The Heart Institute, Division of Molecular Cardiovascular Biology, Cincinnati Children's Hospital Medical Center, Cincinnati, OH, USA.
Internal Medicine, University of Cincinnati College of Medicine, Cincinnati, OH, USA.
Matrix Biol. 2024 Feb;126:1-13. doi: 10.1016/j.matbio.2024.01.001. Epub 2024 Jan 6.
Mouse models of Marfan syndrome (MFS) with Fibrillin 1 (Fbn1) variant C1041G exhibit cardiovascular abnormalities, including myxomatous valve disease (MVD) and aortic aneurism, with structural extracellular matrix (ECM) dysregulation. In this study, we examine the structure-function-mechanics relations of the mitral valve related to specific transitions in ECM composition and organization in progressive MVD in MFS mice from Postnatal day (P)7 to 1 year-of-age.
Mechanistic links between mechanical forces and biological changes in MVD progression were examined in Fbn1 MFS mice. By echocardiography, mitral valve dysfunction is prevalent at 2 months with a decrease in cardiac function at 6 months, followed by a preserved cardiac function at 12 months. Mitral valve (MV) regurgitation occurs in a subset of mice at 2-6 months, while progressive dilatation of the aorta occurs from 2 to 12 months. Mitral valve tissue mechanical assessments using a uniaxial Permeabilizable Fiber System demonstrate decreased stiffness of MFS MVs at all stages. Histological and microscopic analysis of ECM content, structure, and fiber orientation demonstrate that alterations in ECM mechanics, composition, and organization precede functional abnormalities in Fbn1MFS MVs. At 2 months, ECM abnormalities are detected with an increase in proteoglycans and decreased stiffness of the mitral valve. By 6-12 months, collagen fiber remodeling is increased with abnormal fiber organization in MFS mitral valve leaflets. At the same time, matrifibrocyte gene expression characteristic of collagen-rich connective tissue is increased, as detected by RNA in situ hybridization and qPCR. Together, these studies demonstrate early prevalence of proteoglycans at 2 months followed by upregulation of collagen structure and organization with age in MVs of MFS mice.
Altogether, our data indicate dynamic regulation of mitral valve structure, tissue mechanics, and function that reflect changes in ECM composition, organization, and gene expression in progressive MVD. Notably, increased collagen fiber organization and orientation, potentially dependent on increased matrifibrocyte cell activity, is apparent with altered mitral valve mechanics and function in aging MFS mice.
携带 Fibrillin 1(Fbn1)变体 C1041G 的马凡综合征(MFS)小鼠模型表现出心血管异常,包括黏液样瓣膜病(MVD)和主动脉瘤,伴有结构细胞外基质(ECM)失调。在这项研究中,我们研究了与 ECM 组成和组织的特定转变相关的二尖瓣结构-功能-力学关系,以了解在 MFS 小鼠从出生后第 7 天到 1 岁的进行性 MVD 中。
通过超声心动图检查,二尖瓣功能障碍在 2 个月时普遍存在,6 个月时心脏功能下降,12 个月时心脏功能保持不变。2-6 个月时,一部分小鼠出现二尖瓣反流,而主动脉从 2 个月到 12 个月逐渐扩张。使用单轴可渗透纤维系统对二尖瓣组织力学进行评估,结果显示所有阶段的 MFS 二尖瓣的刚度都降低。对 ECM 含量、结构和纤维方向的组织学和显微镜分析表明,ECM 力学、组成和组织的改变先于 Fbn1MFS 二尖瓣的功能异常。在 2 个月时,检测到 ECM 异常,表现为糖胺聚糖增加和二尖瓣硬度降低。6-12 个月时,胶原纤维重塑增加,二尖瓣瓣叶胶原纤维组织异常。与此同时,matrifibrocyte 基因表达特征性的富含胶原的结缔组织增加,这通过 RNA 原位杂交和 qPCR 检测到。综上所述,这些研究表明,MFS 小鼠的二尖瓣在 2 个月时早期出现糖胺聚糖增多,随后随着年龄的增长,胶原结构和组织增多。
总之,我们的数据表明,二尖瓣结构、组织力学和功能的动态调节反映了 ECM 组成、组织和基因表达的变化,这些变化与进行性 MVD 有关。值得注意的是,随着年龄的增长,MFS 小鼠二尖瓣力学和功能的改变,胶原纤维组织和取向的增加,可能依赖于 matrifibrocyte 细胞活性的增加。
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