一种抗有丝分裂和抗血管生成药物 BPR0L075 可克服多药耐药性,并诱导紫杉醇耐药卵巢癌细胞发生有丝分裂灾难。
An antimitotic and antivascular agent BPR0L075 overcomes multidrug resistance and induces mitotic catastrophe in paclitaxel-resistant ovarian cancer cells.
机构信息
Department of Pharmaceutical Sciences, School of Pharmacy, Texas Tech University Health Sciences Center, Amarillo, Texas, United States of America.
出版信息
PLoS One. 2013 Jun 6;8(6):e65686. doi: 10.1371/journal.pone.0065686. Print 2013.
Paclitaxel plays a major role in the treatment of ovarian cancer; however, resistance to paclitaxel is frequently observed. Thus, new therapy that can overcome paclitaxel resistance will be of significant clinical importance. We evaluated antiproliferative effects of an antimitotic and antivascular agent BPR0L075 in paclitaxel-resistant ovarian cancer cells. BPR0L075 displays potent and broad-spectrum cytotoxicity at low nanomolar concentrations (IC50 = 2-7 nM) against both parental ovarian cancer cells (OVCAR-3, SKOV-3, and A2780-1A9) and paclitaxel-resistant sublines (OVCAR-3-TR, SKOV-3-TR, 1A9-PTX10), regardless of the expression levels of the multidrug resistance transporter P-gp and class III β-tubulin or mutation of β-tubulin. BPR0L075 blocks cell cycle at the G2/M phase in paclitaxel-resistant cells while equal concentration of paclitaxel treatment was ineffective. BPR0L075 induces cell death by a dual mechanism in parental and paclitaxel-resistant ovarian cancer cells. In the parental cells (OVCAR-3 and SKOV-3), BPR0L075 induced apoptosis, evidenced by poly(ADP-ribose) polymerase (PARP) cleavage and DNA ladder formation. BPR0L075 induced cell death in paclitaxel-resistant ovarian cancer cells (OVCAR-3-TR and SKOV-3-TR) is primarily due to mitotic catastrophe, evidenced by formation of giant, multinucleated cells and absence of PARP cleavage. Immunoblotting analysis shows that BPR0L075 treatment induced up-regulation of cyclin B1, BubR1, MPM-2, and survivin protein levels and Bcl-XL phosphorylation in parental cells; however, in resistant cells, the endogenous expressions of BubR1 and survivin were depleted, BPR0L075 treatment failed to induce MPM-2 expression and phosphorylation of Bcl-XL. BPR0L075 induced cell death in both parental and paclitaxel-resistant ovarian cancer cells proceed through caspase-3 independent mechanisms. In conclusion, BPR0L075 displays potent cytotoxic effects in ovarian cancer cells with a potential to overcome paclitaxel resistance by bypassing efflux transporters and inducing mitotic catastrophe. BPR0L075 represents a novel microtubule therapeutic to overcome multidrug resistance and trigger alternative cell death by mitotic catastrophe in ovarian cancer cells that are apoptosis-resistant.
紫杉醇在卵巢癌的治疗中起着重要作用;然而,紫杉醇耐药性经常出现。因此,能够克服紫杉醇耐药性的新疗法将具有重要的临床意义。我们评估了抗有丝分裂和抗血管生成剂 BPR0L075 在紫杉醇耐药卵巢癌细胞中的抗增殖作用。BPR0L075 以低纳摩尔浓度(IC50=2-7 nM)对亲本卵巢癌细胞(OVCAR-3、SKOV-3 和 A2780-1A9)和紫杉醇耐药亚系(OVCAR-3-TR、SKOV-3-TR、1A9-PTX10)显示出强大而广谱的细胞毒性,而与多药耐药转运蛋白 P-gp 和 III 类 β-微管蛋白的表达水平或 β-微管蛋白的突变无关。BPR0L075 使紫杉醇耐药细胞的细胞周期在 G2/M 期停滞,而相同浓度的紫杉醇处理则无效。BPR0L075 通过双重机制诱导亲本和紫杉醇耐药卵巢癌细胞死亡。在亲本细胞(OVCAR-3 和 SKOV-3)中,BPR0L075 诱导多聚(ADP-核糖)聚合酶(PARP)裂解和 DNA 梯状形成,从而诱导细胞凋亡。BPR0L075 在紫杉醇耐药卵巢癌细胞(OVCAR-3-TR 和 SKOV-3-TR)中诱导细胞死亡主要是由于有丝分裂灾难,这表现为形成巨大的多核细胞,并且没有 PARP 裂解。免疫印迹分析表明,BPR0L075 处理诱导亲本细胞中环蛋白 B1、BubR1、MPM-2 和 survivin 蛋白水平的上调和 Bcl-XL 磷酸化;然而,在耐药细胞中,BubR1 和 survivin 的内源性表达被耗尽,BPR0L075 处理未能诱导 MPM-2 表达和 Bcl-XL 的磷酸化。BPR0L075 诱导亲本和紫杉醇耐药卵巢癌细胞的细胞死亡均通过 caspase-3 非依赖性机制进行。总之,BPR0L075 在卵巢癌细胞中表现出强大的细胞毒性作用,有可能通过绕过外排转运蛋白和诱导有丝分裂灾难来克服紫杉醇耐药性。BPR0L075 代表一种新型微管治疗药物,可通过有丝分裂灾难克服多药耐药性,并在对凋亡有抗性的卵巢癌细胞中触发替代细胞死亡。
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