Publications by authors named "Jeffrey Y Ying"
All cancer cells must adopt a telomere maintenance mechanism to achieve replicative immortality. Most human cancer cells utilize the enzyme telomerase to maintain telomeres. Alternative splicing of TERT regulates the amount and function of telomerase, however many alternative splicing isoforms of TERT have unknown functions.
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- Telomere shortening in immune cells is linked to aging, affecting immune function (immunosenescence), and while exercise may help boost telomerase activity in some cells, its effects on the thymus remain unclear.
- A study using transgenic mice examined how aging and different exercise models influenced the alternative splicing of human telomerase reverse transcriptase (hTERT) in thymus tissue.
- Results showed that while aging decreases hTERT expression, exercise helped prevent an age-related shift in hTERT splicing ratios, indicating that aging negatively impacts telomerase expression but that exercise can mitigate some of these changes.
Part of the regulation of telomerase activity includes the alternative splicing (AS) of the catalytic subunit telomerase reverse transcriptase (TERT). Although a therapeutic window for telomerase/TERT inhibition exists between cancer cells and somatic cells, stem cells express TERT and rely on telomerase activity for physiological replacement of cells. Therefore, identifying differences in TERT regulation between stem cells and cancer cells is essential for developing telomerase inhibition-based cancer therapies that reduce damage to stem cells.
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