Sosman Jeffrey A, Puzanov Igor, Atkins Michael B
Vanderbilt-Ingram Cancer Center, Division of Hematology/Oncology, Vanderbilt University Medical Center, Nashville, TN 37232, USA.
Clin Cancer Res. 2007 Jan 15;13(2 Pt 2):764s-769s. doi: 10.1158/1078-0432.CCR-06-1975.
The treatment of advanced renal cell carcinoma (RCC) has undergone a major change with the development of potent angiogenesis inhibitors and targeted agents. Several multitargeted tyrosine kinase inhibitors, sorafenib and sunitinib, have already been approved for the treatment of advanced RCC. Temsirolimus (CCI-779), a mammalian target of rapamycin inhibitor, has shown a survival advantage over IFN in advanced, poor-prognosis RCC patients. Bevacizumab, an antibody targeting vascular endothelial growth factor (VEGF) A, has also shown promising clinical activity. Benefits attributable to these agents have been recognized by high objective response rates (sunitinib), significant increases in progression-free survival (sunitinib, sorafenib and bevacizumab), or improved overall survival (temsirolimus). These agents mediate much of their effect through inhibition of the hypoxia-inducible factor (HIF)-VEGF-VEGF receptor axis. Their inhibitory activity for the signaling of platelet-derived growth factor (PDGF) receptor beta or kinases like c-Raf may contribute to the antitumor effects of the multitargeted kinase inhibitors. Nevertheless, all four single agents rarely, if ever, induce complete responses and, at present, all patients develop resistance and, ultimately, progress during therapy. A critical need exists to develop strategies that may increase the degree of the antitumor effects with the hope of inducing more complete responses impeding the onset of or elimination of refractory disease. Combinations of these and other targeted agents may overcome the resistance that develops with single-agent therapy and could be incorporated either as part of initial therapy or later when disease resistance develops. Approaches aimed at combining these agents can be based on the genetics and biology of clear cell RCC. von Hippel-Lindau loss leads to an increase in cellular levels of HIF (HIF-1alpha or HIF-2alpha) leading to increased expression of a number of hypoxia-regulated genes critical to cancer progression. Combinations of targeted agents may block several of these mediators (VEGF, epidermal growth factor receptor, and PDGF), so-called horizontal blockade. Blockade could also take place at two levels of the pathways (vertical blockade), either at HIF and VEGF or at VEGF and VEGF receptor signaling. Many of the above strategies are ongoing and will require careful phase 1 determination of toxicity and even more rigorous phase 2 analysis before moving onto phase 3 trials.
随着强效血管生成抑制剂和靶向药物的发展,晚期肾细胞癌(RCC)的治疗发生了重大变化。几种多靶点酪氨酸激酶抑制剂,如索拉非尼和舒尼替尼,已被批准用于治疗晚期RCC。替西罗莫司(CCI-779)是一种雷帕霉素哺乳动物靶点抑制剂,在晚期、预后不良的RCC患者中显示出比干扰素更具生存优势。贝伐单抗是一种靶向血管内皮生长因子(VEGF)A的抗体,也显示出有前景的临床活性。这些药物带来的益处已通过高客观缓解率(舒尼替尼)、无进展生存期显著延长(舒尼替尼、索拉非尼和贝伐单抗)或总生存期改善(替西罗莫司)得到认可。这些药物大多通过抑制缺氧诱导因子(HIF)-VEGF-VEGF受体轴发挥作用。它们对血小板衍生生长因子(PDGF)受体β或c-Raf等激酶信号传导的抑制活性可能有助于多靶点激酶抑制剂的抗肿瘤作用。然而,这四种单一药物很少能诱导完全缓解,目前,所有患者都会产生耐药性,并最终在治疗过程中病情进展。迫切需要制定策略来增强抗肿瘤效果,以期诱导更完全的缓解,阻止难治性疾病的发生或消除。这些靶向药物与其他药物联合使用可能会克服单药治疗产生的耐药性,可作为初始治疗的一部分,或在疾病出现耐药性后使用。旨在联合使用这些药物的方法可以基于透明细胞RCC的遗传学和生物学特性。冯·希佩尔-林道基因缺失会导致细胞内HIF(HIF-1α或HIF-2α)水平升高,从而导致许多对癌症进展至关重要的缺氧调节基因表达增加。靶向药物联合使用可能会阻断其中几种介质(VEGF、表皮生长因子受体和PDGF),即所谓的横向阻断。阻断也可以在通路的两个水平上进行(纵向阻断),即在HIF和VEGF之间或在VEGF和VEGF受体信号传导之间。上述许多策略仍在进行中,在进入3期试验之前,需要仔细进行1期毒性测定以及更严格的2期分析。
