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间质中的清新气息:间质发育障碍对支气管肺发育不良发病机制的影响。

A breath of fresh air on the mesenchyme: impact of impaired mesenchymal development on the pathogenesis of bronchopulmonary dysplasia.

机构信息

Department of General Pediatrics and Neonatology, University Children's Hospital Giessen , Giessen , Germany ; Department of Internal Medicine II, Universities of Giessen and Marburg Lung Center , Giessen , Germany ; Member of the German Center for Lung Research (DZL) , Giessen , Germany.

Department of Internal Medicine II, Universities of Giessen and Marburg Lung Center , Giessen , Germany ; Member of the German Center for Lung Research (DZL) , Giessen , Germany.

出版信息

Front Med (Lausanne). 2015 Apr 28;2:27. doi: 10.3389/fmed.2015.00027. eCollection 2015.

Abstract

The early mouse embryonic lung, with its robust and apparently reproducible branching pattern, has always fascinated developmental biologists. They have extensively used this embryonic organ to decipher the role of mammalian orthologs of Drosophila genes in controlling the process of branching morphogenesis. During the early pseudoglandular stage, the embryonic lung is formed mostly of tubes that keep on branching. As the branching takes place, progenitor cells located in niches are also amplified and progressively differentiate along the proximo-distal and dorso-ventral axes of the lung. Such elaborate processes require coordinated interactions between signaling molecules arising from and acting on four functional domains: the epithelium, the endothelium, the mesenchyme, and the mesothelium. These interactions, quite well characterized in a relatively simple lung tubular structure remain elusive in the successive developmental and postnatal phases of lung development. In particular, a better understanding of the process underlying the formation of secondary septa, key structural units characteristic of the alveologenesis phase, is still missing. This structure is critical for the formation of a mature lung as it allows the subdivision of saccules in the early neonatal lung into alveoli, thereby considerably expanding the respiratory surface. Interruption of alveologenesis in preterm neonates underlies the pathogenesis of chronic neonatal lung disease known as bronchopulmonary dysplasia. De novo formation of secondary septae appears also to be the limiting factor for lung regeneration in human patients with emphysema. In this review, we will therefore focus on what is known in terms of interactions between the different lung compartments and discuss the current understanding of mesenchymal cell lineage formation in the lung, focusing on secondary septae formation.

摘要

早期的小鼠胚胎肺,其强大且明显可重复的分支模式,一直令发育生物学家着迷。他们广泛地使用这个胚胎器官来破译果蝇基因在哺乳动物同源物在控制分支形态发生过程中的作用。在早期假腺状阶段,胚胎肺主要由保持分支的管组成。随着分支的发生,位于龛中的祖细胞也被扩增,并沿着肺的近-远轴和背-腹轴逐渐分化。这些精细的过程需要来自和作用于四个功能域的信号分子之间的协调相互作用:上皮、内皮、间充质和间皮。这些相互作用在相对简单的肺管状结构中已经得到很好的描述,但在肺发育的连续发育和出生后阶段仍然难以捉摸。特别是,对于形成次级间隔的过程的更好理解,次级间隔是肺泡发生阶段的关键结构单元,仍然缺失。这个结构对于成熟肺的形成至关重要,因为它允许早期新生儿肺中的囊泡在肺泡中细分,从而大大增加了呼吸表面。早产儿的肺泡发生中断是慢性新生儿肺疾病(支气管肺发育不良)的发病机制。在患有肺气肿的人类患者中,次级间隔的新形成似乎也是肺再生的限制因素。因此,在这篇综述中,我们将重点关注不同肺区之间相互作用的已知内容,并讨论目前对肺中间质细胞谱系形成的理解,重点关注次级间隔的形成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/523e/4412070/ac273fccc413/fmed-02-00027-g001.jpg

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