Literature DB >> 10678830

Inhibition of experimental liver cirrhosis in mice by telomerase gene delivery.

K L Rudolph1, S Chang, M Millard, N Schreiber-Agus, R A DePinho.   

Abstract

Accelerated telomere loss has been proposed to be a factor leading to end-stage organ failure in chronic diseases of high cellular turnover such as liver cirrhosis. To test this hypothesis directly, telomerase-deficient mice, null for the essential telomerase RNA (mTR) gene, were subjected to genetic, surgical, and chemical ablation of the liver. Telomere dysfunction was associated with defects in liver regeneration and accelerated the development of liver cirrhosis in response to chronic liver injury. Adenoviral delivery of mTR into the livers of mTR(-/-) mice with short dysfunctional telomeres restored telomerase activity and telomere function, alleviated cirrhotic pathology, and improved liver function. These studies indicate that telomere dysfunction contributes to chronic diseases of continual cellular loss-replacement and encourage the evaluation of "telomerase therapy" for such diseases.

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Year:  2000        PMID: 10678830     DOI: 10.1126/science.287.5456.1253

Source DB:  PubMed          Journal:  Science        ISSN: 0036-8075            Impact factor:   47.728


  115 in total

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Review 3.  How long should telomeres be?

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4.  Telomere shortening impairs organ regeneration by inhibiting cell cycle re-entry of a subpopulation of cells.

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5.  Mitogen stimulation cooperates with telomere shortening to activate DNA damage responses and senescence signaling.

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8.  Short telomeres result in chromosomal instability in hematopoietic cells and precede malignant evolution in human aplastic anemia.

Authors:  R T Calado; J N Cooper; H M Padilla-Nash; E M Sloand; C O Wu; P Scheinberg; T Ried; N S Young
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Review 9.  Cellular lifespan and regenerative medicine.

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Review 10.  Cellular mechanisms of tissue fibrosis. 1. Common and organ-specific mechanisms associated with tissue fibrosis.

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