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胃肠道投射迷走感觉细胞类型的个体发生和营养因子敏感性。

Ontogeny and Trophic Factor Sensitivity of Gastrointestinal Projecting Vagal Sensory Cell Types.

机构信息

The Saban Research Institute, Children's Hospital Los Angeles, Los Angeles, California 90027.

The Saban Research Institute, Children's Hospital Los Angeles, Los Angeles, California 90027

出版信息

eNeuro. 2023 Apr 21;10(4). doi: 10.1523/ENEURO.0511-22.2023. Print 2023 Apr.

Abstract

Vagal sensory neurons (VSNs) located in the nodose ganglion provide information, such as stomach stretch or the presence of ingested nutrients, to the caudal medulla via specialized cell types expressing unique marker genes. Here, we leverage VSN marker genes identified in adult mice to determine when specialized vagal subtypes arise developmentally and the trophic factors that shape their growth. Experiments to screen for trophic factor sensitivity revealed that brain-derived neurotrophic factor (BDNF) and glial cell-derived neurotrophic factor (GDNF) robustly stimulate neurite outgrowth from VSNs Perinatally, BDNF was expressed by neurons of the nodose ganglion itself, while GDNF was expressed by intestinal smooth muscle cells. Thus, BDNF may support VSNs locally, whereas GDNF may act as a target-derived trophic factor supporting the growth of processes at distal innervation sites in the gut. Consistent with this, expression of the GDNF receptor was enriched in VSN cell types that project to the gastrointestinal tract. Last, the mapping of genetic markers in the nodose ganglion demonstrates that defined vagal cell types begin to emerge as early as embryonic day 13, even as VSNs continue to grow to reach gastrointestinal targets. Despite the early onset of expression for some marker genes, the expression patterns of many cell type markers appear immature in prenatal life and mature considerably by the end of the first postnatal week. Together, the data support location-specific roles for BDNF and GDNF in stimulating VSN growth, and a prolonged perinatal timeline for VSN maturation in male and female mice.

摘要

位于结状神经节的迷走感觉神经元 (VSN) 通过表达独特标记基因的特殊细胞类型,将胃伸展或摄入营养物质等信息传递到尾髓。在这里,我们利用在成年小鼠中鉴定的 VSN 标记基因来确定专门的迷走亚型何时在发育中出现,以及塑造它们生长的营养因子。筛选营养因子敏感性的实验表明,脑源性神经营养因子 (BDNF) 和胶质细胞衍生的神经营养因子 (GDNF) 可强有力地刺激 VSN 的轴突生长。围产期,BDNF 由结状神经节本身的神经元表达,而 GDNF 由肠道平滑肌细胞表达。因此,BDNF 可能在局部支持 VSN,而 GDNF 可能作为一种靶向衍生的营养因子,支持肠道远端神经支配部位的过程生长。与此一致的是,GDNF 受体的表达在投射到胃肠道的 VSN 细胞类型中富集。最后,结状神经节中遗传标记的映射表明,定义明确的迷走细胞类型早在胚胎第 13 天就开始出现,即使 VSN 继续生长以到达胃肠道靶点。尽管一些标记基因的表达较早出现,但许多细胞类型标记的表达模式在产前生活中显得不成熟,并在第一周后相当成熟。总之,数据支持 BDNF 和 GDNF 在刺激 VSN 生长方面具有特定位置的作用,以及雄性和雌性小鼠 VSN 成熟的围产期时间延长。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1454/10124152/8a451b0ec720/ENEURO.0511-22.2023_f001.jpg

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