CD38 Dictates Age-Related NAD Decline and Mitochondrial Dysfunction through an SIRT3-Dependent Mechanism

Camacho-Pereira Juliana; Tarrago Mariana G.; Chini Claudia C. S.; Nin Veronica; Escande Carlos; Warner Gina M.; Puranik Amrutesh S.; Schoon Renee A.; Reid Joel M.; Galina Antonio; Chini Eduardo N.

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CD38 Dictates Age-Related NAD Decline and Mitochondrial Dysfunction through an SIRT3-Dependent Mechanism

机译：CD38通过SIRT3依赖性机制决定年龄相关的NAD下降和线粒体功能障碍。

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Nicotinamide adenine dinucleotide (NAD) levels decrease during aging and are involved in age-related metabolic decline. To date, the mechanism responsible for the age-related reduction in NAD has not been elucidated. Here we demonstrate that expression and activity of the NADase CD38 increase with aging and that CD38 is required for the age-related NAD decline and mitochondrial dysfunction via a pathway mediated at least in part by regulation of SIRT3 activity. We also identified CD38 as the main enzyme involved in the degradation of the NAD precursor nicotinamide mononucleotide (NMN) in vivo, indicating that CD38 has a key role in the modulation of NAD-replacement therapy for aging and metabolic diseases.

机译：烟酰胺腺嘌呤二核苷酸（NAD）水平在衰老过程中下降，并与年龄相关的代谢下降有关。迄今为止，尚未阐明导致年龄相关的NAD降低的机制。在这里，我们证明了NADase CD38的表达和活性随着衰老而增加，并且CD38是与年龄相关的NAD下降和线粒体功能障碍所必需的，其途径至少部分是由SIRT3活性的调节介导的。我们还确定CD38为体内降解NAD前体烟酰胺单核苷酸（NMN）的主要酶，表明CD38在调节NAD替代疗法对衰老和代谢性疾病中具有关键作用。

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《Cell metabolism》 |2016年第6期|共13页
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Camacho-Pereira Juliana; Tarrago Mariana G.; Chini Claudia C. S.; Nin Veronica; Escande Carlos; Warner Gina M.; Puranik Amrutesh S.; Schoon Renee A.; Reid Joel M.; Galina Antonio; Chini Eduardo N.;
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正文语种 eng
中图分类内分泌腺疾病及代谢病;
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1. CD38 Dictates Age-Related NAD Decline and Mitochondrial Dysfunction through an SIRT3-Dependent Mechanism [J] . Camacho-Pereira Juliana, Tarrago Mariana G., Chini Claudia C. S., Cell metabolism . 2016,第6期

机译：CD38通过SIRT3依赖性机制决定年龄相关的NAD下降和线粒体功能障碍。
2. The NADase CD38 is induced by factors secreted from senescent cells providing a potential link between senescence and age-related cellular NAD~+ decline [J] . Claudia Chini, Kelly A. Hogan, Gina M. Warner, Biochemical and Biophysical Research Communications . 2019,第2期

机译：NADASED38由来自衰老细胞分泌的因素诱导，提供衰老和年龄相关细胞NAD〜+下降之间的潜在联系
3. Age-related declines in α-Klotho drive progenitor cell mitochondrial dysfunction and impaired muscle regeneration [J] . A. Sahu, H. Mamiya, S. N. Shinde, Nature Communications . 2018,第1期

机译：与年龄相关的α-克洛索氏菌驱动祖细胞线粒体功能障碍和肌肉再生受损
4. MITOCHONDRIAL VARIATION AND THE RISK OF AGE-RELATED MACULAR DEGENERATION ACROSS DIVERSE POPULATIONS [C] . NICOLE A.RESTREPO, SABRINA L.MITCHELL, ROBERT J.GOODLOE, Pacific Symposium on Biocomputing . 2015

机译：线粒体变异和各种人群的年龄相关黄斑变性风险
5. Mitochondrial pore dysfunction, a novel mechanism for age-related disease. [D] . Mott, Justin L. 2003

机译：线粒体毛孔功能障碍，一种与年龄有关的疾病的新机制。
6. CD38 dictates age-related NAD decline and mitochondrial dysfunction through a SIRT3-dependent mechanism [O] . Juliana Camacho-Pereira, Mariana G. Tarragó, Claudia C.S. Chini, -1

机译：CD38通过依赖SIRT3的机制指示与年龄相关的NAD下降和线粒体功能障碍
7. CD38 Dictates Age-Related NAD Decline and Mitochondrial Dysfunction through an SIRT3-Dependent Mechanism [O] . Juliana Camacho-Pereira, Mariana G. Tarragó, Claudia C.S. Chini, 2016

机译：CD38通过SIRT3依赖机构决定年龄相关的NAD下降和线粒体功能障碍

CD38 Dictates Age-Related NAD Decline and Mitochondrial Dysfunction through an SIRT3-Dependent Mechanism

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