Pilot screening of potential matrikines resulting from collagen breakages through ionizing radiation.

IF 1.5 4区 环境科学与生态学 Q3 BIOLOGY Radiation and Environmental Biophysics Pub Date : 2024-08-01 Epub Date: 2024-08-08 DOI:10.1007/s00411-024-01086-z
Juliette Montanari, Lucas Schwob, Aurélie Marie-Brasset, Claire Vinatier, Charlotte Lepleux, Rodolphe Antoine, Jérôme Guicheux, Jean-Christophe Poully, François Chevalier
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Abstract

Little is known regarding radiation-induced matrikines and the possible degradation of extracellular matrix following therapeutic irradiation. The goal of this study was to determine if irradiation can cut collagen proteins at specific sites, inducing potentially biologically active peptides against cartilage cells. Chondrocytes cultured as 3D models were evaluated for extracellular matrix production. Bystander molecules were analyzed in vitro in the conditioned medium of X-irradiated chondrocytes. Preferential breakage sites were analyzed in collagen polypeptide by mass spectrometry and resulting peptides were tested against chondrocytes. 3D models of chondrocytes displayed a light extracellular matrix able to maintain the structure. Irradiated and bystander chondrocytes showed a surprising radiation sensitivity at low doses, characteristic of the presence of bystander factors, particularly following 0.1 Gy. The glycine-proline peptidic bond was observed as a preferential cleavage site and a possible weakness of the collagen polypeptide after irradiation. From the 46 collagen peptides analyzed against chondrocytes culture, 20 peptides induced a reduction of viability and 5 peptides induced an increase of viability at the highest concentration between 0.1 and 1 µg/ml. We conclude that irradiation promoted a site-specific degradation of collagen. The potentially resulting peptides induce negative or positive regulations of chondrocyte growth. Taken together, these results suggest that ionizing radiation causes a degradation of cartilage proteins, leading to a functional unbalance of cartilage homeostasis after exposure, contributing to cartilage dysfunction.

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通过电离辐射对胶原蛋白断裂产生的潜在母因子进行试验性筛选。
人们对辐射诱导的软骨蛋白以及治疗性照射后细胞外基质可能发生的降解知之甚少。本研究的目的是确定辐照是否能在特定部位切割胶原蛋白,从而诱导对软骨细胞具有潜在生物活性的肽。对培养成三维模型的软骨细胞进行了细胞外基质生成评估。体外分析了 X 射线照射软骨细胞条件培养基中的旁观者分子。通过质谱分析了胶原多肽的优先断裂点,并针对软骨细胞对由此产生的肽进行了测试。软骨细胞的三维模型显示,轻质细胞外基质能够维持软骨细胞的结构。辐照软骨细胞和旁观者软骨细胞在低剂量时显示出惊人的辐射敏感性,这是旁观者因子存在的特征,尤其是在 0.1 Gy 之后。据观察,甘氨酸-脯氨酸肽键是辐照后胶原多肽的优先裂解位点和可能的薄弱环节。分析了 46 种胶原蛋白肽对软骨细胞培养的影响,在 0.1 至 1 µg/ml 的最高浓度范围内,20 种肽会导致存活率下降,5 种肽会导致存活率上升。我们的结论是,辐照促进了胶原蛋白的特定部位降解。由此可能产生的肽会诱导软骨细胞生长的负向或正向调节。综上所述,这些结果表明,电离辐射会导致软骨蛋白质降解,从而导致照射后软骨平衡功能失衡,造成软骨功能障碍。
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来源期刊
CiteScore
4.00
自引率
5.90%
发文量
53
审稿时长
>36 weeks
期刊介绍: This journal is devoted to fundamental and applied issues in radiation research and biophysics. The topics may include: Biophysics of ionizing radiation: radiation physics and chemistry, radiation dosimetry, radiobiology, radioecology, biophysical foundations of medical applications of radiation, and radiation protection. Biological effects of radiation: experimental or theoretical work on molecular or cellular effects; relevance of biological effects for risk assessment; biological effects of medical applications of radiation; relevance of radiation for biosphere and in space; modelling of ecosystems; modelling of transport processes of substances in biotic systems. Risk assessment: epidemiological studies of cancer and non-cancer effects; quantification of risk including exposures to radiation and confounding factors Contributions to these topics may include theoretical-mathematical and experimental material, as well as description of new techniques relevant for the study of these issues. They can range from complex radiobiological phenomena to issues in health physics and environmental protection.
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