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Directly converted astrocytes retain the ageing features of the donor fibroblasts and elucidate the astrocytic contribution to human CNS health and disease
Authors:Noemi Gatto,Cleide Dos Santos Souza,Allan C. Shaw,Simon M. Bell,Monika A. Myszczynska,Samantha Powers,Kathrin Meyer,Lydia M. Castelli,Evangelia Karyka,Heather Mortiboys,Mimoun Azzouz,Guillaume M. Hautbergue,N  ra M. M  rkus,Pamela J. Shaw,Laura Ferraiuolo
Affiliation:Noemi Gatto,Cleide Dos Santos Souza,Allan C. Shaw,Simon M. Bell,Monika A. Myszczynska,Samantha Powers,Kathrin Meyer,Lydia M. Castelli,Evangelia Karyka,Heather Mortiboys,Mimoun Azzouz,Guillaume M. Hautbergue,Nóra M. Márkus,Pamela J. Shaw,Laura Ferraiuolo
Abstract:Astrocytes are highly specialised cells, responsible for CNS homeostasis and neuronal activity. Lack of human in vitro systems able to recapitulate the functional changes affecting astrocytes during ageing represents a major limitation to studying mechanisms and potential therapies aiming to preserve neuronal health. Here, we show that induced astrocytes from fibroblasts donors in their childhood or adulthood display age‐related transcriptional differences and functionally diverge in a spectrum of age‐associated features, such as altered nuclear compartmentalisation, nucleocytoplasmic shuttling properties, oxidative stress response and DNA damage response. Remarkably, we also show an age‐related differential response of induced neural progenitor cells derived astrocytes (iNPC‐As) in their ability to support neurons in co‐culture upon pro‐inflammatory stimuli. These results show that iNPC‐As are a renewable, readily available resource of human glia that retain the age‐related features of the donor fibroblasts, making them a unique and valuable model to interrogate human astrocyte function over time in human CNS health and disease.
Keywords:ageing  astrocytes  direct reprogramming  in vitro model  neurodegeneration  neuroinflammation  neuron‐astrocyte crosstalk  nuclear abnormalities  nucleocytoplasmic transport  oxidative stress
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