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在模拟老化骨髓的工程化骨类似物中,增加的变形对于封装细胞的机械反应是可有可无的。

Increased deformations are dispensable for encapsulated cell mechanoresponse in engineered bone analogs mimicking aging bone marrow.

作者信息

Regner Alexander M, DeLeon Maximilien, Gibbons Kalin D, Howard Sean, Nesbitt Derek Q, Darghiasi Seyedeh F, Zavala Anamaria G, Lujan Trevor J, Fitzpatrick Clare K, Farach-Carson Mary C, Wu Danielle, Uzer Gunes

机构信息

Mechanical and Biomedical Engineering Department, Boise State University, USA.

Department of Diagnostic and Biomedical Sciences, UTHealth Houston School of Dentistry, USA.

出版信息

Mechanobiol Med. 2025 Mar;3(1). doi: 10.1016/j.mbm.2024.100097. Epub 2024 Oct 1.

Abstract

Aged individuals and astronauts experience bone loss despite rigorous physical activity. Bone mechanoresponse is in-part regulated by mesenchymal stem cells (MSCs) that respond to mechanical stimuli. Direct delivery of low intensity vibration (LIV) recovers MSC proliferation in senescence and simulated microgravity models, indicating that age-related reductions in mechanical signal delivery within bone marrow may contribute to declining bone mechanoresponse. To answer this question, we developed a 3D bone marrow analog that controls trabecular geometry, marrow mechanics and external stimuli. Validated finite element (FE) models were developed to quantify strain environment within hydrogels during LIV. Bone marrow analogs with gyroid-based trabeculae of scaffold volume fractions (SV/TV) corresponding to adult (25 %) and aged (13 %) mice were printed using polylactic acid (PLA). MSCs encapsulated in migration-permissive hydrogels within printed trabeculae showed robust cell populations on both PLA surface and hydrogel within a week. Following 14 days of LIV treatment (1 g, 100 Hz, 1 h/day), cell proliferation, type-I collagen (Collagen-I) and filamentous actin (F-actin) were quantified for the cells in the hydrogel fraction. While LIV increased all measured outcomes, FE models predicted higher von Mises strains for the 13 % SV/TV groups (0.2 %) when compared to the 25 % SV/TV group (0.1 %). While LIV increased collagen-I volume 34 % more in 13 % SV/TV groups when compared to 25 % SV/TV groups, collagen-I and F-actin measures remained lower in the 13 % SV/TV groups when compared to 25 % SV/TV counterparts, indicating that both LIV-induced strains and scaffold volume fraction (i.e. available scaffold surface) affect cell behavior in the hydrogel phase. Overall, bone marrow analogs offer a robust and repeatable platform to study bone mechanobiology.

摘要

尽管进行了严格的体育活动,老年人和宇航员仍会出现骨质流失。骨力学反应部分受间充质干细胞(MSC)调节,这些细胞对机械刺激作出反应。直接施加低强度振动(LIV)可恢复衰老和模拟微重力模型中的MSC增殖,这表明骨髓内机械信号传递的与年龄相关的减少可能导致骨力学反应下降。为了回答这个问题,我们开发了一种三维骨髓模拟物,可控制小梁几何形状、骨髓力学和外部刺激。开发了经过验证的有限元(FE)模型,以量化LIV期间水凝胶内的应变环境。使用聚乳酸(PLA)打印出具有与成年(25%)和老年(13%)小鼠相对应的支架体积分数(SV/TV)的基于类螺旋结构小梁的骨髓模拟物。封装在打印小梁内允许迁移的水凝胶中的MSC在一周内在PLA表面和水凝胶上均显示出强大的细胞群体。在进行14天的LIV治疗(1g,100Hz,每天1小时)后,对水凝胶部分中的细胞进行细胞增殖、I型胶原蛋白(胶原蛋白-I)和丝状肌动蛋白(F-肌动蛋白)的定量分析。虽然LIV增加了所有测量结果,但FE模型预测,与25%SV/TV组(0.1%)相比,13%SV/TV组的冯·米塞斯应变更高(0.2%)。虽然与25%SV/TV组相比,LIV使13%SV/TV组的胶原蛋白-I体积增加了34%,但与25%SV/TV组相比,13%SV/TV组的胶原蛋白-I和F-肌动蛋白测量值仍然较低,这表明LIV诱导的应变和支架体积分数(即可用支架表面)均影响水凝胶相中的细胞行为。总体而言,骨髓模拟物为研究骨机械生物学提供了一个强大且可重复的平台。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5e7c/12082124/2295a30e7e2e/ga1.jpg

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