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首页> 外文期刊>Eukaryotic cell >CMF22 Is a Broadly Conserved Axonemal Protein and Is Required for Propulsive Motility in Trypanosoma brucei
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CMF22 Is a Broadly Conserved Axonemal Protein and Is Required for Propulsive Motility in Trypanosoma brucei

机译:CMF22是一种广泛保存的轴索蛋白,对于布鲁氏锥虫的推进动力是必需的

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The eukaryotic flagellum (or cilium) is a broadly conserved organelle that provides motility for many pathogenic protozoa and is critical for normal development and physiology in humans. Therefore, defining core components of motile axonemes enhances understanding of eukaryotic biology and provides insight into mechanisms of inherited and infectious diseases in humans. In this study, we show that component of motile flagella 22 (CMF22) is tightly associated with the flagellar axoneme and is likely to have been present in the last eukaryotic common ancestor. The CMF22 amino acid sequence contains predicted IQ and ATPase associated with a variety of cellular activities (AAA) motifs that are conserved among CMF22 orthologues in diverse organisms, hinting at the importance of these domains in CMF22 function. Knockdown by RNA interference (RNAi) and rescue with an RNAi-immune mRNA demonstrated that CMF22 is required for propulsive cell motility in Trypanosoma brucei. Loss of propulsive motility in CMF22-knockdown cells was due to altered flagellar beating patterns, rather than flagellar paralysis, indicating that CMF22 is essential for motility regulation and likely functions as a fundamental regulatory component of motile axonemes. CMF22 association with the axoneme is weakened in mutants that disrupt the nexin-dynein regulatory complex, suggesting potential interaction with this complex. Our results provide insight into the core machinery required for motility of eukaryotic flagella.
机译:真核鞭毛(或纤毛)是一种广泛保存的细胞器,可为许多致病性原生动物提供动力,对人类的正常发育和生理至关重要。因此,定义运动型轴突的核心成分可增强对真核生物的了解,并提供对人类遗传性和传染性疾病机制的深入了解。在这项研究中,我们表明运动鞭毛22(CMF22)的组成部分与鞭毛轴突紧密相关,并且很可能存在于最后的真核生物共同祖先中。 CMF22氨基酸序列包含与各种生物体中CMF22直向同源物之间保守的多种细胞活性(AAA)主题相关的预测的IQ和ATPase,这暗示了这些域在CMF22功能中的重要性。通过RNA干扰(RNAi)进行基因敲除并使用RNAi免疫mRNA进行抢救证明,布鲁氏锥虫的推进细胞运动需要CMF22。 CMF22基因敲低细胞中推进运动力的丧失是由于鞭毛跳动模式的改变,而不是鞭毛麻痹,这表明CMF22对于运动调节至关重要,并且可能作为运动型轴突的基本调节成分。在破坏nexin-dynein调节复合物的突变体中,CMF22与轴突的结合被削弱,表明与该复合物的潜在相互作用。我们的结果提供了真核鞭毛运动所需的核心机制的见解。

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