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布氏锥虫的酸钙小球含有肌醇 1,4,5-三磷酸受体,该受体对于生长和感染力是必需的。

Acidocalcisomes of Trypanosoma brucei have an inositol 1,4,5-trisphosphate receptor that is required for growth and infectivity.

机构信息

Center for Tropical and Emerging Global Diseases and Department of Cellular Biology, University of Georgia, Athens, GA 30602, USA.

出版信息

Proc Natl Acad Sci U S A. 2013 Jan 29;110(5):1887-92. doi: 10.1073/pnas.1216955110. Epub 2013 Jan 14.

Abstract

Acidocalcisomes are acidic calcium stores rich in polyphosphate and found in a diverse range of organisms. The mechanism of Ca(2+) release from these organelles was unknown. Here we present evidence that Trypanosoma brucei acidocalcisomes possess an inositol 1,4,5-trisphosphate receptor (TbIP(3)R) for Ca(2+) release. Localization studies in cell lines expressing TbIP(3)R in its endogenous locus fused to an epitope tag revealed its partial colocalization with the vacuolar proton pyrophosphatase, a marker of acidocalcisomes. IP(3) was able to stimulate Ca(2+) release from a chicken B-lymphocyte cell line in which the genes for all three vertebrate IP(3)Rs have been stably ablated (DT40-3KO) and that were stably expressing TbIP(3)R, providing evidence of its function. IP(3) was also able to release Ca(2+) from permeabilized trypanosomes or isolated acidocalcisomes and photolytic release of IP(3) in intact trypanosomes loaded with Fluo-4 elicited a transient Ca(2+) increase in their cytosol. Ablation of TbIP(3)R by RNA interference caused a significant reduction of IP(3)-mediated Ca(2+) release in trypanosomes and resulted in defects in growth in culture and infectivity in mice. Taken together, the data provide evidence of the presence of a functional IP(3)R as a Ca(2+) release channel in acidocalcisomes of trypanosomes and suggest that a Ca(2+) signaling pathway that involves acidocalcisomes is required for growth and establishment of infection.

摘要

酸钙小体是富含多磷酸盐的酸性钙库,存在于多种生物体中。这些细胞器中 Ca(2+) 释放的机制尚不清楚。本文报道了布氏锥虫酸钙小体存在肌醇 1,4,5-三磷酸受体(TbIP(3)R)介导的 Ca(2+) 释放。在表达 TbIP(3)R 的细胞系中进行的定位研究,其内源基因融合了一个表位标签,结果显示其与液泡质子焦磷酸酶部分共定位,液泡质子焦磷酸酶是酸钙小体的标志物。IP(3)能够刺激已稳定敲除所有三种脊椎动物 IP(3)R 基因的鸡 B 淋巴细胞系(DT40-3KO)和稳定表达 TbIP(3)R 的细胞系释放 Ca(2+),这提供了其功能的证据。IP(3)也能够从通透化的锥虫或分离的酸钙小体中释放 Ca(2+),用光解释放的 IP(3)在 Fluo-4 负载的完整锥虫中引发细胞质中短暂的 Ca(2+)增加。RNA 干扰敲除 TbIP(3)R 导致 IP(3)介导的 Ca(2+)释放在锥虫中显著减少,并导致培养物中的生长缺陷和在小鼠中的感染性缺陷。综上所述,这些数据为酸钙小体中存在功能性 IP(3)R 作为 Ca(2+) 释放通道提供了证据,并表明涉及酸钙小体的 Ca(2+) 信号通路是生长和建立感染所必需的。

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