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首页> 外文期刊>Annals of Surgery >Intraperitoneal treatment for peritoneal mucinous carcinomatosis of appendiceal origin after operative management: long-term follow-up of the Mayo Clinic experience.
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Intraperitoneal treatment for peritoneal mucinous carcinomatosis of appendiceal origin after operative management: long-term follow-up of the Mayo Clinic experience.

机译:腹膜内手术治疗阑尾起源的腹膜粘液性癌病:梅奥诊所经验的长期随访。

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OBJECTIVE: To determine prognostic factors and the impact of intraperitoneal (IP) treatment after surgical resection of peritoneal mucinous carcinomatosis (PMC) of appendiceal origin. SUMMARY OF BACKGROUND DATA: PMC is a rare, malignant, intra-abdominal neoplasm that produces large amounts of mucin. Patients typically present with diffuse peritoneal disease. After surgical treatment, multiple locoregional recurrences are common; recurrences outside the abdomen are infrequent. Treatment regimens include debulking, radiotherapy with IP radioisotopes, and chemotherapies (IP, systemic, or both). Because reported data are variable and heterogeneous, treatment evaluations are challenging. METHODS: We retrospectively reviewed 115 consecutive patients with PMC who underwent maximal surgical resection with or without postoperative therapy between 1985 and 2000 at Mayo Clinic Rochester. After maximal resection, 37 patients received IP 5-fluorouracil, 35 of whom also received IP chromic phosphate P 32. The Kaplan-Meier method was used to estimate overall survival (OS) and disease-free survival. RESULTS: All gross disease was removed in 61% of patients. With a median follow-up of 6.1 years, the median OS was 8.1 years. Median OS for patients receiving versus not receiving IP therapy was 23.5 years versus 7.5 years, respectively. The 5-, 10-, and 15-year OS for those receiving and not receiving IP therapy was 82%, 65%, and 52% versus 60%, 27%, and 15%, respectively. Adverse prognostic factors for OS identified by univariate analysis included partial mucin debulking, adenocarcinoma histology, systemic chemotherapy, diffuse IP disease at presentation, and no IP therapy. On multivariate analysis, diffuse IP disease at presentation and no IP therapy remained significant. A separate analysis was performed for the 70 patients who underwent gross total resection, 51% of whom received IP therapy. Adverse prognostic factors for OS included adenocarcinoma histology, systemic chemotherapy, and no IP therapy. CONCLUSIONS: This large, single-institution, retrospective series with long-term follow-up suggests that IP chromic phosphate P 32 and 5-fluorouracil after maximal surgical resection of PMC of appendiceal origin is associated with improved OS and disease-free survival.
机译:目的:确定手术切除阑尾来源的腹膜粘液性癌(PMC)后的预后因素及其腹膜内(IP)治疗的影响。背景数据概述:PMC是一种罕见的恶性腹腔内肿瘤,会产生大量粘蛋白。患者通常表现为弥漫性腹膜疾病。手术治疗后,多部位复发很常见。腹部以外的复发很少见。治疗方案包括减瘤,用IP放射性同位素进行放射治疗和化学疗法(IP,全身或两者)。由于报告的数据是可变的且异构的,因此治疗评估具有挑战性。方法:我们回顾性回顾了1985年至2000年在梅奥诊所罗切斯特进行的115例连续性PMC患者,这些患者在接受或不接受术后治疗的情况下进行了最大手术切除。最大限度切除后,有37例患者接受了IP 5-氟尿嘧啶治疗,其中35例也接受了IP磷酸铬P 32治疗。Kaplan-Meier方法用于评估总生存期(OS)和无病生存期。结果:61%的患者全部疾病被清除。中位随访时间为6.1年,中位OS​​为8.1年。接受和未接受IP治疗的患者的中位OS分别为23.5年和7.5年。接受和不接受IP疗法者的5年,10年和15年OS分别为82%,65%和52%,而60%,27%和15%分别为。通过单因素分析确定的OS不良预后因素包括部分黏蛋白减集,腺癌组织学,全身化疗,弥漫性IP病就诊以及无IP治疗。在多变量分析中,就诊时出现弥漫性IP疾病且无IP治疗仍然很明显。对70例行总切除的患者进行了单独分析,其中51%接受了IP治疗。 OS的不良预后因素包括腺癌组织学,全身化疗和无IP治疗。结论:这个大型的,单机构的,长期随访的回顾性研究表明,对阑尾来源的PMC进行最大程度的手术切除后,IP磷酸铬P 32和5-氟尿嘧啶可改善OS和无病生存期。

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