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增殖性糖尿病视网膜病变中纤维血管并发症的体外组织培养模型

An Ex Vivo Tissue Culture Model for Fibrovascular Complications in Proliferative Diabetic Retinopathy.

作者信息

Gucciardo Erika, Loukovaara Sirpa, Korhonen Ani, Lehti Kaisa

机构信息

Research Programs Unit, Genome-Scale Biology, Biomedicum Helsinki, University of Helsinki;

Unit of Vitreoretinal Surgery, Ophthalmology, University of Helsinki and Helsinki University Hospital.

出版信息

J Vis Exp. 2019 Jan 25(143). doi: 10.3791/59090.

Abstract

Diabetic retinopathy (DR) is the most common microvascular complication of diabetes and one of the leading causes of blindness in working-age adults. No current animal models of diabetes and oxygen-induced retinopathy develop the full-range progressive changes manifested in human proliferative diabetic retinopathy (PDR). Therefore, understanding of the disease pathogenesis and pathophysiology has relied largely on the use of histological sections and vitreous samples in approaches that only provide steady-state information on the involved pathogenic factors. Increasing evidence indicates that dynamic cell-cell and cell-extracellular matrix (ECM) interactions in the context of three-dimensional (3D) microenvironments are essential for the mechanistic and functional studies towards the development of new treatment strategies. Therefore, we hypothesized that the pathological fibrovascular tissue surgically excised from eyes with PDR could be utilized to reliably unravel the cellular and molecular mechanisms of this devastating disease and to test the potential for novel clinical interventions. Towards this end, we developed a novel method for 3D ex vivo culture of surgically-excised patient-derived fibrovascular tissue (FT), which will serve as a relevant model of human PDR pathophysiology. The FTs are dissected into explants and embedded in fibrin matrix for ex vivo culture and 3D characterization. Whole-mount immunofluorescence of the native FTs and end-point cultures allows thorough investigation of tissue composition and multicellular processes, highlighting the importance of 3D tissue-level characterization for uncovering relevant features of PDR pathophysiology. This model will allow the simultaneous assessment of molecular mechanisms, cellular/tissue processes and treatment responses in the complex context of dynamic biochemical and physical interactions within the PDR tissue architecture and microenvironment. Since this model recapitulates PDR pathophysiology, it will also be amenable for testing or developing new treatments.

摘要

糖尿病视网膜病变(DR)是糖尿病最常见的微血管并发症,也是劳动年龄成年人失明的主要原因之一。目前尚无糖尿病和氧诱导视网膜病变的动物模型能出现人类增殖性糖尿病视网膜病变(PDR)所表现出的全程渐进性变化。因此,对该疾病发病机制和病理生理学的理解在很大程度上依赖于组织学切片和玻璃体样本的使用,而这些方法仅能提供有关相关致病因素的稳态信息。越来越多的证据表明,在三维(3D)微环境背景下的动态细胞间和细胞与细胞外基质(ECM)相互作用对于开发新治疗策略的机制和功能研究至关重要。因此,我们假设从患有PDR的眼睛中手术切除的病理性纤维血管组织可用于可靠地揭示这种毁灭性疾病的细胞和分子机制,并测试新型临床干预措施的潜力。为此,我们开发了一种用于手术切除的患者来源纤维血管组织(FT)的3D体外培养新方法,该方法将作为人类PDR病理生理学的相关模型。将FTs切成外植体并嵌入纤维蛋白基质中进行体外培养和3D表征。对天然FTs和终点培养物进行全组织免疫荧光可全面研究组织组成和多细胞过程,突出了3D组织水平表征对于揭示PDR病理生理学相关特征的重要性。该模型将允许在PDR组织结构和微环境内动态生化和物理相互作用的复杂背景下同时评估分子机制、细胞/组织过程和治疗反应。由于该模型概括了PDR病理生理学,它也将适用于测试或开发新的治疗方法。

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