不同类型 I 型胶原的改变导致成骨不全症小鼠模型中肺和呼吸系统缺陷的严重程度不同。
Distinct type I collagen alterations cause intrinsic lung and respiratory defects of variable severity in mouse models of osteogenesis imperfecta.
机构信息
Department of Physiology & Cell Biology, University of Arkansas for Medical Sciences, Little Rock, AR, USA.
Department of Pediatrics, University of Arkansas for Medical Sciences, Little Rock, AR, USA.
出版信息
J Physiol. 2023 Jan;601(2):355-379. doi: 10.1113/JP283452. Epub 2022 Nov 9.
Type I collagen alterations cause osteogenesis imperfecta (OI), a connective tissue disorder characterized by severe bone fragility. Patients with OI can suffer from significant pulmonary manifestations including severe respiratory distress in the neonatal period and a progressive decline in respiratory function in adulthood. We and others have shown intrinsic lung defects in some mouse models of OI. In this large study, we performed histological, histomorphometric, microcomputed tomography and invasive studies on oim/+, Col1a2 , CrtapKO and oim/oim mice, mimicking mild to moderate to severe OI, with the overall goal of determining the extent of their pulmonary and respiratory mechanics defects and whether these defects correlate with the skeletal disease severity and affect each sex equally. Although with variable severity, OI lung histology consistently showed alveolar simplification with enlarged acinar airspace and reduced alveolar surface. Numerous respiratory mechanics parameters, including respiratory system resistance and elastance, tissue damping, inspiratory capacity, total lung capacity, and others, were significantly and similarly impacted in CrtapKO and oim/oim but not in oim/+ or Col1a2 compared to control mice. Our data indicate that the impact of type I collagen alterations and OI on lung morphology and function positively correlate with the severity of the extracellular matrix deficiency. Moreover, the respiratory defects were more pronounced in male compared to female mice. It will be important to determine whether our observations in mice translate to OI patients and to dissect the respective contribution of intrinsic lung defects vs. extrinsic skeletal defects to impaired lung function in OI. KEY POINTS: Different type I collagen alterations in mouse models of osteogenesis imperfecta (OI) cause similar abnormal lung histology, with alveolar simplification and reduced alveolar surface, reminiscent of emphysema. Several respiratory mechanics parameters are altered in mouse models of OI. The impact of type I collagen alterations and OI on lung morphology and function positively correlate with the severity of the extracellular matrix deficiency. Respiratory defects were more pronounced in male compared to female mice. It will be important to determine whether our observations in mice translate to OI patients and to dissect the respective contribution of intrinsic lung defects vs. extrinsic skeletal defects to impaired lung function in OI.
I 型胶原改变导致成骨不全症(OI),这是一种以严重骨骼脆弱为特征的结缔组织疾病。OI 患者可能会出现严重的肺部表现,包括新生儿期严重呼吸窘迫和成年后呼吸功能逐渐下降。我们和其他人已经在一些 OI 的小鼠模型中发现了内在的肺部缺陷。在这项大型研究中,我们对 oim/+、Col1a2、CrtapKO 和 oim/oim 小鼠进行了组织学、组织形态计量学、微计算机断层扫描和侵袭性研究,模拟了从轻度到中度到重度 OI,总体目标是确定它们的肺部和呼吸力学缺陷的程度,以及这些缺陷是否与骨骼疾病的严重程度相关,是否平等地影响每一种性别。尽管严重程度不同,但 OI 肺部组织学始终显示肺泡简化,肺泡腔增大,肺泡表面减少。与对照小鼠相比,CrtapKO 和 oim/oim 小鼠的许多呼吸力学参数,包括呼吸系统阻力和弹性、组织阻尼、吸气量、总肺活量等,均显著且相似地受到影响,但 oim/+或 Col1a2 小鼠则没有。我们的数据表明,I 型胶原改变和 OI 对肺形态和功能的影响与细胞外基质缺乏的严重程度呈正相关。此外,雄性小鼠的呼吸缺陷比雌性小鼠更明显。重要的是要确定我们在小鼠中的观察结果是否适用于 OI 患者,并剖析内在肺缺陷与外在骨骼缺陷对 OI 肺功能障碍的各自贡献。关键点:不同的 I 型胶原改变在成骨不全症(OI)的小鼠模型中导致相似的异常肺组织学,表现为肺泡简化和肺泡表面减少,类似于肺气肿。OI 小鼠模型中的几个呼吸力学参数发生改变。I 型胶原改变和 OI 对肺形态和功能的影响与细胞外基质缺乏的严重程度呈正相关。与雌性小鼠相比,雄性小鼠的呼吸缺陷更为明显。重要的是要确定我们在小鼠中的观察结果是否适用于 OI 患者,并剖析内在肺缺陷与外在骨骼缺陷对 OI 肺功能障碍的各自贡献。
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