Clinical evaluation of molecular surrogate subtypes in patients with ipsilateral multifocal primary breast cancer.

Slavica Janeva, Ellen Krabbe, Toshima Z Parris, Salmir Nasic, Marie Sundquist, Per Karlsson, Riccardo A Audisio, Roger Olofsson Bagge, Anikó Kovács
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Abstract

Background: When ipsilateral multifocal primary breast cancer (IMBC) is detected, standard routine is to evaluate the largest tumor with immunohistochemistry (IHC). As all foci are not routinely characterized, many patients may not receive optimal adjuvant treatment. Here, we assess the clinical relevance of examining at least two foci present in patients with IMBC.

Methods: Patients diagnosed and treated for IMBC at Sahlgrenska University Hospital (Gothenburg, Sweden) between 2012 and 2017 were screened. In total, 180 patients with ≥ 2 invasive foci (183 specimens) were assessed with IHC and included in this study. Expression of the estrogen (ER) and progesterone (PR) receptors, Ki67, HER2, and tumor grade were used to determine the molecular surrogate subtypes and discordance among the foci was recorded. An additional multidisciplinary team board was then held to re-assess whether treatment recommendations changed due to discordances in molecular surrogate subtype between the different foci.

Results: Discordance in ER, PR, HER2, and Ki67 was found in 2.7%, 19.1%, 7.7%, and 16.9% of invasive foci, respectively. Discordance in the molecular surrogate subtypes was found in 48 of 180 (26.7%) patients, which resulted in therapy changes for 11 patients (6.1%). These patients received additional endocrine therapy (n = 2), chemotherapy (n = 3), and combined chemotherapy and trastuzumab (n = 6).

Conclusion: Taken together, when assessing at least two tumor foci with IHC, regardless of shared morphology or tumor grade between the different foci, 6.1% of patients with IMBC were recommended additional adjuvant treatment. A pathologic assessment using IHC of all foci is therefore recommended to assist in individualized treatment decision making.

Abstract Image

Abstract Image

Abstract Image

同侧多灶性原发性乳腺癌患者分子替代亚型的临床评价。
背景:当检测到同侧多灶性原发性乳腺癌(IMBC)时,标准常规是用免疫组织化学(IHC)评估最大的肿瘤。由于并非所有病灶都具有常规特征,因此许多患者可能无法获得最佳辅助治疗。在这里,我们评估在IMBC患者中检查至少两个病灶的临床相关性。方法:筛选2012年至2017年在瑞典哥德堡萨尔格伦斯卡大学医院诊断和治疗的IMBC患者。共有180例≥2个侵袭性病灶患者(183个标本)接受免疫组化评估并纳入本研究。通过雌激素(ER)和孕激素(PR)受体、Ki67、HER2和肿瘤分级的表达来确定分子替代亚型,并记录病灶之间的不一致。随后召开了一个额外的多学科小组委员会,重新评估治疗建议是否因不同病灶之间的分子替代亚型不一致而改变。结果:侵袭性病灶中ER、PR、HER2、Ki67的不一致性分别为2.7%、19.1%、7.7%、16.9%。180例患者中有48例(26.7%)发现分子替代物亚型不一致,导致11例患者(6.1%)改变治疗。这些患者接受了额外的内分泌治疗(n = 2),化疗(n = 3)以及化疗和曲妥珠单抗联合治疗(n = 6)。综上所述,当用免疫组化评估至少两个肿瘤灶时,无论不同灶之间的共同形态或肿瘤分级如何,6.1%的IMBC患者被推荐额外的辅助治疗。因此,建议对所有病灶进行免疫组化的病理评估,以帮助制定个性化的治疗决策。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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