Impaired cell–cell communication and axon guidance because of pulmonary hypoperfusion during postnatal alveolar development

Author:

Li Debao,Wang Jing,Fang Yuan,Hu Yuqing,Xiao Yingying,Cui Qing,Jiang Chuan,Sun Sijuan,Chen Hao,Ye Lincai,Sun Qi

Abstract

Abstract Background Pulmonary hypoperfusion is common in children with congenital heart diseases (CHDs) or pulmonary hypertension (PH) and causes adult pulmonary dysplasia. Systematic reviews have shown that some children with CHDs or PH have mitigated clinical outcomes with COVID-19. Understanding the effects of pulmonary hypoperfusion on postnatal alveolar development may aid in the development of methods to improve the pulmonary function of children with CHDs or PH and improve their care during the COVID-19 pandemic, which is characterized by cytokine storm and persistent inflammation. Methods and results We created a neonatal pulmonary hypoperfusion model through pulmonary artery banding (PAB) surgery at postnatal day 1 (P1). Alveolar dysplasia was confirmed by gross and histological examination at P21. Transcriptomic analysis of pulmonary tissues at P7(alveolar stage 2) and P14(alveolar stage 4) revealed that the postnatal alveolar development track had been changed due to pulmonary hypoperfusion. Under the condition of pulmonary hypoperfusion, the cell–cell communication and axon guidance, which both determine the final number of alveoli, were lost; instead, there was hyperactive cell cycle activity. The transcriptomic results were further confirmed by the examination of axon guidance and cell cycle markers. Because axon guidance controls inflammation and immune cell activation, the loss of axon guidance may explain the lack of severe COVID-19 cases among children with CHDs or PH accompanied by pulmonary hypoperfusion. Conclusions This study suggested that promoting cellcell communication or supplementation with guidance molecules may treat pulmonary hypoperfusion–induced alveolar dysplasia, and that COVID-19 is less likely to cause a cytokine storm in children with CHD or PH accompanied by pulmonary hypoperfusion. Graphical Abstract

Funder

National Key Research and Development Program of China

Natural Science Foundation of Shanghai

National Natural Science Foundation of China

Science and Technology Innovation Action Plan of Shanghai—Experimental Animal Research

Foundation of Pudong Science and Technology Development

Shanghai Science and Technology Innovation Project

Key Discipline Group Development Fund of Health and Family Planning Commission of Pudong New District

Shanghai Key Clinical Specialty

Publisher

Springer Science and Business Media LLC

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