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Mammographic and Ultrasound Analysis of Breast Masses


A breast mass is one of the most frequent presenting features of breast carcinoma. Benign masses usually have round or oval shapes with pushing or circumscribed borders and do not invade normal surrounding tissue. Malignant masses are often irregularly shaped with indistinct or spiculated margins produced by the tumor infiltrating adjacent normal tissue. Thus radiologists look carefully at mass shapes and margins to determine whether the mass is malignant.

Ultrasound (US) goes hand-in-hand with mammography in breast mass evaluation and shows whether the mass is cystic or solid. US provides real-time evaluation of mass shapes, borders, orientation, and internal characteristics to determine whether the mass is malignant or benign. Detailed principles and interpretation of ultrasonography are explained further in Chapter 5 . This chapter reviews mammographic and US analysis of breast masses.

Mammography for Evaluating Nonpalpable Masses, Asymmetries, and Palpable Masses

In asymptomatic women, screening mammography is a primary screening method for breast cancers in women 40 years of age or older and potentiates the detection of early, clinically occult cancers. When screening mammography detects suspicious findings, such as masses, focal asymmetries, and architectural distortion, diagnostic mammography is generally performed for further evaluation of nonpalpable mammographic findings, as detailed in the American College of Radiology (ACR) Appropriateness Criteria for Nonpalpable Mammographic Findings.

In women with clinically detected palpable masses, diagnostic mammography is the initial imaging modality of choice for evaluating the palpable breast masses in those 40 years of age or older, as indicated in the ACR Appropriateness Criteria for Palpable Breast Masses ( ). For women 30 to 39 years old, either diagnostic mammography or US may be used for initial evaluation, but US is the initial imaging modality in a woman younger than 30 years old.

A true mass is a ball-shaped object that is approximately the same size, shape, and density in orthogonal mammographic projections. Radiologists detect masses because they are whiter than surrounding fibroglandular tissue, are an asymmetric finding compared with the contralateral breast, or display unique distinguishing characteristics from normal background tissue. For example, masses may have distinct edges, are higher density (whiter) than surrounding tissue, are new, or have spiculated margins that make them unique from normal breast tissue.

On two-dimensional (2D) mammography, the radiologist first detects masses because they are different from the surrounding tissue by a distinct mass edge, have higher density, have interval appearance, have architectural distortion, or because there is an asymmetry ( Fig. 4.1 ). The radiologist determines whether the finding is a true mass or overlapping fibroglandular tissue (a fake mass) using mammographic techniques described in Chapter 2 . If the finding is a true mass, the radiologist triangulates its position in the breast and then uses 2D fine-detail spot compression magnification mammography to characterize the mass’ shape, margin, and associated findings such as calcifications ( ). Two-dimensional mammography shows mass shapes and borders best when the mass is displayed against fat, thus, the optimal projection to perform spot magnification mammograms is where the mass lies in fat. If the mass is present or is still suspected, radiologists use US to confirm or exclude a mass lesion and to determine whether detected masses require a histologic diagnosis.

FIG. 4.1, Mammographic technique for evaluating masses. (A and B) Paired 2D mediolateral oblique (MLO) (A) and craniocaudal (B) mammogram show a possible spiculated mass ( arrow ) that overlies fibroglandular tissue. (C) Right MLO tomosynthesis slice (see also Video 4.1 ) shows the mass and spiculations. Note the mass and fibroglandular density contrast has a more narrow gray scale than the 2D mammogram, and the spiculations are enhanced by the reconstruction algorithm. (D) The corresponding ultrasound shows a hypoechoic mass with indistinct margins. (E) Two-dimensional lateromedial mammogram after biopsy with marker placement shows a metallic marker within an air bubble, showing the final location of the biopsied mass in the upper right breast. Biopsy showed invasive lobular carcinoma.

Radiologists reading 2D mammograms often struggle with findings seen on only one standard mammographic projection. Their dilemma is whether the one-view finding is a fake mass produced by overlapping normal tissue, called a summation artifact , or if it is a real mass hidden on the orthogonal view. One-view findings are often focal densities (a white finding that is whiter than the background tissue) called asymmetries, because the focal density is whiter than a mirror image area on the contralateral side. A study by shows that greater than 80% of mammographic asymmetries at screening are summation artifacts. His large prospective study of 61,273 screening mammograms showed that 3.3% (2023 cases) of mammographic screens had one view–only findings. Dr. Sickles’ analysis showed that 54.7% (1086/2023 cases) of one-view findings were confidently dismissed as overlapping tissue by simply seeing the orthogonal view, whereas 29% (587/2023) were recalled and dismissed as normal after diagnostic imaging. None of these findings were cancer at follow-up. In the remaining 36 cases, cancer was found at diagnostic imaging, and 33% of these cancers were lobular cancer. The 2D diagnostic mammographic methods to determine whether one-view findings are masses or normal tissue include repeating the same mammographic view to see if the finding persists, comparing studies with old mammograms, or a 2D diagnostic fine-detail workup including 2D rolled mammographic views, spot compression or spot compression magnification views, and step oblique mammography ( ; Sickles, 2007; ). Targeted US ( ) and tomosynthesis ( ) can also be especially helpful to detect true masses. The Breast Imaging Reporting and Data System (BI-RADS) 2013 definitions of asymmetries and their workup will be discussed in the next section, and the remainder of this section will concentrate on true masses.

Breast tomosynthesis is a useful technique for evaluating masses and possible masses (see Fig. 4.1C ; see ). Studies show that breast tomosynthesis has an advantage over digital mammography in breast cancer diagnosis, with higher cancer detection rates and lower patient recall rates at screening ( ). In the diagnostic setting tomographic slices detect masses hidden on 2D mammograms by uncovering overlapping breast tissue. Tomosynthesis also displays morphologic mass features, helps localize masses, characterizes mass features, and shows the extent of disease in malignancies ( ). In both the screening and diagnostic settings, tomosynthesis also helps clarify if a suspected mass or asymmetry represents a true mass or a summation artifact ( ), resulting in decreased screening recall rates of 15% to 17% in published studies ( ). Tomosynthesis at diagnostic workup is especially helpful to characterize masses that may not show on 2D spot compression ( ) and to localize lesions for US targeting for biopsy ( ; see Fig. 4.1 D–E ).

In contrast, tomosynthesis does not show all masses, particularly masses that have a round shape, are circumscribed, or have an indistinct border in a dense breast. Masses are detected against mammographic backgrounds if they have unique imaging characteristics distinct from the surrounding tissue such as spiculated margins or pleomorphic calcifications. Tomosynthesis is exquisitely sensitive for mass spiculations (see Fig. 4.1C ; see ). Masses not seen by tomosynthesis usually are equal density to normal breast tissue and have nonspiculated borders that blend in with the surrounding tissue so there is no distinct mass margin detectable against the normal breast background ( ). Similar to the silhouette sign of pneumonia against the heart border, a nonspiculated breast mass edge is obscured or silhouetted by glandular tissue, making the mass undetectable. In Andersson’s series, cancers missed by tomosynthesis were found because the patient felt something or the cancer was detected by US or magnetic resonance imaging (MRI). Clinically, this means that palpable findings should undergo US even if the tomosynthesis is negative, especially if the finding lies within dense tissue. The corollary is that a highly suspicious US or MRI finding should undergo histologic sampling even if 2D mammogram or tomosynthesis studies are negative.

Both diagnostic 2D mammography and tomosynthesis are commonly used to evaluate palpable masses under a radiologist’s supervision, as detailed in the ACR Appropriateness Criteria for Palpable Breast Masses ( ). Usually, a technologist places a radiopaque skin marker over the palpable finding and obtains standard craniocaudal and mediolateral views including the marker to show the palpable finding. Special fine-detail mammograms (tangential views, spot compression, or magnification views) may show more detail of the palpable finding. US is used commonly to evaluate palpable breast masses and is the initial imaging modality of choice for women under the age of 30, whereas either diagnostic mammography or US is used as the initial examination for women 30 to 39 years of age. Further details of diagnostic workups of palpable masses are described in later.

