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I型和II型糖尿病临床前模型中的右心室功能障碍

Right ventricular dysfunction in preclinical models of type I and type II diabetes.

作者信息

Polson Sydney M, Thornburg Joshua P, McNair Benjamin D, Cook Christian Z, Straight Elizabeth A, Fontana Kevin C, Hoopes Caleb R, Nair Sreejayan, Bruns Danielle R

机构信息

Kinesiology & Health, University of Wyoming, Laramie, WY, USA.

WWAMI Medical Education, University of Washington, Seattle, WA, USA.

出版信息

Can J Physiol Pharmacol. 2025 Mar 1;103(3):86-97. doi: 10.1139/cjpp-2024-0195. Epub 2024 Dec 18.

Abstract

Diabetic cardiomyopathy (DCM) is a growing clinical entity and major health burden characterized by comorbid diabetes mellitus and heart failure. DCM has been commonly associated with impaired function of the left ventricle (LV); however, DCM likely also occurs in the right ventricle (RV) which has distinct physiology and pathophysiology from the LV. RV dysfunction is the strongest determinant of mortality in several clinical contexts yet remains poorly studied in diabetes. We investigated RV-specific pathophysiology using two models of diabetes-a well-characterized type 2 diabetes (T2DM) model of high-fat diet and low-dose streptozotocin (STZ) in the mouse and a large animal model of type I diabetes in domestic pigs rendered diabetic with STZ. RV global and systolic function deteriorated with diabetes, alongside hypertrophic and fibrotic remodeling. We report evidence of impaired RV insulin sensitivity, dysregulated RV metabolic gene expression, and impaired mitochondrial dynamics. Importantly, while some of these outcomes were similar to those widely reported in the LV, others were not, such as unchanged antioxidant gene expression and regulators of fatty acid uptake. Importantly, these RV-specific changes occurred in both male and female T2DM mice, together emphasizing the importance of distinguishing the RV from the LV when studying DCM and begging the consideration of RV-specific therapies.

摘要

糖尿病性心肌病(DCM)是一种日益常见的临床病症,也是主要的健康负担,其特征为合并糖尿病和心力衰竭。DCM通常与左心室(LV)功能受损有关;然而,DCM也可能发生在右心室(RV),右心室具有与左心室不同的生理和病理生理特点。在多种临床情况下,右心室功能障碍是死亡率的最强决定因素,但在糖尿病患者中对其研究仍较少。我们使用两种糖尿病模型研究右心室特异性病理生理学——一种是在小鼠中通过高脂饮食和低剂量链脲佐菌素(STZ)构建的特征明确的2型糖尿病(T2DM)模型,另一种是在家猪中通过STZ诱导糖尿病建立的I型糖尿病大动物模型。随着糖尿病的发展,右心室整体和收缩功能恶化,同时伴有肥厚和纤维化重塑。我们报告了右心室胰岛素敏感性受损、右心室代谢基因表达失调以及线粒体动力学受损的证据。重要的是,虽然其中一些结果与左心室中广泛报道的结果相似,但其他结果则不同,例如抗氧化基因表达和脂肪酸摄取调节因子未发生变化。重要的是,这些右心室特异性变化在雄性和雌性T2DM小鼠中均出现,这共同强调了在研究DCM时区分右心室和左心室的重要性,并呼吁考虑针对右心室的特异性治疗方法。

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