Regulation of cellular senescence in human fibroblasts /

Benanti, Jennifer Ann.

January 2003

Thesis (Ph. D.)--University of Washington, 2003. / Vita. Includes bibliographical references (leaves 106-118).

Cell Aging. Fibroblasts Fibroblasts

Stereotype beliefs, contextual age, and knowledge of aging in the elderly

Walker, Angela.

January 2003

Thesis (M.A.)--Marshall University, 2003. / Title from document title page. Document formatted into pages; contains iv, 39 p. Includes bibliographical references (p. 25-27).

Older people. Aging

Scalar expansion and normal longevity in Hong Kong /

Cheung, Karen Siu Lan.

January 2003

Thesis (Ph. D.)--Hong Kong University of Science and Technology, 2003. / Includes bibliographical references (leaves 258-273). Also available in electronic version. Access restricted to campus users.

Older people Longevity Aging

Age related changes in preparation of encoding

Strunk, Jonathan

08 June 2015

A hallmark of aging is a decline in episodic memory. These memory impairments in older adults may be related to a shift away from proactive control strategies. Previous research, with young adults, suggests proactive processes can benefit memory encoding. The dual mechanisms of control model suggests changes in the recruitment of proactive and reactive control strategies will influence behavioral outcomes. The current study used EEG to investigated proactive control in episodic memory in aging. Both young and old adults completed a subsequent memory task with audio and visual items. Each item was preceded by a modality consistent cue. Participants also completed the AX-CPT, which is sensitive to the use of proactive strategies. We found both younger and older adults recruited proactive processes only for audio trials. Both groups exhibited proactive patterns of performance on the AX-CPT. Post-stimulus EEG suggests younger and older adults recruited different strategies for processing audio items. Visual items did not show subsequent memory effects in the pre-stimulus time period, but both groups showed post-stimulus effects. These results suggest younger and older adults are able to flexibly recruit proactive strategies that benefit memory performance.

Aging

EEG

Memory

Preparation

On generic protein aggregation and its aging and evolutionary implications

Tsechansky, Mark

02 July 2012

Many neuro-degenerative and metabolic diseases like Parkinson’s and Alzheimer’s are attributed to the effect of mis-folded and aggregated state of proteins in cells. This suggests that the phenomenon of in vivo protein aggregation may be relatively common, perhaps more than currently appreciated. In this study, we aimed to decipher the cause behind an intriguing and potentially related phenomenon observed in yeast cells - a widespread reorganization of hundreds of cytosolic proteins into punctate foci under starvation conditions. The key question that emerges is whether this phenomenon represents organization of proteins into functional assemblies or catastrophic aggregation. This thesis supports the aggregation hypothesis and provides evidence of its role in shaping the dynamics of cellular proteomes. We have been able to demonstrate that the proteins forming foci share a high propensity to aggregate and that these foci may represent sites of homogenous protein aggregation, structures which are typically associated with chaperones. A link between the formation of foci to the yeast aging process has also been established. With evidence correlating protein aggregation propensities to the cellular energy state, we have extended the current "living on the edge" hypothesis (which demonstrates an inverse correlation between protein expression levels and their aggregation propensities). For a specific case of the "purinosome", which is inferred to be a functional enzyme complex responsible for purine biosynthesis, we have shown that the observations may be explained alternatively as a generic protein aggregation phenomenon. This study highlights a systems approach to studying cellular proteins, which can corroborate or provide an alternative explanation to inferences drawn from traditional reductionistic analysis. / text

Protein aggregation

Purinosome

Aging

Effect of the atherogenic phospholipid, lysophosphatidylcholine (LPC),on endothelial senescence

Ko, Choi-lam., 高彩霖.

January 2010

published_or_final_version / Pharmacology / Master / Master of Medical Sciences

Endothelium - Aging.

Lysophospholipids.

Neural basis of prospective memory in normal and abnormal ageing

Gao, Junling, 高峻岭

January 2009

published_or_final_version / Medicine / Doctoral / Doctor of Philosophy

Prospective memory.

Neurophysiology.

Aging.

Post-translational modification of SIRT1 during endothelial senescence and vascular aging : molecular mechanisms and pathophysiological implications

