4.7 Article

Functional genomic analyses highlight a shift in Gpr17-regulated cellular processes in oligodendrocyte progenitor cells and underlying myelin dysregulation in the aged mouse cerebrum

AGING CELL (2021)

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Journal

AGING CELL
Volume 20, Issue 4, Pages -

Publisher

WILEY
DOI: 10.1111/acel.13335

Keywords

ageing; brain; drug discovery; GPR17; myelin; oligodendrocyte; oligodendrocyte precursor; remyelination

Categories

Cell Biology Geriatrics & Gerontology

Funding

  1. Anatomical Society
  2. BBSRC [BB/M029379/1]
  3. MRC [MR/P025811/1]
  4. Multiple Sclerosis Society of the UK [40]
  5. University of Portsmouth
  6. MSCA Seal of Excellence @ UNIPD
  7. NVIDIA Hardware Grant
  8. Italian Ministry of University and Research (MUR)
  9. PRIN - Progetti di Ricerca di Interesse Nazionale (MPA) [2017NSXP8 J]
  10. German Research Council [AZ/115/1-1]
  11. Swiss National Funds [P300PA_171224]
  12. FISM [2017/R/1]
  13. '5 per mile' public funding
  14. BBSRC [BB/M029379/1] Funding Source: UKRI
  15. MRC [MR/P025811/1] Funding Source: UKRI

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Brain ageing is characterized by a decline in neuronal function and cognitive deficits, with myelin disruption being identified as a significant factor contributing to the loss of brain plasticity and repair responses. Through a combined systems biology and neurobiological approach, it was found that oligodendroglial and myelin genes are highly altered in the aging mouse cerebrum, with the G-protein coupled receptor Gpr17 being central to the disruption of OPCs in aging. Systems biology strategies were used to identify therapeutic agents that rejuvenate OPCs and restore myelination in age-related neuropathological contexts.
Brain ageing is characterised by a decline in neuronal function and associated cognitive deficits. There is increasing evidence that myelin disruption is an important factor that contributes to the age-related loss of brain plasticity and repair responses. In the brain, myelin is produced by oligodendrocytes, which are generated throughout life by oligodendrocyte progenitor cells (OPCs). Currently, a leading hypothesis points to ageing as a major reason for the ultimate breakdown of remyelination in Multiple Sclerosis (MS). However, an incomplete understanding of the cellular and molecular processes underlying brain ageing hinders the development of regenerative strategies. Here, our combined systems biology and neurobiological approach demonstrate that oligodendroglial and myelin genes are amongst the most altered in the ageing mouse cerebrum. This was underscored by the identification of causal links between signalling pathways and their downstream transcriptional networks that define oligodendroglial disruption in ageing. The results highlighted that the G-protein coupled receptor Gpr17 is central to the disruption of OPCs in ageing and this was confirmed by genetic fate-mapping and cellular analyses. Finally, we used systems biology strategies to identify therapeutic agents that rejuvenate OPCs and restore myelination in age-related neuropathological contexts.

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