首页> 外文期刊>British journal of ophthalmology >Effect of the cytostatic agent idarubicin on fibroblasts of the human Tenon's capsule compared with mitomycin C.
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Effect of the cytostatic agent idarubicin on fibroblasts of the human Tenon's capsule compared with mitomycin C.

机译:与丝裂霉素C相比,细胞抑制剂伊达比星对人腱囊成纤维细胞的影响。

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BACKGROUND/AIMS: To investigate the in vitro effect of a short time exposure to the anthracycline idarubicin on proliferation, protein synthesis, and motility of human Tenon's capsule fibroblasts in comparison with the antitumour antibiotic mitomycin C. METHODS: After determination of effective concentrations of idarubicin, fibroblasts of the human Tenon's capsule were exposed to idarubicin or mitomycin C at concentrations ranging from 0.1 microg/ml to 1 microg/ml or from 2.5 microg/ml to 250 microg/ml, respectively, for 0.5, 2, or 5 minutes and cultured for 60 days. Cell death by apoptosis caused by idarubicin treatment was confirmed by Hoechst 33258 staining. Further proliferation was explored by cell counting and by (3)H-thymidine uptake. Protein synthesis was measured by (3)H-proline uptake and motility was assessed by agarose droplet motility assay. RESULTS: Idarubicin is able to exert toxicity and to induce apoptosis during a short time exposure of 0.5 minutes at concentrations of 0.3-1 microg/ml resulting in a significant reduction in cell number compared with the control after 60 days. For mitomycin C, higher concentrations and longer expositions were necessary. Even after treatment with 1 microg/ml idarubicin or 250 microg/ml mitomycin C a few cells were able to incorporate (3)H-thymidine. (3)H-proline uptake up to 10 days after exposure to 0.3 microg/ml idarubicin was found not to be decreased. Cell motility was reduced after treatment with 1 microg/ml idarubicin for 5 minutes or with 250 microg/ml mitomycin C for 2 or 5 minutes. For low mitomycin C concentrations, an increase in motility was found during the first 10 days. CONCLUSION: Idarubicin reduces proliferation of human Tenons's capsule fibroblasts after incubation for 0.5 minutes at concentrations as low as 0.3-1 microg/ml. In comparison, mitomycin C requires longer exposure times and higher doses for equal results. Therefore, idarubicin may be useful in the prevention of glaucoma filtering surgery failure.
机译:背景/目的:与抗肿瘤抗生素丝裂霉素C相比,研究短期暴露于蒽环类抗生素阿达比星对人腱囊成纤维细胞增殖,蛋白质合成和运动的体外作用。方法:确定有效浓度的达达比星后将人Tenon胶囊的成纤维细胞分别暴露于idarubicin或丝裂霉素C的浓度范围分别为0.1 microg / ml至1 microg / ml或2.5 microg / ml至250 microg / ml,分别为0.5、2或5分钟,培养60天。 Hoechst 33258染色证实了由依达比星处理引起的凋亡引起的细胞死亡。通过细胞计数和(3)H-胸苷摄取来探索进一步的增殖。通过(3)H-脯氨酸摄取来测量蛋白质合成,并且通过琼脂糖液滴运动性测定来评估运动性。结果:依达比星在浓度为0.3-1 microg / ml的0.5分钟的短时间内暴露时,能够产生毒性并诱导细胞凋亡,与60天后的对照组相比,细胞数量明显减少。对于丝裂霉素C,需要更高的浓度和更长的暴露时间。甚至在用1微克/毫升的idarubicin或250微克/毫升的丝裂霉素C处理后,一些细胞仍能够掺入(3)H-胸苷。 (3)发现在暴露于0.3 microg / ml idarubicin后长达10天的H-脯氨酸摄取没有减少。用1μg/ ml idarubicin处理5分钟或用250μg/ ml丝裂霉素C处理2或5分钟后,细胞运动性降低。对于低的丝裂霉素C浓度,在头10天发现运动性增加。结论:依达比星以低至0.3-1 microg / ml的浓度孵育0.5分钟后,能减少人腱细胞的成纤维细胞增殖。相比之下,丝裂霉素C需要更长的暴露时间和更高的剂量才能获得相同的结果。因此,伊达比星可能有助于预防青光眼滤过手术失败。

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