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铜诱导 IgG 聚集:形成循环蛋白聚集体的潜在驱动力。

Copper-induced aggregation of IgG: a potential driving force for the formation of circulating protein aggregates.

机构信息

Universidad de Buenos Aires, Facultad de Farmacia y Bioquímica, Departamento de Ciencias Químicas, Cátedra de Química General e Inorgánica, Buenos Aires 1113AAD, Argentina.

Consejo Nacional de Investigaciones Científicas y Técnicas, Instituto de Bioquímica y Medicina Molecular Prof. Alberto Boveris (IBIMOL, UBA-CONICET), Buenos Aires 1113AAD, Argentina.

出版信息

Metallomics. 2023 Feb 16;15(2). doi: 10.1093/mtomcs/mfad005.

Abstract

Copper is a highly reactive element involved in a myriad of biological reactions. Thus, while essential for mammalian cells, its concentrations must be kept in check in order to avoid toxicity. This metal participates in redox reactions and may exacerbate oxidative stress in aerobic organisms. Nonetheless, the actual driving force of copper-induced cell death is yet unknown. Likely, free copper ions may target different biomolecules that are crucial for the proper functioning of an organism. In this work, we show that free copper induces protein aggregation in serum. The wide set of proteins present in these biological samples are not equally prone to copper-induced aggregation and some, such as albumin, are highly resistant, whereas γ-globulins are highly sensitive. The identity of the proteins in the aggregates becomes fairly homogeneous as metal concentrations go as low as 20 μM. The identification of the proteins by mass spectrometry indicates a preponderance of IgG and a minor presence of other different proteins. Therefore, free copper in blood may contribute to the formation of circulating protein aggregates with a core of IgG. This may impact health not only due to the activity of aggregated IgG but also due to the many proteins co-aggregated. Understanding whether the γ-globulin core and the heterogeneous subgroup of proteins elicit differential responses in the organisms requires further research.

摘要

铜是一种高度活跃的元素,参与了无数的生物反应。因此,尽管它对哺乳动物细胞是必需的,但为了避免毒性,其浓度必须加以控制。这种金属参与氧化还原反应,并可能加剧需氧生物的氧化应激。尽管如此,铜诱导细胞死亡的实际驱动力仍不清楚。可能是游离的铜离子可能针对对生物体正常功能至关重要的不同生物分子。在这项工作中,我们表明游离铜会诱导血清中的蛋白质聚集。这些生物样本中存在的广泛蛋白质群并不是同等容易受到铜诱导聚集的,有些蛋白质,如白蛋白,具有高度抗性,而γ-球蛋白则非常敏感。随着金属浓度低至 20 μM,聚集物中的蛋白质的身份变得相当均匀。通过质谱鉴定出的蛋白质表明 IgG 占优势,并且存在少量其他不同的蛋白质。因此,血液中的游离铜可能有助于形成含有 IgG 核心的循环蛋白聚集物。这不仅会由于聚集 IgG 的活性,而且还会由于共同聚集的许多蛋白质而对健康产生影响。需要进一步研究以了解 γ-球蛋白核心和异质亚组的蛋白质是否会在生物体中引起不同的反应。

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