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Adult enteric nervous system in health is maintained by a dynamic balance between neuronal apoptosis and neurogenesis

机译:通过神经元凋亡与神经发生之间的动态平衡来维持健康的成人肠神经系统

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摘要

According to current dogma, there is little or no ongoing neurogenesis in the fully developed adult enteric nervous system. This lack of neurogenesis leaves unanswered the question of how enteric neuronal populations are maintained in adult guts, given previous reports of ongoing neuronal death. Here, we confirm that despite ongoing neuronal cell loss because of apoptosis in the myenteric ganglia of the adult small intestine, total myenteric neuronal numbers remain constant. This observed neuronal homeostasis is maintained by new neurons formed in vivo from dividing precursor cells that are located within myenteric ganglia and express both Nestin and p75NTR, but not the pan-glial marker Sox10. Mutation of the phosphatase and tensin homolog gene in this pool of adult precursors leads to an increase in enteric neuronal number, resulting in ganglioneuromatosis, modeling the corresponding disorder in humans. Taken together, our results show significant turnover and neurogenesis of adult enteric neurons and provide a paradigm for understanding the enteric nervous system in health and disease.
机译:根据目前的教条,在完全发达的成人肠神经系统中几乎没有或没有正在进行的神经发生。鉴于先前关于持续性神经元死亡的报道,这种缺乏神经发生的问题仍未解决如何在成年肠道中维持肠道神经元种群的问题。在这里,我们确认,尽管由于成年小肠的肌层神经节中的细胞凋亡导致持续的神经元细胞丢失,但总的肌层神经元数量仍保持恒定。这种观察到的神经元稳态是由新的神经元维持的,该新的神经元是由分裂的前体细胞在体内形成的,这些前体细胞位于肌层神经节内并表达Nestin和p75NTR,但不表达泛神经胶质标记物Sox10。成年前体库中磷酸酶和张力蛋白同源基因的突变导致肠神经元数目增加,导致神经节神经瘤病,模拟了人类的相应疾病。两者合计,我们的研究结果表明成人肠神经元的重要营业额和神经发生,并为理解健康和疾病中的肠神经系统提供了范例。

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