Description of Masses, Asymmetry, and Architectural Distortion Based on Breast Imaging Reporting and Data System 2013 Mammography

Masses

The ACR BI-RADS lexicon defines a breast mass as a three-dimensional (3D) space-occupying lesion seen on at least two mammographic projections. Mass shapes are categorized as oval, round, or irregular ( Figs. 4.2 and 4.3 ; Table 4.1 ). The probability of cancer increases as the mass shape becomes more irregular.

FIG. 4.2, Schematic of mass shapes: oval, round, and irregular. An oval mass is elliptical and can have two or three undulations. A round mass is spherical in shape. An irregular mass usually implies a suspicious lesion.

FIG. 4.3, Mass shapes: oval, round, and irregular. (A) Oval shape. Mammogram shows a low-density oval mass with circumscribed margins representing a simple cyst. Incidentally noted are scattered benign round/punctate calcifications in the breast tissue. (B) Round shape. Mammogram shows a high-density round mass with mostly circumscribed ( arrow ) and partly indistinct ( double arrow ) borders, representing invasive ductal cancer. (C) Irregular shape. Mammogram shows a palpable high-density irregular mass in the upper breast marked with a skin marker that has partly spiculated and indistinct margins ( arrow ) and obscured borders on its inferior aspect ( double arrows), representing invasive ductal cancer.

TABLE 4.1
American College of Radiology 2013 Breast Imaging Reporting and Data System Mammography Lexicon Descriptors for Masses
From American College of Radiology: ACR BI-RADS ® —Mammography. In ACR BI-RADS atlas, breast imaging reporting and data system , ed 5, Reston, VA, 2013, American College of Radiology.
Shape Oval Elliptical or egg-shaped (may include 2–3 undulations)
Round Spherical, ball-shaped, circular, or globular
Irregular Neither round nor oval
Margin Circumscribed At least 75% of the margin is sharply demarcated, with an abrupt transition between the lesion and surrounding tissue
Obscured 25% or more of the margin is hidden by superimposed or adjacent fibroglandular tissue
Microlobulated A margin characterized by short-cycle undulations
Indistinct No clear demarcation of the entire margin or any portion of it from the surrounding tissue
Spiculated Margin is characterized by lines radiating from the mass
Density High density X-ray attenuation of the mass is greater than the expected attenuation of an equal volume of fibroglandular breast tissue
Equal density X-ray attenuation of the mass is the same as the expected attenuation of an equal volume of fibroglandular breast tissue
Low density X-ray attenuation of the mass is less than the expected attenuation of an equal volume of fibroglandular breast tissue
Fat containing Includes all masses containing fat, such as oil cyst, lipoma, or galactocele, as well as mixed-density lesions such as hamartoma

The ACR BI-RADS lexicon defines mass margins as circumscribed (well defined or sharply defined), microlobulated, obscured by surrounding glandular tissue, indistinct, or spiculated ( Fig. 4.4 ; see Table 4.1 ). As the mass margin becomes more spiculated, the probability of cancer increases. Masses with well-circumscribed borders are more likely to be benign ( Fig. 4.5 ; ). Sharply marginated borders indicate no invasion of the surrounding tissue; few cancers have smooth, well-circumscribed borders. An obscured mass has a border hidden by overlapping adjacent fibroglandular tissue, and that border cannot be assessed ( Fig. 4.6 ). Microlobulated masses have small border undulations, like petals on a flower, and are more worrisome for cancer than are masses with circumscribed margins ( Fig. 4.7 ). An indistinct mass has a margin that can be seen but is fuzzy. Indistinct margins are worrisome for carcinoma because the fuzzy border suggests tumor infiltration of surrounding tissue ( Fig. 4.8 ). Finally, spiculated masses are characterized by thin lines radiating from the central portion of the mass and are especially worrisome for cancer ( Fig. 4.9 ; ). When caused by cancer, mass spiculations are caused by productive tumor fibrosis (desmoplastic reaction) or actual tumor infiltration. Tomosynthesis and the synthesized mammograms reconstructed from the tomosynthesis slices are especially sensitive for detecting spiculated masses ( Fig. 4.10 ; ).

FIG. 4.4, Schematic of mass margins: circumscribed, obscured, microlobulated, indistinct, and spiculated. A circumscribed margin is sharply demarcated from the surrounding tissue. Obscured, is used when more than 25% of the entire margin of a mass is hidden by overlapping or adjacent tissue; this descriptor is used usually when the remaining unhidden mass margins are circumscribed. Margins with short-cycle undulations are described as microlobulated margins. When no clear demarcation of the entire margin is seen, the margin is categorized as indistinct (historically “ill-defined”). Spiculated margins are those with thin lines radiating center of the lesion, usually indicating cancer. The probability of cancer increases as mass margin progresses from circumscribed to spiculated.

FIG. 4.5, Mass margin: circumscribed. (A) Photographically magnified mammogram shows a mass with a circumscribed margin. The most of the margin is sharply defined. Part of the margin is obscured by overlapping breast tissue, but is limited to less than 25%, making the use of the descriptor circumscribed appropriate. (B) With tomosynthesis, the entire circumscribed margin is more easily visible (see Video 4.2 ). (C) Ultrasonography shows that the corresponding mass is oval, hypoechoic, and has a circumscribed margin with posterior acoustic enhancement. Pathology was fibroadenoma.

FIG. 4.6, Mass margin: obscured. (A) Photographically magnified mammogram shows a round high-density mass. The identifiable parts of the margin are circumscribed ( arrowheads ), but more than 25% of the margin is obscured by overlapping breast tissue. Thus the use of the descriptor obscured is appropriate for this mass. (B) The corresponding ultrasonography shows an irregular, hypoechoic mass with circumscribed superficial and deep margins, and an angular margin ( arrow ) that is suspicious for malignancy. Biopsy showed invasive ductal carcinoma.

FIG. 4.7, Mass margin: microlobulated. (A) Photographically magnified mammogram shows a high-density, round irregular mass with microlobulated margins. (B) The corresponding ultrasound shows a hypoechoic irregular mass with microlobulated margins. Biopsy showed invasive ductal carcinoma.

FIG. 4.8, Mass margin: indistinct. (A) Craniocaudal mammogram shows a round mass in the medial left breast ( arrow ). The differential is a focal area of glandular tissue, a cyst, or a solid mass. (B) Magnification mammogram shows the mass has indistinct margins rather than circumscribed borders ( arrow ). This shows the importance of fine-detail views and of being suspicious of medial breast masses. A biopsy showed invasive ductal cancer.

FIG. 4.9, Mass margin: spiculated. (A) Photographically magnified mammogram shows an irregular mass with a spiculated margin characterized by numerous fine lines radiating from the mass. There are a few associated pleomorphic calcifications along the superior margin. (B) Tomosynthesis (see ) visualizes the radiating lines from the mass with less overlapping tissue. (C) Corresponding ultrasound shows a hypoechoic irregular mass with spiculated and indistinct margins. Biopsy showed invasive ductal carcinoma.

FIG. 4.10, Spiculation and distortion shown better on synthesized views and tomosynthesis. (A) Craniocaudal (CC) 2D mammogram of dense tissue shows possible spiculation and flattening of the normally scalloped glandular tissue edge of the outer left breast. (B) Synthesized 2D CC mammogram reconstructed from tomosynthesis slices shows distortion ( arrows ) in the outer breast better than the conventional 2D mammogram. (C) Tomosynthesis slice shows a spiculated mass ( arrows ) in the outer left breast, causing the distortion and flattening of the adjacent tissue, better than on conventional 2D (A) or synthesized 2D mammograms (B). Biopsy showed invasive lobular cancer (see also ).

