Author
Listed:
- Tom Vulliamy
(Faculty of Medicine, Imperial College School of Science, Technology and Medicine, Hammersmith Hospital)
- Anna Marrone
(Faculty of Medicine, Imperial College School of Science, Technology and Medicine, Hammersmith Hospital)
- Frederick Goldman
(The University of Iowa Hospitals and Clinics)
- Andrew Dearlove
(MRC UK, HGMP Resource Centre)
- Monica Bessler
(Washington University School of Medicine)
- Philip J. Mason
(Faculty of Medicine, Imperial College School of Science, Technology and Medicine, Hammersmith Hospital)
- Inderjeet Dokal
(Faculty of Medicine, Imperial College School of Science, Technology and Medicine, Hammersmith Hospital)
Abstract
Dyskeratosis congenita is a progressive bone-marrow failure syndrome that is characterized by abnormal skin pigmentation, leukoplakia and nail dystrophy1,2. X-linked, autosomal recessive and autosomal dominant inheritance have been found in different pedigrees. The X-linked form of the disease is due to mutations in the gene DKC1 in band 2, sub-band 8 of the long arm of the X chromosome (ref. 3). The affected protein, dyskerin, is a nucleolar protein that is found associated with the H/ACA class of small nucleolar RNAs and is involved in pseudo-uridylation of specific residues of ribosomal RNA4. Dyskerin is also associated with telomerase RNA (hTR)5, which contains a H/ACA consensus sequence6,7. Here we map the gene responsible for dyskeratosis congenita in a large pedigree with autosomal dominant inheritance. Affected members of this family have an 821-base-pair deletion on chromosome 3q that removes the 3′ 74 bases of hTR. Mutations in hTR were found in two other families with autosomal dominant dyskeratosis congenita.
Suggested Citation
Tom Vulliamy & Anna Marrone & Frederick Goldman & Andrew Dearlove & Monica Bessler & Philip J. Mason & Inderjeet Dokal, 2001.
"The RNA component of telomerase is mutated in autosomal dominant dyskeratosis congenita,"
Nature, Nature, vol. 413(6854), pages 432-435, September.
Handle:
RePEc:nat:nature:v:413:y:2001:i:6854:d:10.1038_35096585
DOI: 10.1038/35096585
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