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果蝇性别决定基因 Sex-lethal 可以绕过其性别决定基因靶标 transformer,从而调节雌性行为的某些方面。

Drosophila switch gene Sex-lethal can bypass its switch-gene target transformer to regulate aspects of female behavior.

机构信息

Division of Genetics, Genomics and Development, Department of Molecular and Cell Biology, University of California, Berkeley, CA 94720.

出版信息

Proc Natl Acad Sci U S A. 2013 Nov 19;110(47):E4474-81. doi: 10.1073/pnas.1319063110. Epub 2013 Nov 4.

Abstract

The switch gene Sex-lethal (Sxl) was thought to elicit all aspects of Drosophila female somatic differentiation other than size dimorphism by controlling only the switch gene transformer (tra). Here we show instead that Sxl controls an aspect of female sexual behavior by acting on a target other than or in addition to tra. We inferred the existence of this unknown Sxl target from the observation that a constitutively feminizing tra transgene that restores fertility to tra(-) females failed to restore fertility to Sxl-mutant females that were adult viable but functionally tra(-). The sterility of these mutant females was caused by an ovulation failure. Because tra expression is not sufficient to render these Sxl-mutant females fertile, we refer to this pathway as the tra-insufficient feminization (TIF) branch of the sex-determination regulatory pathway. Using a transgene that conditionally expresses two Sxl feminizing isoforms, we find that the TIF branch is required developmentally for neurons that also sex-specifically express fruitless, a tra gene target controlling sexual behavior. Thus, in a subset of fruitless neurons, targets of the TIF and tra pathways appear to collaborate to control ovulation. In most insects, Sxl has no sex-specific functions, and tra, rather than Sxl, is both the target of the primary sex signal and the gene that maintains the female developmental commitment via positive autoregulation. The TIF pathway may represent an ancestral female-specific function acquired by Sxl in an early evolutionary step toward its becoming the regulator of tra in Drosophila.

摘要

性致死(Sex-lethal,Sxl)开关基因被认为通过仅控制转换基因转化器(transformer,tra)来引发除大小二型外的所有果蝇雌性体分化方面。然而,我们发现 Sxl 通过作用于除 tra 之外或之外的靶基因来控制雌性性行为的一个方面。我们从以下观察结果推断出这个未知 Sxl 靶基因的存在:一个组成型雌性化的 tra 转基因,可恢复 tra(-)雌性的生育能力,但不能恢复成年存活但功能上 tra(-)的 Sxl 突变体雌性的生育能力。这些突变体雌性的不育是由于排卵失败引起的。由于 tra 表达不足以使这些 Sxl 突变体雌性具有生育能力,我们将该途径称为性别决定调控途径的 tra 不足雌性化(tra-insufficient feminization,TIF)分支。使用条件表达两种 Sxl 雌性化异构体的转基因,我们发现 TIF 分支在发育过程中是必需的,用于特异性表达 fruitless 的神经元,fruitless 是一个控制性行为的 tra 基因靶标。因此,在一小部分 fruitless 神经元中,TIF 和 tra 途径的靶基因似乎协同控制排卵。在大多数昆虫中,Sxl 没有性别特异性功能,tra 而不是 Sxl,既是主要性别信号的靶基因,也是通过正反馈调节来维持雌性发育承诺的基因。TIF 途径可能代表了 Sxl 在向成为 Drosophila tra 调节因子的早期进化步骤中获得的一个祖先雌性特异性功能。

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