Title of article
Very Short Telomeres in the Peripheral Blood of Patients with X-Linked and Autosomal Dyskeratosis Congenita
Author/Authors
Tom J. Vulliamy، نويسنده , , Stuart W. Knight، نويسنده , , Philip J. Mason، نويسنده , , Inderjeet Dokal، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2001
Pages
5
From page
353
To page
357
Abstract
Dyskeratosis congenita (DC) is an inherited bone marrow failure syndrome in which patients undergo premature ageing and have a predisposition to malignancy. X-linked and autosomal (dominant and recessive) forms of the disease are recognized. The gene responsible for X-linked DC (DKC1) encodes a highly conserved protein called dyskerin that is believed to be essential in ribosome biogenesis and may also be involved in telomerase RNP assembly. Here we show that in X-linked DC, peripheral blood cells have dramatically reduced telomere lengths but normal levels of telomerase activity. We also find that subjects with autosomal DC have significantly shorter telomeres than age-matched normal controls suggesting that both forms of the disease are associated with rapid telomere shortening in hemopoietic stem cells. The further characterization of these genes will not only lead to a better understanding of the biology of DC but may also provide further insights into the maintenance of telomeres and the biology of aplastic anemia, ageing, and cancer.
Keywords
telomerase. , ageing , aplastic anemia , dyskerin , telomeres , dyskeratosis congenita , DKC1
Journal title
Blood Cells, Molecules and Diseases
Serial Year
2001
Journal title
Blood Cells, Molecules and Diseases
Record number
498400
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