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斑马鱼Meis蛋白的功能是稳定Pbx蛋白并调节后脑模式形成。

Zebrafish Meis functions to stabilize Pbx proteins and regulate hindbrain patterning.

作者信息

Waskiewicz A J, Rikhof H A, Hernandez R E, Moens C B

机构信息

Howard Hughes Medical Institute, Division of Basic Sciences and Program in Developmental Biology, B2-152, Fred Hutchinson Cancer Research Center, 1100 Fairview Ave. N., Seattle, WA 98109, USA.

出版信息

Development. 2001 Nov;128(21):4139-51. doi: 10.1242/dev.128.21.4139.

DOI:10.1242/dev.128.21.4139
PMID:11684652
Abstract

Homeodomain-containing Hox proteins regulate segmental identity in Drosophila in concert with two partners known as Extradenticle (Exd) and Homothorax (Hth). These partners are themselves DNA-binding, homeodomain proteins, and probably function by revealing the intrinsic specificity of Hox proteins. Vertebrate orthologs of Exd and Hth, known as Pbx and Meis (named for a myeloid ecotropic leukemia virus integration site), respectively, are encoded by multigene families and are present in multimeric complexes together with vertebrate Hox proteins. Previous results have demonstrated that the zygotically encoded Pbx4/Lazarus (Lzr) protein is required for segmentation of the zebrafish hindbrain and proper expression and function of Hox genes. We demonstrate that Meis functions in the same pathway as Pbx in zebrafish hindbrain development, as expression of a dominant-negative mutant Meis results in phenotypes that are remarkably similar to that of lzr mutants. Surprisingly, expression of Meis protein partially rescues the lzr(-) phenotype. Lzr protein levels are increased in embryos overexpressing Meis and are reduced for lzr mutants that cannot bind to Meis. This implies a mechanism whereby Meis rescues lzr mutants by stabilizing maternally encoded Lzr. Our results define two functions of Meis during zebrafish hindbrain segmentation: that of a DNA-binding partner of Pbx proteins, and that of a post-transcriptional regulator of Pbx protein levels.

摘要

含同源结构域的Hox蛋白与另外两个名为Extradenticle(Exd)和Homothorax(Hth)的蛋白协同调节果蝇中的节段身份。这些蛋白本身就是具有DNA结合能力的同源结构域蛋白,可能通过揭示Hox蛋白的内在特异性来发挥作用。Exd和Hth在脊椎动物中的直系同源物分别称为Pbx和Meis(以髓系嗜亲性白血病病毒整合位点命名),由多基因家族编码,并与脊椎动物Hox蛋白一起存在于多聚体复合物中。先前的研究结果表明,合子编码的Pbx4/Lazarus(Lzr)蛋白是斑马鱼后脑分割以及Hox基因正确表达和功能所必需的。我们证明,在斑马鱼后脑发育中,Meis与Pbx在同一途径中发挥作用,因为显性负性突变体Meis的表达所导致的表型与lzr突变体的表型非常相似。令人惊讶的是,Meis蛋白的表达部分挽救了lzr(-)表型。在过表达Meis的胚胎中,Lzr蛋白水平升高,而对于无法与Meis结合的lzr突变体,Lzr蛋白水平降低。这意味着一种机制,即Meis通过稳定母源编码的Lzr来挽救lzr突变体。我们的结果确定了Meis在斑马鱼后脑分割过程中的两种功能:作为Pbx蛋白的DNA结合伴侣,以及作为Pbx蛋白水平的转录后调节因子。

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Development. 2001 Nov;128(21):4139-51. doi: 10.1242/dev.128.21.4139.
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