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Chemotherapy-induced diarrhea

机译:化疗引起的腹泻

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Chemotherapy-induced diarrhea is a well-documented side effect of many cancer treatments and is associated with increased morbidity and mortality. Chemotherapy-induced diarrhea negatively impacts patient quality of life and treatment outcome by requiring dose limitations or treatment interruption. The chemotherapeutic agent CPT-11 (irinotecan) has shown promising results as a single agent and in combination chemotherapy for the treatment of colorectal and small cell lung cancer. However, delayed onset diarrhea is considered to be its major dose-limiting toxicity. In some cases, it can be life threatening. To prevent CPT-11-induced delayed diarrhea, oral alkalization (OA) and control of defecation (CD) [Int J Cancer 92: 269-275, 2001] were developed based on fundamental studies [Int J Cancer 83: 491-496, 1999; Cancer Res 62: 179-187, 2002]. Oral administration of antibiotics [Cancer Res 56: 3752-3757, 1996; Clin Cancer Res 7: 1136-1141, 2001] or kampo medicine [Jpn J Cancer Res 86: 978-984, 1995; Jpn J Cancer Res 86: 985-989, 1995] to decrease beta-glucuronidase activity derived from bacteria in the large intestine was also reported to be successful in preventing delayed diarrhea. When CPT-11-induced delayed diarrhea occurs, the conventional treatment is loperamide [J Natl Cancer Inst 86: 446-449, 1994], and the early recognition and treatment of diarrhea with this opioid has reduced, although not entirely eliminated, patient morbidity. Other therapies are needed to treat patients with loperamide-refractory CPT-11 induced diarrhea, and the successful use of the somatostatin analogue octreotide has been reported [Support Care Cancer 9: 258-260, 2001; Ann Oncol 12: 227-229, 2001; Proc Am Soc Clin Oncol 21: 387a, 2002].
机译:化学疗法引起的腹泻是许多癌症治疗方法的有据可查的副作用,并与发病率和死亡率增加相关。化学疗法引起的腹泻需要限制剂量或中断治疗,从而对患者的生活质量和治疗结果产生负面影响。化疗药物CPT-11(伊立替康)作为单一药物和联合化疗在结直肠癌和小细胞肺癌治疗中已显示出令人鼓舞的结果。然而,延迟发作性腹泻被认为是其主要的剂量限制性毒性。在某些情况下,可能会危及生命。为防止CPT-11-引起的延迟性腹泻,根据基础研究[Int J Cancer 83:491-496,口服碱化(OA)和控制排便(CD)[Int J Cancer 92:269-275,2001] 1999年; Cancer Res 62:179-187,2002]。口服抗生素[Cancer Res 56:3752-3757,1996; Clin Cancer Res 7:1136-1141,2001]或kampo medicine [Jpn J Cancer Res 86:978-984,1995; [Jpn J Cancer Res 86:985-989,1995]降低大肠细菌中的β-葡糖醛酸糖苷酶活性也被报道成功地预防了延迟性腹泻。当发生CPT-11-引起的延迟性腹泻时,常规治疗是洛哌丁胺[J Natl Cancer Inst 86:446-449,1994],尽管这种阿片类药物虽然并未完全消除,但对早期腹泻的识别和治疗有所降低,但患者的发病率却有所降低。 。还需要其他疗法来治疗洛哌丁胺难治性CPT-11诱导的腹泻,并且已报道成功使用生长抑素类似物奥曲肽[Support Care Cancer 9:258-260,2001; Ann Oncol 12:227-229,2001; [Proc Am Soc Clin Oncol 21:387a,2002]。

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