Vitamin D as a Shield against Aging

Int J Mol Sci. 2023 Feb 25;24(5):4546. doi: 10.3390/ijms24054546.

Abstract

Aging can be seen as a physiological progression of biomolecular damage and the accumulation of defective cellular components, which trigger and amplify the process, toward whole-body function weakening. Senescence initiates at the cellular level and consists in an inability to maintain homeostasis, characterized by the overexpression/aberrant expression of inflammatory/immune/stress responses. Aging is associated with significant modifications in immune system cells, toward a decline in immunosurveillance, which, in turn, leads to chronic elevation of inflammation/oxidative stress, increasing the risk of (co)morbidities. Albeit aging is a natural and unavoidable process, it can be regulated by some factors, like lifestyle and diet. Nutrition, indeed, tackles the mechanisms underlying molecular/cellular aging. Many micronutrients, i.e., vitamins and elements, can impact cell function. This review focuses on the role exerted by vitamin D in geroprotection, based on its ability to shape cellular/intracellular processes and drive the immune response toward immune protection against infections and age-related diseases. To this aim, the main biomolecular paths underlying immunosenescence and inflammaging are identified as biotargets of vitamin D. Topics such as heart and skeletal muscle cell function/dysfunction, depending on vitamin D status, are addressed, with comments on hypovitaminosis D correction by food and supplementation. Albeit research has progressed, still limitations exist in translating knowledge into clinical practice, making it necessary to focus attention on the role of vitamin D in aging, especially considering the growing number of older individuals.

Keywords: cardiomyocytes; immunocytes; immunosenescence; inflammaging; molecular mechanisms; skeletal muscle cells; vitamin D.

Publication types

  • Review

MeSH terms

  • Aging / metabolism
  • Cellular Senescence
  • Humans
  • Immunosenescence*
  • Inflammation
  • Vitamin D* / metabolism
  • Vitamins

Substances

  • Vitamin D
  • Vitamins

Grants and funding

This research received no external funding.