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首页> 外文期刊>Journal of Clinical Oncology >Prognostic Impact of Deficient DNA Mismatch Repair in Patients With Stage III Colon Cancer From a Randomized Trial of FOLFOX-Based Adjuvant Chemotherapy.
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Prognostic Impact of Deficient DNA Mismatch Repair in Patients With Stage III Colon Cancer From a Randomized Trial of FOLFOX-Based Adjuvant Chemotherapy.

机译:从基于FOLFOX的辅助化疗的随机试验中,DNA错配修复不足对III期结肠癌患者的预后影响。

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The association of deficient DNA mismatch repair (dMMR) with prognosis in patients with colon cancer treated with adjuvant fluorouracil, leucovorin, and oxaliplatin (FOLFOX) chemotherapy remains unknown.Resected, stage III colon carcinomas from patients (N = 2,686) randomly assigned to FOLFOX ± cetuximab (North Central Cancer Treatment Group N0147 trial) were analyzed for mismatch repair (MMR) protein expression and mutations in BRAF(V600E) (exon 15) and KRAS (codons 12 and 13). Association of biomarkers with disease-free survival (DFS) was determined using Cox models. A validation cohort (Cancer and Leukemia Group B 88903 trial) was used.dMMR was detected in 314 (12%) of 2,580 tumors, of which 49.3% and 10.6% had BRAF(V600E) or KRAS mutations, respectively. MMR status was not prognostic overall (adjusted hazard ratio [HR], 0.82; 95% CI, 0.64 to 1.07; P = .14), yet significant interactions were found between MMR and primary tumor site (Pinteraction = .009) and lymph node category (N1 v N2; Pinteraction = .014). Favorable DFS was observed for dMMR versus proficient MMR proximal tumors (HR, 0.71; 95% CI, 0.53 to 0.94; P = .018) but not dMMR distal tumors (HR, 1.71; 95% CI, 0.99 to 2.95; P = .056), adjusting for mutations and covariates. Any survival benefit of dMMR was lost in N2 tumors. Mutations in BRAF(V600E) (HR, 1.37; 95% CI, 1.08 to 1.70; P = .009) or KRAS (HR, 1.44; 95% CI, 1.21 to 1.70; P < .001) were independently associated with worse DFS. The observed MMR by tumor site interaction was validated in an independent cohort of stage III colon cancers (Pinteraction = .037).The prognostic impact of MMR depended on tumor site, and this interaction was validated in an independent cohort. Among dMMR cancers, proximal tumors had favorable outcome, whereas distal or N2 tumors had poor outcome. BRAF or KRAS mutations were independently associated with adverse outcome.
机译:辅助性氟尿嘧啶,亚叶酸钙和奥沙利铂(FOLFOX)化疗治疗的结肠癌患者中DNA错配修复(dMMR)不足与预后的相关性。来自患者的切除的III期结肠癌(N = 2,686)被随机分配至FOLFOX对±西妥昔单抗(北部中央癌症治疗组N0147试验)进行了BRAF(V600E)(第15外显子)和KRAS(第12和13号密码子)错配修复(MMR)蛋白表达和突变分析。使用Cox模型确定生物标志物与无病生存期(DFS)的关联。使用验证队列(癌症和白血病B组88903试验)。在2,580个肿瘤中,有314个(12%)检测到dMMR,其中分别有BRAF(V600E)或KRAS突变的49.3%和10.6%。 MMR状态并非整体预后(危险比[HR]为0.82; 95%CI为0.64至1.07; P = .14),但是MMR与原发肿瘤部位之间存在显着相互作用(相互作用= .009)。类别(N1 v N2;互动= 0.014)。相对于熟练的MMR近端肿瘤(HR,0.71; 95%CI,0.53至0.94; P = .018),dMMR观察到良好的DFS,而dMMR远端肿瘤(HR,1.71; 95%CI,0.99至2.95; P =。 056),调整突变和协变量。 dMMR的任何生存益处在N2肿瘤中丧失。 BRAF(V600E)(HR,1.37; 95%CI,1.08至1.70; P = .009)或KRAS(HR,1.44; 95%CI,1.21至1.70; P <.001)的突变与DFS较差独立相关。在一个独立的III期结肠癌队列中验证了通过肿瘤部位相互作用观察到的MMR(Pinteraction = .037)。MMR的预后影响取决于肿瘤部位,并且在一个独立队列中验证了这种相互作用。在dMMR癌症中,近端肿瘤的预后良好,而远端或N2肿瘤的预后差。 BRAF或KRAS突变与不良结局独立相关。

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