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先天性通气不足相关延髓神经元的遗传学鉴定。

Genetic identification of medullary neurons underlying congenital hypoventilation.

机构信息

The Brainstem Group, Institute for Cell Biology and Neurobiology, Charité Universitätsmedizin Berlin, corporate member of Freie Universität Berlin and Humboldt-Universität zu Berlin, Berlin, Germany.

German Center for Neurodegenerative Diseases (DZNE), 10117 Berlin, Germany.

出版信息

Sci Adv. 2024 Jun 21;10(25):eadj0720. doi: 10.1126/sciadv.adj0720. Epub 2024 Jun 19.

Abstract

Mutations in the transcription factors encoded by or correlate with congenital central hypoventilation disorders. These conditions are typically characterized by pronounced hypoventilation, central apnea, and diminished chemoreflexes, particularly to abnormally high levels of arterial PCO. The dysfunctional neurons causing these respiratory disorders are largely unknown. Here, we show that distinct, and previously undescribed, sets of medullary neurons coexpressing both transcription factors (dB2 neurons) account for specific respiratory functions and phenotypes seen in congenital hypoventilation. By combining intersectional chemogenetics, intersectional labeling, lineage tracing, and conditional mutagenesis, we uncovered subgroups of dB2 neurons with key functions in (i) respiratory tidal volumes, (ii) the hypercarbic reflex, (iii) neonatal respiratory stability, and (iv) neonatal survival. These data provide functional evidence for the critical role of distinct medullary dB2 neurons in neonatal respiratory physiology. In summary, our work identifies distinct subgroups of dB2 neurons regulating breathing homeostasis, dysfunction of which causes respiratory phenotypes associated with congenital hypoventilation.

摘要

或编码的转录因子中的突变与先天性中枢性通气不足障碍相关。这些病症的典型特征是明显的通气不足、中枢性呼吸暂停和化学感受反射减弱,特别是对异常高的动脉 PCO 水平。导致这些呼吸障碍的功能失调神经元在很大程度上是未知的。在这里,我们表明,表达这两种转录因子(dB2 神经元)的不同的、以前未描述的一组延髓神经元负责先天性通气不足中所见的特定呼吸功能和表型。通过结合交叉化学遗传学、交叉标记、谱系追踪和条件性突变,我们发现了 dB2 神经元的亚群,它们在(i)呼吸潮气量、(ii)高碳酸血症反射、(iii)新生儿呼吸稳定性和(iv)新生儿存活率方面具有关键功能。这些数据为特定延髓 dB2 神经元在新生儿呼吸生理中的关键作用提供了功能证据。总之,我们的工作确定了调节呼吸动态平衡的不同 dB2 神经元亚群,其功能障碍导致与先天性通气不足相关的呼吸表型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9a26/11186509/b76b1322d54a/sciadv.adj0720-f1.jpg

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