首页> 外文期刊>European journal of gynaecological oncology >Octreotide is the favorable alternative for cisplatin resistance reversal of ovarian cancer in vitro and in nude mice in vivo
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Octreotide is the favorable alternative for cisplatin resistance reversal of ovarian cancer in vitro and in nude mice in vivo

机译:奥曲肽是体外和体内裸鼠卵巢癌顺铂耐药性逆转的有利替代药物

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摘要

This study aimed to observe the effects of octreotide (OCT) on cisplatin resistance reversal of cancer cells in vitro and in nude mice in vivo. MTT method and flow cytometry were used to investigate the effect of cisplatin, OCT or the combination of these two compounds on the proliferation and apoptosis of SKOV3-DDP cells. The size and weight of xenograft tumors from the nude mice model were measured. Real-time PCR was used to detect the mRNA expression of SSTR2, MDR1, MRP2, GST-π and EGFR in SKOV3/DDP cells following the different treatment. At the concentration of 2.5-20 g/ml, OCT significantly reduced IC50 (p < 0.05) and promoted apoptosis (p < 0.05) of SKOV3-DDP cells' response to cisplatin. Unchanged expression was found in SSTR2 on the SKOV3/DDP cell in vitro after OCT treatment, but increased expression in vivo (p < 0.05). OCT increased GST-π expression (p < 0.05) and reduced MRP2 and EGFR expression (p < 0.05) in a dose-dependent manner. The similar results were obtained in mice in vivo experiment, except the reduced expression of GST-π. It is suggested that OCT could inhibit ovarian cancer proliferation and promote apoptosis, via the cell surface SSTR2, and reverse cisplatin resistance through inhibition of MRP2, EGFR, and even GST-π expressions.
机译:这项研究旨在观察奥曲肽(OCT)对体外和体内裸鼠癌细胞对顺铂耐药性逆转的影响。采用MTT法和流式细胞术研究了顺铂,OCT或这两种化合物的组合对SKOV3-DDP细胞增殖和凋亡的影响。测量来自裸鼠模型的异种移植肿瘤的大小和重量。实时荧光定量PCR检测不同处理后SKOV3 / DDP细胞中SSTR2,MDR1,MRP2,GST-π和EGFR的mRNA表达。在2.5-20 g / ml的浓度下,OCT显着降低了SKOV3-DDP细胞对顺铂反应的IC50(p <0.05)并促进了细胞凋亡(p <0.05)。 OCT处理后,在体外SKOV3 / DDP细胞的SSTR2中未发现表达改变,但在体内表达增加(p <0.05)。 OCT以剂量依赖性方式增加GST-π表达(p <0.05)并降低MRP2和EGFR表达(p <0.05)。在小鼠体内实验中获得了相似的结果,除了GST-π的表达降低。提示OCT可通过细胞表面SSTR2抑制卵巢癌的增殖并促进细胞凋亡,并通过抑制MRP2,EGFR甚至GST-π的表达来逆转顺铂耐药性。

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