Biogenesis and maintenance of the apicoplast in model apicomplexan parasites

顶端体 生物 生物发生 质体 顶复亚门 细胞器生物发生 细胞器 基因组 TSG101型 计算生物学 中心体 细胞生物学 遗传学 基因 恶性疟原虫 细胞周期 微泡 疟疾 叶绿体 小RNA 免疫学
作者
Ying Zhang,Chun-Ren Wang,Honglin Jia
出处
期刊:Parasitology International [Elsevier]
卷期号:81: 102270-102270 被引量:2
标识
DOI:10.1016/j.parint.2020.102270
摘要

The apicoplast is a non-photosynthetic relict plastid of Apicomplexa that evolved from a secondary symbiotic system. During its evolution, most of the genes derived from its alga ancestor were lost. Only genes involved in several valuable metabolic pathways, such as the synthesis of isoprenoid precursors, heme, and fatty acids, have been transferred to the host genome and retained to help these parasites adapt to a complex life cycle and various living environments. The biological function of an apicoplast is essential for most apicomplexan parasites. Considering their potential as drug targets, the metabolic functions of this symbiotic organelle have been intensively investigated through computational and biological means. Moreover, we know that not only organellar metabolic functions are linked with other organelles, but also their biogenesis processes have developed and evolved to tailor their biological functions and proper inheritance. Several distinct features have been found in the biogenesis process of apicoplasts. For example, the apicoplast borrows a dynamin-related protein (DrpA) from its host to implement organelle division. The autophagy system has also been repurposed for linking the apicoplast and centrosome during replication and the division process. However, many vital questions remain to be answered about how these parasites maintain and properly inherit this symbiotic organelle. Here we review our current knowledge about its biogenesis process and discuss several critical questions remaining to be answered in this field.

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