Improved characterization of sub-centimeter enhancing breast masses on MRI with radiomics and machine learning in BRCA mutation carriers

This was a retrospective Health Insurance Portability and Accountability Act–compliant study conducted at Memorial Sloan Kettering Cancer Center. The study was approved by the Institutional Review Board (protocol number 19-119) and the need for written informed consent was waived.

A review of the Department of Radiology database was performed to identify consecutive patients with genetic testing results available and who had an MRI from November 2013 to February 2019 that led to a biopsy or a short-term follow-up. We identified 430 patients. Our inclusion criteria were as follows: BRCA 1– or BRCA 2–positive patients; breast masses with the longest diameter ≤ 10 mm; and BI-RADS 3, 4, or 5 on MRI further assessed with follow-up or vacuum-assisted breast biopsy (MRI or ultrasound-guided) yielding benign or malignant histology. Findings described as non-mass enhancements on MRI were not included. We excluded patients with mutations other than BRCA 1 and 2 and those with a follow-up of less than 2 years when biopsy was not performed (BI-RADS 3 and BI-RADS 4 when target was not visualized at the time of biopsy).

Breast MRI was performed on either a 1.5-T or a 3-T magnet (Sigma; GE) using an 8-channel or 16-channel dedicated surface breast coil. The imaging sequences are included in Table 1.

All images were independently assessed by two dedicated fellowship-trained breast radiologists in one session (R1: R.L., and R2: I.D., both with 4 years of experience in breast imaging and interpreting breast MRI) blinded to the final histopathological diagnoses and prior or subsequent conventional and MRI imaging. For each lesion, the following morphological features were assessed according to the BI-RADS lexicon on post-contrast-enhanced T1-weighted images: lesion shape, margin, and internal enhancement characteristics. Readers also assigned a BI-RADS classification. Lesion size was measured as the single largest diameter. On T2-weighted and DW images, signal intensity, morphology, background parenchymal enhancement (BPE), and fibroglandular tissue (FGT) for each breast were also assessed. Time–intensity kinetic curve analysis (signal enhancement in relation to time after contrast injection) was performed on a dedicated workstation with a commercially available computer-aided diagnosis system (OsiriX, OsiriX Foundation) by R1. The reader qualitatively measured the kinetic curve pattern described as washout, plateau, or persistent, according to the BI-RADS lexicon. The location of lesions within the breast (anterior, middle, or posterior depth) was also assessed by R1.

After independent review was conducted, the cases in which there was disagreement between the two readers were re-reviewed in consensus to generate an overall consensus assessment.

Preferentially, histopathology was used as the reference standard established by either image-guided needle biopsy or surgery. In two patients who had benign high-risk lesions on biopsy, the histological report from the surgical biopsy was recorded to confirm the benign nature of the lesion. When biopsy was not performed, stability of more than 2 years on follow-up MRI was considered benign.

Digital Imaging and Communications in Medicine (DICOM) images from the DCE-MRI and non-contrast-enhanced T1-weighted MRI were loaded into the open-source image processing tool OsiriX. Both radiologists reviewed the images in consensus before delineating the ROIs and R1manually delineated the ROIs, tracing the borders of each lesion to include the entire enhancing lesion.

Given the small size of the lesions sampled yielding a small number of pixels per slice, an in-house code written in MATLAB (The MathWorks, Inc.) was used to input the ROIs into the open-source CERR software environment (freely available through GitHub) which calculated the radiomics features [17]. Data was reduced to 16 gray levels and only an interpixel distance of one was considered (for small lesions, higher interpixel distances are not appropriate and would reduce counting statistics drastically). CERR analysis resulted in 102 radiomics features sub-divided into six categories: 22 first-order features, 26 features based on the gray level co-occurrence matrix (GLCM), 16 features based on the run length matrix (RLM), 16 features based on the size zone matrix (SZM), 17 features based on the neighborhood gray level dependence matrix, and 5 features based on the neighborhood gray tone difference matrix. Since patients were scanned at either 1.5 T (27 benign cases and 17 malignant cases) or 3 T (49 benign cases and 23 malignant cases), ComBat harmonization (Supplemental Info A1) was employed prior to statistical analysis to remove center effects [18].

Univariate analysis was initially performed to select significant radiomics features able to differentiate between benign and malignant lesions. An AUC cutoff of ≥ 0.65 was used to reduce the number of features of interest. Correlation analysis was then employed to further remove redundant features. For any significant correlations in which the Spearman rank correlation coefficient > 0.9, the feature with the lowest AUC was removed from consideration. This resulted in a more manageable number of features for subsequent multivariate modeling. Using a fine Gaussian support vector machine, perfect separation of benign and malignant cases was obtained. To limit data overfitting, a fivefold cross-validation was employed to develop a robust ML model which should produce similar results for new data.

Statistical analysis was conducted using SAS (version 9.4, SAS Institute). Continuous variables were summarized using means (± standard deviation) and medians (range); categorical variables were summarized using proportions. Univariate analysis using the chi-square test or Fisher’s exact test was performed to assess associations between the imaging parameters (from independent and consensus assessment) with disease status (malignant vs. benign). p values < 0.05 were considered significant. To determine inter-observer agreement, weighted Cohen’s κ was used to assess ordinal parameters, while simple Cohen’s κ was used to assess the inter-reader agreement for nominal parameters.

For radiomics data, statistical analysis was performed using SPSS (version 25, IBM Corp.) and MATLAB (R2017b, The MathWorks, Inc.). Univariate analysis was performed to identify radiomics features that were significantly different between malignant and benign lesions. Since the number of patients was not large (especially in the malignant cohort), normality in the malignant and benign cohort distributions was tested using the Shapiro–Wilk test and Q-Q plots. For a minority (21/102) of normally distributed features, a two-tailed independent t test was used to determine the significant features. For the majority of non-normally distributed features (81/102), the Mann–Whitney U test for two independent samples was used to determine the significant features.

The study population included 96 patients (Fig. 1).

Table 2 and Fig. 2 show the patient and breast lesion characteristics. Figures 3 and 4 are examples of benign and malignant breast masses included in this study. After segmentation, the median benign lesion size was 514.5 pixels (range 85–2425 pixels) and the median malignant lesion size was 816 pixels (range 66–2116 pixels).

Table 3 shows the results from univariate analysis according to independent assessments by the two radiologists.

Table 4 shows the results from univariate analysis according to overall consensus assessment as well as according to singular assessment performed for kinetics and lesion location, BRCA mutation status, and menopausal status. In consensus reading, there was no significant association with disease status based on margin (p = 0.11), shape (p = 0.97), enhancement pattern (p = 0.05), T2 signal intensity (p = 0.16), DWI (p = 0.54), BPE (p = 0.32), and BRCA mutation status (BRCA1 vs. BRCA2, p = 0.79). There was a statistically significant association with disease status based on lesion location within the breast (p = 0.03), menopausal status (p = 0.0001), and BI-RADS classification (p < 0.001).