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Signalling in malaria parasites – The MALSIG consortium

机译:疟原虫中的信号传递– MALSIG联盟

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Depending on their developmental stage in the life cycle, malaria parasites develop within or outside host cells, and in extremely diverse contexts such as the vertebrate liver and blood circulation, or the insect midgut and hemocoel. Cellular and molecular mechanisms enabling the parasite to sense and respond to the intra- and the extra-cellular environments are therefore key elements for the proliferation and transmission of Plasmodium, and therefore are, from a public health perspective, strategic targets in the fight against this deadly disease. The MALSIG consortium, which was initiated in February 2009, was designed with the primary objective to integrate research ongoing in Europe and India on i) the properties of Plasmodium signalling molecules, and ii) developmental processes occurring at various points of the parasite life cycle. On one hand, functional studies of individual genes and their products in Plasmodium falciparum (and in the technically more manageable rodent model Plasmodium berghei) are providing information on parasite protein kinases and phosphatases, and of the molecules governing cyclic nucleotide metabolism and calcium signalling. On the other hand, cellular and molecular studies are elucidating key steps of parasite development such as merozoite invasion and egress in blood and liver parasite stages, control of DNA replication in asexual and sexual development, membrane dynamics and trafficking, production of gametocytes in the vertebrate host and further parasite development in the mosquito. This article, which synthetically reviews such signalling molecules and cellular processes, aims to provide a glimpse of the global frame in which the activities of the MALSIG consortium will develop over the next three years.
机译:根据其生命周期的发育阶段,疟疾寄生虫会在宿主细胞内或宿主外以及在极为多样的环境中发展,例如脊椎动物的肝脏和血液循环,或昆虫的中肠和嗜血菌。因此,使寄生虫能够感知和响应细胞内和细胞外环境的细胞和分子机制是疟原虫增殖和传播的关键要素,因此,从公共卫生的角度来看,这是与之抗争的战略目标致命的疾病。 MALSIG联盟始于2009年2月,其主要目的是整合欧洲和印度正在进行的有关以下方面的研究:i)疟原虫信号分子的特性,ii)寄生虫生命周期各个阶段发生的发育过程。一方面,恶性疟原虫(以及在技术上更易于管理的啮齿动物模型伯氏疟原虫)中单个基因及其产物的功能研究正在提供有关寄生虫蛋白激酶和磷酸酶以及控制环核苷酸代谢和钙信号传导的分子的信息。另一方面,细胞和分子研究正在阐明寄生虫发育的关键步骤,例如裂殖子在血液和肝脏寄生虫阶段的侵袭和流出,无性和性发育中DNA复制的控制,膜动力学和运输,脊椎动物配子细胞的产生在蚊子中宿主并进一步寄生虫。本文对这些信号分子和细胞过程进行了综合综述,旨在提供一个全球框架的概览,MALSIG联盟的活动将在未来三年内发展。

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