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Steven S.S. Poon

Quality and Reliability (Greece)

Publishes on Telomeres, Telomerase, and Senescence, Electrostatic Discharge in Electronics, Chromosomal and Genetic Variations. 90 papers and 4.2k citations.

90Publications
4.2kTotal Citations
Telomeres, Telomerase, and SenescenceElectrostatic Discharge in ElectronicsChromosomal and Genetic VariationsCell Image Analysis TechniquesImage Processing Techniques and Applications

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Top publicationsby citations

Telomeres in the mouse have large inter-chromosomal variations in the number of T <sub>2</sub> AG <sub>3</sub>  repeats
J. M. J. M. Zijlmans, Uwe M. Martens, Steven S.S. Poon et al.|Proceedings of the National Academy of Sciences|1997
Cited by 495Open Access

The ultra-long telomeres that have been observed in mice are not in accordance with the concept that critical telomere shortening is related to aging and immortalization. Here, we have used quantitative fluorescence in situ hybridization to estimate (T2AG3)n lengths of individual telomeres in various mouse strains. Telomere lengths were very heterogeneous, but specific chromosomes of bone marrow cells and skin fibroblasts from individual mice had similar telomere lengths. We estimate that the shortest telomeres are around 10 kb in length, indicating that each mouse cell has a few telomeres with (T2AG3)n lengths within the range of human telomeres. These short telomeres may be critical in limiting the replicative potential of murine cells.

Collapse of Telomere Homeostasis in Hematopoietic Cells Caused by Heterozygous Mutations in Telomerase Genes
Geraldine Aubert, Gabriela M. Baerlocher, Irma Vulto et al.|PLoS Genetics|2012
Cited by 257Open Access

Telomerase activity is readily detectable in extracts from human hematopoietic stem and progenitor cells, but appears unable to maintain telomere length with proliferation in vitro and with age in vivo. We performed a detailed study of the telomere length by flow FISH analysis in leukocytes from 835 healthy individuals and 60 individuals with reduced telomerase activity. Healthy individuals showed a broad range in average telomere length in granulocytes and lymphocytes at any given age. The average telomere length declined with age at a rate that differed between age-specific breakpoints and between cell types. Gender differences between leukocyte telomere lengths were observed for all cell subsets studied; interestingly, this trend could already be detected at birth. Heterozygous carriers for mutations in either the telomerase reverse transcriptase (hTERT) or the telomerase RNA template (hTERC) gene displayed striking and comparable telomere length deficits. Further, non-carrier relatives of such heterozygous individuals had somewhat shorter leukocyte telomere lengths than expected; this difference was most profound for granulocytes. Failure to maintain telomere homeostasis as a result of partial telomerase deficiency is thought to trigger cell senescence or cell death, eventually causing tissue failure syndromes. Our data are consistent with these statements and suggest that the likelihood of similar processes occurring in normal individuals increases with age. Our work highlights the essential role of telomerase in the hematopoietic system and supports the notion that telomerase levels in hematopoietic cells, while limiting and unable to prevent overall telomere shortening, are nevertheless crucial to maintain telomere homeostasis with age.