The aging mouse CNS is protected by an autophagy-dependent microglia population promoted by IL-34.
Rasmus BerglundYufei ChengEliane PiketMilena Z AdzemovicManuel ZeitelhoferTomas OlssonAndre Ortlieb Guerreiro-CacaisMaja JagodicPublished in: Nature communications (2024)
Microglia harness an unutilized health-promoting potential in age-related neurodegenerative and neuroinflammatory diseases, conditions like progressive multiple sclerosis (MS). Our research unveils an microglia population emerging in the cortical brain regions of aging mice, marked by ERK1/2, Akt, and AMPK phosphorylation patterns and a transcriptome indicative of activated autophagy - a process critical for cellular adaptability. By deleting the core autophagy gene Ulk1 in microglia, we reduce this population in the central nervous system of aged mice. Notably, this population is found dependent on IL-34, rather than CSF1, although both are ligands for CSF1R. When aging mice are exposed to autoimmune neuroinflammation, the loss of autophagy-dependent microglia leads to neural and glial cell death and increased mortality. Conversely, microglial expansion mediated by IL-34 exhibits a protective effect. These findings shed light on an autophagy-dependent neuroprotective microglia population as a potential target for treating age-related neuroinflammatory conditions, including progressive MS.
Keyphrases
- cell death
- multiple sclerosis
- neuropathic pain
- inflammatory response
- signaling pathway
- endoplasmic reticulum stress
- oxidative stress
- healthcare
- traumatic brain injury
- mass spectrometry
- spinal cord injury
- white matter
- high fat diet induced
- gene expression
- ms ms
- public health
- spinal cord
- adipose tissue
- cell cycle arrest
- type diabetes
- human health
- rna seq
- pi k akt
- copy number
- dna methylation
- transcription factor
- cognitive impairment
- functional connectivity
- genome wide analysis