MR-guided vacuum-assisted breast biopsy of MRI-only lesions: a single center experience

This retrospective single-center study was institutional review board (IRB)-approved and informed consent was waived. In our tertiary care breast cancer assessment center, we collected data from the institutional database for all consecutive women with non-palpable MRI breast lesions that were occult both on mammography and ultrasound, and for whom successful MR-guided biopsy was performed due to suspicious (BI-RADS 4 or 5) findings on CE-MRI. MRI-only cases were included in which a final diagnosis had been established either by open surgery, in case of malignant and high-risk lesions, or imaging follow-up, in case of benign lesions. A minimum of 12 months imaging follow-up, to establish a standard of reference, has been applied [21, 22].

There were 467 consecutive patients (mean age 52, range 18–87 years) who underwent 487 MR-guided biopsies in our department during 11/2006 to 7/2013 and who were included in this study (Fig. 1).

All MR-guided biopsies were performed on a 1.5-Tesla (T) system (Magnetom Avanto, Siemens Medical Solutions®, Erlangen, Germany) using a dedicated double breast imaging and intervention coil (InVivo, Philips, Netherlands). A short imaging protocol for lesion localization, consisting of a dynamic contrast-enhanced T1-weighted, spoiled gradient echo (fast low angle shot, FLASH-3D) sequence [repetition time/echo time (TR/TE) 11/4.76 ms; spatial resolution 0.7 × 0.7 × 3 mm; 64 slices; acquisition time 58 sec] was acquired before and repeated once or twice after the intravenous (IV) application of 0.15 mmol/kg body weight of Gd-DOTA (Dotarem, Guerbet, France) with an automatic injector (Spectris, Medrad, Germany) at 3 ml/s. Automatically scaled subtraction images were obtained by subtracting pre-contrast images from post-contrast images using the vendor-supplied software.

Intervention planning was performed without additional software by manually referencing the MRI lesion localization to that of an MRI-compatible marker with positive T1-weighted contrast. After obtaining written, informed consent for the procedure, vacuum-assisted biopsy using three different 8- to 10-gauge devices (Vacora [V], Bard Biopsy Systems, Tampa, USA; Mammotome [M], Devicor Medical Products, Cincinnati, USA; or ATEC [A], Hologic, Indianapolis, USA) was performed by one of four experienced, board-certified radiologists (T.H.H., K.P, P.K., B.A.T.). The following needles were used for A (9-gauge Atec MRI needle, Hologic, Indianapolis, USA), M (8-gauge MRI needle, Devicor Medical Products, Cincinnati, USA), V (10-gauge MRI needle, Bard Biopsy Systems, Tampa, USA). The following markers were used for A (Atec TriMark, Hologic), M (Mammomark 3.5 mm, Devicor Medical Products) and V (BiomarC 1 × 5 mm, Carbon Medical Technologies, MI, USA). M and A are MR-guided, console-based vacuum biopsy systems, whereas V is a hand-held vacuum biopsy system. All radiologists performed at least 20 MR-guided biopsies with each respective device. One radiologist who had performed more than 200 MR-guided biopsies in different institutions using different devices supervised the first 15 cases of the other 3 radiologists. The selection of each device was based solely on its availability during the study period and never on lesion type or needle size.

The FLASH-3D sequence above was repeated to verify needle positioning during the procedure. The number of samples obtained was 12–24, depending on lesion size and location [23]. The biopsy site was marked with MRI-compatible clip markers. To verify biopsy site and clip position and to exclude potential complications, such as major bleeding, a final FLASH-3D sequence was obtained. The results of histopathological analysis, which was performed by an experienced, board-certified breast pathologist (M.R.), were compared with the MR imaging results in interdisciplinary consensus. The B classification was applied for histological diagnosis [24]. In cases of discrepancy between imaging and histopathology, and in case of lesions with uncertain malignant potential (B3), open biopsy was performed after wire localization by board-certified, experienced breast surgeons. In case of a benign finding, there was MR imaging follow-up of at least 12 months. Reasons for surgery on a benign VABB result were suspicion of poor targeting, e.g. epithelial hyperplasia without atypia as histological diagnosis on MR-guided VABB when a solid mass lesion was seen on MRI — such findings are deemed discrepant and usually undergo surgery in our department.