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Telomerase gene therapy in adult and old mice delays aging and increases longevity without increasing cancer

机译:成年和成年小鼠端粒酶基因治疗可延缓衰老并延长寿命,而不会增加癌症

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AbstractA major goal in aging research is to improve health during aging. In the case of mice, genetic manipulations that shorten or lengthen telomeres result, respectively, in decreased or increased longevity. Based on this, we have tested the effects of a telomerase gene therapy in adult (1 year of age) and old (2 years of age) mice. Treatment of 1- and 2-year old mice with an adeno associated virus (AAV) of wide tropism expressing mouse TERT had remarkable beneficial effects on health and fitness, including insulin sensitivity, osteoporosis, neuromuscular coordination and several molecular biomarkers of aging. Importantly, telomerase-treated mice did not develop more cancer than their control littermates, suggesting that the known tumorigenic activity of telomerase is severely decreased when expressed in adult or old organisms using AAV vectors. Finally, telomerase-treated mice, both at 1-year and at 2-year of age, had an increase in median lifespan of 24 and 13%, respectively. These beneficial effects were not observed with a catalytically inactive TERT, demonstrating that they require telomerase activity. Together, these results constitute a proof-of-principle of a role of TERT in delaying physiological aging and extending longevity in normal mice through a telomerase-based treatment, and demonstrate the feasibility of anti-aging gene therapy.See accompanying article http://dx.doi.org/10.1002/emmm.201200246
机译:摘要衰老研究的主要目标是改善衰老过程中的健康状况。对于小鼠,缩短或延长端粒的基因操作分别导致寿命降低或增加。基于此,我们测试了端粒酶基因治疗对成年(1岁)和年老(2岁)小鼠的影响。用表达小鼠TERT的广泛向性性腺相关病毒(AAV)治疗1岁和2岁小鼠对健康和健身具有显着的有益作用,包括胰岛素敏感性,骨质疏松症,神经肌肉协调作用和一些衰老的分子生物标志物。重要的是,端粒酶治疗的小鼠没有比其同窝同窝小鼠发展出更多的癌症,这表明当使用AAV载体在成年或旧生物中表达时,端粒酶的已知致癌活性会大大降低。最后,端粒酶治疗的小鼠在1岁和2岁时的平均寿命分别增加了24%和13%。在催化失活的TERT中未观察到这些有益效果,表明它们需要端粒酶活性。总之,这些结果构成了TERT通过基于端粒酶的治疗延缓正常小鼠的生理衰老和延长其寿命的作用的原理证明,并证明了抗衰老基因疗法的可行性。 /dx.doi.org/10.1002/emmm.201200246

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