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调控纤维化中的淋巴管:理解生物学以改善建模。

Regulating Lymphatic Vasculature in Fibrosis: Understanding the Biology to Improve the Modeling.

机构信息

Department of Biomedical Engineering, Worcester Polytechnic Institute, 100 Institute Rd., Worcester, MA, 01609, USA.

出版信息

Adv Biol (Weinh). 2023 May;7(5):e2200158. doi: 10.1002/adbi.202200158. Epub 2023 Feb 15.

Abstract

Fibrosis occurs in many chronic diseases with lymphatic vascular insufficiency (e.g., kidney disease, tumors, and lymphedema). New lymphatic capillary growth can be triggered by fibrosis-related tissue stiffening and soluble factors, but questions remain for how related biomechanical, biophysical, and biochemical cues affect lymphatic vascular growth and function. The current preclinical standard for studying lymphatics is animal modeling, but in vitro and in vivo outcomes often do not align. In vitro models can also be limited in their ability to separate vascular growth and function as individual outcomes, and fibrosis is not traditionally included in model design. Tissue engineering provides an opportunity to address in vitro limitations and mimic microenvironmental features that impact lymphatic vasculature. This review discusses fibrosis-related lymphatic vascular growth and function in disease and the current state of in vitro lymphatic vascular models while highlighting relevant knowledge gaps. Additional insights into the future of in vitro lymphatic vascular models demonstrate how prioritizing fibrosis alongside lymphatics will help capture the complexity and dynamics of lymphatics in disease. Overall, this review aims to emphasize that an advanced understanding of lymphatics within a fibrotic disease-enabled through more accurate preclinical modeling-will significantly impact therapeutic development toward restoring lymphatic vessel growth and function in patients.

摘要

纤维化发生在许多伴有淋巴血管功能不全的慢性疾病中(例如,肾脏疾病、肿瘤和淋巴水肿)。纤维化相关的组织僵硬和可溶性因子可触发新的淋巴管毛细血管生长,但对于相关生物力学、生物物理学和生物化学线索如何影响淋巴管生长和功能,仍存在一些问题。目前研究淋巴管的临床前标准是动物模型,但体外和体内的结果往往不一致。体外模型也可能在将血管生长和功能作为单独的结果进行分离的能力上存在局限性,而且纤维化通常不包含在模型设计中。组织工程提供了一个机会,可以解决体外的局限性,并模拟影响淋巴管的微环境特征。这篇综述讨论了疾病中与纤维化相关的淋巴血管生长和功能,以及当前的体外淋巴血管模型的状态,同时突出了相关的知识空白。对体外淋巴血管模型未来的进一步研究表明,如何将纤维化与淋巴管一起作为优先事项,将有助于捕捉疾病中淋巴管的复杂性和动态性。总的来说,这篇综述旨在强调,通过更准确的临床前建模来深入了解纤维化疾病中的淋巴管,将极大地影响治疗性药物的开发,以恢复患者的淋巴管生长和功能。

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