Essential role of limiting telomeres in the pathogenesis of Werner syndrome

Sandy Chang; Asha S. Multani; Noelia G. Cabrera; Maria L. Naylor; Purnima Laud; David Lombard; Sen Pathak; Leonard Guarente; Ronald A. DePinho

doi:10.1038/ng1389

Essential role of limiting telomeres in the pathogenesis of Werner syndrome

Sandy Chang, Asha S. Multani, Noelia G. Cabrera, Maria L. Naylor, Purnima Laud, David Lombard, Sen Pathak, Leonard Guarente, Ronald A. DePinho

Genetics

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398 Scopus citations

Abstract

Mutational inactivation of the gene WRN causes Werner syndrome, an autosomal recessive disease characterized by premature aging, elevated genomic instability and increased cancer incidence. The capacity of enforced telomerase expression to rescue premature senescence of cultured cells from individuals with Werner syndrome and the lack of a disease phenotype in Wrn-deficient mice with long telomeres implicate telomere attrition in the pathogenesis of Werner syndrome. Here, we show that the varied and complex cellular phenotypes of Werner syndrome are precipitated by exhaustion of telomere reserves in mice. In late-generation mice null with respect to both Wrn and Terc (encoding the telomerase RNA component), telomere dysfunction elicits a classical Werner-like premature aging syndrome typified by premature death, hair graying, alopecia, osteoporosis, type II diabetes and cataracts. This mouse model also showed accelerated replicative senescence and accumulation of DNA-damage foci in cultured cells, as well as increased chromosomal instability and cancer, particularly nonepithelial malignancies typical of Werner syndrome. These genetic data indicate that the delayed manifestation of the complex pleiotropic of Wrn deficiency relates to telomere shortening.

Original language	English (US)
Pages (from-to)	877-882
Number of pages	6
Journal	Nature Genetics
Volume	36
Issue number	8
DOIs	https://doi.org/10.1038/ng1389
State	Published - Aug 2004

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Genetics

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title = "Essential role of limiting telomeres in the pathogenesis of Werner syndrome",

abstract = "Mutational inactivation of the gene WRN causes Werner syndrome, an autosomal recessive disease characterized by premature aging, elevated genomic instability and increased cancer incidence. The capacity of enforced telomerase expression to rescue premature senescence of cultured cells from individuals with Werner syndrome and the lack of a disease phenotype in Wrn-deficient mice with long telomeres implicate telomere attrition in the pathogenesis of Werner syndrome. Here, we show that the varied and complex cellular phenotypes of Werner syndrome are precipitated by exhaustion of telomere reserves in mice. In late-generation mice null with respect to both Wrn and Terc (encoding the telomerase RNA component), telomere dysfunction elicits a classical Werner-like premature aging syndrome typified by premature death, hair graying, alopecia, osteoporosis, type II diabetes and cataracts. This mouse model also showed accelerated replicative senescence and accumulation of DNA-damage foci in cultured cells, as well as increased chromosomal instability and cancer, particularly nonepithelial malignancies typical of Werner syndrome. These genetic data indicate that the delayed manifestation of the complex pleiotropic of Wrn deficiency relates to telomere shortening.",

author = "Sandy Chang and Multani, {Asha S.} and Cabrera, {Noelia G.} and Naylor, {Maria L.} and Purnima Laud and David Lombard and Sen Pathak and Leonard Guarente and DePinho, {Ronald A.}",

note = "Funding Information: We thank P. Carpenter for the γH2AX and 53BP1 antibodies and K. K. Wong, R. Maser and members of the laboratory of S.C. for comments. S.C. is supported by a KO8 Mentored Award from the NIA and an Ellison New Scholar in Aging Award from the Ellison Medical Foundation. R.A.D. is an American Cancer Society Professor and a Steven and Michele Kirsch Investigator.",

year = "2004",

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AU - Chang, Sandy

AU - Multani, Asha S.

AU - Cabrera, Noelia G.

AU - Naylor, Maria L.

AU - Laud, Purnima

AU - Lombard, David

AU - Pathak, Sen

AU - Guarente, Leonard

AU - DePinho, Ronald A.

N1 - Funding Information: We thank P. Carpenter for the γH2AX and 53BP1 antibodies and K. K. Wong, R. Maser and members of the laboratory of S.C. for comments. S.C. is supported by a KO8 Mentored Award from the NIA and an Ellison New Scholar in Aging Award from the Ellison Medical Foundation. R.A.D. is an American Cancer Society Professor and a Steven and Michele Kirsch Investigator.

PY - 2004/8

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N2 - Mutational inactivation of the gene WRN causes Werner syndrome, an autosomal recessive disease characterized by premature aging, elevated genomic instability and increased cancer incidence. The capacity of enforced telomerase expression to rescue premature senescence of cultured cells from individuals with Werner syndrome and the lack of a disease phenotype in Wrn-deficient mice with long telomeres implicate telomere attrition in the pathogenesis of Werner syndrome. Here, we show that the varied and complex cellular phenotypes of Werner syndrome are precipitated by exhaustion of telomere reserves in mice. In late-generation mice null with respect to both Wrn and Terc (encoding the telomerase RNA component), telomere dysfunction elicits a classical Werner-like premature aging syndrome typified by premature death, hair graying, alopecia, osteoporosis, type II diabetes and cataracts. This mouse model also showed accelerated replicative senescence and accumulation of DNA-damage foci in cultured cells, as well as increased chromosomal instability and cancer, particularly nonepithelial malignancies typical of Werner syndrome. These genetic data indicate that the delayed manifestation of the complex pleiotropic of Wrn deficiency relates to telomere shortening.

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Essential role of limiting telomeres in the pathogenesis of Werner syndrome

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