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从人体远流出道中分离和鉴定新型原代细胞。

Isolation and characterization of novel primary cells from the human distal outflow pathway.

机构信息

Department of Ophthalmology, Mayo Clinic, 200 First Street SW, Rochester, MN, 55905, USA.

出版信息

Sci Rep. 2021 Feb 17;11(1):4034. doi: 10.1038/s41598-021-83558-6.

Abstract

Ocular hypertension occurs due to increased resistance to aqueous humor removal through the conventional outflow pathway. Unlike the proximal region of the conventional outflow pathway, the distal region has not been well studied, mostly due to lack of model systems. Here we describe isolation and characterization of human primary vascular distal outflow pathway (VDOP) cells from the distal region of the conventional outflow pathway. Tissue from the distal region was isolated from human corneo-scleral rims, digested with collagenase type I (100 U/ml) and placed on gelatin coated plates to allow cellular growth in Dulbecco's Modified Eagle's Medium (low glucose) containing fetal bovine serum and antibiotic/antimycotic. VDOP cells showed consistent proliferation for up to 7 passages, retained endothelial-like nature of the parent tissues and showed a unique marker phenotype of LectinVEGFR2CD34NG2 that was distinct from neighboring trabecular meshwork (LectinVEGFR2CD34NG2) and Schlemm's canal (LectinVEGFR2CD34NG2) cells. Dexamethasone treated VDOP cells did not express myocilin and did not form cross-linked actin networks, in contrast to trabecular meshwork cells. These data show that VDOP cells are unique to the distal outflow region and can be used as a viable in vitro model system to understand the biology of the distal outflow pathway and intraocular pressure regulation.

摘要

眼内压升高是由于通过传统流出途径的房水清除阻力增加所致。与传统流出途径的近端区域不同,远端区域尚未得到很好的研究,主要是因为缺乏模型系统。在这里,我们描述了从传统流出途径的远端区域分离和鉴定人原发性血管远端流出途径(VDOP)细胞的方法。从人角巩膜缘分离远端区域的组织,用 I 型胶原酶(100 U/ml)消化,并放置在涂有明胶的平板上,使细胞在含胎牛血清和抗生素/抗真菌药物的 Dulbecco 修改的 Eagle 培养基(低糖)中生长。VDOP 细胞可稳定增殖多达 7 代,保留了亲本组织的内皮样性质,并表现出独特的标记表型 LectinVEGFR2CD34NG2,与邻近的小梁网(LectinVEGFR2CD34NG2)和施莱姆氏管(LectinVEGFR2CD34NG2)细胞明显不同。与小梁网细胞不同,用地塞米松处理的 VDOP 细胞不表达肌球蛋白,也不形成交联的肌动蛋白网络。这些数据表明,VDOP 细胞是远端流出区域所特有的,可作为一种可行的体外模型系统,用于了解远端流出途径和眼内压调节的生物学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e216/7890058/29a19a32fcd2/41598_2021_83558_Fig1_HTML.jpg

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