Characterisation of HER2-Driven Morphometric Signature in Breast Cancer and Prediction of Risk of Recurrence

IF 2.9 2区医学 Q2 ONCOLOGY

Cancer Medicine Pub Date : 2025-04-17 DOI:10.1002/cam4.70852

N. M. Atallah, S. Makhlouf, M. Nabil, A. Ibrahim, M. S. Toss, N. P. Mongan, E. Rakha

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Abstract

Introduction

Human epidermal growth factor receptor 2-positive (HER2-positive) breast cancer (BC) is a heterogeneous disease. In this study, we hypothesised that the degree of HER2 oncogenic activity, and hence response to anti-HER2 therapy is translated into a morphological signature that can be of prognostic/predictive value.

Methods

We developed a HER2-driven signature based on a set of morphometric features identified through digital image analysis and visual assessment in a sizable cohort of BC patients. HER2-enriched molecular sub-type (HER2-E) was used for validation, and pathway enrichment analysis was performed to assess HER2 pathway activity in the signature-positive cases. The predictive utility of this signature was evaluated in post-adjuvant HER2-positive BC patients.

Results

A total of 57 morphometric features were evaluated; of them, 22 features were significantly associated with HER2 positivity. HER2 IHC score 3+/oestrogen receptor-negative tumours were significantly associated with HER2-related morphometric features compared to other HER2 classes including HER2 IHC 2+ with gene amplification, and they showed the least intra-tumour morphological heterogeneity. Tumours displaying HER2-driven morphometric signature showed the strongest association with PAM50 HER2-E sub-type and were enriched with ERBB signalling pathway compared to signature-negative cases. BC patients with positive HER2 morphometric signature showed prolonged distant metastasis-free survival post-adjuvant anti-HER2 therapy (p = 0.007). The clinico-morphometric prognostic index demonstrated an 87% accuracy in predicting recurrence risk.

Conclusion

Our findings underscore the strong prognostic and predictive correlation between HER2 histo-morphometric features and response to targeted anti-HER2 therapy.

Abstract Image

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乳腺癌中her2驱动的形态学特征表征及复发风险预测

人表皮生长因子受体2阳性（her2阳性）乳腺癌（BC）是一种异质性疾病。在这项研究中，我们假设HER2的致癌活性程度以及对抗HER2治疗的反应可以转化为具有预后/预测价值的形态学特征。方法：基于一组通过数字图像分析和视觉评估确定的形态学特征，我们开发了一种her2驱动的特征。使用HER2富集分子亚型（HER2- e）进行验证，并进行途径富集分析以评估特征阳性病例中HER2途径的活性。在辅助治疗后her2阳性BC患者中评估了这一特征的预测效用。结果共评估了57个形态学特征；其中22个特征与HER2阳性显著相关。HER2 IHC评分3+/雌激素受体阴性肿瘤与HER2相关的形态学特征显著相关，与其他HER2类别（包括HER2 IHC 2+基因扩增）相比，它们表现出最小的肿瘤内形态学异质性。与特征阴性的肿瘤相比，显示her2驱动形态特征的肿瘤与PAM50 HER2-E亚型的相关性最强，并且富含ERBB信号通路。HER2形态学特征阳性的BC患者在抗HER2辅助治疗后无远处转移生存期延长（p = 0.007）。临床形态学预测指数在预测复发风险方面准确率为87%。结论：我们的研究结果强调了HER2组织形态学特征与靶向抗HER2治疗反应之间的预后和预测相关性。

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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来源期刊

Cancer Medicine ONCOLOGY-

CiteScore

5.50

自引率

2.50%

发文量

907

审稿时长

19 weeks

期刊介绍： Cancer Medicine is a peer-reviewed, open access, interdisciplinary journal providing rapid publication of research from global biomedical researchers across the cancer sciences. The journal will consider submissions from all oncologic specialties, including, but not limited to, the following areas: Clinical Cancer Research Translational research ∙ clinical trials ∙ chemotherapy ∙ radiation therapy ∙ surgical therapy ∙ clinical observations ∙ clinical guidelines ∙ genetic consultation ∙ ethical considerations Cancer Biology: Molecular biology ∙ cellular biology ∙ molecular genetics ∙ genomics ∙ immunology ∙ epigenetics ∙ metabolic studies ∙ proteomics ∙ cytopathology ∙ carcinogenesis ∙ drug discovery and delivery. Cancer Prevention: Behavioral science ∙ psychosocial studies ∙ screening ∙ nutrition ∙ epidemiology and prevention ∙ community outreach. Bioinformatics: Gene expressions profiles ∙ gene regulation networks ∙ genome bioinformatics ∙ pathwayanalysis ∙ prognostic biomarkers. Cancer Medicine publishes original research articles, systematic reviews, meta-analyses, and research methods papers, along with invited editorials and commentaries. Original research papers must report well-conducted research with conclusions supported by the data presented in the paper.