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PfPuf2 是 Puf 家族 RNA 结合蛋白,调控疟原虫(Plasmodium falciparum)有性生殖和性别分化。

The Puf-family RNA-binding protein PfPuf2 regulates sexual development and sex differentiation in the malaria parasite Plasmodium falciparum.

机构信息

Department of Entomology, The Pennsylvania State University, University Park, PA 16802, USA.

出版信息

J Cell Sci. 2010 Apr 1;123(Pt 7):1039-49. doi: 10.1242/jcs.059824. Epub 2010 Mar 2.

Abstract

Translation regulation plays an important role during gametocytogenesis in the malaria parasite, a process that is obligatory for the transmission of the parasite through mosquito vectors. In this study we determined the function of PfPuf2, a member of the Puf family of translational repressors, in gametocytogenesis of Plasmodium falciparum. Tagging of the endogenous PfPuf2 protein with green fluorescent protein showed that PfPuf2 was expressed in both male and female gametocytes, and the protein was localized in the cytoplasm of the parasite. Targeted disruption of the PfPuf2 gene did not affect asexual growth of the parasite, but promoted the formation of gametocytes and differentiation of male gametocytes. Complementation studies were performed to confirm that the resultant phenotypic changes were due to disruption of the PfPuf2 gene. Episomal expression of PfPuf2 under its cognate promoter almost restored the gametocytogenesis rate in a PfPuf2 disruptant to the level of the wild-type parasite. It also partially restored the effect of PfPuf2 disruption on male-female sex ratio. In addition, episomal overexpression of PfPuf2 under its cognate promoter but with a higher concentration of the selection drug or under the constitutive hsp86 promoter in both the PfPuf2-disruptant and wild-type 3D7 lines, further dramatically reduced gametocytogenesis rates and sex ratios. These findings suggest that in this early branch of eukaryotes the function of PfPuf2 is consistent with the ancestral function of suppressing differentiation proposed for Puf-family proteins.

摘要

翻译调控在疟原虫配子体发生中起着重要作用,这是寄生虫通过蚊子媒介传播所必需的。在这项研究中,我们确定了 PfPuf2(翻译抑制因子 Puf 家族的一员)在恶性疟原虫配子体发生中的功能。PfPuf2 内源性蛋白与绿色荧光蛋白的标记显示 PfPuf2 在雄配子体和雌配子体中均有表达,该蛋白定位于寄生虫的细胞质中。PfPuf2 基因的靶向敲除不影响寄生虫的无性生长,但促进了配子体的形成和雄配子体的分化。通过互补研究证实,产生的表型变化是由于 PfPuf2 基因的敲除所致。PfPuf2 在其同源启动子下的附加表达几乎将 PfPuf2 敲除突变体中的配子体发生率恢复到野生型寄生虫的水平。它还部分恢复了 PfPuf2 敲除对雌雄性别比的影响。此外,PfPuf2 在其同源启动子下的附加表达(但选择药物浓度较高)或在 PfPuf2 敲除突变体和野生型 3D7 系中组成型 hsp86 启动子下的过表达,进一步显著降低了配子体发生率和性别比。这些发现表明,在这种真核生物的早期分支中,PfPuf2 的功能与 Puf 家族蛋白所提出的抑制分化的祖先功能一致。

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