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dmd-3, adoublesex-related gene regulated bytra-1, governs sex-specific morphogenesis inC. elegans

生物 双性恋 形态发生 细胞生物学 性二态性 遗传学 Wnt信号通路 融合蛋白 性别分化 雌雄同体 基因 生态学 重组DNA RNA剪接 核糖核酸 内分泌学
作者
D. Adam Mason,Jeremy S. Rabinowitz,Douglas S. Portman
出处
期刊:Development [The Company of Biologists]
卷期号:135 (14): 2373-2382 被引量:82
标识
DOI:10.1242/dev.017046
摘要

Although sexual dimorphism is ubiquitous in animals, the means by which sex determination mechanisms trigger specific modifications to shared structures is not well understood. In C. elegans, tail tip morphology is highly dimorphic: whereas hermaphrodites have a whip-like, tapered tail tip, the male tail is blunt-ended and round. Here we show that the male-specific cell fusion and retraction that generate the adult tail are controlled by the previously undescribed doublesex-related DM gene dmd-3, with a secondary contribution from the paralogous gene mab-3. In dmd-3 mutants, cell fusion and retraction in the male tail tip are severely defective, while in mab-3; dmd-3 double mutants, these processes are completely absent. Conversely, expression of dmd-3 in the hermaphrodite tail tip is sufficient to trigger fusion and retraction. The master sexual regulator tra-1 normally represses dmd-3expression in the hermaphrodite tail tip, accounting for the sexual specificity of tail tip morphogenesis. Temporal cues control the timing of tail remodeling in males by regulating dmd-3 expression, and Wnt signaling promotes this process by maintaining and enhancing dmd-3expression in the tail tip. Downstream, dmd-3 and mab-3regulate effectors of morphogenesis including the cell fusion gene eff-1. Together, our results reveal a regulatory network for male tail morphogenesis in which dmd-3 and mab-3 together occupy the central node. These findings indicate that an important conserved function of DM genes is to link the general sex determination hierarchy to specific effectors of differentiation and morphogenesis.
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