Grants and Contracts Details
Description
Aging is characterized by an altered immune function and stress response. It becomes increasingly clear
that, at least in part, this is due to alterations in ability of the cells to respond to different stress inducers.
The hypothesis to be tested in this proposal is that aging-induced up-regulation of neutral
sphingomyelianse-2 (NSMase-2) activity underlies the exaggerated response of hepatocytes IL-1 beta
during aging. We further hypothesized that aging-associated increases in NSMase-2 activity are
consequence of the decreases in the cellular glutathione level. Therefore, the long-term objective of our
study is to understand the relation between aging, the altered cellular response to inflammation, and the
state of oxidative stress. The following specific aim are proposed: Specific aim 1. To test the role of
NSMase-2 as a mediator of aging-induced hyperresponsiveness to IL-1b. Studies in this specific aim will
decipher the contribution of NSMase-2 to the IL-1 b hyperresponsiveness of aged animals. Gene silencing
approach will be used in vitro. in hepatocytes isolated from old rats, and in vivo, in aged animals. Specific
aim 2. To study the IL-1 b hyperresponsiveness in calorie-restricted aged rats. Calorie-restriction (CR) is
known to increase the life span of experimental animals and to attenuate the onset of oxidative stress,
including preventing aging-induced GSH/GSSH decline. Thus we hypothesized that CR attenuates IL-1 B
hyperresponsiveness of liver. This will be tested in vivo and in vitro. If NSMase-2 mediates IL-1 b
hyperresponsiveness by acting down-stream of GSH/GSSH changes, then NSMase-2 overexpression in
aged CR should restore the aging-associated IL-1 b hyperresponsiveness. This will be tested by
adenoviral -mediated expression of NSMase-2 in isolated hepatocytes and intact liver from aged CR rats.
Specific aim 3: To study the role of GSH in aging-associated NSMase-2 activation and IL-1 b
hyperresponsiveness. These studies will whether GSH depletion in aging and NSMase-2 activation are
causatively linked and will establish a link between the onset of oxidative stress and the IL-1b
hyperesponsivness in aged animals. The proposed studies will provide novel understanding on the cellular
mechanisms involved in the onset of aging and may have practical application in the development of new
anti-inflammatory drugs for the elderly.
Status | Finished |
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Effective start/end date | 2/15/07 → 1/31/13 |
Funding
- National Institute on Aging: $1,446,681.00
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