考古人骨和牙本质中抗体保存不良

Ross Kendall, Jessica Hendy, M. Collins, A. Millard, R. Gowland
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引用次数: 13

摘要

基于蛋白质组学的考古学方法的发展促使了对考古人骨和牙本质中非胶原蛋白(特别是免疫球蛋白G (IgG))存活情况的调查。十多年前,关于提取的、具有免疫反应性的考古IgG,以及通过1D和2D SDS-PAGE凝胶的Western blots检测IgG分子的可变产率的报道已经发表。如果IgG确实可以从考古骨骼材料中恢复,它将为探索疾病的历史提供非凡的机会——例如,应用功能性抗疟疾IgG来研究过去的疟疾模式。最近,该领域已经从免疫学方法转向通过质谱法使用鸟枪蛋白质组学。利用先前发表的技术,本研究试图提取和表征考古IgG蛋白。在只有一种提取方法中,免疫球蛋白衍生的肽被鉴定出来,这些肽显示出广泛的降解证据。除了一种方法外,所有方法都不能提取免疫球蛋白,同时观察到蛋白质降解的模式,这表明IgG可能不是检测疾病相关抗原的合适靶标。这项研究强调了利用新兴技术重新审视以前“成功”的生物分子方法的重要性。
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Poor preservation of antibodies in archaeological human bone and dentine
Abstract The growth of proteomics-based methods in archaeology prompted an investigation of the survival of non-collagenous proteins, specifically immunoglobulin G (IgG), in archaeological human bone and dentine. Over a decade ago reports were published on extracted, immunoreactive archaeological IgG, and the variable yields of IgG molecules detected by Western blots of 1D and 2D SDS-PAGE gels. If IgG can indeed be recovered from archaeological skeletal material, it offers remarkable opportunities for exploring the history of disease - for example in applying functional anti-malarial IgGs to study past patterns of malaria. More recently, the field has seen a move away from immunological approaches and towards the use of shotgun proteomics via mass spectrometry. Using previously published techniques, this study attempted to extract and characterize archaeological IgG proteins. In only one extraction method were immunoglobulin derived peptides identified, and these displayed extensive evidence of degradation. The failure to extract immunoglobulins by all but one method, along with observed patterns of protein degradation, suggests that IgG may be an unsuitable target for detecting disease-associated antigens. This research highlights the importance of revisiting previously ‘successful’ biomolecular methodologies using emerging technologies.
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