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Determination of extracellular matrix collagen fibril architectures and pathological remodeling by polarization dependent second harmonic microscopy

机译:偏振相关二次谐波显微镜确定细胞外基质胶原原纤维的结构和病理重塑

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摘要

Polarization dependence second harmonic generation (P-SHG) microscopy is gaining increase popularity for in situ quantification of fibrillar protein architectures. In this report, we combine P-SHG microscopy, new linear least square (LLS) fitting and modeling to determine and convert the complex second-order non-linear optical anisotropy parameter ρ of several collagen rich tissues into a simple geometric organization of collagen fibrils. Modeling integrates a priori knowledge of polyhelical organization of collagen molecule polymers forming fibrils and bundles of fibrils as well as Poisson photonic shot noise of the detection system. The results, which accurately predict the known sub-microscopic hierarchical organization of collagen fibrils in several tissues, suggest that they can be subdivided into three classes according to their microscopic and macroscopic hierarchical organization of collagen fibrils. They also show, for the first time to our knowledge, intrahepatic spatial discrimination between genuine fibrotic and non-fibrotic vessels. CCl4-treated livers are characterized by an increase in the percentage of fibrotic vessels and their remodeling involves peri-portal compaction and alignment of collagen fibrils that should contribute to portal hypertension. This integrated P-SHG image analysis method is a powerful tool that should open new avenue for the determination of pathophysiological and chemo-mechanical cues impacting collagen fibrils organization.
机译:极化相关的二次谐波产生(P-SHG)显微镜在原纤维蛋白结构的定量分析中越来越受欢迎。在本报告中,我们结合了P-SHG显微镜,新的线性最小二乘(LLS)拟合和建模,以确定并将一些富含胶原的组织的复杂的二阶非线性光学各向异性参数ρ转换为胶原纤维的简单几何结构。建模集成了形成分子纤维和纤维束以及检测系统的泊松光子散粒噪声的胶原分子聚合物的多螺旋组织的先验知识。结果准确地预测了几种组织中已知的胶原纤维的亚微观层次结构,结果表明,根据胶原纤维的微观和宏观层次结构,它们可以分为三类。据我们所知,它们还首次显示了真正的纤维化和非纤维化血管之间的肝内空间区别。经CCl4处理的肝脏的特点是纤维化血管百分比增加,其重塑涉及门静脉周围的压实和胶原纤维的排列,这会导致门脉高压。这种整合的P-SHG图像分析方法是一种功能强大的工具,应该为确定影响胶原蛋白原纤维组织的病理生理学和化学机械学线索开辟新途径。

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