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PfMAP-2 对疟原虫恶性疟原虫的雄性配子体发生是必需的。

PfMAP-2 is essential for male gametogenesis in the malaria parasite Plasmodium falciparum.

机构信息

Department of Medical Parasitology and Infection Biology, Swiss Tropical and Public Health Institute, 4051, Basel, Switzerland.

University of Basel, 4001, Basel, Switzerland.

出版信息

Sci Rep. 2020 Jul 17;10(1):11930. doi: 10.1038/s41598-020-68717-5.

Abstract

In malaria parasites, male gametogenesis is a proliferative stage essential for parasite transmission to the mosquito vector. It is a rapid process involving three rounds of genome replication alternating with closed endomitoses, and assembly of axonemes to produce eight flagellated motile microgametes. Studies in Plasmodium berghei have highlighted tight regulation of gametogenesis by a network of kinases. The P. berghei MAPK homologue PbMAP-2 is dispensable for asexual development but important at the induction of axoneme motility. However, in P. falciparum, causing the most severe form of human malaria, PfMAP-2 was suggested to be essential for asexual proliferation indicating distinct functions for MAP-2 in these two Plasmodium species. We here show that PfMAP-2 is dispensable for asexual growth but important for male gametogenesis in vitro. Similar to PbMAP-2, PfMAP-2 is required for initiating axonemal beating but not for prior DNA replication or axoneme formation. In addition, single and double null mutants of PfMAP-2 and the second P. falciparum MAPK homologue PfMAP-1 show no defect in asexual proliferation, sexual commitment or gametocytogenesis. Our results suggest that MAPK activity plays no major role in the biology of both asexual and sexual blood stage parasites up until the point of male gametogenesis.

摘要

在疟原虫中,雄性配子发生是寄生虫传播给蚊子媒介所必需的增殖阶段。这是一个快速的过程,涉及三轮基因组复制,与有丝分裂交替进行,并组装轴丝产生八个鞭毛运动的精子。在伯氏疟原虫中的研究强调了由激酶网络对配子发生的紧密调控。疟原虫 MAPK 同源物 PbMAP-2 对于无性发育不是必需的,但对于轴丝运动的诱导是重要的。然而,在引起最严重形式的人类疟疾的恶性疟原虫中,PfMAP-2 被认为对于无性增殖是必需的,这表明 MAP-2 在这两种疟原虫中具有不同的功能。我们在这里表明 PfMAP-2 对于体外无性生长是可有可无的,但对于雄性配子发生是重要的。与 PbMAP-2 相似,PfMAP-2 对于启动轴丝跳动是必需的,但对于先前的 DNA 复制或轴丝形成不是必需的。此外,PfMAP-2 和第二种恶性疟原虫 MAPK 同源物 PfMAP-1 的单突变体和双突变体在无性增殖、性承诺或配子发生中没有缺陷。我们的结果表明,MAPK 活性在无性和有性血液阶段寄生虫的生物学中直到雄性配子发生阶段都没有发挥主要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/76e7/7368081/a31fb6406398/41598_2020_68717_Fig1_HTML.jpg

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