Mass density describes the mass whiteness compared with an equal volume of fibroglandular tissue ( Figs. 4.11 and 4.12 ; see Table 4.1 ).

FIG. 4.11, Schematics of mass density. Mass density is classified as high, equal, and low density based on the relative mass density compared with an equal volume of normal breast tissue. A fat-containing mass contains very low density identical to fat density ( arrow ). The fat density may comprise the entire mass, such as an oil cyst or lipoma, or part of the mass, as in a lymph node or hamartoma.

FIG. 4.12, Mass density: high-density, equal-density, low-density, and fat-containing masses. (A) Mammogram shows a high-density mass ( arrow ) with spiculated margins, representing invasive ductal cancer. (B) Equal density. Mammogram shows an equal-density oval mass with mostly circumscribed margins, representing invasive ductal cancer. (C) Low density. Mammogram shows a low-density mass adjacent to the pectoralis ( arrow ), representing a simple cyst. Note scattered benign round/punctate calcifications in the breast tissue. (D) Fat containing. Spot compression magnification view shows a fat-containing, thin-walled mass with a radiolucent center and faint calcifications along its rim ( arrow ) in the area of a previous biopsy, representing an oil cyst.

High-density masses are whiter than fibroglandular tissue, and low-density masses are darker than fibroglandular tissue. High-density masses are especially worrisome for cancer, because they may contain cells with a higher atomic number than normal glandular tissue and fat. Low-density masses and masses with density equal to that of surrounding fibroglandular tissue are less worrisome for cancer. However, low-density cancers, such as mucinous cancers, do exist and mimic breast cysts. These cancers are low density because they contain mucin, which is fluid density.

Fat-containing masses on 2D mammography are almost always benign, except for the rare liposarcoma or tumors surrounding fat on tomosynthesis. Fat-containing masses include lymph nodes, oil cysts (see Fig. 4.12D ), hamartomas, and fat necrosis, all of which are benign. However, tomosynthesis may show fat in both benign and malignant masses, and the fat seen on tomosynthesis may not be evident on 2D mammography ( ). Cancers may appear to contain fat if the cancer shape is very irregular and has trapped fat in between arms of the tumor. This means that the old mammographic rule that masses containing fat are always benign does not apply to tomosynthesis. To avoid misdiagnosis of cancers that contain fat on tomosynthesis slices, radiologists analyze the mass for suspicious margins or shapes and proceed with biopsy based on the worst mass features, even if the mass contains fat (see section: Masses Containing Fat ).

Asymmetry

The ACR BI-RADS mammography lexicon term asymmetry is used for mammography and not for US or MRI, although enhancing findings at MRI may be called symmetric or asymmetric. On mammography, asymmetries are white areas, more in one breast than in the other, and may represent asymmetric fibroglandular tissue or masses obscured by adjacent tissue. The finding must be included in the field of view on two orthogonal projections to qualify as an asymmetry. Asymmetries themselves do not qualify as masses on mammography. The ACR lexicon divides asymmetries into four categories: asymmetry, global asymmetry, focal asymmetry , and developing asymmetry ( Table 4.2 ; Fig. 4.13 ). A focal asymmetry and developing asymmetry have a higher likelihood of representing true masses, including breast cancer.

TABLE 4.2
American College of Radiology Breast Imaging Reporting and Data System Mammography Lexicon Descriptors for Asymmetry
From American College of Radiology: ACR BI-RADS ® —Mammography. In ACR BI-RADS atlas, breast imaging reporting and data system , ed 5, Reston, VA, 2013, American College of Radiology; Leung JWT, Sickles EA. Developing asymmetry identified on mammography: correlation with imaging outcomes and pathologic findings. AJR Am J Roentgenol 188:667–675.
Asymmetry An area of fibroglandular-density tissue that is seen in one standard mammographic view and likely represents summation
Global asymmetry An area of fibroglandular-density tissue that occupies at least one quadrant and likely represents normal asymmetry between breasts
Focal asymmetry An area of fibroglandular-density tissue that is seen in two mammographic views but does not fulfill criteria of mass
Developing asymmetry A focal asymmetry that is new, larger, or more conspicuous than on a previous examination, 15% are cancer ( )

FIG. 4.13, Schematics of asymmetry: asymmetry, global asymmetry, focal asymmetry, and developing asymmetry.

The first category of asymmetries is asymmetry , which is a small area (less than one quadrant of the breast volume) of fibroglandular-density tissue seen only on one mammographic projection. The asymmetry is either invisible or looks like normal fibroglandular tissue on the orthogonal view. Most one-view asymmetries represent overlapping tissues producing a “fake mass” or summation artifact ( Fig. 4.14 ; ).

FIG. 4.14, Asymmetry: asymmetry—summation artifact, stable. (A and B) Paired mediolateral oblique (A) and craniocaudal (CC) (B) screening mammograms shows an asymmetry ( arrow ) in the left inner breast that is visible only on left CC view. (C–E) Photography magnified left CC views of annual screening mammograms (2-year [C] and 1-year [D] prior studies and the current study [E]) show this one-view asymmetry has been stable over years, which supports the diagnosis as a summation artifact of normal breast tissue. (F) On tomosynthesis (photography magnified left CC projection), this asymmetry has no central density, unlike a typical mass (see also ).

Because some asymmetries proved to be cancer, radiologists often recalled women with asymmetries from 2D screening mammography. Breast tomosynthesis decreases asymmetry recalls from screening because tomosynthesis either shows the mass as a true finding by removing glandular tissue in front of and behind the mass, or proves that the mass is fake, comprised of superimposed tissue on contiguous slices (see Fig. 4.14 ; see ). However, not all asymmetries that persist as asymmetries/possible masses on tomosynthesis are true masses on workup. A possible mass may represent a summation artifact even on tomosynthesis, especially if there is suboptimal compression. These summation artifact asymmetries will spread out into their normal glandular components if there is sufficient compression, as with spot compression tomosynthesis ( Fig. 4.15 ; ). This means that tomosynthesis examinations require good compression to correctly demonstrate asymmetries as normal overlapping glandular tissue.

FIG. 4.15, Asymmetry: asymmetry—summation artifact. (A and B) Paired mediolateral oblique (A) and craniocaudal (CC; B) screening mammograms show an asymmetry ( box ) in the inner right breast that is visible only on the right CC view. (C) The one-view asymmetry ( box ) persists on the tomosynthesis slice (also see ) of the right CC projection caused by inadequate compression. (D) Spot compression right CC tomosynthesis study slice using greater compression on the asymmetry (also see ) shows normal overlapping normal tissue at the corresponding area ( box ), and US of the right breast was negative. The asymmetry was diagnosed as a summation artifact of overlapping normal breast tissue and shows the importance of good compression with tomosynthesis.

