COSA-1 mediated pro-crossover complex formation promotes meiotic crossing over in C. elegans

Author:

Yang Yuejun1,Wang Nan1,Liu Guoteng1,Nan Wencong1,Wang Bin2,Gartner Anton3ORCID,Zhang Hongtao1,Hong Ye1ORCID

Affiliation:

1. Shandong Provincial Key Laboratory of Animal Cell and Developmental Biology, School of Life Sciences, Shandong University , Qingdao , Shandong  266237 , China

2. National Key Laboratory of Non-food Biomass and Enzyme Technology, Guangxi Academy of Sciences , Nanning , China

3. Institute for Basic Sciences Center for Genomic Integrity, Graduate School for Health Sciences and Technology and Department for Biological Sciences, Ulsan National Institute of Science and Technology , Ulsan , Republic of Korea

Abstract

Abstract Accurate chromosome segregation during meiosis requires the establishment of at least one crossover (CO) between each pair of homologous chromosomes. CO formation depends on a group of conserved pro-CO proteins, which colocalize at CO-designated sites during late meiotic prophase I. However, it remains unclear whether these pro-CO proteins form a functional complex and how they promote meiotic CO formation in vivo. Here, we show that COSA-1, a key component required for CO formation, interacts with other pro-CO factors, MSH-5 and ZHP-3, via its N-terminal disordered region. Point mutations that impair these interactions do not affect CO designation, but they strongly hinder the accumulation of COSA-1 at CO-designated sites and result in defective CO formation. These defects can be partially bypassed by artificially tethering an interaction-compromised COSA-1 derivate to ZHP-3. Furthermore, we revealed that the accumulation of COSA-1 into distinct foci is required to assemble functional ‘recombination nodules’. These prevent early CO-designated recombination intermediates from being dismantled by the RTEL-1 helicase and protect late recombination intermediates, such as Holliday junctions, until they are resolved by CO-specific resolvases. Altogether, our findings provide insight into COSA-1 mediated pro-CO complex assembly and its contribution to CO formation.

Funder

National Natural Science Foundation of China

Natural Science Foundation of Shandong Province

Natural Science Foundation of the Jiangsu Province

Programs of Shandong University Qilu Young Scholars

Double-First Class Initiative of Shandong University School of Life Sciences

Future Plan for Young Scholars of Shandong University

Natural Science Foundation

Korea Basic Science Institute

Publisher

Oxford University Press (OUP)

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