Regorafenib synergizes with TAS102 against multiple gastrointestinal cancers and overcomes cancer stemness, trifluridine-induced angiogenesis, ERK1/2 and STAT3 signaling regardless of KRAS or BRAF mutational status.

Q2 Medicine
Jun Zhang, Lanlan Zhou, Shuai Zhao, Wafik S El-Deiry
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引用次数: 0

Abstract

Single-agent TAS102 (trifluridine/tipiracil) and regorafenib are FDA-approved treatments for metastatic colorectal cancer (mCRC). We previously reported that regorafenib combined with a fluoropyrimidine can delay disease progression in clinical case reports of multidrug-resistant mCRC patients. We hypothesized that the combination of TAS102 and regorafenib may be active in CRC and other gastrointestinal (GI) cancers and may in the future provide a treatment option for patients with advanced GI cancer. We investigated the therapeutic effect of TAS102 in combination with regorafenib in preclinical studies employing cell culture, colonosphere assays that enrich for cancer stem cells, and in vivo. TAS102 in combination with regorafenib has synergistic activity against multiple GI cancers in vitro including colorectal and gastric cancer, but not liver cancer cells. TAS102 inhibits colonosphere formation and this effect is potentiated by regorafenib. In vivo anti-tumor effects of TAS102 plus regorafenib appear to be due to anti-proliferative effects, necrosis and angiogenesis inhibition. Growth inhibition by TAS102 plus regorafenib occurs in xenografted tumors regardless of p53, KRAS or BRAF mutations, although more potent tumor suppression was observed with wild-type p53. Regorafenib significantly inhibits TAS102-induced angiogenesis and microvessel density in xenografted tumors, as well inhibits TAS102-induced ERK1/2 activation regardless of RAS or BRAF status in vivo. TAS102 plus regorafenib is a synergistic drug combination in preclinical models of GI cancer, with regorafenib suppressing TAS102-induced increase in microvessel density and p-ERK as contributing mechanisms. The TAS102 plus regorafenib drug combination may be further tested in gastric and other GI cancers.

瑞戈非尼与 TAS102 对多种胃肠道癌症具有协同作用,并且无论 KRAS 或 BRAF 突变状态如何,都能克服癌症干性、三氟利定诱导的血管生成、ERK1/2 和 STAT3 信号转导。
单药 TAS102(三氟脲啶/替吡拉西)和瑞戈非尼是美国 FDA 批准的治疗转移性结直肠癌(mCRC)的药物。我们曾报道过,在耐多药 mCRC 患者的临床病例报告中,瑞戈非尼与氟嘧啶联用可延缓疾病进展。我们推测,TAS102 和瑞戈非尼联合用药可能对 CRC 和其他胃肠道(GI)癌症有积极作用,将来可能为晚期胃肠道癌症患者提供一种治疗选择。在临床前研究中,我们采用细胞培养、富集癌症干细胞的结肠球试验和体内试验等方法,研究了TAS102与瑞戈非尼联用的治疗效果。TAS102 与瑞戈非尼联用在体外对包括结直肠癌和胃癌在内的多种消化道癌症具有协同活性,但对肝癌细胞没有协同活性。TAS102 可抑制结肠球囊的形成,而瑞戈非尼可增强这种效应。TAS102 加上瑞戈非尼的体内抗肿瘤作用似乎是由于抗增殖作用、坏死和血管生成抑制。无论 p53、KRAS 或 BRAF 是否发生突变,TAS102 加瑞戈非尼都能抑制异种移植肿瘤的生长,但野生型 p53 对肿瘤的抑制作用更强。瑞戈非尼能显著抑制TAS102诱导的血管生成和异种移植肿瘤中的微血管密度,还能抑制TAS102诱导的ERK1/2活化,与体内的RAS或BRAF状态无关。在消化道癌症的临床前模型中,TAS102 加瑞戈非尼是一种协同作用的药物组合,瑞戈非尼抑制 TAS102- 诱导的微血管密度和 p-ERK 的增加是其作用机制。TAS102 加瑞戈非尼的药物组合可能会在胃癌和其他消化道癌症中进行进一步测试。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Oncotarget
Oncotarget Oncogenes-CELL BIOLOGY
CiteScore
6.60
自引率
0.00%
发文量
129
审稿时长
1.5 months
期刊介绍: Information not localized
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