Department of Chemical Biology, School of Life Sciences, Guangdong Provincial Key Laboratory of Cell Microenvironment and Disease Research, Shenzhen Key Laboratory of Cell Microenvironment, Southern University of Science and Technology, 518055 Shenzhen, China.
Proc Natl Acad Sci U S A. 2023 May 23;120(21):e2303698120. doi: 10.1073/pnas.2303698120. Epub 2023 May 15.
Hybrid incompatibility as a kind of reproductive isolation contributes to speciation. The nucleocytoplasmic incompatibility between eggs and sperm (×) leads to specific loss of paternal chromosomes 3L and 4L. The hybrids die before gastrulation, of which the lethal causes remain largely unclear. Here, we show that the activation of the tumor suppressor protein P53 at late blastula stage contributes to this early lethality. We find that in stage 9 embryos, P53-binding motif is the most enriched one in the up-regulated Assay for Transposase-Accessible Chromatin with high-throughput sequencing (ATAC-seq) peaks between × and wild-type controls, which correlates with an abrupt stabilization of P53 protein in × hybrids at stage 9. Inhibition of P53 activity via either knockout or overexpression of a dominant-negative P53 mutant or Murine double minute 2 proto-oncogene (Mdm2), a negative regulator of P53, by mRNA injection can rescue the × early lethality. Our results suggest a causal function of P53 on hybrid lethality prior to gastrulation.
杂种不育性作为一种生殖隔离有助于物种形成。卵子和精子之间的核质不相容性(×)导致特定的父本染色体 3L 和 4L 的丢失。杂种在原肠胚形成之前死亡,其致死原因在很大程度上尚不清楚。在这里,我们表明晚期囊胚期肿瘤抑制蛋白 P53 的激活有助于这种早期致死性。我们发现,在第 9 期胚胎中,P53 结合基序是上调的 Assay for Transposase-Accessible Chromatin with high-throughput sequencing (ATAC-seq) 峰中最丰富的一个,在 × 和野生型对照之间,这与 × 杂种中 P53 蛋白在第 9 期的突然稳定相关。通过 mRNA 注射敲除或过表达显性负 P53 突变体或 P53 负调节剂 Murine double minute 2 原癌基因(Mdm2),可以抑制 P53 活性,从而挽救 × 的早期致死性。我们的结果表明,P53 在原肠胚形成之前对杂种致死性有因果作用。
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