Bai, Bo, 白波

January 2013

Endothelial senescence represents one of the major characteristics of vascular aging contributing to the development of cardiovascular diseases. SIRT1 is a NAD+-dependent enzyme catalyzing the deacetylation reaction of various signaling molecules and exerts beneficial effects against aging-associated pathologies. SIRT1 is a potent regulator antagonizing endothelial senescence. Both expression and activity of SIRT1 are down-regulated in senescent endothelial cells. However, the molecular mechanisms underlying the loss-of-SIRT1 function during the occurrence of endothelial senescence remain unknown. The present study reveals that phosphorylation at serine 47(S47) contributes to the loss-of-SIRT1 function during endothelial senescence. In both replicative and premature senescent endothelial cells, increased phosphorylation of SIRT1 at S47 was closely associated with the severity of cellular senescence. Replacing serine 47 residue with a phospho-mimicking aspartic acid residue impaired the anti-senescence activity of this protein. In addition, phosphorylation of SIRT1 at serine 47 inhibited its nuclear-cytoplasmic shuttling and protein-protein interactions with LKB1, a senescence-promoting kinase and telomeric repeat-binding factor 2–interacting protein 1, a telomere and inflammation regulator. As a result, the anti-inflammatory function of SIRT1 was also abolished by phosphorylation at serine 47. Cyclin dependent kinase 5 (CDK5) was identified as an upstream kinase responsible for phosphorylation of SIRT1 at serine 47. During the endothelial senescence, the activity of this kinase was up-regulated which was attributed to the augmented P25, a regulatory subunit of CDK5. Inhibition of this kinase by roscovitine, a CDK5 inhibitor, decreased the phosphorylation of SIRT1 at serine 47, reduced cellular senescence, promoted the cytoplasmic translocation of SIRT1 and attenuated the inflammation in endothelial cells triggered by tumor necrosis factor α. Moreover, the kinase activity of CDK5 was significantly elevated in aorta tissues of apolipoprotein E–deficient mice. Chronic administration of roscovitine alleviated endothelial senescence, vascular inflammation and the development of arterial atherosclerosis. These results collectively suggest that CDK 5 is responsible for the phosphorylation of SIRT1 at serine 47, which impairs the anti-senescence activity of enzyme and contributes to loss-of-SIRT1 function during vascular aging. By inhibiting this kinase, SIRT1 function can be improved, in turn preventing the development of endothelial senescence and slowing down the process of vascular aging. In addition to phosphorylation, I have also performed a preliminary study on the ubiquitination of SIRT1. The results demonstrated that SIRT1 ubiquitination was mediated by a Cullin-1-RING E3 ligase complex. Knocking down of cullin-1 enhanced SIRT1 protein expression, promoted proliferation and inhibited senescence in endothelial cells. This discovery may provide novel insights on the anti-vascular aging therapeutic development based on SIRT1 modification. / published_or_final_version / Pharmacology and Pharmacy / Doctoral / Doctor of Philosophy

Vascular endothelium - Aging

Sirtuins

Over-expression of human SIRT1 prevents ageing-induced endothelial dysfunction : eNOS dependent and independent mechanisms

Li, Jie, 李杰

January 2013

In blood vessel of mature animal, endothelial cells remain quiescent for years, before apoptosis and being replaced by newly generated endothelial cells. During aging, this turnover process is accelerated and the fast generated endothelial cells become dysfunctional. Endothelial dysfunction in blood vessel is characterized by the imbalanced production of endothelium-dependent relaxing factors (EDRF) and endothelium-dependent contracting factors (EDCF). The NAD-dependent deacetylase SIRT1 is an anti-aging protein with therapeutic potential for aging related cardiovascular diseases. Endothelium-specific over-expression of human SIRT1 promotes endothelium-dependent vasodilatation and endothelium-selective inhibition of human SIRT1 inhibit it. It is accepted that SIRT1 plays a protective role in endothelium dysfunction. However, the underlying mechanisms remain unclear. In the present study, the endothelial functions of a transgenic mouse model with endothelium-selective over-expression of human SIRT1 (hSIRT1) were evaluated and compared with those of wild type mice. Aging-induced deterioration in endothelium-dependent vasodilatation was observed in wild type but not hSIRT1 mice. Endothelium-specific over-expression of SIRT1 prevented aging-induced reduction of NO bioavailability in aortae, without changing endothelial nitric oxide synthase (eNOS) expression levels. Enhanced phosphorylation of eNOS at serine 1177 was detected in hSIRT1 mice aorta. In the presence of Nω-Nitro-L-arginine methyl ester (L-NAME), the nitric oxide synthase (NOS) inhibitor, EDCF induced contraction to acetylcholine was significantly decreased in carotid arteries of hSIRT1 mice. Cyclooxygenase-2 (COX-2) expression was induced by aging in wild-type mice but not in hSIRT1 mice. Thus, both the augmented NO bioavailability and the reduced production of COX-2-derived EDCF in hSIRT1 mice enhanced their endothelial function. To further explore the eNOS-independent mechanism underlying the vasoprotective role of SIRT1, the eNOS deficient and hSIRT1 endothelium-specific over-expression (eNOS-hSIRT1) mice was generated. Decreased endothelium-dependent contraction to acetylcholine was observed in both the carotid artery and aorta of eNOS-hSIRT1 mice, when compared to the controlled eNOS deficient mice. Besides, ATP induced endothelium-dependent contraction, which was COX-dependent, was also decreased in aortae of eNOS-hSIRT1 mice. Thus, the improved endothelial function induced by the endothelium-selective overexpression of SIRT1 was partly attributed to the reduced COX function, independent of eNOS signaling pathway. In summary, endothelium-selective overexpression of human SIRT1 prevented aging-induced impairment of endothelial function via both eNOS dependent and independent mechanisms. / published_or_final_version / Pharmacology and Pharmacy / Master / Master of Philosophy

Vascular endothelium - Aging

Sirtuins

Aging and Metalsmithing

Rice, Erin M.

20 November 2015

<p> Recently I have chosen to work with the concept of aging. This concept is shown through the use of architectural structures and medical instruments in order to create reliquaries and vessels. These reliquaries are composed of hand blown glass, metal, and other materials including silicone and latex medical tubing, enamel, and resin. </p><p> These reliquaries are my exploration into the idea of what is deemed precious and important. Time is one of the most valuable resources we have and it is impossible to contain. Through the aging process we begin to have less and less time and occasionally have medical procedures done in order to lengthen our life span or improve our quality of life. </p><p> Some of these reliquaries contain objects, while others have been left empty in order to allow the viewer to ponder what the piece might contain. Many of the vessels have medical undertones that enable the viewer to relate to common life experiences, while others contain architectural and industrial elements in order to show the relation to the machine made structures that surround us.</p>

Fine arts|Aging