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Columnar Cell Change, Flat Epithelial Atypia, and Atypical Ductal Epithelial Hyperplasia


Introduction: Screening and Detection

As the imaging modalities used for breast cancer screening and diagnosis have improved, the types of specimens evaluated by pathologists for risk-associated lesions have changed. In contemporary practice, atypical ductal hyperplasia (ADH) and atypical lobular hyperplasia (ALH) are much more likely to be diagnosed in image-guided core needle biopsy (CNB) specimens versus excisional biopsies. The adoption of digital mammography has resulted in more CNBs for microcalcifications with more diagnoses of columnar cell lesions (CCLs) and ADH. Three-dimensional digital breast tomosynthesis may identify more atypical lesions and radial scars (RSs) associated with architectural distortion.

In CNBs, the frequency of atypical hyperplasia is approximately 4%. The frequency of ADH, ALH, and lobular carcinoma in situ (LCIS) may be as high as 10% to 15% in vacuum-assisted stereotactic CNBs specifically. Flat epithelial atypia (FEA) and benign papillomas are present in 1% and 2% to 3% of CNBs, respectively. RSs account for approximately 1% to 2% of breast CNBs. If 8% of the estimated 1.5 million image-guided CNBs performed annually in the United States contain ADH, ALH, LCIS, FEA, or an RS, approximately 120,000 women could be referred for surgery based on these diagnoses each year. This chapter focuses on the assessment of microscopic features, the selected application of immunohistochemistry (IHC), and the risk of carcinoma associated with CCL and ADH.

Columnar Cell Lesions: Benign and Atypical

Alterations of the terminal duct lobular unit (TDLU) by the spectrum of CCL have been known for well over 100 years. This spectrum of simple CCLs and CCLs with atypical cytology has generated a wide variety of different pathological designations ( Table 19.1 ), including abnormal involution, adenoid cystic change of senile parenchymatous hypertrophy, hyperplastic unfolded lobules, blunt duct adenosis (BDA), low-grade clinging carcinoma, columnar alteration with prominent apical snouts, atypical cystic lobules, enlarged lobular units with columnar alteration (ELUCAs), hyperplastic enlarged lobular units (HELUs), and flat ductal intraepithelial neoplasia (DIN1a). The variety of different names, taken together, describes the salient microscopic features that have attracted the attention of so many pathologists. These alterations involve replacement of the normal TDLU acinar cells with columnar cells, which may on occasion appear atypical, may be cystically dilated, are often enlarged, and may have apical cellular snouts.

Table 19.1
Terminology previously applied to flat epithelial atypia of the breast.
Clinging carcinoma
Atypical cystic lobules
Columnar alteration with prominent apical snouts and secretions with atypia
Columnar cell change with atypia
Columnar cell hyperplasia with atypia
Hypersecretory hyperplasia with atypia
Ductal intraepithelial neoplasia of the flat monomorphic type

Clinical Presentation and Imaging

Most patients with columnar cell change (CCC) and FEA are found to have calcifications on mammographic screening. The observed mammographic calcifications are almost always seen to be intimately involved with CCC and FEA on microscopic sections of breast core biopsies (determinate calcifications). The calcifications are often irregular, within the lumen, and sometimes associated with flocculent intraluminal secretion material. On rare occasions, there may be marked dilatation of ducts with eosinophilic material simulating thyroid follicles. The epithelium should be scrutinized in these areas because this type of luminal content is rarely seen with fibrocystic change. Less commonly, CCLs may be seen in a breast biopsy in which the calcifications are seen in other areas of the breast tissue (nondeterminate calcifications).

CCL ranks fifth among the common findings associated with mammographic calcifications, behind fibrocystic change, fibroadenoma, ductal carcinoma in situ (DCIS), and sclerosing adenosis. Mammographic calcifications ( Fig. 19.1 ) may appear rounded, branching, amorphous, indistinct, or pleomorphic and are usually interpreted as suspicious; in the United States, they are most often assigned Breast Imaging Reporting and Data System (BI-RADS) category 4, which is indication for biopsy. Images with suspicious calcium are typically followed up with biopsies with vacuum assistance to maximize tissue volume, or execute complete removal of calcium.

Fig. 19.1, Typical mammographic appearance of microcalcifications with flat epithelial atypia.

Gross Pathology

There are no specific gross tissue findings of CCC or FEA.

