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转铁蛋白在后发性白内障中的作用及作为晶状体上皮细胞的存活因子。

Transferrin in after-cataract and as a survival factor for lens epithelium.

作者信息

Davidson M G, Harned J, Grimes A M, Duncan G, Wormstone I M, McGahan M C

机构信息

Department of Companion Animal and Special Species, College of Veterinary Medicine, North Carolina State University, Raleigh, NC 27606, USA.

出版信息

Exp Eye Res. 1998 Feb;66(2):207-15. doi: 10.1006/exer.1997.0413.

Abstract

The Fe-transport protein, transferrin (Tf), is synthesized and secreted by whole lenses and cultured lens epithelial cells. Because of Tf's central role in cell growth and proliferation, its participation in lens cell proliferation following cataract extraction was explored using a rabbit model of after-cataract. Varying amounts of the central anterior lens capsule were removed (0, 35, or 80%) following extraction of the lens. The Tf content of and secretion by after-cataract lens capsular sacs containing regenerated lens tissue was determined ex vivo at 0, 3, 5, 7 and 9 weeks post-surgery. In all cases Tf content of and secretion by the lens sacs was higher than that of their contralateral controls (whole lenses). Tf secretion was up to 5-fold higher and metabolic labeling studies indicated secretion of newly synthesized Tf. The sacs contained up to 10 times the concentration of Tf as the control lenses. Human lens after-cataract capsular bags also secreted Tf. The function of Tf as a survival factor was tested on cultured lens epithelial cells. Cells cultured in serum-free medium had a survival rate of only 20-34% if the medium was changed each day. If the medium was never changed during this period, the survival rate was 43-52%, suggesting secretion of essential growth factors by these cells. Addition of 200 microg ml-1 Tf to the medium during each daily change increased survival to levels attained when the medium was not changed. Addition of Tf antibodies to the culture medium during each daily change decreased cell survival to 14%. Apparently Tf acts as a survival factor for lens epithelia and its synthesis is up-regulated in after-cataract lens sacs. These factors suggest that Tf may play an important role in the pathogenesis of lens epithelial cell proliferation and after-cataract formation following cataract surgery.

摘要

铁转运蛋白转铁蛋白(Tf)由完整晶状体和培养的晶状体上皮细胞合成并分泌。由于Tf在细胞生长和增殖中起核心作用,因此使用后发性白内障兔模型探讨了其在白内障摘除术后晶状体细胞增殖中的作用。晶状体摘除后,去除不同量的中央前囊膜(0%、35%或80%)。在术后0、3、5、7和9周,对含有再生晶状体组织的后发性白内障晶状体囊袋的Tf含量和分泌情况进行离体测定。在所有情况下,晶状体囊袋的Tf含量和分泌均高于其对侧对照(完整晶状体)。Tf分泌量高达对照的5倍,代谢标记研究表明有新合成的Tf分泌。囊袋中的Tf浓度高达对照晶状体的10倍。人后发性白内障囊袋也分泌Tf。在培养的晶状体上皮细胞上测试了Tf作为存活因子的功能。在无血清培养基中培养的细胞,如果每天更换培养基,存活率仅为20% - 34%。如果在此期间不更换培养基,存活率为43% - 52%,这表明这些细胞分泌了必需的生长因子。在每天更换培养基时添加200μg/ml的Tf可使存活率提高到不更换培养基时的水平。在每天更换培养基时向培养基中添加Tf抗体可使细胞存活率降至14%。显然,Tf作为晶状体上皮细胞的存活因子,其合成在白内障术后的后发性白内障晶状体囊中上调。这些因素表明,Tf可能在白内障手术后晶状体上皮细胞增殖和后发性白内障形成的发病机制中起重要作用。

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