Department of Molecular and Cell Biology, University of California, Berkeley, Berkeley, United States.
California Institute for Quantitative Biosciences, Berkeley, United States.
Elife. 2023 Jan 26;12:e84492. doi: 10.7554/eLife.84492.
Meiotic chromosome segregation relies on synapsis and crossover (CO) recombination between homologous chromosomes. These processes require multiple steps that are coordinated by the meiotic cell cycle and monitored by surveillance mechanisms. In diverse species, failures in chromosome synapsis can trigger a cell cycle delay and/or lead to apoptosis. How this key step in 'homolog engagement' is sensed and transduced by meiotic cells is unknown. Here we report that in , recruitment of the Polo-like kinase PLK-2 to the synaptonemal complex triggers phosphorylation and inactivation of CHK-2, an early meiotic kinase required for pairing, synapsis, and double-strand break (DSB) induction. Inactivation of CHK-2 terminates DSB formation and enables CO designation and cell cycle progression. These findings illuminate how meiotic cells ensure CO formation and accurate chromosome segregation.
减数分裂染色体分离依赖于同源染色体之间的联会和交叉(CO)重组。这些过程需要多个步骤,由减数分裂细胞周期协调,并由监测机制监控。在不同的物种中,染色体联会的失败会引发细胞周期延迟和/或导致细胞凋亡。减数分裂细胞如何感知和转导这个“同源物结合”的关键步骤尚不清楚。在这里,我们报告说,在 中,Polo 样激酶 PLK-2 被招募到联会复合体上,触发了早期减数分裂激酶 CHK-2 的磷酸化和失活,该激酶对于配对、联会和双链断裂(DSB)诱导是必需的。CHK-2 的失活终止了 DSB 的形成,并使 CO 的指定和细胞周期的进展成为可能。这些发现阐明了减数分裂细胞如何确保 CO 的形成和染色体的正确分离。
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