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肌球蛋白 A 的磷酸化调节滑行运动,对疟原虫传播至关重要。

Phosphorylation of myosin A regulates gliding motility and is essential for Plasmodium transmission.

机构信息

Integrative Parasitology, Center for Infectious Diseases, University of Heidelberg Medical School, Heidelberg, Germany.

German Center for Infection Research, DZIF Partner Site Heidelberg, Heidelberg, Germany.

出版信息

EMBO Rep. 2022 Jul 5;23(7):e54857. doi: 10.15252/embr.202254857. Epub 2022 May 4.

Abstract

Malaria-causing parasites rely on an actin-myosin-based motor for the invasion of different host cells and tissue traversal in mosquitoes and vertebrates. The unusual myosin A of Plasmodium spp. has a unique N-terminal extension, which is important for red blood cell invasion by P. falciparum merozoites in vitro and harbors a phosphorylation site at serine 19. Here, using the rodent-infecting P. berghei we show that phosphorylation of serine 19 increases ookinete but not sporozoite motility and is essential for efficient transmission of Plasmodium by mosquitoes as S19A mutants show defects in mosquito salivary gland entry. S19A along with E6R mutations slow ookinetes and salivary gland sporozoites in both 2D and 3D environments. In contrast to data from purified proteins, both E6R and S19D mutations lower force generation by sporozoites. Our data show that the phosphorylation cycle of S19 influences parasite migration and force generation and is critical for optimal migration of parasites during transmission from and to the mosquito.

摘要

疟原虫寄生虫依赖肌动球蛋白为基础的运动,用于入侵不同的宿主细胞和在蚊子和脊椎动物中组织迁移。疟原虫属的不寻常肌球蛋白 A 具有独特的 N 端延伸,这对于疟原虫裂殖子体外入侵红细胞是很重要的,并且在丝氨酸 19 上具有一个磷酸化位点。在这里,我们使用感染啮齿动物的 P. berghei 表明丝氨酸 19 的磷酸化增加了动合子但不是子孢子的运动能力,并且对于蚊子的高效传播是必不可少的,因为 S19A 突变体在蚊子唾液腺进入中显示出缺陷。S19A 与 E6R 突变一起在 2D 和 3D 环境中减缓动合子和唾液腺子孢子的运动。与纯化蛋白的数据相反,E6R 和 S19D 突变都会降低子孢子的力产生。我们的数据表明,S19 的磷酸化循环影响寄生虫的迁移和力产生,并且对于从蚊子到蚊子的传播过程中寄生虫的最佳迁移是至关重要的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/254e/9253774/21c68de26b57/EMBR-23-e54857-g006.jpg

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