A large study from England ( ) demonstrated a tendency for higher specificity for 2D plus tomosynthesis compared with 2D alone for distortion/asymmetry because tomosynthesis showed either overlapping tissue or an underlying mass. In another study ( ), lesions on tomosynthesis were seen as a more specific and localized pattern (eg, mass or focal asymmetry rather than asymmetry) than those on 2D mammogram; cancers were more often constantly visible on tomosynthesis than on 2D mammography, and asymmetries were more often classified as focal asymmetry on tomosynthesis. Decreased recalls from screening in the author’s own practice were often caused by tomosynthesis showing overlapping tissue that could be dismissed as benign, versus true distortion/mass that might be cancer.

showed that asymmetries that represent normal, benign overlapping tissue are nonpalpable, contain no mass and no architectural distortion, and have no associated suspicious calcifications. Their study showed that asymmetries (formerly called asymmetric breast tissue) are present on mammograms in up to 3% of cases, and if benign, are stable on consecutive studies (see Fig. 4.14 ). In reviewing 8406 2D mammograms, showed that 221/8406 (3%) screens had asymmetric breast tissue and were not cancer if the asymmetry did not form a mass, was nonpalpable, and had no architectural distortion or calcifications. During the 36- to 42-month follow-up study period, 20 patients underwent excisional biopsy for clinical findings showing two breast cancer and one lymphoma cases, all of which were palpable. The remaining 17 biopsies were benign, and there were no breast cancers found in the remaining 201 patients with asymmetries. The study abstract concluded with the statement:

...an asymmetric volume of breast tissue, asymmetrically dense breast tissue, or asymmetrically prominent ducts that do not form a mass, do not contain microcalcifications, or do not produce architectural distortion should be view with concern only when associated with a palpable asymmetry, and are otherwise normal variations.

BI-RADS 2013 states that a global asymmetry is large, containing one quadrant or more of fibroglandular-like breast tissue compared with the same location in the contralateral breast, and is a real finding because it is displayed on two orthogonal projections. Global asymmetries are usually interspersed with fat and have no convex outward borders to suggest a mass. Similar to the smaller benign asymmetry, global asymmetries are benign if they are not new and have no associated architectural distortion, palpable findings, or suspicious calcifications. The nonpalpable global asymmetry is either an intrinsic normal variant ( Fig. 4.16 A ) or is caused by surgical removal of glandular tissue in the contralateral breast ( Fig. 4.16B ). If nonpalpable, the global asymmetry can be assessed as a BI-RADS 2 Benign Finding and returned to screening. However, if the finding is new, palpable, or is actually a mass instead of a global asymmetry, it may represent cancer and needs workup.

FIG. 4.16, Asymmetry: global asymmetry. Normal breast tissue variant and postbiopsy tissue removal. (A) Global asymmetry as a normal variant. Paired mediolateral oblique (MLO; left ) and craniocaudal (CC; right ) screening mammograms show more fibroglandular tissue in the right breast than the left, of greater than 25% of the breast volume (global asymmetry), and unchanged for 2 years. Note BB markers on the nipples. (B) Global asymmetry caused by surgery. Paired MLO ( left ) and CC ( right ) screening mammograms show more fibroglandular tissue in the right breast than the left, also of greater than 25% of the breast volume, and caused by surgical removal of breast tissue in the lower left breast (pathology showed papilloma, calcifications, and usual ductal hyperplasia). Given the clinical history, these are benign findings. Note the left linear skin scar marker and a postbiopsy metallic marker from benign biopsy in the left breast.

A focal asymmetry is defined as a more fibroglandular-like density in one breast compared with the other, both in a corresponding location, is seen on two orthogonal views, and is less than one quadrant in size (smaller than the global asymmetry). The focal asymmetry also lacks outward convex borders seen in masses, and may be interspersed with fat. It may be challenging to identify focal asymmetries, because comparison to the contralateral breast is especially important to identify the asymmetry on two views, and the findings must be included in the field of view on both projections. Some focal asymmetries may be dismissed as benign at screening ( Fig. 4.17 ), whereas others require workup. Scientific publications assess the focal asymmetry as a BI-RADS category 3 Probably Benign finding if called back from screening and is worked up, with a 0.5% to 1% probability of cancer if there are no masses at workup and it is stable over a 2-to 3-year mammographic follow-up period ( ).

FIG. 4.17, Asymmetry: focal asymmetry. Summation artifact. (B) Paired mediolateral oblique (MLO; A) and craniocaudal (CC; B) screening mammograms show a focal asymmetry with upper outer left breast ( arrows ). It is more obvious on the CC view because it is a summation of overlapping tissue that is spread out on the MLO view and stable for 24 months. Unlike a true mass, which is more conspicuous on both views and has convex outward borders, this benign asymmetry has concave outward borders and is interspersed with fat.

As stated in BI-RADS 2013, focal asymmetries that are less than 1 cm are of concern because they may represent nonpalpable cancers ( Fig. 4.18 ; ). It is of particular concern if the focal asymmetry recalled from screening has associated architectural distortion or calcifications. On occasion a focal asymmetry is found to be a true mass at diagnostic mammography or targeted US and might be cancer ( Fig. 4.19 ).

FIG. 4.18, Asymmetry: focal asymmetry/mass. Atypical ductal hyperplasia. (A and B) Mediolateral oblique (A) and craniocaudal (B) mammograms of left breast show a focal asymmetry ( arrows ). (C) This focal asymmetry persists as a mass of the same density and size on spot compression tomosynthesis (see also ), unlike the summation artifact demonstrated in Fig. 4.15 and , which spread out into normal glandular elements. Wire-localized excisional biopsy showed atypical ductal hyperplasia.

FIG. 4.19, Asymmetry: focal asymmetry. Breast cancer and cysts. (A and B) Paired mediolateral oblique (A) and craniocaudal (B) screening mammograms show a focal asymmetry with possible architectural distortion in the left upper outer breast. (C and D) Ultrasound shows multiple cysts (C) and a 3.6-cm irregular hypoechoic shadowing mass (D). (E) Contrast-enhanced magnetic resonance image shows a 3.1-cm segmental clumped nonmass enhancement with rapid initial and washout delayed kinetics and adjacent low signal cysts. Biopsy showed invasive carcinoma with desmoplastic stroma. In retrospect, the focal asymmetry consisted of breast cancer and multiple cysts.

A developing asymmetry is a focal asymmetry that, when compared with older mammograms, is new, larger, or more conspicuous than on prior studies (BI-RADS 2013; Fig. 4.20 ).

FIG. 4.20, Asymmetry: developing asymmetry. Breast cancer. Mediolateral oblique (MLO) and craniocaudal (CC) screening mammograms of the right breast 4 years before (A and B) and currently (C and D) show a new increased density (focal asymmetry; box ) that looks like a mass behind the nipple on the MLO view but partly spreads out in the inner breast on the CC view, hidden by adjacent tissue. Workup showed a mass and biopsy showed tubular cancer.

The 2007 study by showed that developing asymmetries were present in 0.16% (292 cases) of 180,801 screening mammograms and 0.11% (32 cases) of diagnostic mammograms. At screening mammography, 12.8% of the developing asymmetries were cancer. The Leung and Sickles study and a follow-up study by showed that the developing asymmetry in the diagnostic setting has a likelihood of 26.7% of malignancy if found in follow-up of BI-RADS category 3 lesions, if shown after a benign concordant biopsy or if developing in the first 5 years after breast conservation. Because the percentage of cancer is above the 2% Probably Benign category 3 threshold, developing asymmetries should undergo biopsy if they are not normal overlapping tissue at workup.

Occasionally, nonpuerperal (nonlactating) mastitis may show a developing asymmetry with rare associated architectural distortion ( ), which can be difficult to distinguish from breast carcinoma. Puerperal or postpartum mastitis caused by lactation also produces the same radiologic features as developing asymmetry but clinically, women present with a clinical history of fever and pain, and their mammograms commonly show breast edema with the developing asymmetry.