Microscopic Pathology

The current World Health Organization (WHO) classification (5th Edition) provides three diagnostic categories: CCC, columnar cell hyperplasia (CCH), and FEA. The 5th Edition of the WHO classification also includes CCC with atypia and CCH with atypia as acceptable terms. Use of the terms clinging carcinoma (monomorphic type), atypical cystic lobules , and atypical lobules type A is not recommended. The frequent association of FEA with ADH, low-grade DCIS, tubular carcinomas, and lobular neoplasia lends support to the concept of a low-grade breast neoplasia pathway. Management recommendations vary, but many patients with FEA diagnosed on CNB are offered surgical excision to exclude coexisting carcinoma (see “Clinical Relevance, Management, and Risk/Prognosis”).

CCC involves dilated acinar spaces of the TDLU that may have irregular contours and are lined by columnar epithelial cells with ovoid nuclei oriented perpendicularly to the basement membrane. The nuclei are bland, have a fine chromatin, and have no visible nucleoli. The columnar cells have scant apical cytoplasm and apical cytoplasmic blebs or snouts that are extruded into the lumen ( Fig. 19.2 ). The flocculent secretions subsequently formed are invariably calcified to some degree.

Fig. 19.2, Columnar cell change (CCC). ( A ) Low-magnification appearance of CCC with dilatation of terminal duct lobular unit. ( B ) CCC with elongated bland nuclei and abundant apical snouts. ( C ) Granular calcific debris in the lumen of a terminal duct with CCC. ( D ) CCC with dilatation of the lobular unit and prominent apical snouts with luminal content. ( E ) Granular luminal content in this focus of CCC. Note bland cytology. ( F ) Higher magnification shows elongated oval bland nuclei, some overlapping, with prominent apical snouts. ( G ) Ki-67 index is invariably less than 3%. ( H ) Estrogen receptor (ER) in an area of CCC shows diffuse strong immunostaining of nuclei representing ER upregulation compared with the adjacent lobule where focal nuclear ER expression is usual.

CCH has the same overall appearance at low magnification, with irregularly dilated TDLUs. The cells lining these acini have identical morphological features, although there is cellular stratification of more than two cell layers ( Fig. 19.3 ). There may be cellular crowding or overlapping and, rarely, small tufts or mounds of cells, but no blunt micropapillary projections. Flocculent secretions and calcifications are universal.

Key Diagnostic Points

Flat epithelial atypia

  • Enlarged TDLUs; dilated acini have smooth contours.

  • Low-grade monomorphic cytology in one or more layers of epithelial cells with increased nuclear/cytoplasmic ratios and loss of polarity.

  • Apical snouts and blebs with flocculent secretions; calcifications may show concentric lamellar morphology.

  • No architectural complexity.

  • Frequently associated with ADH, low-grade DCIS, tubular carcinoma, and lobular neoplasia.

  • CCC/CCH and FEA are positive for estrogen receptors (ER) and negative for high molecular weight cytokeratin.

Fig. 19.3, Columnar cell hyperplasia. ( A ) Crowding and pseudostratification of bland nuclei with prominent apical snouts. ( B ) Stratification with bland nuclei and apical cytoplasmic snouts. ( C ) Crowding and stratification of bland oval nuclei and luminal apical blebs. ( D ) Multiple layers of elongated bland nuclei that maintain polarity.

In FEA, the dilated acini of the TDLU are single layered, or lined by three to five flat layers of epithelial cells with low-grade monomorphic cytology, increased nuclear/cytoplasmic ratios, and loss of polarity. The cell population is mostly low cuboidal and sometimes columnar, and the enlarged acini have more regular, round contours. The cytomorphology of these cells is clearly abnormal, manifested as a low-grade monomorphic atypia, in which the nuclei are generally larger, more than twice the size of the nuclei seen in CCC/CCH, rounded, and clearly abnormal in shape, with abnormally shaped nuclear membranes, mild hyperchromasia, occasional small nucleoli, and increased nucleus-to-cytoplasm (N/C) ratios ( Figs. 19.4 to 19.15 ). The cytomorphological features of these cells are virtually identical to those of ADH and low-grade DCIS when present on the same slide. Architecturally, FEA may manifest cellular stratification, but there are no blunt, club-shaped micropapillary projections or Roman bridges ( Fig. 19.16 ). In addition, FEA, including the stratified type, may demonstrate cytoplasmic apocrine features. Recognize that the term flat does not exclude cellular stratification, but it does exclude the architectural manifestations of ADH, namely, rigid bars, arches, and blunt micropapillae. Cytoplasmic blebs/snouts are present but, in general, are reduced. Mitotic figures are very uncommon but may be observed. The diagnosis of FEA must not rest on the presence of mitotic figures. The terminology applied to FEA throughout the years is supplied in Table 19.1 . An algorithmic approach to aid in the differential diagnosis and morphological assessment of columnar cell alterations is illustrated in Fig. 19.17 . Several studies have documented the reproducibility of the diagnosis of FEA and distinction from CCL, with pathologist agreement of 92% and kappa value of 0.83.

