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Clinical experience of the first digital mammographic unit in Australia in its first year of use

Emma Pun, W F Eddie Lau, Robin Cassumbhoy, Anthony J Taranto and Alexander G Pitman
Med J Aust 2007; 187 (10): 576-579. || doi: 10.5694/j.1326-5377.2007.tb01420.x
Published online: 19 November 2007

Abstract

More than one in eight women will develop breast cancer in their lifetime,1 and it is the most common cause of cancer mortality in Australian women.2 Mammography remains the mainstay of early breast cancer diagnosis, and its performance depends on image quality.3 Mammographic screening has been in use for 20–30 years,4 and reduces breast cancer mortality in women aged 40 years and over.5,6 In women aged 50–69 years, mortality decreases by 20%–35% at 14 years of follow-up; efficacy in 40–49-year-old women is slightly lower.7

A technical limitation of conventional screen-film mammography (CM) occurs when there is insufficient contrast in radiographic density between normal breast parenchyma and cancer. About 10%–20% of palpable breast cancers are not visible on CM for this reason.8 As women age, less dense breast fat replaces normally dense breast parenchyma, so density contrast limitations have a greater impact on younger women.

Digital mammography (DM) has demonstrated superior diagnostic accuracy over CM for cancer detection in women with dense breasts and women under 50 years old, and evidence exists for its superior demonstration of microcalcifications.9-11 About 8% of facilities in the United States have now converted from CM to DM,12 and the number is growing.

Peter MacCallum Cancer Centre (“Peter Mac”) is a quaternary specialist teaching hospital affiliated with the University of Melbourne and is Australia’s only stand-alone dedicated oncology centre. Its breast service provides diagnostic, surgical, radiation and medical oncological care to breast cancer patients. Peter Mac’s Familial Cancer Clinic (FCC) is Australia’s largest screening facility for women at high genetic risk of breast cancer; Peter Mac is not a BreastScreen centre.

In April 2004, Peter Mac became the first site in Australia to offer DM. Here, we report on the first year of its use at our centre.

Our early experience
Evolving management of microcalcifications

In some of our diagnostic DM studies, we found that comparison with the patient’s earlier CM imaging showed a greater number or a more extensive distribution of microcalcifications. Microcalcifications may be a manifestation of ductal carcinoma-in-situ (DCIS). They are classifiable as malignant, indeterminate or benign, depending on individual microcalcification and cluster morphology. All else being equal, progression of microcalcifications is also suspicious for malignancy. However, because DM has been shown to demonstrate microcalcifications better than CM,9-11 two explanations were possible in these women:

We therefore developed a unit policy designed to determine which of these two explanations applied to individual patients. Cases where the reading radiologist considered the microcalcifications to have malignant individual or cluster morphology, or considered the interval progression of indeterminate microcalcifications to be suspicious for cancer, were recommended for stereotactic biopsy. If a unit review by the breast surgeon (and sometimes an external radiologist from BreastScreen) supported the reader’s opinion, a biopsy was performed (Group A). In cases where the new microcalcifications found on DM lacked any individual suspicious morphology (as decided either by the reader or unit review), our policy was to bring the patient back for a 6-month comparison study to confirm microcalcification stability (Group B).

Implications

In adopting DM, we took technical, practical and other considerations into account.

Technical considerations

DM offers several technical advances over CM. In CM, the breast image is created directly on mammographic x-ray film, which acts as the sole vehicle for the three imaging steps: acquisition, display and storage. Overall image quality is a compromise between these steps. Once acquired, the image cannot be altered. Traditional methods of improving a reader’s viewing performance are a very dark room, a handheld loupe and a bright light.14 If greater magnification is required, the patient has to return for focal compression magnification views (with further radiation exposure).

In DM, the steps of image acquisition, display and storage are separated, allowing optimisation of every step.15 DM images are acquired in the same way as CM, but a digital detector replaces the x-ray film cassette. Unlike CM, DM allows manipulation of the stored image. The reader can adjust contrast and intensity, and magnify and move the image, all without acquiring further views (Box 4). Since a digital mammogram is a data file, it can be copied, sent via a network, burned to CD or printed on a mammographic-quality x-ray laser printer. Multiple copies can be reviewed simultaneously at different sites. The capacity for the technologist to immediately view the acquired images for quality assurance and to transmit the data files to a central reading site could make DM an excellent choice for mobile BreastScreen units operating in rural and remote areas.

Clinical considerations

The sensitivity of DM is at least equal to CM for detection of breast cancer.17-21 A recent study of over 49 000 women showed DM to be more diagnostically accurate than CM in women under 50 years of age, women with radiographically dense breasts and pre- or peri-menopausal women.21 Underlying this clinical finding is the proven superior contrast resolution of DM, giving it maximal impact in radiographically dense breast tissue that may mask a dense cancerous mass.22 In our patient cohort, we subjectively found that imaging of dense breasts improved with DM compared with CM (Box 5). With growing debate about whether to invite women aged 40–49 years to screening by BreastScreen, the greater accuracy of DM in dense breasts is particularly pertinent.23

Further, evidence is mounting that DM may provide superior image quality at an equal or lower breast glandular dose than CM.8,21 This matters particularly for women at high genetic risk of breast cancer, who may undergo frequent mammographic screening from a relatively young age.

Evidence is also accumulating in radiological literature that DM is superior to CM for demonstration of microcalcifications.9-11 Box 6 demonstrates the example of a woman referred for HNL and wide local excision of DCIS, where DM showed a more extensive distribution of malignant calcifications, thus necessitating a change in management to mastectomy.

Our microcalcification follow-up data strongly suggest that new indeterminate microcalcifications found on initial DM largely reflect the greater detection ability of DM over CM rather than progressive microcalcification. Of the 56 women with new microcalcifications detected, only four had a malignant or premalignant histology, and 35 of 38 without malignant morphology had stable imaging findings on follow-up. As a result of these findings, our unit policy is now to treat any new microcalcifications found on DM (when compared with prior CM) solely on the individual and cluster morphology of the microcalcification. Accordingly, we recommend that where such microcalcifications have no individual suspicious morphological features or suspicious clustering characteristics, routine mammographic review with DM, rather than biopsy, is appropriate management.

  • Emma Pun1
  • W F Eddie Lau1
  • Robin Cassumbhoy1
  • Anthony J Taranto1
  • Alexander G Pitman2

  • 1 Department of Diagnostic Imaging, Peter MacCallum Cancer Centre, Melbourne, VIC.
  • 2 Department of Medical Imaging, St Vincent’s Hospital, Melbourne, VIC.


Correspondence: Eddie.Lau@petermac.org

Acknowledgements: 

We are grateful to BreastScreen Victoria, St Vincent’s Health (Associate Professor Jennifer Cawson, Chief Radiologist) for providing backup mammographic service during Peter Mac’s changeover from CM to DM. We acknowledge Associate Professor Cawson’s help and support as our external reference breast radiologist during the subsequent setup and validation of our DM service.

Competing interests:

None identified.

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