Architectural Distortion

Architectural distortion is defined as linear alterations of breast parenchyma pulled into a central focus, without a definite visible mass, resulting in radiating spiculations or thin lines pointing toward the center, like a star ( Fig. 4.21 ). Distortion also describes the pulling in or straightening of any edge of the glandular tissue boundary with fat (see Fig. 4.10 ). This was called the “tent sign” and attributed to Dr. Lazslo Tabar. When associated with asymmetry or calcifications, architectural distortion is even more suspicious for cancer. In contrast, architectural distortion associated with a history of surgical biopsy represents a postbiopsy scar and is benign. Because postbiopsy scars can be indicated by placement of a linear metallic marker on the skin over the postbiopsy scar, many facilities place radiopaque skin markers on skin scars to show that underlying distortion represents a benign scar. However, architectural distortion is suspicious for malignancy or radial scar if there is no history of trauma or surgery, and it requires biopsy. Architectural distortion is seen on 2D mammography and is even more exquisitely depicted on tomosynthesis. Architectural distortion seen on tomosynthesis may be invisible or subtle on 2D mammography, but still represents cancer or radial scar ( Fig. 4.22 ; ).

FIG. 4.21, Architectural distortion: breast cancer. (A) Paired craniocaudal (CC) mammograms show architectural distortion ( circle ) and possible focal asymmetry in the central left breast. (B) Spot compressed magnified CC view better depicts the distortion as a suspicious spiculated finding. (C) Ultrasound shows a hypoechoic irregular mass with indistinct margins with acoustic shadowing. Biopsy showed invasive ductal carcinoma.

FIG. 4.22, Architectural distortion: radial scar. (A and B) Mediolateral oblique (A) and craniocaudal (CC) (B) screening mammograms show architectural distortion ( arrows ) in the outer right breast. (C) Spot compressed CC tomosynthesis slice (see also Video 4.8 ) shows distortion and a possible 7-mm mass not seen by US. Wire-localized biopsy showed radial scar.

For findings seen only on tomosynthesis and undetected by US, biopsy may be done under tomosynthesis guidance ( ). Architectural distortion may be a finding by itself or may be an associated finding (see section: Associated Features of Masses ).

Associated Features of Masses

Associated findings of masses worrisome for cancer ( Box 4.1 ) include skin or nipple retraction ( Figs. 4.23 and 4.24 ; ), skin thickening ( Fig. 4.25 ), or trabecular thickening ( Fig. 4.26 ); axillary adenopathy ( Fig. 4.27 ); architectural distortion; and calcifications ( Fig. 4.28 ).

BOX 4.1
American College of Radiology Breast Imaging Reporting and Data System Associated Findings
From American College of Radiology: ACR BI-RADS ® —Mammography. In ACR BI-RADS atlas, breast imaging reporting and data system , ed 5, Reston, VA, 2013, American College of Radiology.

  • Skin retraction

  • Nipple retraction

  • Skin thickening

  • Trabecular thickening

  • Skin lesion

  • Axillary adenopathy

  • Architectural distortion

  • Calcifications

FIG. 4.23, Associated feature: skin retraction. Breast cancer. (A and B) Mediolateral oblique (MLO; A) and craniocaudal (B) mammograms show a skin marker over a high-density palpable spiculated mass in the upper outer left breast causing skin retraction ( arrows ). (C) Magnification MLO view shows a high-density mass with spiculations extending to the skin, causing the skin tethering. Biopsy showed invasive ductal cancer.

FIG. 4.24, Associated feature: nipple retraction. Recurrent breast cancer. (A) Craniocaudal (CC) mammogram in a patient with a previous history of right lumpectomy and radiation therapy for cancer shows linear scar markers and mild postbiopsy distortion in the retroareolar region. (B–D) Nine years after (A) diagnostic mammogram was performed because she developed lump and nipple inversion. Right CC mammogram (B) shows a retroareolar developing asymmetry with nipple retraction. Right CC tomosynthesis slice (C; see also ) and spot compressed magnification CC mammogram with scar marker (D) depict an irregular mass with spiculations extending to the nipple. Note a normal dense calcification and vascular calcifications on B–D, new from the previous study (A). Biopsy showed invasive ductal carcinoma.

FIG. 4.25, Associated features: skin thickening. Inflammatory cancer. (A) Previous right mediolateral oblique (MLO) mammogram obtained 1 year prior shows no apparent abnormality. (B) The patient presented with skin redness and thickening of the central two-thirds of the right breast. Current right MLO mammogram shows widespread breast edema, trabecular thickening, and diffuse skin thickening most readily apparent in the lower breast ( arrowheads ). Axillary lymph nodes ( arrow ) are enlarged compared with the previous study. (C and D) Ultrasound shows diffuse abnormal increased echogenicity throughout the right breast (C), skin thickening, and an enlarged lymph node (D) with a lobulated border and impingement of the fatty hilum. Although a specific breast mass was not identified, biopsy of the skin showed angiolymphatic spaces containing carcinoma cells compatible with the clinical diagnosis of inflammatory cancer. Axillary lymph node biopsy showed metastatic carcinoma, consistent with ductal carcinoma of the breast.

FIG. 4.26, Associated features: skin thickening and trabecular thickening. (A) Prior mediolateral oblique mammogram shows normal tissue and the normal dark fat below the skin with thin Cooper’s ligaments. (B) Current lateromedial mammogram shows a new irregular high-density mass ( arrows ) with new trabecular thickening ( box ), shown by coarser white strands in the normally black subcutaneous fat and scalloping of the normally straight skin line ( arrowhead ). Biopsy of the mass showed invasive ductal carcinoma.

FIG. 4.27, Associated features: axillary adenopathy. Metastatic lymph node from breast cancer. Left breast mediolateral oblique view shows a 3.5-cm oval high-density left axillary mass ( arrow ) near a BB marker and circular mole marker, representing a metastatic lymph node. The primary invasive ductal cancer is an oval mass with indistinct margins ( arrowhead ) under another BB marker in the mid left breast that is much smaller than the metastasis. Note that lymphadenopathy may be a dominant or an only indicator of breast cancer, because even small cancers can metastasize.

FIG. 4.28, Associated features: calcifications. Three different cases with breast cancer. (A) Cropped magnified mammogram shows a suspicious irregular mass containing pleomorphic calcifications, representing grade II invasive ductal cancer (IDC) and ductal carcinoma in situ (DCIS). (B) Another patient has a suspicious dense mass and fine pleomorphic calcifications within and adjacent to the mass. Excisional biopsy showed high-grade DCIS. (C) Spiculated mass, representing IDC, has fine-linear and pleomorphic calcifications within it and extending into the surrounding tissue, representing DCIS. Note the linear scar marker overlying this breast cancer recurrence near the prior postbiopsy scar. Radiologists report both the mass and calcification extent to ensure the surgeon removes all suspicious findings.

Associated calcifications within or adjacent to a suspect mass are important for two reasons. First, suspicious, pleomorphic calcifications inside a benign-appearing mass may be the only clue that the mass is a cancer. Second, if the mass is cancer, calcifications around it may represent ductal carcinoma in situ (DCIS). Patient management includes sampling both the mass and surrounding suspicious calcifications ( Box 4.2 ). If both prove to be cancer, the surgeon will excise the extent of the suspicious calcifications to remove the cancer in its entirety (see Fig. 4.28B–C ).

BOX 4.2
Masses and Microcalcifications

Beware of pleomorphic calcifications adjacent to a suspicious breast mass that is biopsy-proven invasive cancer. The adjacent calcifications should undergo biopsy because the calcifications may represent ductal carcinoma in situ.

At histology, DCIS constituting more than 25% of an invasive ductal cancer is called an extensive intraductal component (EIC); such a cancer is called EIC-positive (EIC + ). Because EIC tumors have an increased risk of local recurrence, breast-conserving surgery is less successful. This is one of the reasons to always look for calcifications when a suspicious mass is present.

Other important associated mammographic findings suggestive of cancer are skin thickening, which may indicate breast edema or focal tumor invasion; skin retraction or nipple retraction as a result of focal tumor tethering; axillary adenopathy indicating axillary lymph node metastases; and architectural distortion.

