EGFR 基因突变阳性状态与病理分期和组织学亚型相结合是 pN0-1 肺腺癌复发的危险因素：一项回顾性多中心分析。

Positive EGFR mutation status is a risk of recurrence in pN0-1 lung adenocarcinoma when combined with pathological stage and histological subtype: A retrospective multi-center analysis.

机构信息

Department of Surgical Oncology, Research Institute for Radiation Biology and Medicine, Hiroshima University, Hiroshima, Japan.

Department of Thoracic Surgery, Kanagawa Cancer Center, Yokohama, Kanagawa, Japan.

出版信息

Lung Cancer. 2020 Mar;141:107-113. doi: 10.1016/j.lungcan.2020.01.018. Epub 2020 Jan 30.

DOI:10.1016/j.lungcan.2020.01.018

PMID:32035371

Abstract

OBJECTIVES

Recurrence risk of resected lung adenocarcinoma is represented by pathological stage (pStage), histological subtype, and potentially by EGFR mutation. However, the relationship among these factors and their combined impact on prognosis are unclear.

MATERIALS AND METHODS

Using a multicenter database, we retrospectively investigated the prognostic impact of EGFR mutation status in relation to pStage and histological subtype in resected pN0-1M0 lung adenocarcinoma.

RESULTS

Among 1155 pN0-1M0 adenocarcinoma cases, pStage 0 and IA1-IB were confirmed predominantly in EGFR-positive cases. AIS, MIA, and lepidic predominant adenocarcinoma were also more frequently found in EGFR-positive cases and showed no/little recurrence regardless of EGFR mutation status. The 5-year recurrence-free survival (RFS) of papillary, acinar, solid, and micropapillary predominant adenocarcinoma was stratified by pStage (IA1-IB, IIA-IIIA) or histological malignant subtype (intermediate or high malignant subtype), and more finely subdivided by EGFR mutation status. Positive EGFR mutation cases showed worse RFS in both classifications. Low malignant subtype and pStage IA1-IB intermediate malignant subtype showed low frequency of recurrence. Whereas, in pStage IA1-IB high malignant subtype and pStage IIA-IIIA cases, EGFR-positive cases showed poorer 5-year RFS than EGFR-negative (49.6% and 75.6%, respectively, hazard ratio [HR] = 1.84, 95% CI = 1.38-7.42, p <  0.01) and multivariate analysis indicated positive EGFR mutation status was significantly related to poorer PRF (HR = 2.005, 95% CI = 1.029-3.906, p =  0.041).

CONCLUSION

EGFR mutation harbored primarily in early-stage or low-malignant histological subtypes with no/little recurrence. In pN0-1M0 adenocarcinoma with higher risk of recurrence, positive EGFR mutation cases showed worse RFS. EGFR mutation status enables better stratification of recurrence risk when considering pStage and histological malignant subtype.

摘要

目的

切除的肺腺癌的复发风险由病理分期（pStage）、组织学亚型以及可能的 EGFR 突变来表示。然而，这些因素之间的关系及其对预后的综合影响尚不清楚。

材料和方法

我们使用多中心数据库回顾性研究了 EGFR 突变状态与切除的 pN0-1M0 肺腺癌的 pStage 和组织学亚型之间的关系对预后的影响。

结果

在 1155 例 pN0-1M0 腺癌病例中，pStage 0 和 IA1-IB 主要出现在 EGFR 阳性病例中。AIS、MIA 和贴壁为主型腺癌也更常见于 EGFR 阳性病例，且无论 EGFR 突变状态如何，均无/很少复发。按 pStage（IA1-IB、IIA-IIIA）或组织学恶性亚型（中或高恶性亚型）对乳头型、腺泡型、实体型和微乳头型为主型腺癌进行分层，并根据 EGFR 突变状态进一步细分，5 年无复发生存率（RFS）。在这两种分类中，EGFR 阳性突变病例的 RFS 均较差。低恶性亚型和 pStage IA1-IB 中恶性亚型的复发频率较低。然而，在 pStage IA1-IB 高恶性亚型和 pStage IIA-IIIA 病例中，EGFR 阳性病例的 5 年 RFS 比 EGFR 阴性病例差（分别为 49.6%和 75.6%，风险比[HR] = 1.84，95%CI = 1.38-7.42，p < 0.01），多变量分析表明 EGFR 阳性突变状态与较差的 PRF 显著相关（HR = 2.005，95%CI = 1.029-3.906，p = 0.041）。

结论

EGFR 突变主要存在于无复发或复发风险低的早期或低恶性组织学亚型中。在具有较高复发风险的 pN0-1M0 腺癌中，EGFR 阳性病例的 RFS 较差。EGFR 突变状态有助于在考虑 pStage 和组织学恶性亚型时更好地分层复发风险。

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EGFR 基因突变阳性状态与病理分期和组织学亚型相结合是 pN0-1 肺腺癌复发的危险因素：一项回顾性多中心分析。

Positive EGFR mutation status is a risk of recurrence in pN0-1 lung adenocarcinoma when combined with pathological stage and histological subtype: A retrospective multi-center analysis.

机构信息

出版信息

OBJECTIVES

MATERIALS AND METHODS

RESULTS

CONCLUSION

目的

材料和方法

结果

结论

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