Death receptor-associated pro-apoptotic signaling in aged skeletal muscle

Pistilli, Emidio E.; Jackson, Janna R.; Alway, Stephen E.

doi:10.1007/s10495-006-0194-6

Cited by 104 publications

(73 citation statements)

References 63 publications

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“…Thus IL-15 seems to function, at least in part, to inhibit apoptosis by blocking the signaling downstream of the TNFR. This is relevant in aging muscle because the extrinsic apoptotic pathway is very active in aged skeletal muscle (31). We speculate that the changes in IL-15 mRNA observed in the current study may represent an attempt to counter the pro-apoptotic environment typically observed in aged skeletal muscle.…”

Section: Discussionmentioning

confidence: 65%

Interleukin-15 responses to aging and unloading-induced skeletal muscle atrophy

Pistilli

Siu²,

Alway

2007

American Journal of Physiology-Cell Physiology

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Section: Discussionmentioning

confidence: 65%

Interleukin-15 responses to aging and unloading-induced skeletal muscle atrophy

Pistilli

Siu²,

Alway

2007

American Journal of Physiology-Cell Physiology

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“…FBN rats. Caspase-8 and caspase-3 activity were both greater in aged skeletal muscles and aged muscles also had greater protein content of Fas-associated death domain protein (FADD) and BH3-interacting death domain agonist (Bid) [14]. However, increasing IL-15 systemically in a similarly aged group of rodents did attenuate the incidence of apoptosis in skeletal muscle.…”

Section: Interleukin-15 As An Apoptosis Inhibitormentioning

confidence: 97%

Systemic elevation of interleukin-15 in vivo promotes apoptosis in skeletal muscles of young adult and aged rats

Pistilli

2008

Biochemical and Biophysical Research Communications

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In this study, we tested the hypothesis that systemic elevation of IL-15 would attenuate apoptosis in skeletal muscles of aged rats. IL-15 was administered to young adult (n=6) and aged (n=6) rats for 14 days. Apoptosis was quantified using an ELISA assay and verified through TUNEL staining of muscle sections. As expected, apoptosis was greater in muscles from aged control rats, compared to age-matched control. Apoptosis was also greater in the muscles from young adult and aged rats treated with IL-15. These increases in apoptosis were associated with decreases in muscle mass of IL-15 treated rats. These data do not support our initial hypothesis and suggest that systemic elevation of IL-15 promotes apoptosis in skeletal muscle. The proposed anti-apoptotic property of IL-15 may be specific to cell-type and/or the degree of muscle pathology present; however, additional research is required to more clearly decipher its role in skeletal muscle.

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“…In particular, the death receptor-mediated pathway, triggered by TNF-α, is thought to play a significant role in age-related muscle loss [14,17,19,20], owing to its ability to promote muscle protein wasting [63,64] and myonuclear apoptosis [14,17,19,20,65]. Interestingly, the transduction of TNF- α signaling during aging may be fiber-type specific[14].…”

Section: The Involvement Of Apoptosis In the Pathogenesis Of Sarcopeniamentioning

confidence: 99%

Multiple Pathways to the Same End: Mechanisms of Myonuclear Apoptosis in Sarcopenia of Aging

Marzetti

Privitera

Simili

et al. 2010

The Scientific World JOURNAL

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Sarcopenia, the age-related decline in muscle mass and function, represents a significant health issue due to the high prevalence of frailty and disability associated with this condition. Nevertheless, the cellular mechanisms responsible for the loss of muscle mass in old age are still largely unknown. An altered regulation of myocyte apoptosis has recently emerged as a possible contributor to the pathogenesis of sarcopenia. Studies in animal models have shown that the severity of skeletal muscle apoptosis increases over the course of aging and correlates with the degree of muscle mass and strength decline. Several apoptotic pathways are operative in aged muscles, with the mitochondria- and TNF-α-mediated pathways likely being the most relevant to sarcopenia. However, despite the growing number of studies on the subject, a definite mechanistic link between myocyte apoptosis and age-related muscle atrophy has not yet been established. Furthermore, the evidence on the role played by apoptosis in human sarcopenia is still sparse. Clearly, further research is required to better define the involvement of myocyte apoptosis in the pathogenesis of muscle loss at advanced age. This knowledge will likely help in the design of more effective therapeutic strategies to preserve muscle mass into old age, thus fostering independence of the elderly population and reducing the socioeconomic burden associated with sarcopenia.

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Death receptor-associated pro-apoptotic signaling in aged skeletal muscle

Cited by 104 publications

References 63 publications

Interleukin-15 responses to aging and unloading-induced skeletal muscle atrophy

Interleukin-15 responses to aging and unloading-induced skeletal muscle atrophy

Systemic elevation of interleukin-15 in vivo promotes apoptosis in skeletal muscles of young adult and aged rats

Multiple Pathways to the Same End: Mechanisms of Myonuclear Apoptosis in Sarcopenia of Aging

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