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直肠癌根治术后异时性肿瘤性病变的影响因素

Influencing factors of metachronous tumor lesions after radical resection of rectal cancer

  • 摘要:
    目的 探究直肠癌根治术后发生异时性肿瘤性病变的危险因素。
    方法 纳入2012年10月至2018年6月在中山大学附属第六医院接受直肠癌根治术的直肠癌患者,收集患者一般资料、初始结肠镜及截至2025年3月的随访结肠镜等相关临床信息。采用Kaplan-Meier风险函数比较早发性直肠癌与晚发性直肠癌发生异时性肿瘤性病变的差异;采用单因素和多因素Cox比例风险模型,分析直肠癌根治术后异时性肿瘤性病变发生的影响因素。
    结果 共757例患者纳入研究,随访时间为30(15, 58)个月。Kaplan-Meier风险函数显示:与晚发性直肠癌组相比,早发性直肠癌组异时性肿瘤性病变的发生风险明显下降(P<0.001)。Cox比例风险模型分析显示:早发性直肠癌(HR=0.508,95%CI:0.344~0.749)是直肠癌术后异时性肿瘤性病变的保护因素;PIK3CA突变(HR=2.360,95%CI:1.340~4.158)和同时性进展性腺瘤(HR=2.094,95%CI:1.401~3.129)是直肠癌术后异时性肿瘤性病变的危险因素。
    结论 早发性直肠癌患者无需频繁的结肠镜监测,临床应考虑对PIK3CA突变和存在同时性进展性腺瘤的直肠癌根治术后患者进行强化监测。

     

    Abstract:
    Objective To investigate risk factors for metachronous tumor lesions after radical resection of rectal cancer (RC).
    Methods Patients who underwent radical resection for RC at The Sixth Affiliated Hospital, Sun Yat-sen University between October 2012 and June 2018 were selected. General patient data, initial colonoscopy findings, and follow-up colonoscopy results before Marth 2025 were collected. Kaplan-Meier analysis was used to compare the cumulative incidence of metachronous tumor lesions between early-onset (EO) and average-onset (AO) RC groups. Univariate and multivariate Cox proportional hazards models were employed to analyze factors associated with developing metachronous tumor lesions after surgery.
    Results A total of 757 patients were included, with a follow-up duration of 30 (15, 58) months. Kaplan-Meier analysis demonstrated a significantly lower cumulative risk of metachronous tumor lesions in the EO-RC group compared to the AO-RC group (P<0.001). Multivariate Cox regression analysis identified EO-RC as a protective factor against metachronous tumor lesions (HR=0.508, 95%CI: 0.344-0.749). Conversely, PIK3CA mutation (HR=2.360, 95%CI: 1.340-4.158) and synchronous advanced adenoma (HR=2.094, 95%CI: 1.401-3.129) were identified as independent risk factors.
    Conclusions Patients with EO-RC may not require intensified colonoscopy surveillance postoperatively. However, intensified surveillance strategies should be considered for RC patients harboring PIK3CA mutations or presenting with synchronous advanced adenomas.

     

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