Cell Death and Disease (Feb 2021)

The N-terminal BRCT domain determines MCPH1 function in brain development and fertility

  • Xiaoqian Liu,
  • Nadine Schneble-Löhnert,
  • Martina Kristofova,
  • Xiaobing Qing,
  • Jan Labisch,
  • Susanne Hofmann,
  • Sandra Ehrenberg,
  • Mara Sannai,
  • Tjard Jörß,
  • Alessandro Ori,
  • Maren Godmann,
  • Zhao-Qi Wang

DOI
https://doi.org/10.1038/s41419-021-03406-3
Journal volume & issue
Vol. 12, no. 2
pp. 1 – 16

Abstract

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Abstract MCPH1 is a causal gene for the neurodevelopmental disorder, human primary microcephaly (MCPH1, OMIM251200). Most pathogenic mutations are located in the N-terminal region of the gene, which encodes a BRCT domain, suggesting an important function of this domain in brain size determination. To investigate the specific function of the N-terminal BRCT domain in vivo, we generated a mouse model lacking the N’-BRCT domain of MCPH1 (referred as Mcph1-ΔBR1). These mutant mice are viable, but exhibit reduced brain size, with a thinner cortex due to a reduction of neuroprogenitor populations and premature neurogenic differentiation. Mcph1-ΔBR1 mice (both male and female) are infertile; however, almost all female mutants develop ovary tumours. Mcph1-ΔBR1 MEF cells exhibit a defect in DNA damage response and DNA repair, and show the premature chromosome condensation (PCC) phenotype, a hallmark of MCPH1 patient cells and also Mcph1 knockout cells. In comparison with Mcph1 complete knockout mice, Mcph1-ΔBR1 mice faithfully reproduce all phenotypes, indicating an essential role of the N-terminal BRCT domain for the physiological function of MCPH1 in the control of brain size and gonad development as well as in multiple cellular processes.