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Citations to this article

Lifespan of mice and primates correlates with immunoproteasome expression
Andrew M. Pickering, … , Marcus Lehr, Richard A. Miller
Andrew M. Pickering, … , Marcus Lehr, Richard A. Miller
Published April 13, 2015
Citation Information: J Clin Invest. 2015;125(5):2059-2068. https://doi.org/10.1172/JCI80514.
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Research Article Aging Article has an altmetric score of 16

Lifespan of mice and primates correlates with immunoproteasome expression

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Abstract

There is large variation in lifespan among different species, and there is evidence that modulation of proteasome function may contribute to longevity determination. Comparative biology provides a powerful tool for identifying genes and pathways that control the rate of aging. Here, we evaluated skin-derived fibroblasts and demonstrate that among primate species, longevity correlated with an elevation in proteasomal activity as well as immunoproteasome expression at both the mRNA and protein levels. Immunoproteasome enhancement occurred with a concurrent increase in other elements involved in MHC class I antigen presentation, including β-2 microglobulin, (TAP1), and TAP2. Fibroblasts from long-lived primates also appeared more responsive to IFN-γ than cells from short-lived primate species, and this increase in IFN-γ responsiveness correlated with elevated expression of the IFN-γ receptor protein IFNGR2. Elevation of immunoproteasome and proteasome activity was also observed in the livers of long-lived Snell dwarf mice and in mice exposed to drugs that have been shown to extend lifespan, including rapamycin, 17-α-estradiol, and nordihydroguaiaretic acid. This work suggests that augmented immunoproteasome function may contribute to lifespan differences in mice and among primate species.

Authors

Andrew M. Pickering, Marcus Lehr, Richard A. Miller

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Total citations by year

Year: 2025 2024 2023 2022 2021 2020 2019 2018 2017 2016 2015 Total
Citations: 1 1 3 1 3 2 4 4 6 7 4 36
Citation information
This citation data is accumulated from CrossRef, which receives citation information from participating publishers, including this journal. Not all publishers participate in CrossRef, so this information is not comprehensive. Additionally, data may not reflect the most current citations to this article, and the data may differ from citation information available from other sources (for example, Google Scholar, Web of Science, and Scopus).

Citations to this article in year 2016 (7)

Title and authors Publication Year
Molecular pathology endpoints useful for aging studies
LJ Niedernhofer, JL Kirkland, W Ladiges
Ageing Research Reviews 2016
Growth Hormone Receptor Deficiency Protects against Age-Related NLRP3 Inflammasome Activation and Immune Senescence
O Spadaro, EL Goldberg, CD Camell, YH Youm, JJ Kopchick, KY Nguyen, A Bartke, LY Sun, VD Dixit
Cell Reports 2016
The Immunoproteasome in oxidative stress, aging, and disease
HK Johnston-Carey, LC Pomatto, KJ Davies
Critical Reviews in Biochemistry and Molecular Biology 2016
Unraveling the message: insights into comparative genomics of the naked mole-rat
KN Lewis, I Soifer, E Melamud, M Roy, RS McIsaac, M Hibbs, R Buffenstein
Mammalian Genome 2016
Gene expression signatures of human cell and tissue longevity
I Seim, S Ma, VN Gladyshev
npj Aging and Mechanisms of Disease 2016
Cell culture-based profiling across mammals reveals DNA repair and metabolism as determinants of species longevity
S Ma, A Upneja, A Galecki, YM Tsai, CF Burant, S Raskind, Q Zhang, ZD Zhang, A Seluanov, V Gorbunova, CB Clish, RA Miller, VN Gladyshev
eLife 2016
Pharmaceutical inhibition of mTOR in the common marmoset: effect of rapamycin on regulators of proteostasis in a non-human primate
Lelegren M, Liu Y, Ross C, Tardif S, Salmon AB
Pathobiology of Aging & Age Related Diseases 2016

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