Tissue material properties, whole-bone morphology and mechanical behavior in the Fbn1C1041G/+ mouse model of Marfan syndrome

Q1 Medicine

Matrix Biology Plus Pub Date : 2024-06-15 DOI:10.1016/j.mbplus.2024.100155

Elizabeth A. Zimmermann , Taylor DeVet , Myriam Cilla , Laia Albiol , Kyle Kavaseri , Christine Andrea , Catherine Julien , Kerstin Tiedemann , Arash Panahifar , Sima A. Alidokht , Richard Chromik , Svetlana V. Komarova , Dieter P. Reinhardt , Paul Zaslansky , Bettina M. Willie

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引用次数: 0

Abstract

Marfan syndrome (MFS) is a connective tissue disorder caused by pathogenic mutations in FBN1. In bone, the protein fibrillin-1 is found in the extracellular matrix where it provides structural support of elastic fiber formation, stability for basement membrane, and regulates the bioavailability of growth factors. Individuals with MFS exhibit a range of skeletal complications including low bone mineral density and long bone overgrowth. However, it remains unknown if the bone phenotype is caused by alteration of fibrillin-1′s structural function or distortion of its interactions with bone cells. To assess the structural effects of the fibrillin-1 mutation, we characterized bone curvature, microarchitecture, composition, porosity, and mechanical behavior in the Fbn1^C1041G/+ mouse model of MFS. Tibiae of 10, 26, and 52-week-old female Fbn1^C1041G/+ and littermate control (LC) mice were analyzed. Mechanical behavior was assessed via in vivo strain gauging, finite element analysis, ex vivo three-point bending, and nanoindentation. Tibial bone morphology and curvature were assessed with micro computed tomography (μCT). Bone composition was measured with Fourier transform infrared (FTIR) imaging. Vascular and osteocyte lacunar porosity were assessed by synchrotron computed tomography. Fbn1^C1041G/+ mice exhibited long bone overgrowth and osteopenia consistent with the MFS phenotype. Trabecular thickness was lower in Fbn1^C1041G/+ mice but cortical bone microarchitecture was similar in Fbn1^C1041G/+ and LC mice. Whole bone curvature was straighter below the tibio-fibular junction in the medial–lateral direction and more curved above in LC compared to Fbn1^C1041G/+ mice. The bone matrix crystallinity was 4 % lower in Fbn1^C1041G/+ mice compared to LC, implying that mineral platelets in LCs have greater crystal size and perfection than Fbn1^C1041G/+ mice. Structural and mechanical properties were similar between genotypes. Cortical diaphyseal lacunar porosity was lower in Fbn1^C1041G/+ mice compared to LC; this was a result of the average volume of an individual osteocyte lacunae being smaller. These data provide valuable insights into the bone phenotype and its contribution to fracture risk in this commonly used mouse model of MFS.

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马凡氏综合征 Fbn1C1041G/+ 小鼠模型的组织材料特性、全骨形态和机械性能

马凡综合征（MFS）是一种由 FBN1 基因突变引起的结缔组织疾病。在骨骼中，蛋白质纤维素-1 存在于细胞外基质中，为弹性纤维的形成提供结构支持，稳定基底膜，并调节生长因子的生物利用度。骨质疏松症患者会表现出一系列骨骼并发症，包括低骨矿物质密度和长骨过度生长。然而，骨表型是由纤维蛋白-1的结构功能改变还是由其与骨细胞的相互作用发生扭曲引起的，目前仍不得而知。为了评估纤连蛋白-1突变对结构的影响，我们对Fbn1C1041G/+小鼠MFS模型的骨弯曲度、微结构、成分、孔隙率和机械行为进行了鉴定。我们对 10、26 和 52 周大的雌性 Fbn1C1041G/+ 小鼠和同窝对照（LC）小鼠的胫骨进行了分析。通过体内应变测量、有限元分析、体外三点弯曲和纳米压痕法评估了机械行为。胫骨形态和弧度通过微型计算机断层扫描（μCT）进行评估。傅立叶变换红外（FTIR）成像测量了骨成分。血管和骨细胞裂隙孔隙度通过同步辐射计算机断层扫描进行评估。Fbn1C1041G/+ 小鼠表现出与 MFS 表型一致的长骨过度生长和骨质疏松。Fbn1C1041G/+ 小鼠的骨小梁厚度较低，但 Fbn1C1041G/+ 和 LC 小鼠的皮质骨微结构相似。与 Fbn1C1041G/+ 小鼠相比，LC 小鼠胫腓骨交界处以下的整体骨弯曲度在内侧-外侧方向更直，而在上方则更弯曲。Fbn1C1041G/+ 小鼠的骨基质结晶度比 LC 小鼠低 4%，这意味着 LC 小鼠的矿物质血小板比 Fbn1C1041G/+ 小鼠的晶体尺寸更大、更完美。不同基因型小鼠的结构和机械性能相似。与 LC 相比，Fbn1C1041G/+ 小鼠皮质骺裂隙孔隙率较低；这是由于单个骨细胞裂隙的平均体积较小。这些数据为我们深入了解这种常用的 MFS 小鼠模型的骨表型及其对骨折风险的影响提供了宝贵的信息。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Matrix Biology Plus Medicine-Histology

CiteScore

9.00

自引率

0.00%

发文量

审稿时长

105 days