The Cellular Senescence Stress Response in Post-Mitotic Brain Cells: Cell Survival at the Expense of Tissue Degeneration

Eric Sah; Sudarshan Krishnamurthy; Mohamed Y Ahmidouch; Gregory J Gillispie; Carol Milligan; Miranda E Orr

doi:10.3390/life11030229

The Cellular Senescence Stress Response in Post-Mitotic Brain Cells: Cell Survival at the Expense of Tissue Degeneration

Life (Basel). 2021 Mar 11;11(3):229. doi: 10.3390/life11030229.

Authors

Eric Sah¹, Sudarshan Krishnamurthy^{1

2}, Mohamed Y Ahmidouch^{1

3}, Gregory J Gillispie^{1

4}, Carol Milligan⁵, Miranda E Orr^{1

4

6}

Affiliations

¹ Department of Internal Medicine, Section on Gerontology and Geriatric Medicine, Wake Forest School of Medicine, Winston-Salem, NC 27157, USA.
² Bowman Gray Center for Medical Education, Wake Forest School of Medicine, Winston-Salem, NC 27101, USA.
³ Departments of Biology and Chemistry, Wake Forest University, Winston-Salem, NC 27109, USA.
⁴ Sticht Center for Healthy Aging and Alzheimer's Prevention, Wake Forest School of Medicine, Winston-Salem, NC 27157, USA.
⁵ Department of Neurobiology and Anatomy, Wake Forest School of Medicine, Winston-Salem, NC 27157, USA.
⁶ Salisbury VA Medical Center, Salisbury, NC 28144, USA.

Abstract

In 1960, Rita Levi-Montalcini and Barbara Booker made an observation that transformed neuroscience: as neurons mature, they become apoptosis resistant. The following year Leonard Hayflick and Paul Moorhead described a stable replicative arrest of cells in vitro, termed "senescence". For nearly 60 years, the cell biology fields of neuroscience and senescence ran in parallel, each separately defining phenotypes and uncovering molecular mediators to explain the 1960s observations of their founding mothers and fathers, respectively. During this time neuroscientists have consistently observed the remarkable ability of neurons to survive. Despite residing in environments of chronic inflammation and degeneration, as occurs in numerous neurodegenerative diseases, often times the neurons with highest levels of pathology resist death. Similarly, cellular senescence (hereon referred to simply as "senescence") now is recognized as a complex stress response that culminates with a change in cell fate. Instead of reacting to cellular/DNA damage by proliferation or apoptosis, senescent cells survive in a stable cell cycle arrest. Senescent cells simultaneously contribute to chronic tissue degeneration by secreting deleterious molecules that negatively impact surrounding cells. These fields have finally collided. Neuroscientists have begun applying concepts of senescence to the brain, including post-mitotic cells. This initially presented conceptual challenges to senescence cell biologists. Nonetheless, efforts to understand senescence in the context of brain aging and neurodegenerative disease and injury emerged and are advancing the field. The present review uses pre-defined criteria to evaluate evidence for post-mitotic brain cell senescence. A closer interaction between neuro and senescent cell biologists has potential to advance both disciplines and explain fundamental questions that have plagued their fields for decades.

Keywords: Alzheimer’s disease; amyotrophic lateral sclerosis; biology of aging; brain; cellular senescence; geroscience; neurodegeneration; neuronal senescence; post-mitotic; tauopathy.

Publication types

Review

Abstract

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