Further Characterization of Masses with Ultrasonography

US goes hand-in-hand with mammography in breast mass evaluation. A major advantage of US is the ability to directly correlate the clinical and imaging findings. It provides real-time evaluation of mass shapes, borders, orientation, and internal characteristics to determine whether the mass is cystic or solid or malignant or benign. Many masses that are not well characterized on mammography can be characterized as benign using US. US is often used for further assessment of possible masses after mammography and is the initial imaging modality in the evaluation of clinically detected palpable masses in a women younger than 30 years of age. Detailed principles and interpretation of ultrasonography are explained further in Chapter 5 .

Ultrasound Technique and Analysis of Masses

The ACR BI-RADS US lexicon describes terms and features of breast masses that are key for the diagnosis of cancer ( Table 4.3 ). As shown by , ultrasonographic features are basically different between malignant and benign solid masses ( Box 4.3 ). Illustrations of these features are shown in Chapter 5 , with the most important US features of cancer detailed under the categories of mass shape (irregular), margin (not circumscribed), and orientation (not parallel to the chest wall).

TABLE 4.3
American College of Radiology Breast Imaging Reporting and Data System Ultrasound Lexicon Descriptors for Masses
From American College of Radiology: ACR BI-RADS ® —Ultrasound. In ACR BI-RADS atlas, breast imaging reporting and data system , ed 5, Reston, VA, 2013, American College of Radiology.
Shape Orientation Margin Echo Pattern Posterior Acoustic Features Associated Features Calcifications
Oval
Round
Irregular		 Parallel
Not parallel		 Circumscribed
Not circumscribed
Indistinct
Angular
Microlobulated
Spiculated		 Anechoic
Hyperechoic
Complex
Hypoechoic
Isoechoic
Heterogeneous		 None
Enhancement
Shadowing
Combined		 Architectural distortion
Duct changes
Skin changes
Skin thickening
Skin retraction
Edema
Vascularity
Absent
Internal vascularity
Vessels in rim
Elasticity assessment
Soft
Intermediate
Hard		 Calcifications in a mass
Calcifications outside of a mass
Intraductal calcifications

BOX 4.3
Ultrasound Features of Solid Breast Masses: Malignant versus Benign
Modified from Stavros AT, Thickman D, Rapp CL, et al: Solid breast nodules: use of sonography to distinguish between benign and malignant lesions, Radiology 196:123–134, 1995.

Malignant

  • Irregular shape

  • Not-parallel orientation (taller than wide)

  • Not-circumscribed margin (indistinct, angulated, microlobulated, and spiculated)

  • Very hypoechoic

  • Acoustic shadowing

  • Microcalcifications

  • Duct extension

  • Branch pattern

  • Hard elasticity assessment

Benign

  • Oval shape

  • Parallel orientation (wider than tall)

  • Circumscribed margin

  • Intense homogeneous hyperechogenicity

  • Four or fewer gentle lobulations

  • Thin echogenic pseudocapsule/ellipsoid shape

  • No malignant characteristics

US evaluation of breast masses begins with determining whether the mass is cystic or solid. Simple cysts are anechoic (all black inside), round or oval shaped with circumscribed margins, have an abrupt interface with surrounding tissue, have a thin posterior wall, and are enhanced through sound transmission (have a white tail on the side of the mass opposite of the transducer, like a comet tail). Simple cysts are dismissed as benign.

In contrast, solid breast masses have internal echoes and could be either malignant or benign. To determine whether a mass is cancer on US, the radiologist evaluates the mass shape, margins, and orientation. The most suspicious mass shape is irregular. The most suspicious mass margin is not circumscribed, including margins that are indistinct (including echogenic halo), angular, microlobulated, and spiculated. The most suspicious orientation is not-parallel orientation in which the long axis of the mass is perpendicular to the chest wall. Not parallel is also known as “taller than wide” by and is of concern that the mass is growing through normal tissue planes. Other suspicious descriptors are a heterogeneous or complex cystic and solid internal echo pattern, posterior acoustic shadowing , or architectural distortion of the surrounding breast tissue. The presence and location of associated calcifications are helpful in describing masses on US.

After scanning, the technologist takes representative pictures of the mass and labels the images to clarify the mass’ location in the breast. The ACR Practice Parameter for the Performance of a Breast Ultrasound Examination, Labeling, includes facility name and location, examination date, patient’s first and last name, which breast was scanned (left or right), position of the mass in terms of breast clock face or diagram annotation, the finding’s location in centimeters from the nipple, and the technologist’s initials. Other information helpful in finding the mass on subsequent studies includes the scan angle (radial or antiradial and transverse or longitudinal). The technologist captures the image without and with measuring calipers on the mass ( Box 4.4 ). It is also helpful to indicate whether the mass is palpable or nonpalpable. The ACR Practice Parameter encourages real-time scanning by the interpreter. Many facilities capture cine or moving images in addition to static images.

BOX 4.4
American College of Radiology Recommendations for Breast Ultrasound Labeling a

a 2014 ACR Practice Parameter for the Performance of the Breast Ultrasound Examination

  • Right or left breast

  • Mass position in terms of clock face or quadrant

  • Number of centimeters from the nipple

  • Scan plane (radial/antiradial and transverse/long)

  • Initials of person performing the scan

  • Orthogonal images of mass without and with measuring calipers

Benign US findings include no malignant features, oval or round shape, an abrupt circumscribed margin, intense homogeneous internal hyperechogenicity, fewer than four gentle lobulations, parallel (wider than tall) configuration (parallel to the chest wall), no posterior acoustic shadowing, and a thin echogenic capsule ( ). Because benign and malignant features in solid masses overlap, common sense plays a major role in patient management for solid masses, especially if the mass looks benign but the clinical scenario is suspicious (for example, new benign-appearing mass in a patient with a strong family history of breast cancer).

Correlating Palpable and Nonpalpable Masses on Mammography and Ultrasound

A common clinical problem is the palpable breast mass. The ACR Appropriateness Criteria for Palpable Breast Masses ( ) specifies guidelines to tailor imaging examinations for palpable masses. For example, the ACR Criteria recommends initial mammography for women aged ≥40 years old, usually with US as the second test. For pregnant or lactating women, or women aged ≤30 years old, US is the first study. Either US or mammography can be done first in women between these ages.

When US is the only study for a palpable mass, one correlates US findings with the palpable mass at real-time imaging. One method to correlate US findings to the mass is to place an examining finger or a cotton-tipped swab directly on the palpable mass and scan over the finger or cotton-tipped swab on the mass to generate a ring-down shadow. Subsequent removal of the finger or cotton-tipped swab from under the probe produces a scan of the palpable finding. Then the radiologist, technologist, and patient have no doubt that the palpable finding has been scanned, because this technique ensures that the transducer is placed directly on the palpable finding.

To correlate palpable US and mammographic findings when US is the first study, the radiologist or technologist scans the palpable mass and if there is a US-detected mass, the sonographer places a finger or cotton-tipped swab on the skin over the mass. The sonographer then marks the skin with indelible ink and places a metallic skin marker, such as a BB, over the palpable finding. Subsequently, the mammography technologist performs the mammogram. If the marker is at or near the mammographic finding, the palpable, mammographic, and US findings all correlate with each other.

To correlate nonpalpable US findings with mammographic findings when mammography is the first study, the sonographer looks at the mammogram to determine where to scan and what to expect on US. If there is a US finding that might correlate with the mammographic finding, the sonographer places a finger, cotton-tipped swab, or large unwound paper clip under the transducer so that a ring-down shadow is superimposed over the finding. The sonographer removes the transducer, marks the skin over the mass with an indelible ink marker, and places a metallic skin marker on the ink spot. The mammography technologist takes orthogonal mammographic views. The skin marker over the US finding should be in the same location as the mammographic finding on the films. It should be expected that even if the mammogram and US findings are the same, the mammographic finding might be 1 cm or more away from the skin marker on the films because the skin marker will be compressed away from the mass on the mammogram by the compression paddle.

