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鉴定人卵巢癌细胞中对顺铂耐药具有特异性的可重复低质量SELDI蛋白质谱。

Identification of reproducible low mass SELDI protein profiles specific to cisplatin resistance in human ovarian cancer cells.

作者信息

Britten Richard A, Hardy Carrie, Vlahou Antonia, Gregory Betsy, Giri P Shankar, Drake Richard

机构信息

Department of Radiation Oncology, 600 Gresham Drive, Norfolk, VA 23507, USA.

出版信息

Oncol Rep. 2005 Nov;14(5):1323-30.

Abstract

Platinum compounds are the most effective drugs in the fight against ovarian cancer. Unfortunately, many ovarian tumors are not eradicated by chemotherapy due to the emergence of drug-resistant clones during therapy, and hence 5-year survival rate of women afflicted with this disease is just 18%. In the continued absence of an effective early detection test for ovarian cancer, there is a considerable need to develop treatment strategies that can either circumvent (e.g. gene therapy) or prevent the development of platinum resistance. A prerequisite for the development of such treatments is a detailed knowledge of factors that confer tumor cell resistance to platinum compounds. We have used surface-enhanced laser desorption/ionization time of flight mass spectrometry (SELDI-TOF-MS or SELDI) to identify low mass proteins that are uniquely expressed in ovarian tumor cells that are platinum-resistant. Only two polypeptide peaks (m/z 5041 and 7324) were consistently altered following the induction of cisplatin resistance in the OAW42 and 2780 cell lines. These peaks appear to be specific to cisplatin resistance as they are not altered in the same manner in a melphalan-resistant variant of OAW42. The exact identity of the polypeptide peaks is unknown, but appears to be unrelated to changes in several proteins that have been historically associated with cisplatin resistance. These data suggest that SELDI-based proteomic profiling may be useful in monitoring the emergence of cisplatin-resistant tumor cell clones.

摘要

铂类化合物是对抗卵巢癌最有效的药物。不幸的是,由于治疗期间耐药克隆的出现,许多卵巢肿瘤无法通过化疗根除,因此患这种疾病的女性的5年生存率仅为18%。在仍然缺乏有效的卵巢癌早期检测测试的情况下,迫切需要开发能够规避(如基因治疗)或预防铂耐药性发展的治疗策略。开发此类治疗方法的一个先决条件是详细了解赋予肿瘤细胞对铂类化合物耐药性的因素。我们使用表面增强激光解吸/电离飞行时间质谱(SELDI-TOF-MS或SELDI)来鉴定在铂耐药的卵巢肿瘤细胞中独特表达的低质量蛋白质。在OAW42和2780细胞系中诱导顺铂耐药后,只有两个多肽峰(m/z 5041和7324)持续发生变化。这些峰似乎是顺铂耐药所特有的,因为它们在OAW42的美法仑耐药变体中没有以相同的方式改变。多肽峰的确切身份尚不清楚,但似乎与一些历史上与顺铂耐药相关的蛋白质的变化无关。这些数据表明,基于SELDI的蛋白质组学分析可能有助于监测顺铂耐药肿瘤细胞克隆的出现。

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