Loss of lamin-B1 and defective nuclear morphology are hallmarks of astrocyte senescence in vitro and in the aging human hippocampus.
Isadora MatiasLuan Pereira DinizIsabella Vivarini DamicoAna Paula Bergamo AraujoLaís da Silva NevesGabriele VargasRenata E P LeiteClaudia K SuemotoRicardo NitriniWilson Jacob-FilhoLea T GrinbergElly M HolJinte MiddeldorpFlávia Carvalho Alcantara GomesPublished in: Aging cell (2021)
The increase in senescent cells in tissues, including the brain, is a general feature of normal aging and age-related pathologies. Senescent cells exhibit a specific phenotype, which includes an altered nuclear morphology and transcriptomic changes. Astrocytes undergo senescence in vitro and in age-associated neurodegenerative diseases, but little is known about whether this process also occurs in physiological aging, as well as its functional implication. Here, we investigated astrocyte senescence in vitro, in old mouse brains, and in post-mortem human brain tissue of elderly. We identified a significant loss of lamin-B1, a major component of the nuclear lamina, as a hallmark of senescent astrocytes. We showed a severe reduction of lamin-B1 in the dentate gyrus of aged mice, including in hippocampal astrocytes, and in the granular cell layer of the hippocampus of post-mortem human tissue from non-demented elderly. The lamin-B1 reduction was associated with nuclear deformations, represented by an increased incidence of invaginated nuclei and loss of nuclear circularity in senescent astrocytes in vitro and in the aging human hippocampus. We also found differences in lamin-B1 levels and astrocyte nuclear morphology between the granular cell layer and polymorphic layer in the elderly human hippocampus, suggesting an intra-regional-dependent aging response of human astrocytes. Moreover, we described senescence-associated impaired neuritogenic and synaptogenic capacity of mouse astrocytes. Our findings show that reduction of lamin-B1 is a conserved feature of hippocampal cells aging, including astrocytes, and shed light on significant defects in nuclear lamina structure which may contribute to astrocyte dysfunctions during aging.
Keyphrases
- endothelial cells
- induced apoptosis
- induced pluripotent stem cells
- pluripotent stem cells
- dna damage
- cerebral ischemia
- single cell
- cell cycle arrest
- type diabetes
- gene expression
- signaling pathway
- stem cells
- oxidative stress
- metabolic syndrome
- middle aged
- functional connectivity
- resting state
- rna seq
- community dwelling
- mass spectrometry
- early onset
- subarachnoid hemorrhage
- insulin resistance
- pi k akt