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Prognostic value of fibrosis ratio in metastatic lymph nodes of node-positive advanced gastric cancer

机译:纤维化比率在淋巴结阳性晚期胃癌转移淋巴结中的预后价值

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摘要

Lymph node metastasis plays a crucial role in predicting prognosis in advanced gastric cancer (AGC). In the present study, we formulated a fibrosis ratio (FR), defined as the number of metastatic lymph nodes with fibrosis divided by the total number of lymph nodes, and sought to determine whether it can be used to predict the prognosis of patients with AGC and improve on existing node staging. We retrospectively analyzed 161 patients who underwent curative resection for node-positive AGC between 2001 and 2010, evaluating the association between FR, lymph node ratio (LNR), and micrometastasis, and the relationship between FR and clinicopathologic findings, overall survival (OS) and disease-free survival (DFS). A high FR was significantly related to T stage (P < .001), N stage (P < .001), tumor stage (P < .001), lymphatic invasion (P < .001), and venous invasion (P = .007). FR was significantly correlated with an increased number of metastatic lymph nodes (P = .001, R = 0.869) and LNR (P = .001, R = 0.943), but not with total harvested lymph nodes. Patients with micrometastases had a lower FR, compared with those without micrometastases (P < .001). A survival analysis showed poor OS for patients in the entire cohort (P < .001); N1 (P = .002), N2 (P = .004), N3a (P = .010), and N3b (P = .003) stages; and groups with high LNR (P = .013) and low LNR (P = .001). DFS was also poor for the entire cohort (P < .001) and the N2 (P = .013), N3b (P = .002), high-LNR (P = .036), and low-LNR (P = .001) groups, but not the N1 or N3a group. Univariate and multivariate analyses revealed that high FR was an independent prognostic factor for OS (hazard ratio [HR], 2.780; CI, 1.655–4.670; P < .001) and DFS (HR, 2.051; CI, 1.199–3.508; P = .009) in AGC. Collectively, our findings indicate that high FR is associated with adverse clinicopathologic parameters in AGC, clearly establishing nodal fibrosis as a pathological finding with value in predicting poor prognosis of patients with AGC. Thus, combining current N stage and LNR diagnostics with FR could improve prognostic prediction in AGC.
机译:淋巴结转移在预测晚期胃癌(AGC)的预后中起着至关重要的作用。在本研究中,我们制定了纤维化率(FR),定义为纤维化转移性淋巴结的数目除以淋巴结的总数,并试图确定其是否可用于预测AGC患者的预后并改进现有节点的暂存。我们回顾性分析了2001年至2010年间接受根治性AGC根治性切除术的161例患者,评估了FR,淋巴结比率(LNR)和微转移之间的关联,以及FR与临床病理结果,总生存期(OS)和无病生存期(DFS)。高FR与T期(P <0.001),N期(P <0.001),肿瘤期(P <0.001),淋巴管浸润(P <0.001)和静脉浸润(P =)显着相关。 007)。 FR与转移性淋巴结数目的增加(P = 0.001,R = 0.869)和LNR(P = 0.001,R = 0.943)显着相关,但与总收获的淋巴结无关。与无微转移的患者相比,有微转移的患者的FR较低(P <0.001)。生存分析显示整个队列的患者的OS较差(P <.001); N1(P = .002),N2(P = .004),N3a(P = .010)和N3b(P = .003)阶段;以及LNR高(P = .013)和LNR低( P = .001)的组。整个队列( P <.001)和N2( P = .013),N3b( P =)的DFS也很差。 002),高LNR( P = .036)和低LNR( P = .001)组,但不包括N1或N3a组。单因素和多因素分析表明,高FR是OS的独立预后因素(危险比[HR]为2.780; CI为1.655-4.670; P <.001)和DFS(HR为2.051; CI) ,1.199–3.508; P = .009)。总的来说,我们的发现表明高FR与AGC中不良的临床病理参数有关,从而明确将淋巴结纤维化确定为病理学发现,具有预测AGC患者预后不良的价值。因此,将当前的N期和LNR诊断与FR结合可以改善AGC的预后预测。

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