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Competence for Chemical Reprogramming of Sexual Fate Correlates with an Intersexual Molecular Signature in Caenorhabditis elegans

机译:化学命运的性命重编程能力与秀丽隐杆线虫的两性分子特征相关。

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摘要

In multicellular organisms, genetic programs guide cells to adopt cell fates as tissues are formed during development, maintained in adults, and repaired after injury. Here we explore how a small molecule in the environment can switch a genetic program from one fate to another. Wild-type Caenorhabditis elegans XX adult hermaphrodites make oocytes continuously, but certain mutant XX adults make sperm instead in an otherwise hermaphrodite soma. Thus, ; XX adults make only sperm, but they can be switched from sperm to oocyte production by treatment with a small-molecule MEK inhibitor. To ask whether this chemical reprogramming is common, we tested six XX sperm-only mutants, but found only one other capable of cell fate switching, ; . Therefore, reprogramming competence relies on genotype, with only certain mutants capable of responding to the MEK inhibitor with a cell fate change. To gain insight into the molecular basis of competence for chemical reprogramming, we compared polyadenylated transcriptomes of competent and noncompetent XX sperm-only mutants in the absence of the MEK inhibitor and hence in the absence of cell fate reprogramming. Despite their cellular production of sperm, competent mutants were enriched for oogenic messenger RNAs relative to mutants lacking competence for chemical reprogramming. In addition, competent mutants expressed the oocyte-specific protein , whereas those lacking competence did not. Therefore, mutants competent for reprogramming possess an intersexual molecular profile at both RNA and protein levels. We suggest that this intersexual molecular signature is diagnostic of an intermediate network state that poises the germline tissue for changing its cellular fate in response to environmental cues.
机译:在多细胞生物中,遗传程序指导细胞采取细胞命运,因为组织在发育过程中形成,在成人中维持并在受伤后进行修复。在这里,我们探索环境中的小分子如何将遗传程序从一种命运转变为另一种命运。野生型秀丽隐杆线虫XX成年雌雄同体连续制造卵母细胞,但是某些XX突变体成年雌性则在其他雌雄同体的体中制造精子。因此, XX个成年人仅产生精子,但可以通过使用小分子MEK抑制剂治疗将其从精子转换为卵母细胞。为了询问这种化学重编程是否普遍,我们测试了六个XX个仅精子的突变体,但发现只有另一个能够进行细胞命运转换。 。因此,重编程能力取决于基因型,只有某些突变体能够通过细胞命运变化来响应MEK抑制剂。为了深入了解化学重编程能力的分子基础,我们比较了在没有MEK抑制剂的情况下,因此在没有细胞命运重编程的情况下,有能力和无能力的XX精子突变体的多腺苷酸转录组。尽管它们的细胞产生精子,但相对于缺乏化学重编程能力的突变体,能胜任的突变体在致卵信使RNA方面更丰富。此外,有能力的突变体表达了卵母细胞特异性蛋白,而缺乏能力的突变体则没有。因此,能够重编程的突变体在RNA和蛋白质水平上都具有两性分子特征。我们建议,这种性间分子特征是对中间网络状态的诊断,该状态为种系组织蓄势待发,以响应环境线索改变其细胞命运。

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