A neonatal rat model of pulmonary vein stenosis

Author:

Li Debao,Qiu Lisheng,Hong Haifa,Chen Hao,Zhao Peibin,Xiao Yingying,Zhang Hao,Sun Qi,Ye LincaiORCID

Abstract

Abstract Objectives Pulmonary vein stenosis (PVS), one of the most challenging clinical problems in congenital heart disease, leads to secondary pulmonary arterial hypertension (PAH) and right ventricular (RV) hypertrophy. Due to the lack of a rodent model, the mechanisms underlying PVS and its associated secondary effects are largely unknown, and treatments are minimally successful. This study developed a neonatal rat PVS model with the aim of increasing our understanding of the mechanisms and developing possible treatments for PVS. Methods PVS was created at postnatal day 1 (P1) by banding pulmonary veins that receive blood from the right anterior and mid lobes. The condition was confirmed using echocardiography, computed tomography (CT), gross anatomic examination, hematoxylin and eosin (H&E) staining, fibrosis staining, and immunofluorescence. Lung and RV remodeling under the condition of PVS were evaluated using H&E staining, fibrosis staining, and immunofluorescence. Results At P21, echocardiography revealed a change in wave form and a decrease in pulmonary artery acceleration time—indicators of PAH—at the transpulmonary valve site in the PVS group. CT at P21 showed a decrease in pulmonary vein diameter in the PVS group. At P30 in the PVS group, gross anatomic examination showed pulmonary congestion, H&E staining showed wall thickening and lumen narrowing in the upstream pulmonary veins, and immunofluorescence showed an increase in the smooth muscle layers in the upstream pulmonary veins. In addition, at P30 in the PVS group, lung remodeling was evidenced by hyperemia, thickening of pulmonary small vessel walls and smooth muscle layers, and reduction of the number of alveoli. RV remodeling was evidenced by an increase in RV free wall thickness. Conclusions A neonatal rat model of PVS was successfully established, showing secondary lung and RV remodeling. This model may serve as a useful platform for understanding the mechanisms and treatments for PVS.

Funder

National Key R&D Program of China

Natural Science Foundation of Shanghai

Science and Technology Innovation Plan Of Shanghai Science and Technology Commission

National Natural Science Foundation of China

Foundation of Pudong Science and Technology Development

Health and Family Planning Committee of Pudong New Area

Shanghai Key Clinical Specialty(shslczdzk), Biomedical and Engineering (Science) Interdisciplinary Study Fund of Shanghai Jiaotong University

Innovation Project of Distinguished Medical Team in Ningbo

Publisher

Springer Science and Business Media LLC

Subject

General Biochemistry, Genetics and Molecular Biology

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