Sensitivity of Contrast-Enhanced Breast MRI vs X-ray Mammography Based on Cancer Histology, Tumor Grading, Receptor Status, and Molecular Subtype: A Supplemental Analysis of 2 Large Phase III Studies

IF 1.8 Q3 ONCOLOGY

Breast Cancer : Basic and Clinical Research Pub Date : 2022-01-01 DOI:10.1177/11782234221092155

J. Endrikat, G. Schmidt, D. Haverstock, Olaf Weber, Z. Trnkova, J. Barkhausen

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引用次数: 2

Abstract

Background: The impact of certain tumor parameters on the sensitivity of imaging tools is unknown. The purpose was to study the impact of breast cancer histology, tumor grading, single receptor status, and molecular subtype on the sensitivity of contrast-enhanced breast magnetic resonance imaging (CE-BMRI) vs X-ray mammography (XRM) to detect breast cancer. Materials and Methods: We ran a supplemental analysis of 2 global Phase III studies which recruited patients with histologically proven breast cancers. The sensitivity of CE-BMRI vs XRM to detect cancer lesions with different histologies, tumor grading, single receptor status, and molecular subtype was compared. Six blinded readers for each study evaluated the images. Results were summarized as the “Mean Reader.” For each reader, sensitivity was defined as the proportion of detected lesions vs the total number of lesions identified by the standard of reference. Two-sided 95% confidence intervals were calculated for within-group proportions, and for the difference between CE-BMRI and XRM, using a normal approximation to the binomial distribution. Results: In 778 patients, 1273 cancer lesions were detected. A total of 435 patients had 1 lesion, 254 had 2 lesions, and 77 had 3 or more lesions. The sensitivity of CE-BMRI was significantly higher compared with XRM irrespective of the histology. The largest difference was seen for invasive lobular carcinoma (22.3%) and ductal carcinoma in situ (19%). Across all 3 tumor grades, the sensitivity advantage of CE-BMRI over XRM ranged from 15.7% to 18.5%. Contrast-enhanced breast magnetic resonance imaging showed higher sensitivity compared with XRM irrespective of single receptor expressions (15.3%-19.4%). The sensitivities for both imaging methods were numerically higher for the more aggressive ER– (estrogen receptor), PR– (progesterone receptor), and HER2+ (human epidermal growth factor receptor 2) tumors. Irrespective of molecular subtype, sensitivity of CE-BMRI was 14.8% to 18.9% higher compared with XRM. Conclusions: Contrast-enhanced breast magnetic resonance imaging showed significantly higher sensitivity compared with XRM independent of tumor histology, tumor grading, single receptor status, and molecular subtype. Trial Registration: ClinicalTrials.gov: NCT01067976 and NCT01104584.

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基于肿瘤组织学、肿瘤分级、受体状态和分子亚型的对比增强乳房MRI与x线乳房x线摄影的敏感性:对2项大型III期研究的补充分析

背景:某些肿瘤参数对成像工具灵敏度的影响尚不清楚。目的是研究乳腺癌组织学、肿瘤分级、单受体状态和分子亚型对乳腺磁共振造影(CE-BMRI)与x线乳房x线摄影(XRM)检测乳腺癌敏感性的影响。材料和方法:我们对2项全球III期研究进行了补充分析，这些研究招募了组织学证实的乳腺癌患者。比较CE-BMRI与XRM对不同组织学、肿瘤分级、单一受体状态、分子亚型的肿瘤病变的检测敏感性。每项研究有6名盲眼读者对图片进行评估。结果被总结为“平均读者”。对于每个阅读器，灵敏度定义为检测到的病变与参考标准确定的病变总数的比例。使用二项分布的正态近似，计算组内比例和CE-BMRI与XRM之间差异的双侧95%置信区间。结果:778例患者中检出1273个癌灶。1个病灶435例，2个病灶254例，3个及以上病灶77例。无论组织学如何，CE-BMRI的敏感性明显高于XRM。浸润性小叶癌(22.3%)和导管原位癌(19%)的差异最大。在所有3种肿瘤分级中，CE-BMRI相对于XRM的敏感性优势在15.7%至18.5%之间。与XRM相比，对比增强的乳房磁共振成像显示更高的灵敏度，而不考虑单一受体的表达(15.3%-19.4%)。对于侵袭性更强的ER -(雌激素受体)、PR -(孕激素受体)和HER2+(人表皮生长因子受体2)肿瘤，两种成像方法的敏感性在数值上都更高。无论分子亚型如何，CE-BMRI的敏感性比XRM高14.8%至18.9%。结论:与肿瘤组织学、肿瘤分级、单受体状态、分子亚型无关，乳腺磁共振增强成像的敏感性明显高于XRM。试验注册:ClinicalTrials.gov: NCT01067976和NCT01104584。

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

Breast Cancer : Basic and Clinical Research ONCOLOGY-

CiteScore

5.10

自引率

3.40%

发文量

审稿时长

8 weeks

期刊介绍： Breast Cancer: Basic and Clinical Research is an international, open access, peer-reviewed, journal which considers manuscripts on all areas of breast cancer research and treatment. We welcome original research, short notes, case studies and review articles related to breast cancer-related research. Specific areas of interest include, but are not limited to, breast cancer sub types, pathobiology, metastasis, genetics and epigenetics, mammary gland biology, breast cancer models, prevention, detection, therapy and clinical interventions, and epidemiology and population genetics.