Fig. 19.4, Flat epithelial atypia (FEA). ( A ) Low magnification demonstrates a bluer appearance attributed to cellular crowding. Note numerous coarse calcifications. ( B ) FEA with rounded, mildly hyperchromatic nuclei and monotonous morphology.

Fig. 19.5, Slightly dilated flat epithelial atypia (FEA). ( A ) Attenuated cells have monomorphic rounded nuclei. ( B ) Higher magnification of slightly dilated FEA with mildly hyperchromatic rounded nuclei. Loss of apical snouts yields a relative higher nucleus-to-cytoplasm ratio. ( C ) Monomorphic atypia and blunting of apical snouts. ( D ) Calcific debris and monomorphic rounded atypical cells.

Fig. 19.6, Monomorphic atypia of flat epithelial atypia and luminal calcific debris and apical blebs.

Fig. 19.7, Flat epithelial atypia with granular luminal content and monomorphic atypia. Small nucleoli are evident in some cells.

Fig. 19.8, Colloid-like flat epithelial atypia (FEA). ( A ) Low magnification of dilated colloid-like FEA. ( B ) Colloid-like FEA in which these cells have apocrine features and monomorphic atypia. ( C ) Colloid-like FEA shows monomorphic atypia and attenuation of cells with loss of apical snouts. ( D ) Low magnification of dilated colloid-like FEA. This simulates fibrocystic change. ( E ) Colloid-like FEA shows dilatation and blue cellular appearance at medium magnification. ( F ) Higher magnification shows monomorphic atypia within the area of colloid-like FEA (arrow) .

Fig. 19.9, Flat epithelial atypia (FEA) with apocrine features. ( A ) Multilayered FEA with apocrine cytoplasm shows calcific luminal debris. ( B ) Medium magnification of FEA with apocrine features. Note multilayered epithelium, prominent apical snouts, and calcific luminal debris. ( C ) Higher magnification of FEA with apocrine features and calcific debris. Small nucleoli appear in some nuclei. ( D ) This FEA with apocrine features has vacuolated cytoplasm and calcific debris. ( E ) This focus of FEA shows architectural abnormality of atypical duct hyperplasia on the left side of the image with focal early cribriform architecture. ( F ) Apocrine variant of FEA shows monomorphic atypia. ( G ) Apocrine variant of FEA with tenacious luminal secretions and characteristic monomorphic atypia. ( H ) High magnification shows monomorphic atypia and presence of some nucleoli in focal areas. ( I ) Tenacious luminal material in this area of apocrine FEA with characteristic monomorphic cytology.

Fig. 19.10, The right half of this lobule shows flat epithelial atypia. At this magnification, the cells appear bluer and more cellular.

Fig. 19.11, This lobule is virtually completely replaced by flat epithelial atypia, appears bluer, and shows focal cribriform architecture in the middle top of the image.

Fig. 19.12, Multilayered flat epithelial atypia (FEA). ( A ) This entire lobule has been replaced by FEA of the multilayered type with focal architectural abnormality. Compare with the adjacent normal lobule in the upper right. ( B ) Higher magnification of the multilayered FEA and focally cribriform architecture in this lobule.

Fig. 19.13, Cytokeratin 5 in this lobule of flat epithelial atypia (FEA) shows no expression in the FEA but strong expression in the luminal area of usual ductal epithelial hyperplasia.

Fig. 19.14, Estrogen receptor (ER) shows diffuse immunostaining because of ER upregulation, a typical pattern with flat epithelial atypia.

Fig. 19.15, Low-power magnification shows prominent flat epithelial atypia in dilated acini, foci of atypical ductal hyperplasia with Roman arches, and invasive tubular carcinoma on the top half of the image.

Fig. 19.16, Flat epithelial atypia (FEA) adjacent to atypical ductal hyperplasia (ADH). ( A ) The left side of this image shows FEA with apocrine features and the lower right illustrates ADH with cribriform architecture. ( B ) Arch formation in this area of FEA demonstrates identical monomorphic cytology in the bridge as well as in the adjacent epithelium. Note mucinous luminal content. ( C ) FEA, stratified, adjacent to ADH with cribriform architecture. ( D ) FEA conjoined to an area of ADH manifested by micropapillary clubbing. ( E ) Higher magnification of monomorphic cytology of FEA with identical cytological features in the micropapillary clubs.

Fig. 19.17, Algorithmic approach to morphological assessment of columnar-related lesions. ADH , Atypical ductal hyperplasia; CCC , columnar cell change; CCH , columnar cell hyperplasia; DCIS , ductal carcinoma in situ; FEA , flat epithelial atypia.

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