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Pfetin as a Risk Factor of Recurrence in Gastrointestinal Stromal Tumors

机译:Pfetin是胃肠道间质瘤复发的危险因素

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Background. Despite complete resection of gastrointestinal stromal tumors (GIST), recurrent and/or metastatic disease occurs, often depending on the grade of malignancy. As such, markers are needed that accurately predict patients at high risk for recurrence. Previously our group reported Pfetin as a prognostic biomarker for GIST. In order to create an approach for predicting risk of recurrence, we incorporated Pfetin expression with clinicopathological data to produce a predictive model.Object. Forty-five patients with localized primary GIST were treated with complete gross surgical resection surgically at our institution between 1995 and 2010 were included. The majority of tumors originated in the stomach (38 cases), as well as small intestine (6 cases) and rectum (1 case).Method. (1) We performed retrospective analysis of the connection between Pfetin expression, clinicopathological data, and incidences of recurrence, using bivariate and multivariate analyses. (2) The reactivity of the monoclonal antibody against Pfetin was examined by immunohistochemistry.Pfetin. We have reported Pfetin, identified microarray technology, and compared between statistically different GISTs for good and poor prognoses and for prognostic marker.Results. There were 7 cases of recurrences. (1) By univariate analysis, tumor size, mitoses, exposure to abdominal cavity, and complete tumor removal predicted risk of recurrence. (2) Pfetin-negative cases were significantly related to recurrence (P= 0.002).Conclusions. This analysis demonstrates that lack of Pfetin expression is an additional predictor of recurrence in resected GIST. Further study may determine the role of this variable added to the current predictive model for selection of adjuvant therapy.
机译:背景。尽管已经完全切除了胃肠道间质瘤(GIST),但仍会复发和/或转移性疾病,这通常取决于恶性程度。因此,需要能够准确预测高复发风险患者的标记物。先前,我们的研究小组将Pfetin报告为GIST的预后生物标志物。为了创建一种预测复发风险的方法,我们将Pfetin表达与临床病理数据相结合以产生预测模型。 1995年至2010年间,我们机构对45例局灶性原发性GIST患者进行了彻底的大手术切除。肿瘤多数起源于胃(38例),小肠(6例)和直肠(1例)。 (1)我们使用双变量和多变量分析对Pfetin表达,临床病理数据与复发率之间的关系进行了回顾性分析。 (2)通过免疫组织化学检查了单克隆抗体对Pfetin的反应性。我们已经报告了Pfetin,已确定的微阵列技术,并在统计学上不同的GIST之间进行了比较,以评估预后的好坏和预后的标志物。有7例复发。 (1)通过单因素分析,肿瘤大小,有丝分裂,暴露于腹腔以及完全切除肿瘤可预测复发风险。 (2)Pfetin阴性病例与复发率显着相关(P = 0.002)。该分析表明,缺乏Pfetin表达是切除的GIST复发的另一个预测因素。进一步的研究可能会确定将此变量添加到当前预测模型中以选择辅助治疗的作用。

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