| Literature DB >> 34429357 |
Anna Katharina Schlusche1,2, Sabine Ulrike Vay3, Niklas Kleinenkuhnen3, Steffi Sandke4, Rafael Campos-Martín3, Marta Florio5, Wieland Huttner5, Achim Tresch3,6, Jochen Roeper7, Maria Adele Rueger3,8, Igor Jakovcevski1,2,8, Malte Stockebrand1,2, Dirk Isbrandt9,2,8.
Abstract
The development of the cerebral cortex relies on the controlled division of neural stem and progenitor cells. The requirement for precise spatiotemporal control of proliferation and cell fate places a high demand on the cell division machinery, and defective cell division can cause microcephaly and other brain malformations. Cell-extrinsic and -intrinsic factors govern the capacity of cortical progenitors to produce large numbers of neurons and glia within a short developmental time window. In particular, ion channels shape the intrinsic biophysical properties of precursor cells and neurons and control their membrane potential throughout the cell cycle. We found that hyperpolarization-activated cyclic nucleotide-gated cation (HCN) channel subunits are expressed in mouse, rat, and human neural progenitors. Loss of HCN channel function in rat neural stem cells impaired their proliferation by affecting the cell-cycle progression, causing G1 accumulation and dysregulation of genes associated with human microcephaly. Transgene-mediated, dominant-negative loss of HCN channel function in the embryonic mouse telencephalon resulted in pronounced microcephaly. Together, our findings suggest a role for HCN channel subunits as a part of a general mechanism influencing cortical development in mammals.Entities:
Keywords: HCN channelopathy; brain development; cell cycle; microcephaly
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Year: 2021 PMID: 34429357 PMCID: PMC8536352 DOI: 10.1073/pnas.2009393118
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205