Sometimes it is still uncertain whether a US and mammographic finding are one and the same even after US/mammography skin marking. If the patient agrees to a biopsy of the US finding, the radiologist places a metallic marker into the mass using a US-guided, percutaneously placed needle after the biopsy ( Fig. 4.29 ). Postbiopsy mammograms will show the marker in the mass if the US and mammography findings are the same. If the mass was only seen by tomosynthesis, marker placement in the mass should be confirmed by postbiopsy tomosynthesis.

FIG. 4.29, Ultrasound (US)-guided marker placement to correlate nonpalpable US and mammography findings. (A) A patient with a nonpalpable mass seen only on the mediolateral oblique (MLO) view underwent US, showing an indistinct, not-parallel mass with an echogenic rim and acoustic shadowing. (B) After US-guided core biopsy with marker placement in the mass, a BB skin marker was placed over the skin where US showed the mass. (C) The MLO view shows the mass and marker ( arrow ) and the skin BB over the mass, proving the US-detected finding represents mammographic mass. Biopsy showed invasive ductal carcinoma. Note the metallic linear scar marker on the skin over a previous biopsy.

Alternatively, a retractable hookwire may be placed in the mass under US. A mammogram with the wire in place will show that the US finding and the mammographic finding represent the same mass. The radiologist can subsequently remove the retractable hookwire.

The mammography and US report for a breast mass should describe if the mass is palpable; the size, shape, margin, and density of the mass; its location and associated findings; and any change from previous examinations, if known. The report should also include US finding descriptors and whether it correlates with the mammographic finding. Finally, each report that includes a mammogram should be assigned an ACR BI-RADS final assessment code indicating the level of suspicion for cancer and follow-up management recommendations ( Box 4.5 ).

BOX 4.5
American College of Radiology Breast Imaging Reporting and Data System Mass Reporting
From American College of Radiology: ACR BI-RADS ® —Mammography. In ACR BI-RADS atlas, breast imaging reporting and data system , ed 5, Reston, VA, 2013, American College of Radiology.

  • Size and location

  • Mass type and modifiers (shape, margin, and density)

  • Associated calcifications

  • Associated findings

  • How changed if previously present

  • Summary and BI-RADS code (0–6)

BI-RADS, Breast Imaging Reporting and Data System.

Mammographic and Ultrasound Atlas of Masses

Masses with Spiculated Borders and Sclerosing Features

Masses with spiculated borders and sclerosing features suggest malignancy ( Box 4.6 ). The benign (but high-risk) radial scar also appears as a spiculated mass on both 2D mammography and tomosynthesis and is a common cause of false-positive breast biopsies. On occasion, inflammatory or fibrotic lesions also may appear as spiculated masses

BOX 4.6
Differential Diagnosis of Spiculated Masses

  • Invasive ductal carcinoma

  • Invasive lobular carcinoma

  • Tubular cancer

  • Postbiopsy scar

  • Radial scar

  • Fat necrosis (atypical)

  • Sclerosing adenosis

  • Proliferative fibrocystic change (rare)

Cancer

Invasive Ductal Carcinoma

Invasive ductal carcinoma is the most common breast cancer and accounts for approximately 90% of all cancers. Also known as invasive ductal carcinoma not otherwise specified (NOS), invasive ductal carcinoma usually grows as a hard irregular mass in the breast ( Fig. 4.30 ; ). The classic appearance of invasive ductal carcinoma is a high-density irregular or spiculated mass, occasionally containing or associated with adjacent pleomorphic calcifications representing DCIS. On the mammogram, the mass should be about the same size and density on two orthogonal mammographic views. Spot compression magnification views may show unsuspected calcifications in or around the mass or unsuspected irregular borders.

FIG. 4.30, Spiculated mass: invasive ductal carcinoma. (A) Magnification craniocaudal (CC) mammogram shows a spiculated mass. (B) Tomosynthesis of left CC projection slice (see also ) shows spiculations and microcalcifications within the mass more clearly. (C) The corresponding ultrasound shows a hypoechoic mass with indistinct, spiculated margins. Biopsy showed invasive ductal carcinoma.

Mammographic spiculated masses are often round, irregular, or spiculated on US and commonly produce acoustic shadowing as a result of either productive fibrosis or tumor extension. When present, acoustic spiculation looks like thin radiating lines extending from the tumor into surrounding breast structures, occasionally causing tissue distortion. In a dense white breast, the US spicules are dark against the white glandular tissue. In a fatty breast, the spicules are white against the dark fatty background.

On MRI, the usual appearance of invasive ductal cancer is a brightly enhancing irregular mass with or without spiculation; enhancement is initially rapid, with a late-phase plateau or washout curve. Rim enhancement and heterogeneous enhancement are other worrisome signs for invasive ductal cancer on MRI.

Invasive Lobular Carcinoma

Invasive lobular carcinoma (ILC) is most commonly seen as an equal-density or high-density noncalcified mass, occasionally showing spiculations or ill-defined borders ( Fig. 4.31 ; see also Fig. 4.1 ). and showed that 50% of ILC may have a density equal or lower than surrounding glandular tissue and showed that some ILC may contain lucent areas. ILC has a higher rate of bilaterality and multifocality than does invasive ductal cancer. It accounts for less than 10% of all invasive cancers, but historically it is the most difficult breast cancer to see on mammograms ( Box 4.7 ). ILC gives radiologists a bad name because it can be missed by mammography, at a rate reported by to be as high as 21%. This failure can be partly explained by the growth pattern of the carcinoma. Classically, ILC grows in single lines of tumor cells infiltrating the surrounding glandular tissue and may not produce a mass, making it difficult to see by mammography and difficult to feel by physical examination. It usually does not contain microcalcifications. It often infiltrates the breast, is often seen on only one view, and may cause only subtle distortion of the surrounding glandular tissue. When actually seen on the mammogram, ILC masses are often of equal or higher density than fibroglandular tissue and are seen because of the mass itself or its effect on surrounding tissue, such as architectural distortion and straightening of Cooper’s ligaments. As with any mass, distortion, flattening, and tenting of glandular tissue caused by ILC are most easily seen in locations in which Cooper’s ligaments extend out into surrounding fat, such as in the retroglandular fat or along the edge of the normal, scalloped fibroglandular tissue (see Figs. 4.10 and 4.25 ).

FIG. 4.31, Spiculated mass: invasive lobular cancer in two different cases. (A) Spot compression craniocaudal mammogram shows a spiculated mass causing distortion ( arrow ) and flattening of the nipple. Thin straight lines extend from the tumor into subcutaneous fat, indicating its presence. (B) In another patient, there is a spiculated mass ( arrow ) at the edge of the film at the chest wall on a right mediolateral oblique view. The cancer looks very similar to the rest of the breast tissue and is seen only because of the spiculations extending into the fat, and also because it is a density in “no man’s land” in which there is usually only fat near the chest wall.

BOX 4.7
Features of Invasive Lobular Carcinoma

  • 10% of all breast cancers

  • Grows in single-cell files

  • Hardest tumor to see on mammography

  • Often seen on one view

  • Causes mass or architectural distortion

  • Calcifications not a feature

On US, ILC is a hypoechoic, irregular, spiculated, or ill-defined mass that may or may not have acoustic shadowing. When ILC becomes very large, only the acoustic shadowing may be apparent; the mass itself can be difficult to see because of its large size. On MRI, ILC looks like a spiculated mass but may have variable enhancing patterns; it can look like a mass, like a distortion of tissue, or like nodular regions connected by strands of tissue. Its enhancement kinetics can be similar to those of normal breast tissue and can thus be a cause of false-negative MRI examinations. However, ILC is detected more readily by MRI compared with mammography and US, rendering ILC a common indication for breast MRI when assessing extent of disease. In a 2015 study, showed that women with ILC were significantly associated with having other foci of cancer in the involved breast when evaluated with MRI ( p = 0.02).

