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Analysis of old proteins unmasks dynamic gradient of cartilage turnover in human limbs

机译:对旧蛋白质的分析揭示了人体四肢软骨翻转的动态梯度

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摘要

Unlike highly regenerative animals, such as axolotls, humans are believed to be unable to counteract cumulative damage, such as repetitive joint use and injury that lead to the breakdown of cartilage and the development of osteoarthritis. Turnover of insoluble collagen has been suggested to be very limited in human adult cartilage. The goal of this study was to explore protein turnover in articular cartilage from human lower limb joints. Analyzing molecular clocks in the form of nonenzymatically deamidated proteins, we unmasked a position-dependent gradient (distal high, proximal low) of protein turnover, indicative of a gradient of tissue anabolism reflecting innate tissue repair capacity in human lower limb cartilages that is associated with expression of limb-regenerative microRNAs. This association shows a potential link to a capacity, albeit limited, for regeneration that might be exploited to enhance joint repair and establish a basis for human limb regeneration.
机译:与诸如re等高度再生的动物不同,人类被认为无法抵抗累积性损害,例如反复使用关节和导致软骨破裂和骨关节炎发展的伤害。已提出在成人软骨中不溶性胶原蛋白的周转非常有限。这项研究的目的是探讨人类下肢关节软骨蛋白的更新。分析非酶脱酰胺蛋白形式的分子钟,我们揭示了蛋白质更新的位置依赖性梯度(远侧高,近侧低),表明组织合成代谢的梯度反映了人类下肢软骨与生俱来的组织修复能力肢体再生microRNA的表达。这种联系显示了与再生能力的潜在联系,尽管能力有限,但可以用来增强关节修复能力并为人类肢体再生奠定基础。

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