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Quantitative nanohistological investigation of scleroderma: an atomic force microscopy-based approach to disease characterization

机译:硬皮病的定量纳米组织学研究:基于原子力显微镜的疾病表征方法

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摘要

Scleroderma (or systemic sclerosis, SSc) is a disease caused by excess crosslinking of collagen. The skin stiffens and becomes painful, while internally, organ function can be compromised by the less elastic collagen. Diagnosis of SSc is often only possible in advanced cases by which treatment time is limited. A more detailed analysis of SSc may provide better future treatment options and information of disease progression. Recently, the histological stain picrosirius red showing collagen register has been combined with atomic force microscopy (AFM) to study SSc. Skin from healthy individuals and SSc patients was biopsied, stained and studied using AFM. By investigating the crosslinking of collagen at a smaller hierarchical stage, the effects of SSc were more pronounced. Changes in morphology and Young’s elastic modulus were observed and quantified; giving rise to a novel technique, we have termed “quantitative nanohistology”. An increase in nanoscale stiffness in the collagen for SSc compared with healthy individuals was seen by a significant increase in the Young’s modulus profile for the collagen. These markers of stiffer collagen in SSc are similar to the symptoms experienced by patients, giving additional hope that in the future, nanohistology using AFM can be readily applied as a clinical tool, providing detailed information of the state of collagen.
机译:硬皮病(或全身性硬化症,SSc)是由胶原蛋白过度交联引起的疾病。皮肤变硬并变得疼痛,而在内部,弹性较低的胶原蛋白会损害器官功能。 SSc的诊断通常仅在治疗时间受到限制的晚期病例中才可能。对SSc进行更详细的分析可能会提供更好的未来治疗选择和疾病进展信息。最近,显示胶原注册的组织学染色picrosirius红已与原子力显微镜(AFM)结合用于研究SSc。使用AFM对健康个体和SSc患者的皮肤进行活检,染色和研究。通过研究胶原蛋白在较小层次上的交联,SSc的作用更加明显。观察并量化了形态和杨氏弹性模量的变化;为了产生一种新技术,我们将其称为“定量纳米组织学”。与健康个体相比,SSc胶原蛋白的纳米级刚度有所增加,这是因为胶原蛋白的杨氏模量显着增加。 SSc中胶原蛋白变硬的这些标记类似于患者所经历的症状,这给人们带来了更多希望,即将来使用AFM的纳米组织学可以很容易地用作临床工具,从而提供胶原蛋白状态的详细信息。

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