En route towards a personalized medicine approach: Innovative therapeutic modalities for connective tissue disorders

IF 4.5 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Charlene Redhead, Nandaraj Taye, Dirk Hubmacher
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引用次数: 0

Abstract

Connective tissue disorders can be caused by pathogenic variants (mutations) in genes encoding extracellular matrix (ECM) proteins. Such disorders typically manifest during development or postnatal growth and result in significant morbidity and mortality. The development of curative treatments for connective tissue disorders is hampered in part by the inability of many mature connective tissues to efficiently regenerate. To be most effective, therapeutic strategies designed to preserve or restore tissue function will likely need to be initiated during phases of significant endogenous connective tissue remodeling and organ sculpting postnatally and directly target the underlying ECM protein mutations. With recent advances in whole exome sequencing, in-vitro and in-vivo disease modeling, and the development of mutation-specific molecular therapeutic modalities, it is now feasible to directly correct disease-causing mutations underlying connective tissue disorders and ameliorate their pathogenic consequences. These technological advances may lead to potentially curative personalized medicine approaches for connective tissue disorders that have previously been considered incurable. In this review, we highlight innovative therapeutic modalities including gene replacement, exon skipping, DNA/mRNA editing, and pharmacological approaches that were used to preserve or restore tissue function in the context of connective tissue disorders. Inherent to a successful application of these approaches is the need to deepen the understanding of mechanisms that regulate ECM formation and homeostasis, and to decipher how individual mutations in ECM proteins compromise ECM and connective tissue development and function.

走向个性化医学方法:结缔组织疾病的创新治疗模式。
结缔组织疾病可由编码细胞外基质(ECM)蛋白的基因的致病性变异(突变)引起。这种疾病通常在发育或产后生长期间表现出来,并导致显著的发病率和死亡率。结缔组织疾病治疗方法的发展在一定程度上受到许多成熟结缔组织无法有效再生的阻碍。为了最有效,设计用于保存或恢复组织功能的治疗策略可能需要在出生后显著的内源性结缔组织重塑和器官雕刻阶段启动,并直接针对潜在的ECM蛋白突变。随着全外显子组测序、体外和体内疾病建模以及突变特异性分子治疗模式的发展,现在可以直接纠正结缔组织疾病的致病突变并改善其致病后果。这些技术进步可能会为以前被认为无法治愈的结缔组织疾病带来潜在的个性化治疗方法。在这篇综述中,我们强调了创新的治疗模式,包括基因置换、外显子跳过、DNA/mRNA编辑,以及在结缔组织疾病中用于保护或恢复组织功能的药理学方法。成功应用这些方法的本质是需要加深对调节ECM形成和稳态的机制的理解,并破译ECM蛋白的个体突变如何影响ECM和结缔组织的发育和功能。
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
Matrix Biology 生物-生化与分子生物学
CiteScore
11.40
自引率
4.30%
发文量
77
审稿时长
45 days
期刊介绍: Matrix Biology (established in 1980 as Collagen and Related Research) is a cutting-edge journal that is devoted to publishing the latest results in matrix biology research. We welcome articles that reside at the nexus of understanding the cellular and molecular pathophysiology of the extracellular matrix. Matrix Biology focusses on solving elusive questions, opening new avenues of thought and discovery, and challenging longstanding biological paradigms.
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