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活检诊断的乳腺导管原位癌的临床病理随访:一项对575例患者的单机构研究

Clinicopathological Follow-up of Breast DCIS Diagnosed on Biopsies: A Single Institutional Study of 575 Patients.

作者信息

Yan Mingfei, Bomeisl Phillip, Gilmore Hannah, Harbhajanka Aparna

机构信息

24575University Hospitals Cleveland Medical Center, Cleveland, OH, USA.

出版信息

Int J Surg Pathol. 2021 Dec;29(8):836-843. doi: 10.1177/10668969211012088. Epub 2021 Apr 23.

Abstract

Stratifying ductal carcinoma in situ (DCIS) patients into different upgrading risk groups is important in exploiting more precise therapeutic options. Evaluation of estrogen receptor/progesterone receptor/human epidermal growth factor receptor 2 (ER/PR/HER2) status and axillary lymph node metastatic status for DCIS and their upgraded invasive counterparts can also provide diagnostic and therapeutic implications. We retrospectively studied 575 patients with first-time diagnosis of DCIS on biopsies, and followed up their final diagnosis, ER/PR/HER2 status, and axillary lymph node involvement on excisions. As a result, biopsy-diagnosed DCIS had an overall 19.1% risk to be upgraded on subsequent excisions, with 4.7% being upgraded to microinvasive carcinoma (pT1mi) and 14.4% to overt invasive carcinoma (⩾pT1a). Factors significantly associated with higher upgrading risk on multivariate analysis include biopsy guidance by ultrasound ( <.001), DCIS with suspicious microinvasion ( < .001), and DCIS diagnosed in left breast ( = .026). DCIS diagnosed in younger patients (⩽40 years old) or DCIS with high nuclear grade showed higher upgrading risk only on univariate analysis. About 80% ER + /PR + and ER/PR DCIS remained the same ER/PR status after being upgraded, and ER + /PR   DCIS had the highest risk (63.6%) of having HER2 amplification in upgraded invasive carcinoma. For upgraded DCIS, microinvasive carcinoma was more likely to have HER2 amplification (50%) than overt invasive carcinoma (29.5%). Besides, pure DCIS had a low risk of axillary lymph node macrometastasis (0.74%), while the risk increased in DCIS with microinvasion (4.4%) and was highest in overt invasive carcinoma (14.7%). The findings of this study are clinically relevant with respect to criteria that might be used in selecting patients for de-escalation trials.

摘要

将原位导管癌(DCIS)患者分层为不同的升级风险组对于采用更精确的治疗方案至关重要。评估DCIS及其升级后的浸润性对应物的雌激素受体/孕激素受体/人表皮生长因子受体2(ER/PR/HER2)状态和腋窝淋巴结转移状态也可为诊断和治疗提供指导。我们回顾性研究了575例首次经活检诊断为DCIS的患者,并随访了其最终诊断、ER/PR/HER2状态以及切除标本中的腋窝淋巴结受累情况。结果显示,活检诊断为DCIS的患者在后续切除术中总体有19.1%的升级风险,其中4.7%升级为微浸润癌(pT1mi),14.4%升级为浸润性癌(⩾pT1a)。多因素分析显示,与升级风险较高显著相关的因素包括超声引导活检(<0.001)、伴有可疑微浸润的DCIS(<0.001)以及左乳诊断的DCIS(=0.026)。仅在单因素分析中,年轻患者(⩽40岁)诊断的DCIS或核分级高的DCIS显示出较高的升级风险。约80%的ER+/PR+和ER/PR DCIS升级后ER/PR状态保持不变,且ER+/PR-DCIS在升级后的浸润性癌中HER2扩增风险最高(63.6%)。对于升级后的DCIS,微浸润癌比浸润性癌更易发生HER2扩增(50%比29.5%)。此外,单纯DCIS腋窝淋巴结大转移风险较低(0.74%),而伴有微浸润的DCIS风险增加(4.4%),在浸润性癌中风险最高(14.7%)。本研究结果对于可能用于选择患者进行降阶梯试验的标准具有临床相关性。

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