Hybrid hydrogel–extracellular matrix scaffolds identify biochemical and mechanical signatures of cardiac ageing

IF 37.2 1区 材料科学 Q1 CHEMISTRY, PHYSICAL
Avery Rui Sun, Md Faris H. Ramli, Xingyu Shen, Karthikbabu Kannivadi Ramakanth, Dixiao Chen, Yang Hu, Prasanna Vidyasekar, Roger S. Foo, Yuchen Long, Jin Zhu, Matthew Ackers-Johnson, Jennifer L. Young
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Abstract

Extracellular matrix remodelling of cardiac tissue is a key contributor to age-related cardiovascular disease and dysfunction. Such remodelling is multifaceted including changes to the biochemical composition, architecture and mechanics, clouding our understanding of how and which extracellular matrix properties contribute to a dysfunctional state. Here we describe a decellularized extracellular matrix–synthetic hydrogel hybrid scaffold that independently confers two distinct matrix properties—ligand presentation and stiffness—to cultured cells in vitro, allowing for the identification of their specific roles in cardiac ageing. The hybrid scaffold maintains native matrix composition and organization of young or aged murine cardiac tissue, whereas its mechanical properties can be independently tuned to mimic young or aged tissue stiffness. Seeding these scaffolds with murine primary cardiac fibroblasts, we identify distinct age- and matrix-dependent mechanisms of cardiac fibroblast activation, matrix remodelling and senescence. Importantly, we show that the ligand presentation of a young extracellular matrix can outweigh the profibrotic stiffness cues typically present in an aged extracellular matrix in maintaining or driving cardiac fibroblast quiescence. Ultimately, these tunable scaffolds can enable the discovery of specific extracellular targets to prevent ageing dysfunction and promote rejuvenation.

Abstract Image

混合水凝胶-细胞外基质支架识别心脏老化的生化和机械特征
心脏组织的细胞外基质重构是与年龄相关的心血管疾病和功能障碍的关键因素。这种重塑是多方面的,包括生物化学组成、结构和力学的变化,使我们对细胞外基质特性如何以及哪些特性导致功能失调状态的理解变得模糊。在这里,我们描述了一种脱细胞细胞外基质-合成水凝胶混合支架,它独立地赋予体外培养细胞两种不同的基质特性-配体呈现和刚度,从而可以识别它们在心脏老化中的特定作用。混合支架维持了年轻或年老小鼠心脏组织的天然基质组成和组织,而其机械性能可以独立调整以模拟年轻或年老组织的刚度。在这些支架中植入小鼠原代心脏成纤维细胞,我们确定了心脏成纤维细胞激活、基质重塑和衰老的不同年龄和基质依赖机制。重要的是,我们表明年轻细胞外基质的配体呈现可以超过通常存在于衰老细胞外基质中的促纤维化僵硬线索,以维持或驱动心脏成纤维细胞静止。最终,这些可调节的支架可以发现特定的细胞外目标,以防止衰老功能障碍和促进返老还童。
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来源期刊
Nature Materials
Nature Materials 工程技术-材料科学:综合
CiteScore
62.20
自引率
0.70%
发文量
221
审稿时长
3.2 months
期刊介绍: Nature Materials is a monthly multi-disciplinary journal aimed at bringing together cutting-edge research across the entire spectrum of materials science and engineering. It covers all applied and fundamental aspects of the synthesis/processing, structure/composition, properties, and performance of materials. The journal recognizes that materials research has an increasing impact on classical disciplines such as physics, chemistry, and biology. Additionally, Nature Materials provides a forum for the development of a common identity among materials scientists and encourages interdisciplinary collaboration. It takes an integrated and balanced approach to all areas of materials research, fostering the exchange of ideas between scientists involved in different disciplines. Nature Materials is an invaluable resource for scientists in academia and industry who are active in discovering and developing materials and materials-related concepts. It offers engaging and informative papers of exceptional significance and quality, with the aim of influencing the development of society in the future.
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