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Volume 3 Issue 10, October 2023

SIRT2 safeguards primate cardiac aging

In this issue, Ye et al. investigated the molecular mechanisms that govern cardiac aging in primates. They identify SIRT2 as a pivotal protein that exhibits a geroprotective role in safeguarding the primate heart and demonstrate the therapeutic potential of SIRT2-based gene therapy to protect against age-related cardiac dysfunction. The cover image illustrates the cardioprotective role of SIRT2, depicting its expression as a reparative thread embroidered onto a knitted heart.

See Ye et al.

Image: Yizhu Wang. Cover Design: Lauren Heslop

Editorial

  • Research Highlights, News & Views and Research Briefings are three article formats used in this journal to highlight primary research. We explain the shared and unique features of these formats and describe how we are starting to use artificial intelligence to help produce one of them.

    Editorial

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Correspondence

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Comment & Opinion

  • Given the unique requirements of older adults, age-friendly product design is becoming increasingly important to promote independence and enhance quality of life. The Global Centre for Modern Ageing calls for a comprehensive, standardized and evidence-based assessment process to incorporate the perspectives of older adults into the design process.

    • Navaz Naghavi
    • Saeed Pahlevansharif
    World View
  • The intestinal epithelium serves as a barrier that facilitates interaction between intrinsic and environmental factors. Aging is accompanied by the gradual deterioration of this barrier. We postulate that barrier dysfunction results from defects in epithelial membrane trafficking that exacerbate age-related metabolic imbalances. Herein, we integrate barrier integrity, protein homeostasis, membrane trafficking and intracellular lipid sensing into an age-determining mechanism.

    • Lexus Tatge
    • Rene Solano Fonseca
    • Peter M. Douglas
    Comment
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Research Highlights

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News & Views

  • Human aging is associated with increased rates of many cardiac diseases and tissue remodeling. However, disentangling the mechanisms that underlie normal heart aging from disease processes is challenging. A study now addresses this gap by investigating healthy primate cardiac aging and provides evidence that SIRT2 signaling may regulate cardioprotective effects.

    • Laura Cox
    • Michael Olivier
    News & Views
  • A recent publication in Nature Aging suggests that DOPA decarboxylase may serve as an emerging biomarker that can identify neurodegenerative disorders that are characterized by dopaminergic cell loss. Here we discuss how this finding can assist clinicians and researchers in the differential diagnosis of individuals who present with parkinsonism or cognitive decline.

    • Marcel M. Verbeek
    • Bastiaan R. Bloem
    News & Views
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Research Briefings

  • Senescent cells accumulate with age and promote tissue decline. A broad genomic screen reveals that senescent cells can be eliminated from aged mice by interfering with their unique secretory program. Reducing the capacity of the endoplasmic reticulum by inhibiting the YAP–TEAD complex sensitizes senescent cells to apoptosis.

    Research Briefing
  • Microglia exhibit unexpected sex differences in gene expression and accessibility and compromised inflammatory responses during the aging process in mice. We established a mouse model with accelerated microglial turnover (3xDR), which results in aged microglia in non-aged brains. Analysis of this model revealed that aged microglia themselves contribute to cognitive decline.

    Research Briefing
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Reviews

  • Parkhitko et al. discuss combinatorial approaches targeting underlying mechanisms of aging across species and describe frameworks to analyze these interactions and their cross-species translational potential.

    • Andrey A. Parkhitko
    • Elizabeth Filine
    • Marc Tatar
    Review Article
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