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首页> 外文期刊>Medical oncology >Patients with distal intestinal gastric cancer have superior outcome with addition of taxanes to combination chemotherapy, while proximal intestinal and diffuse gastric cancers do not: does biology and location predict chemotherapy benefit?
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Patients with distal intestinal gastric cancer have superior outcome with addition of taxanes to combination chemotherapy, while proximal intestinal and diffuse gastric cancers do not: does biology and location predict chemotherapy benefit?

机译:远端肠胃癌患者在联合化疗中加入紫杉烷类药物可获得更好的疗效,而近端肠癌和弥漫性胃癌患者则不行:生物学和部位对化疗有好处吗?

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Gastric cancer, with one million new cases observed annually, and its dismal prognosis, is one of the leading causes of cancer-related mortalities. Systemic chemotherapy is the main treatment modality in advanced gastric cancer patients. We aim to evaluate the predictive role of tumor localization and histopathology on choosing three or two-drug combination regimens. Consecutive 110 metastatic gastric adenocarcinoma patients who were admitted to the Baskent University Department of Medical Oncology and the Van Research and Training Hospital were included in the study. Data of patients were analyzed retrospectively. Median age of patients was 58 years (range 30-80). Proximal intestinal, distal intestinal, and diffuse gastric cancers were found in 35 (32 %), 64 (58 %), and 11 (10 %) patients, respectively. 5-fluoracil and platinum (PF) and PFtax were administered to 47 (43 %) and 63 (57 %) patients, respectively. Median progression-free survival (PFS) was 4.0 (95 % CI 2.5-5.6) and 7.4 months (95 % CI 6.0-8.7) for PF and PFtax groups, (p = 0.034). When we used tumor localization as strata in the PFS survival curve, PFtax produced significantly higher PFS rates only in distal intestinal-type gastric cancer, compared with PF (p = 0.03). Median overall survival (OS) was 9.0 (95 % CI 5.2-12.3) and 17.3 months (95 % CI 7.8-27) for PF and PFtax groups, (p = 0.010). When we used tumor localization as strata in the OS survival curve, PFtax produced significantly higher OS rates only in distal intestinal-type gastric cancer compared with PF (p = 0.015). Pathology and tumor location in gastric cancers may affect the outcome, the addition of taxanes as a third drug may significantly increase PFS and OS rate purely in distal intestinal-type gastric cancer but not in patients with proximal and diffuse-type gastric cancers.
机译:胃癌每年观察到一百万例新病例,其预后不佳,是与癌症有关的死亡率的主要原因之一。全身化疗是晚期胃癌患者的主要治疗方式。我们旨在评估肿瘤定位和组织病理学在选择三种或两种药物联合治疗方案中的预测作用。这项研究包括连续入选Baskent大学医学肿瘤学系和Van研究与培训医院的110例转移性胃腺癌患者。回顾性分析患者资料。患者的中位年龄为58岁(范围30-80)。分别在35(32%),64(58%)和11(10%)患者中发现了近端肠癌,远端肠癌和弥漫性胃癌。分别对47名患者(43%)和63名患者(57%)分别使用了5-氟尿嘧啶和铂(PF)和PFtax。 PF和PFtax组的中位无进展生存期(PFS)为4.0(95%CI 2.5-5.6)和7.4个月(95%CI 6.0-8.7)(p = 0.034)。当我们在PFS生存曲线中将肿瘤定位用作分层时,与PF相比,PFtax仅在远侧肠型胃癌中产生明显更高的PFS率(p = 0.03)。 PF和PFtax组的中位总生存期(OS)为9.0(95%CI 5.2-12.3)和17.3个月(95%CI 7.8-27)(p = 0.010)。当我们将肿瘤定位作为OS生存曲线的分层时,PFtax仅在远侧肠型胃癌中产生的OS率显着高于PF(p = 0.015)。胃癌的病理学和肿瘤位置可能会影响预后,紫杉烷类作为第三种药物的加入可能纯粹在远端肠型胃癌中显着提高PFS和OS率,而在近端和弥漫型胃癌患者中则不然。

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