and through the bite of infected mosquitoes. Evidence for complete LS development was supported by the transition to blood-stage infection in mice engrafted with human erythrocytes. Additionally, this model was successfully evaluated for its utility in testing antimalarial therapeutics, as supported by primaquine acting as a causal prophylactic against P. falciparum. Presented here is a new platform for the study of human Plasmodium infection with the potential to aid in drug discovery.

摘要

疟原虫早期感染疟原虫和间日疟原虫需要寄生虫在宿主肝细胞内复制,称为肝期(LS)。然而,由于物种特异性的挑战,对人类 LS 感染动力学的了解有限。本文报道了一种可重复、易于操作且成本适中的体内模型,用于在小鼠中研究人类疟原虫 LS;异位 huLiver 模型。异位 huLiver 肿瘤通过皮下注射 HC-04 细胞系产生,并显示可被新鲜分离的子孢子和受感染蚊子的叮咬感染。通过用人红细胞移植的小鼠中出现血液期感染,证明了完全 LS 发育的证据。此外,该模型在测试抗疟治疗药物的实用性方面取得了成功,支持了伯氨喹作为疟原虫的因果预防药物。本文提出了一种新的研究人类疟原虫感染的平台,具有辅助药物发现的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cb2d/10019673/2bb2a6c0a179/pone.0279144.g001.jpg

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