Tubular Carcinoma

Tubular carcinoma is a generally slow-growing tumor with a bilateral incidence of 12% to 40%. On mammography, tubular cancer is a dense or equal-density spiculated mass with occasional microcalcifications ( Fig. 4.32 ). On occasion it may be apparent on the previous mammogram because of its slow growth. Although controversial, some pathologists believe that radial scars may be a precursor to tubular carcinoma. Generally, tubular carcinoma has a good prognosis and a lower incidence of metastases than does invasive ductal cancer. On US, tubular cancers are hypoechoic, irregular masses that occasionally produce acoustic shadowing.

Postbiopsy Scar

On mammograms, a new postbiopsy scar is round, ill-defined, and contains air and fluid; after healing, an old postbiopsy scar looks like a spiculated mass that is impossible to distinguish from cancer. In the immediate postoperative period, postbiopsy scars show air and fluid in a round or oval mass at the biopsy site, with adjacent skin thickening where the surgeon has closed the skin. Because the surgeon does not close the excised cavity with sutures, the cavity is left to fill with fluid (seroma) that may contain blood. The fluid is resorbed to varying degrees over time, with fluid occasionally persisting for several years as a round or oval mass in the biopsy site. In other cases the fluid resorbs completely, and the surrounding glandular tissue is drawn into a central dense nidus of scar tissue. As a result, the mammogram shows a centrally dense spiculated mass (the scar) with straightening of the surrounding Cooper’s ligaments and indrawing of normal glandular tissue, simulating a spiculated breast cancer ( Fig. 4.33 ; ). In some patients, no dense central nidus occurs, and the scar appears as a focal architectural distortion with radiating thin white lines from a central point. On US, a postbiopsy scar is a hypoechoic mass with acoustic spiculation and shadowing, similar to cancer. There should be thickening of the patient’s skin where the skin scar lies and distortion of subcutaneous tissue extending from the patient’s skin scar, down the plane of the incision, and finally leading to the postbiopsy scar.

FIG. 4.32, Spiculated mass: tubular cancer with mammographic and ultrasound correlation. (A) Spot compression mammogram shows a palpable spiculated mass ( arrow ) under a BB skin marker in extremely dense tissue. (B) Ultrasound shows a not-parallel spiculated irregular mass. (C) Specimen radiograph better shows the typical spiculations radiating from the mass ( arrow ) around a localizing hookwire.

FIG. 4.33, Spiculated mass: postbiopsy scar. (A) Photographic magnification 2D mammogram shows a spiculated mass directly under a linear scar marker over a postbiopsy site, representing a postbiopsy scar. (B) Tomosynthesis slice (see also ) shows the postbiopsy scar to greater advantage.

The postbiopsy scar is not of concern for cancer if it occupies a surgical site ( Box 4.8 ). To distinguish postbiopsy scars from cancer, the radiologist reviews surgical biopsy locations on the breast history form and reviews older films to see if the scar is at the same location as the resected finding. Some facilities place a radiopaque linear metallic scar marker on the patient’s skin scar to show the skin scar location on the mammogram (see Fig. 4.33 ; see ). The metallic linear scar marker should be on top of the architectural distortion thought to represent postbiopsy scar. If the mammographic scar does not correspond to a postbiopsy site, it is a mass, should be considered suspicious, and should undergo workup and biopsy ( Fig. 4.34 ). However, increased density, growth, or changing of the normally convex postbiopsy scar to a concave margin suggests breast cancer recurrence and needs workup (see Chapter 8 ).

BOX 4.8
How to Confirm Postbiopsy Scars

To determine whether a spiculated mass is a postbiopsy scar, correlate the “scar” to a linear scar marker on the skin showing the location of the previous biopsy, and correlate the scar location with the targeted finding on old prebiopsy mammograms. If the postbiopsy scar is nowhere near the linear scar marker, or if the scar has developed in a location other than the targeted, excised finding, it is not a scar and should undergo biopsy.

FIG. 4.34, Spiculated mass: postbiopsy scar and new cancer away from scar marker. Mediolateral oblique mammogram shows a postbiopsy scar ( arrowheads ) from resection of a papillary cancer with a new spiculated mass ( arrow) in the upper breast. The new mass in the upper breast cannot represent a postbiopsy scar because it is far away from the linear scar marker. Biopsy showed invasive ductal cancer.

Radial Scar

A radial scar has nothing to do with a postbiopsy scar but is a common name for a benign proliferative breast lesion that looks like a spiculated cancerous mass or postbiopsy scar on mammograms. Both radial scars and their larger variants, called complex sclerosing lesions, may include adenosis and hyperplasia. In autopsy series, small radial scars are common but often may not be apparent on 2D mammography. The central part of a radial scar undergoes atrophy, resulting in a scarlike formation, with pulling in of the surrounding glandular tissue that produces a spiculated mass. On occasion, because of entrapment of breast ductules, the radial scar may be difficult for pathologists to distinguish from infiltrating ductal carcinoma. However, both epithelial and myoepithelial cells in benign radial scars distinguish them from breast cancer. Radial scars may contain or be associated with atypical ductal hyperplasia, atypical lobular hyperplasia, lobular carcinoma in situ, or cancer. This is one of the rationales for surgical excision. Some pathologists believe that a radial scar may be a precursor to tubular carcinoma and should be excised, although this position is controversial.

On mammography, a radial scar appears as a spiculated mass with either a dark or white central area that may or may not have associated microcalcifications ( Figs. 4.35 and 4.36 ; ). It is a myth that radial scars have dark centers in the mass on mammography and can be distinguished from breast cancers, which have white-centered masses. Scientific studies have shown that radial scars and breast cancer can both have either white or dark centers on mammograms. This means that all spiculated masses not representing a postbiopsy scar should be sampled histologically ( Box 4.9 ).

FIG. 4.35, Spiculated mass: radial scar with spot compression tomosynthesis studies. (A and B) Left mediolateral oblique (MLO; A) and craniocaudal (B) views show a focal asymmetry with possible architectural distortion ( arrows ) in the upper outer left breast. (C) Spot compressed MLO tomosynthesis slice shows architectural distortion more clearly (also see ). (D) Corresponding ultrasound shows heterogeneous hypoechoic area surrounded by several cysts. Excisional biopsy showed radial scar. Obstruction of mammary ducts by radial scar likely caused the surrounding cysts.

FIG. 4.36, Spiculated mass: radial scar with mammographic and ultrasound correlation. (A) Photographically magnified mammogram shows a vague spiculated mass ( arrow ) with a dense white center in the upper part of the breast. (B) Ultrasound shows an irregular hypoechoic mass, simulating cancer. Biopsy showed radial scar, which is indistinguishable from cancer on imaging.

BOX 4.9
Radial Scar versus Cancer

Radial scars cannot be distinguished from cancer on mammography. Spiculated masses not representing postbiopsy scar tissue require a histologic diagnosis.

Because tomosynthesis is extremely sensitive in detecting spiculation or distortion, many radial scars are now found by tomosynthesis that were invisible on 2D mammography. Unfortunately, a radial scar cannot be distinguished from cancer even on tomosynthesis, thus it requires a biopsy and is a cause for false-positive studies.

On US, a radial scar is a hypoechoic mass, with or without acoustic shadowing (see Figs. 4.35 and 4.36 ; ).

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