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基质细胞信号蛋白 Lonely heart 中的不同结构域对于 . 的心脏细胞外基质形成和心脏功能至关重要。

Distinct domains in the matricellular protein Lonely heart are crucial for cardiac extracellular matrix formation and heart function in .

机构信息

From the Departments of Zoology and Developmental Biology and.

Genetics, Faculty of Biology & Chemistry, University of Osnabrück Barbarastrasse 11, 49076 Osnabrück, Germany.

出版信息

J Biol Chem. 2018 May 18;293(20):7864-7879. doi: 10.1074/jbc.M117.817940. Epub 2018 Mar 29.

DOI:10.1074/jbc.M117.817940
PMID:29599288
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5961049/
Abstract

The biomechanical properties of extracellular matrices (ECMs) are critical to many biological processes, including cell-cell communication and cell migration and function. The correct balance between stiffness and elasticity is essential to the function of numerous tissues, including blood vessels and the lymphatic system, and depends on ECM constituents (the "matrisome") and on their level of interconnection. However, despite its physiological relevance, the matrisome composition and organization remain poorly understood. Previously, we reported that the ADAMTS-like protein Lonely heart (Loh) is critical for recruiting the type IV collagen-like protein Pericardin to the cardiac ECM. Here, we utilized as a simple and genetically amenable invertebrate model for studying Loh-mediated recruitment of tissue-specific ECM components such as Pericardin to the ECM. We focused on the functional relevance of distinct Loh domains to protein localization and Pericardin recruitment. Analysis of Loh deletion constructs revealed that one thrombospondin type 1 repeat (TSR1-1), which has an embedded WW motif, is critical for anchoring Loh to the ECM. Two other thrombospondin repeats, TSR1-2 and TSR1-4, the latter containing a CTCG motif, appeared to be dispensable for tethering Loh to the ECM but were crucial for proper interaction with and recruitment of Pericardin. Moreover, our results also suggested that Pericardin in the cardiac ECM primarily ensures the structural integrity of the heart, rather than increasing tissue flexibility. In conclusion, our work provides new insights into the roles of thrombospondin type 1 repeats and advances our understanding of cardiac ECM assembly and function.

摘要

细胞外基质(ECM)的生物力学特性对许多生物学过程至关重要,包括细胞间通讯、细胞迁移和功能。刚度和弹性之间的正确平衡对于许多组织的功能至关重要,包括血管和淋巴系统,这取决于 ECM 成分(“基质组”)及其连接程度。然而,尽管其具有生理相关性,但基质组的组成和组织仍知之甚少。此前,我们报道 ADAMTS 样蛋白 Lonely heart(Loh)对于招募 IV 型胶原蛋白样蛋白 Pericardin 到心脏 ECM 中至关重要。在这里,我们利用作为一种简单且遗传上易于处理的无脊椎动物模型,研究 Loh 介导的组织特异性 ECM 成分(如 Pericardin)向 ECM 的募集。我们专注于不同 Loh 结构域对蛋白质定位和 Pericardin 募集的功能相关性。对 Loh 缺失构建体的分析表明,一个包含 WW 基序的血栓素样蛋白 1 重复序列(TSR1-1)对于将 Loh 锚定到 ECM 至关重要。另外两个血栓素重复序列,TSR1-2 和 TSR1-4,后者包含一个 CTCG 基序,似乎对于将 Loh 束缚到 ECM 是可有可无的,但对于与 Pericardin 的正确相互作用和募集至关重要。此外,我们的结果还表明,心脏 ECM 中的 Pericardin 主要确保心脏的结构完整性,而不是增加组织的柔韧性。总之,我们的工作为血栓素样蛋白 1 重复序列的作用提供了新的见解,并推进了我们对心脏 ECM 组装和功能的理解。

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