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NK-2类同源框基因在果蝇和小鼠心脏发育中的不同作用。

Divergent roles for NK-2 class homeobox genes in cardiogenesis in flies and mice.

作者信息

Ranganayakulu G, Elliott D A, Harvey R P, Olson E N

机构信息

Department of Molecular Biology and Oncology, The University of Texas Southwestern Medical Center, Dallas, Tx 75235-9148, USA.

出版信息

Development. 1998 Aug;125(16):3037-48. doi: 10.1242/dev.125.16.3037.

DOI:10.1242/dev.125.16.3037
PMID:9671578
Abstract

Recent evidence suggests that cardiogenesis in organisms as diverse as insects and vertebrates is controlled by an ancient and evolutionarily conserved transcriptional pathway. In Drosophila, the NK-2 class homeobox gene tinman (tin) is expressed in cardiac and visceral mesodermal progenitors and is essential for their specification. In vertebrates, the tin homologue Nkx2-5/Csx and related genes are expressed in early cardiac and visceral mesodermal progenitors. To test for an early cardiogenic function for Nkx2-5 and to examine whether cardiogenic mechanisms are conserved, we introduced the mouse Nkx2-5 gene and various mutant and chimeric derivatives into the Drosophila germline, and tested for their ability to rescue the tin mutant phenotype. While tin itself strongly rescued both heart and visceral mesoderm, Nkx2-5 rescued only visceral mesoderm. Other vertebrate 'non-cardiac' NK-2 genes rescued neither. We mapped the cardiogenic domain of tin to a unique region at its N terminus and, when transferred to Nkx2-5, this region conferred a strong ability to rescue heart. Thus, the cardiac and visceral mesodermal functions of NK-2 homeogenes are separable in the Drosophila assay. The results suggest that, while tin and Nkx2-5 show close functional kinship, their mode of deployment in cardiogenesis has diverged possibly because of differences in their interactions with accessory factors. The distinct cardiogenic programs in vertebrates and flies may be built upon a common and perhaps more ancient program for specification of visceral muscle.

摘要

最近的证据表明,在昆虫和脊椎动物等多种生物中,心脏发生受一条古老且在进化上保守的转录途径控制。在果蝇中,NK-2类同源异型框基因tinman(tin)在心脏和内脏中胚层祖细胞中表达,对其特化至关重要。在脊椎动物中,tin的同源物Nkx2-5/Csx及相关基因在早期心脏和内脏中胚层祖细胞中表达。为了测试Nkx2-5的早期心脏发生功能,并研究心脏发生机制是否保守,我们将小鼠Nkx2-5基因以及各种突变体和嵌合衍生物导入果蝇种系,并测试它们挽救tin突变体表型的能力。虽然tin本身能强烈挽救心脏和内脏中胚层,但Nkx2-5仅能挽救内脏中胚层。其他脊椎动物的“非心脏”NK-2基因都无法挽救。我们将tin的心脏发生结构域定位到其N端的一个独特区域,当将该区域转移到Nkx2-5时,它赋予了很强的挽救心脏的能力。因此,在果蝇实验中,NK-2同源基因的心脏和内脏中胚层功能是可分离的。结果表明,虽然tin和Nkx2-5显示出密切的功能亲缘关系,但它们在心脏发生中的作用模式可能已经不同,这可能是由于它们与辅助因子相互作用的差异。脊椎动物和果蝇中不同的心脏发生程序可能建立在一个共同的、也许更古老的内脏肌肉特化程序之上。

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Development. 1998 Aug;125(16):3037-48. doi: 10.1242/dev.125.16.3037.
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