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刚地弓形虫热休克蛋白90是一个潜在的药物靶点,其表达和亚细胞定位受发育调控。

Toxoplasma gondii Hsp90 is a potential drug target whose expression and subcellular localization are developmentally regulated.

作者信息

Echeverria Pablo C, Matrajt Mariana, Harb Omar S, Zappia María P, Costas Monica A, Roos David S, Dubremetz Jean François, Angel Sergio O

机构信息

Laboratorio de Parasitología Molecular, UB2, IIB-INTECH, CONICET-UNSAM, Camino de Circunvalación Laguna Km. 6, C.C 164, (B7130IIWA)Chascomús, Prov. Buenos Aires, Argentina.

出版信息

J Mol Biol. 2005 Jul 22;350(4):723-34. doi: 10.1016/j.jmb.2005.05.031.

Abstract

Two replicative forms characterize the asexual cycle of the protozoan parasite Toxoplasma gondii: rapidly growing tachyzoites and slowly dividing encysted bradyzoites. The mechanisms that regulate the transition between these two stages are not clearly understood. However, stress inducers that also activate heat shock protein expression can trigger formation of bradyzoites in vitro. Here, we studied the association of the T.gondii Hsp90 with modulation of parasite differentiation and response to stress stimuli using RH DeltaUPRT parasites and the cystogenic strain ME49 and a clone derivative of that strain, PK. Our results show that Hsp90 transcript and protein levels increase under stress or bradyzoite differentiation conditions. Moreover, fluorescence microscopy studies revealed that Hsp90 is present in the cytosol of tachyzoites and both in the nucleus and cytosol of mature bradyzoites, suggesting a correlation between its subcellular organization and these two developmental stages. To further characterize the role for Hsp90 in bradyzoite differentiation, T.gondii tachyzoite mutants that are defective in differentiation showed the same staining pattern as tachyzoites under differentiation conditions. In addition, geldanamycin, a benzoquinone ansamycin antibiotic capable of binding and disrupting the function of Hsp90, blocked conversion both from the tachyzoite to bradyzoite and the bradyzoite to tachyzoite stage, suggesting an essential role for this protein in the regulation of stage interconversion. These results thus suggest Hsp90 may play a role in stage switch.

摘要

两种复制形式表征了原生动物寄生虫刚地弓形虫的无性繁殖周期

快速生长的速殖子和缓慢分裂的包囊缓殖子。调节这两个阶段之间转变的机制尚不清楚。然而,也能激活热休克蛋白表达的应激诱导剂可在体外触发缓殖子的形成。在此,我们使用RH DeltaUPRT寄生虫、产孢囊菌株ME49及其克隆衍生物PK,研究了刚地弓形虫热休克蛋白90(Hsp90)与寄生虫分化调节及应激刺激反应之间的关联。我们的结果表明,在应激或缓殖子分化条件下,Hsp90的转录本和蛋白质水平会升高。此外,荧光显微镜研究显示,Hsp90存在于速殖子的细胞质中,也存在于成熟缓殖子的细胞核和细胞质中,这表明其亚细胞定位与这两个发育阶段之间存在相关性。为了进一步阐明Hsp90在缓殖子分化中的作用,在分化方面存在缺陷的刚地弓形虫速殖子突变体在分化条件下显示出与速殖子相同的染色模式。此外,格尔德霉素是一种能够结合并破坏Hsp90功能的苯醌安莎霉素类抗生素,它阻断了从速殖子到缓殖子以及从缓殖子到速殖子阶段的转变,表明该蛋白在阶段相互转换的调节中起着至关重要的作用。因此,这些结果表明Hsp90可能在阶段转换中发挥作用。

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