Publications by authors named "Chelsea G Drown"
Article Synopsis
- Studying essential genes in live mice is difficult due to irreversible genetic changes and slow protein depletion.
- The first-generation auxin-inducible-degron (AID) system works well for cultured cells but is toxic to mice, limiting its use.
- The optimized second-generation AID system allows for conditional loss of key protein CEP192 in mice without toxicity, enabling rapid and sustained protein depletion for better understanding of protein function.
Hepatocyte polyploidization is a tightly controlled process that is initiated at weaning and increases with age. The proliferation of polyploid hepatocytes in vivo is restricted by the PIDDosome-P53 axis, but how this pathway is triggered remains unclear. Given that increased hepatocyte ploidy protects against malignant transformation, the evolutionary driver that sets the upper limit for hepatocyte ploidy remains unknown.
View Article and Find Full Text PDFMulticiliated cells (MCCs) are terminally differentiated epithelia that assemble multiple motile cilia used to promote fluid flow. To template these cilia, MCCs dramatically expand their centriole content during a process known as centriole amplification. In cycling cells, the master regulator of centriole assembly Polo-like kinase 4 (PLK4) is essential for centriole duplication; however recent work has questioned the role of PLK4 in centriole assembly in MCCs.
View Article and Find Full Text PDFCentrosomes are microtubule-organizing centers comprised of a pair of centrioles and the surrounding pericentriolar material. Abnormalities in centriole number are associated with cell division errors and can contribute to diseases such as cancer. Centriole duplication is limited to once per cell cycle and is controlled by the dosage-sensitive Polo-like kinase 4 (PLK4).
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