Micromechanics of lung capillaries across mouse lifespan and in positive- vs negative-pressure ventilation.

Kathryn Regan, Lauren Castle, Robert LeBourdais, Abdulrahman Kobayter, Linzheng Shi, Winita Wangsrikhun, Gabrielle Grifno, Rohin Banerji, Athanasios Batgidis, Bela Suki, Hadi T Nia
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Abstract

The lung undergoes continuous remodeling throughout normal development and aging, including changes to alveolar and capillary structure and function. While histological methods allow static analysis of these age-related changes, characterizing the changes that occur in response to mechanical stimuli remains difficult, particularly over a dynamic, physiologically relevant range in a functioning lung. Alveolar and capillary distension - the change in diameter of alveoli and capillaries, respectively, in response to pressure changes - is one such process, where dynamically controlling and monitoring the diameter of the same capillary or alveolus is essential to infer its mechanical properties. We overcome these limitations by utilizing the recently developed crystal ribcage to image the alveoli and vasculature of a functional mouse lung across the lifespan in postnatal (6-7 days), young adult (12-18 weeks), and aged (20+ months) mice. Using a range of biologically relevant vascular (0-15 cmH2O) and transpulmonary (3-12 cmH2O) pressures, we directly quantify vascular and alveolar distention in the functional lung as we precisely adjust pulmonary pressures. Our results show differences in age-related alveolar and vascular distensibility: when we increase transpulmonary alveolar or vascular pressure, vessels in postnatal lungs expand less and undergo less radial and axial strain, under each respective pressure type, suggesting stiffer capillaries than in older lungs. However, while vessels in young adult and aged lungs respond similarly to variations in vascular pressure, differences in elasticity start to emerge at the alveolar scale in response to transpulmonary alveolar pressure changes. Our results further indicate that differing effects of ventilation mode (i.e., positive vs negative) present themselves at the capillary level, with vessels under positive pressure undergoing more compression than when under negative-pressure conditions. These findings contribute both to the understanding of the functional changes that occur within the lung across the lifespan, as well as to the debate of ventilation effects on lung microphysiology.

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肺部在正常发育和衰老过程中不断发生重塑,包括肺泡和毛细血管结构与功能的变化。虽然组织学方法可以对这些与年龄相关的变化进行静态分析,但要描述机械刺激下发生的变化仍然很困难,尤其是在动态的、与生理相关的肺功能范围内。肺泡和毛细血管扩张--肺泡和毛细血管的直径分别随压力变化而变化--就是这样一个过程,动态控制和监测同一毛细血管或肺泡的直径对推断其机械特性至关重要。我们利用最近开发的水晶肋骨,对出生后(6-7 天)、幼年(12-18 周)和老年(20 个月)小鼠肺泡和血管进行了成像,从而克服了这些局限性。我们使用一系列与生物相关的血管压力(0-15 cmH2O)和跨肺压力(3-12 cmH2O),在精确调节肺部压力的同时,直接量化功能性肺部的血管和肺泡膨胀情况。我们的结果显示了与年龄相关的肺泡和血管扩张性差异:当我们增加肺泡或血管的跨肺压力时,在每种压力类型下,出生后肺部血管的扩张程度较小,径向和轴向应变也较小,这表明毛细血管比老年肺部更硬。然而,虽然年轻成人肺和老年肺的血管对血管压力变化的反应相似,但在肺泡尺度上,血管弹性的差异开始出现,以应对肺泡转压的变化。我们的研究结果进一步表明,通气模式(即正压与负压)的不同影响表现在毛细血管层面,正压条件下的血管比负压条件下的血管受到更多的压缩。这些发现有助于人们理解肺在整个生命周期中发生的功能变化,也有助于讨论通气对肺微生理学的影响。
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