iScience (Feb 2024)

Sirt6 regulates the proliferation of neural precursor cells and cortical neurogenesis in mice

  • Yufei Wei,
  • Xinhuan Wang,
  • Zhihua Ma,
  • Pan Xiang,
  • Gaoao Liu,
  • Bin Yin,
  • Lin Hou,
  • Pengcheng Shu,
  • Wei Liu,
  • Xiaozhong Peng

Journal volume & issue
Vol. 27, no. 2
p. 108706

Abstract

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Summary: Sirt6, a member of the class III histone deacetylases (HDACs), functions in the regulation of genomic stability, DNA repair, cancer, metabolism and aging. Sirt6 deficiency is lethal, and newborn SIRT6-null cynomolgus monkeys show unfinished brain development. After the generation of a cortex-specific Sirt6 conditional knockout mouse model, we investigated the specific deletion of Sirt6 in NPCs at E10.5. This study found that Sirt6 deficiency causes excessive proliferation of neural precursor cells (NPCs) and retards differentiation. The results suggest that endogenous Sirt6 in NPCs regulates histone acetylation and limits stemness-related genes, including Notch1, in order to participate in NPC fate determination. These findings help elucidate Sirt6’s role in brain development and in NPC fate determination while providing data on species generality and differentiation.

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