转移性乳腺癌原发部位和复发部位生物标志物不一致及其临床意义研究:来自印度的一项单一机构研究

IF 0.6 Q4 ONCOLOGY South Asian Journal of Cancer Pub Date : 2023-12-08 DOI:10.1055/s-0043-1775807
S. Shanthala, U. Amirtham, C. Gopal, Suma M. N., Linu Jacob, Govind Babu
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引用次数: 0

摘要

原发和转移部位之间受体的免疫表型差异显著影响治疗结果。目前的国际指南建议对可接近的转移性病变进行重新活检,以重新评估组织生物标志物。虽然关于生物标志物变化的现有文献存在矛盾和异质性,但缺乏对印度乳腺癌患者队列的类似研究。在此背景下,我们旨在评估原发和复发部位活检之间生物标志物变化的频率,以及它们与转移性乳腺癌(MBC)患者的各种临床病理特征(包括转移类型和治疗)的关系。这是一项在单一中心进行的双视角研究。回顾了配对的原发性和复发性MBC患者的免疫组化(IHC)表达情况,分析了雌激素受体(ER)、孕激素受体(PR)、人表皮生长因子2 (HER2)和Ki-67的表达。根据ER、PR和HER2的Allred评分评估受体的一致性、缺失和获得。Ki-67基于14%的临界值进行评估。此外,研究了受体变化与年龄、绝经状态、形态、分级、分期、转移部位、活检间隔和治疗的关系。在进展时,41.18%的局部复发和58.82%的转移部位进行了活检。尽管ER和PR的差异高达47%和68.6%,但ER、PR和HER2的真实受体转化率分别为9.8%、21.56%和5.88%。年龄与ER不一致性有显著相关性(p = 0.029)。PR的丧失与Ki-67的增加显著相关。在所有转移部位中,肺与PR和Ki-67一致性显著相关(p = 0.008和p = 0.0425)。受体的不一致与活检部位(局部复发或转移部位)无关,也与活检间隔时间、既往化疗或激素治疗无关。总之,疾病的转移进展伴随着ER的年龄依赖性不一致。PR与ER相关的异常变化表明,与ER无关的通路可能影响MBC中PR的表达。此外,PR丢失与Ki-67增加的同时表明随着疾病进展具有侵袭性表型。因此,对样本进行受体表达的后续检测有助于确定预后和指导治疗决策。
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Study of Biomarker Discordance between Primary and Recurrent Sites and its Clinical Implications in Metastatic Breast Cancer : A Single Institutional Study from India
Abstract S. Shanthala Immunophenotypic discordance of receptors between primary and metastatic sites significantly impacts treatment outcomes. Current international guidelines recommend rebiopsy of accessible metastatic lesions to reassess tissue biomarkers. While existing literature on biomarker changes is conflicting and heterogeneous, similar studies on the Indian cohort of breast cancer patients are lacking. In this context, we aimed to evaluate the frequencies of biomarker changes between biopsies from primary and recurrent sites, and their association with various clinicopathological characteristics, including the type of metastasis and treatment in metastatic breast cancer (MBC) patients. This is an ambispective study performed at a single center. Immunohistochemical (IHC) expression of paired primary and recurrence samples of MBC patients was reviewed for the expression of estrogen receptor (ER), progesterone receptor (PR), human epidermal growth factor 2 (HER2), and Ki-67. Concordance, loss, and gain of receptors were assessed based on the Allred scores for ER, PR, and HER2. Ki-67 was assessed based on a 14% cutoff. Further, receptor changes were studied in relation to age, menopausal status, morphology, grade, stage, metastatic sites, interval between biopsies, and treatment. At progression, biopsies were obtained from 41.18% of locoregional recurrence and 58.82% of metastatic sites. Despite high discordance of 47% for ER and 68.6% for PR, true receptor conversion was observed in 9.8%, 21.56%, and 5.88% for ER, PR, and HER2, respectively. There was a significant correlation between age and ER discordance ( p  = 0.029). Loss in PR significantly correlated with a gain in Ki-67. Of all the metastatic sites, the lung was significantly associated with PR and Ki-67 concordance ( p  = 0.008 and p  = 0.0425, respectively). Discordance of receptors was neither related to the sites of biopsy (local recurrence or metastatic site) nor to the time interval between biopsies, prior chemotherapy, or hormone therapy. In conclusion, metastatic progression of the disease is accompanied by age-dependent discordance of ER. Unparalleled changes in PR in relation to ER suggest that ER-independent pathways may influence PR expression in MBC. Furthermore, the concurrence of PR loss with Ki-67 gain indicates an aggressive phenotype with disease progression. Hence, follow-up testing of samples for receptor expression is beneficial in determining prognosis and guiding therapeutic decisions.
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