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Sequential treatment in disseminated well- and intermediate-differentiated pancreatic neuroendocrine tumors: Common sense or low rationale?

机译:继发性高分化和中分化胰腺神经内分泌肿瘤的序贯治疗:常识还是基本原理?

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摘要

Fortunately, the landscape of the systemic treatment for grade 1 and 2 pancreatic neuroendocrine tumors has changed in the last decade with at least four different alternatives approved in the field. Chemotherapy, somatostatin analogues, sunitinib and everolimus remind valid options according to the most referenced international guidelines. However, and although this is something done in the routine practice, there is a lack of evidence for the use of any of these strategies after failure to the others. Moreover, further sequential alternatives in third or fourth line have never been tested prospectively. The need for a better understanding of the rationale to sequence different systemic options is even greater in non-pancreatic neuroendocrine tumors since available therapies are scarce. Sequential strategies in other solid tumors have led to a clear improvement in overall survival. This is also believed to occur in neuroendocrine tumors but no clear data on it has been delivered yet. We postulate that the different mode of action of the systemic options available for the treatment of neuroendocrine tumors may avoid the complete resistance of one option after the other and that sequential use of these agents will be translated into a longer overall survival of patients. Prospective and randomized trials that seek for the activity of drugs after failure to another systemic alternatives are highly needed in this field of neuroendocrine tumors.
机译:幸运的是,在过去的十年中,针对1级和2级胰腺神经内分泌肿瘤的全身性治疗方法发生了变化,该领域已批准了至少四种不同的替代方法。化疗,生长抑素类似物,舒尼替尼和依维莫司提示根据国际参考指南最多的有效选择。但是,尽管这是常规操作中完成的工作,但是在其他策略失败之后,仍缺乏证据证明可以使用这些策略。此外,第三行或第四行中的其他顺序替代方案从未经过过预期的测试。由于缺乏可用的治疗方法,因此在非胰腺神经内分泌肿瘤中,更好地了解对不同全身选择进行排序的原理的需求就更大。其他实体瘤中的顺序治疗策略已导致总体生存率明显提高。据信这也发生在神经内分泌肿瘤中,但尚无明确数据。我们推测,可用于神经内分泌肿瘤治疗的全身选择的不同作用方式可能会避免一种选择对另一种选择的完全抵抗,并且顺序使用这些药物将转化为更长的患者总生存期。在神经内分泌肿瘤领域中,迫切需要进行前瞻性和随机试验,以寻找在无法使用其他系统替代药物后药物的活性。

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