Guarnieri G, Sarchielli E, Comeglio P, Herrera-Puerta E, Piaceri I, Nacmias B, Benelli M, Kelsey G, Maggi M, Gallina P, Vannelli GB, Morelli A
Epigenetics
TNF伪 is the main proinflammatory cytokine implicated in the pathogenesis of neurodegenerative disorders, but it also modulates physiological functions in both the developing and adult brain. In this study, we investigated a potential direct role of TNF伪 in determining phenotypic changes of a recently established cellular model of human basal forebrain cholinergic neuroblasts isolated from the nucleus basalis of Meynert (hfNBMs). Exposing hfNBMs to TNF伪 reduced the expression of immature markers, such as nestin and 尾-tubulin III, and inhibited primary cilium formation. On the contrary, TNF伪 increased the expression of TNF伪 receptor TNFR2 and the mature neuron marker MAP2, also promoting neurite elongation. Moreover, TNF伪 affected nerve growth factor receptor expression. We also found that TNF伪 induced the expression of DNA-methylation enzymes and, accordingly, downregulated genes involved in neuronal development through epigenetic mechanisms, as demonstrated by methylome analysis. In summary, TNF伪 showed a dual role on hfNBMs phenotypic plasticity, exerting a negative influence on neurogenesis despite a positive effect on differentiation, through mechanisms that remain to be elucidated. Our results help to clarify the complexity of TNF伪 effects in human neurons and suggest that manipulation of TNF伪 signaling could provide a potential therapeutic approach against neurodegenerative disorders.
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International journal of molecular sciences, PMID: 32854421