eNOS Activity Is Reduced in Senescent Human Endothelial Cells

Matsushita, Hisashi; Chang, Edwin; Glassford, Alexander J.; Cooke, John P.; Chiu, Choy‐Pik; Tsao, Philip S.

doi:10.1161/hh2101.098443

Cited by 261 publications

(170 citation statements)

References 41 publications

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“…In human iliac arteries, endothelial cells at the bifurcation have shorter telomeres, consistent with a focal acceleration of senescence (3). Senescent human endothelial cells produce less nitric oxide (NO ⅐ ), generate more superoxide anion (O 2 ⅐-), and are more adhesive for monocytes, effects that can be reversed by transfection with the gene encoding telomerase (4).…”

Section: Program In Vascular Medicine and Biology Stanford Universitmentioning

confidence: 99%

Flow, NO, and atherogenesis

Cooke

2003

Proc. Natl. Acad. Sci. U.S.A.

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126

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Section: Program In Vascular Medicine and Biology Stanford Universitmentioning

confidence: 99%

Flow, NO, and atherogenesis

Cooke

2003

Proc. Natl. Acad. Sci. U.S.A.

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126

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“…This decline in NO availability is a consequence of an impaired eNOS activity as well as of a progressive NO inactivation through increasing levels of superoxide anions. 108,109 As a result, aged vessels exhibit compromised vasodilatory properties that cause increased vascular resistance and impaired perfusion. Moreover, reduced NO bioavailability prompts vascular inflammation and atherogenesis and impedes endothelial repair.…”

Section: Nitric Oxide Signaling In Aging Vessels Is Regulated By Sirt1mentioning

confidence: 99%

FOXOs and Sirtuins in Vascular Growth, Maintenance, and Aging

Oellerich

Potente

2012

Circulation Research

136

128

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“…127,128 Decreases in both NO production and eNOS activity in human umbilical vein endothelial cells and human aortic endothelial cells (HAECs) are associated with aging. 129,130 Matsushita et al 130 demonstrated that shear stress-induced increase in NO production was diminished in senescent HAECs and that stable expression of TERT restored the decreased eNOS expression and NO production associated with aging. Minamino et al 131 reported that HAECs from human atherosclerotic lesions presented phenotypes of senescent cells and decreases in eNOS expression and eNOS activity.…”

Section: Endothelial Cell Senescencementioning

confidence: 99%

Endothelial dysfunction and hypertension in aging

2012

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Hypertension is one of the common diseases in the elderly. The prevalence of hypertension markedly increases with advancing age. Both aging and hypertension have a critical role in cardiovascular and cerebrovascular complications. Although aging and hypertension, either independently or collectively, impair endothelial function, aging and hypertension may have similar cascades for the pathogenesis and development of endothelial dysfunction. Nitric oxide (NO) has an important role in regulation of vascular tone. Decrease in NO bioavailability by endothelial dysfunction would lead to elevation of blood pressure. An imbalance of reduced production of NO or increased production of reactive oxygen species, mainly superoxide, may promote endothelial dysfunction. One possible mechanism by which the prevalence of hypertension is increased in relation to aging may be advancing endothelial dysfunction associated with aging through an increase in oxidative stress. In addition, endothelial cell senescence is also involved in aging-related endothelial dysfunction. In this review, we focus on recent findings and interactions between endothelial function, oxidative stress and hypertension in aging.

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eNOS Activity Is Reduced in Senescent Human Endothelial Cells

Cited by 261 publications

References 41 publications

Flow, NO, and atherogenesis

Flow, NO, and atherogenesis

FOXOs and Sirtuins in Vascular Growth, Maintenance, and Aging

Endothelial dysfunction and hypertension in aging

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