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首页> 外文期刊>Development >A Zn-finger/FH2-domain containing protein, FOZI-1, acts redundantly with CeMyoD to specify striated body wall muscle fates in the Caenorhabditis elegans postembryonic mesoderm.
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A Zn-finger/FH2-domain containing protein, FOZI-1, acts redundantly with CeMyoD to specify striated body wall muscle fates in the Caenorhabditis elegans postembryonic mesoderm.

机译:含有锌指/ FH2结构域的蛋白质FOZI-1与CeMyoD重复发挥作用,以指定秀丽隐杆线虫胚后中胚层的横纹体壁肌肉命运。

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Striated muscle development in vertebrates requires the redundant functions of multiple members of the MyoD family. Invertebrates such as Drosophila and Caenorhabditis elegans contain only one MyoD homolog in each organism. Earlier observations suggest that factors outside of the MyoD family might function redundantly with MyoD in striated muscle fate specification in these organisms. However, the identity of these factors has remained elusive. Here, we describe the identification and characterization of FOZI-1, a putative transcription factor that functions redundantly with CeMyoD (HLH-1) in striated body wall muscle (BWM) fate specification in the C. elegans postembryonic mesoderm. fozi-1 encodes a novel nuclear-localized protein with motifs characteristic of both transcription factors and actin-binding proteins. We show that FOZI-1 shares the same expression pattern as CeMyoD in the postembryonic mesodermal lineage, the M lineage, and that fozi-1-null mutants exhibit similar M lineage-null defects to those found in animals lacking CeMyoD in the M lineage (e.g. loss of a fraction of M lineage-derived BWMs). Interestingly, fozi-1-null mutants with a reduced level of CeMyoD lack most, if not all, M lineage-derived BWMs. Our results indicate that FOZI-1 and the Hox factor MAB-5 function redundantly with CeMyoD in the specification of the striated BWM fate in the C. elegans postembryonic mesoderm, implicating a remarkable level of complexity for the production of a simple striated musculature in C. elegans.
机译:脊椎动物的横纹肌发育需要MyoD家族多个成员的冗余功能。果蝇和秀丽隐杆线虫等无脊椎动物在每种生物中仅包含一个MyoD同源物。较早的观察结果表明,在这些生物的横纹肌命运规范中,MyoD家族以外的因素可能与MyoD冗余发挥作用。但是,这些因素的身份仍然难以捉摸。在这里,我们描述了FOZI-1的鉴定和特征,FOZI-1是在C. elegans胚胎后中胚层的横纹体壁肌肉(BWM)命运规范中与CeMyoD(HLH-1)冗余起作用的推定转录因子。 fozi-1编码具有定位转录因子和肌动蛋白结合蛋白特征的新型核定位蛋白。我们显示FOZI-1在胚后中胚层谱系,M谱系中与CeMyoD共享相同的表达模式,并且fozi-1-null突变体表现出与在M谱系中缺乏CeMyoD的动物中发现的相似的M谱系-空缺陷(例如,丢失了M个沿袭来源的BWM的一部分)。有趣的是,CeMyoD水平降低的fozi-1空突变体缺乏大多数(如果不是全部)M谱系来源的BWM。我们的结果表明,FOZI-1和Hox因子MAB-5在C. elegans胚胎后中胚层的横纹BWM命运规范中与CeMyoD重复发挥作用,对于在C中产生简单的横纹肌肉组织牵涉到显着的复杂性水平线虫。

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