Characterization of a murine model of endothelial dysfunction induced by chronic intraperitoneal administration of angiotensin II

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作者
Celeste Trejo-Moreno
Enrique Jiménez-Ferrer
Gabriela Castro-Martínez
Marisol Méndez-Martínez
María Angélica Santana
Gerardo Arrellín-Rosas
José Pedraza-Chaverri
Omar Noel Medina-Campos
Beatriz Hernández-Téllez
Oscar Ramírez-Pliego
Maribel Herrera-Ruiz
Jacquelynne Cervantes-Torres
Zimri Aziel Alvarado-Ojeda
Alejandro Costet-Mejía
Gladis Fragoso
Gabriela Rosas-Salgado
机构
[1] Universidad Autónoma del Estado de Morelos,Facultad de Medicina
[2] Instituto Mexicano del Seguro Social,Centro de Investigación Biomédica del Sur
[3] Universidad Autónoma Metropolitana-Xochimilco,Departamento de Sistemas Biológicos
[4] Universidad Autónoma del Estado de Morelos,Centro de Investigación en Dinámica Celular
[5] Universidad Panamericana,Facultad de Ciencias de la Salud
[6] Universidad Nacional Autónoma de México,Facultad de Química
[7] Universidad Nacional Autónoma de México,Facultad de Medicina
[8] Universidad Nacional Autónoma de México,Instituto de Investigaciones Biomédicas
[9] Universidad Autónoma Metropolitana-Iztapalapa,Posgrado en Biología Experimental
来源
Scientific Reports | / 11卷
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摘要
Endothelial dysfunction (ED) is a key factor for the development of cardiovascular diseases. Due to its chronic, life-threatening nature, ED only can be studied experimentally in animal models. Therefore, this work was aimed to characterize a murine model of ED induced by a daily intraperitoneal administration of angiotensin II (AGII) for 10 weeks. Oxidative stress, inflammation, vascular remodeling, hypertension, and damage to various target organs were evaluated in treated animals. The results indicated that a chronic intraperitoneal administration of AGII increases the production of systemic soluble VCAM, ROS and ICAM-1 expression, and the production of TNFα, IL1β, IL17A, IL4, TGFβ, and IL10 in the kidney, as well as blood pressure levels; it also promotes vascular remodeling and induces non-alcoholic fatty liver disease, glomerulosclerosis, and proliferative retinopathy. Therefore, the model herein proposed can be a representative model for ED; additionally, it is easy to implement, safe, rapid, and inexpensive.
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