Fibrocystic breast changes

Last updated: June 13, 2023

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Summary

Fibrocystic breast changes is a nonspecific term that includes a heterogeneous spectrum of breast conditions. Women between 20 and 50 years of age are most commonly affected. Histologically, fibrocystic changes are divided into nonproliferative breast lesions (e.g., simple breast cysts, apocrine metaplasia) and proliferative breast lesions (e.g., ductal epithelial hyperplasia, sclerosing adenosis). Patients typically present with premenstrual bilateral multifocal breast pain with or without palpable nodules, which may be tender. The diagnosis is made during the workup of symptoms (e.g., mastalgia, palpable breast mass, nipple discharge) or incidentally on clinical breast examination and/or imaging. Tissue biopsy, usually a core-needle biopsy, is indicated if there is a clinical suspicion of malignancy. Management of breast lesions without cellular atypia is primarily symptomatic. Proliferative breast lesions with cellular atypia require surgical excision as they are associated with an increased risk of breast cancer.

Epidemiology

Most common benign lesion of the breast
Peak age: 20–50 years
Up to 50% of women are affected during their lifetime.

Epidemiological data refers to the US, unless otherwise specified.

Clinical features

Premenstrual bilateral multifocal breast pain (cyclic mastalgia)
Tender or nontender breast nodules
Clear or slightly milky nipple discharge

Subtypes and variants

Nonproliferative breast lesions ^[2]^[3]^[4]

Simple breast cysts: circumscribed fluid-filled lesions (blue dome cysts)
Stromal fibrosis (no malignant potential)
Apocrine metaplasia

Proliferative breast lesions (with or without cellular atypia) ^[2]^[4]

Sclerosing adenosis
- Proliferation of small ductules and acini in the lobules
- Stromal fibrosis ^[5]
- Calcifications (slightly increased risk of breast cancer)
Ductal epithelial hyperplasia (ductal hyperplasia)
- Epithelial hyperplasia of terminal duct cells and lobular epithelium
- The presence of atypical cells is associated with an increased risk of breast cancer.
- Papillary proliferation (papillomatosis) is a type of ductal hyperplasia that has a papillary histopathological appearance.
Radial scar
Fibroadenoma
Intraductal papilloma

Fibrocystic disease of the breast Fibrocystic breast changes

Diagnostics

General principles ^[2]^[6]

Obtain a thorough medical history and perform a CBE in all patient
Diagnostic workup should be guided by clinical findings.
See also “Breast mass,” “Mastalgia,” “Nipple discharge,” and “Breast cysts” as needed.

All patients with a palpable breast mass should be evaluated appropriately, even those with suspected fibrocystic breast changes. ^[2]

Imaging

Follow age-appropriate diagnostic workup for a palpable breast mass. The imaging findings in fibrocystic breast changes are heterogeneous and include the following.

Breast ultrasound

Scattered calcifications
Clustered microcysts ^[7]^[8]
Simple or complicated cysts (see “Breast cysts” for details). ^[9]^[10]
Distorted breast parenchyma ^[10]^[11]

Oval retroareolar breast mass

Mammography ^[11]^[12]

Focal asymmetry
Architectural distortion
Round or oval masses with circumscribed borders
Calcifications

Breast calcifications

MRI breast with and without contrast (not routinely obtained) ^[4]

Nonmass enhancement
Isointense or hypointense masses with fluid components
Low-intensity T1 weighted round or oval masses

Biopsy

In patients with suspicious clinical and/or imaging findings, a tissue biopsy is indicated to rule out malignancy.” See “Histologic subtypes” for findings ^[4]^[13]

Core needle biopsy (CNB): preferred for most lesions ^[13]
Excisional biopsy: Consider in the following situations ^[2]
- CNB findings suggestive of radial scar, atypical hyperplasia ^[2]
- Imaging and needle biopsy findings are discordant.

Management

Nonproliferative breast lesions or proliferative breast lesions without atypia

Symptomatic management ^[6]
- Proper breast support (i.e., a well-fitting bra)
- Consider topical NSAIDs, tamoxifen; , or danazol for moderate to severe symptoms.
- See “Management of mastalgia” for details.
Management of breast cysts (e.g., surveillance, FNAC, or excision)
Age-appropriate routine breast cancer surveillance is sufficient. ^[2]

Proliferative breast lesions with atypia (specifically atypical ductal hyperplasia) ^[2]

Surgical excision, followed by close surveillance for breast cancer with CBE and imaging ^[2]
Chemoprevention (e.g., tamoxifen, raloxifene, or aromatase inhibitors) can be considered for further risk reduction. ^[2]

Atypical ductal hyperplasia is associated with an increased risk of breast cancer in both the affected and contralateral breast. ^[2]

Prognosis

Nonproliferative breast lesions are not associated with an increased risk of breast cancer.
Proliferative breast lesions with atypical cells (e.g., ductal epithelial hyperplasia) are associated with an increased risk of cancer.

References

ACOG. Practice Bulletin No. 164 Diagnosis and management of benign breast disorders. Obstetrics & Gynecology. 2016; 127 (6): p.e141-e156.doi: 10.1097/aog.0000000000001482 . | Open in Read by QxMD
Zendehdel M, Niakan B, Keshtkar A, Rafiei E, Salamat F. Subtypes of Benign Breast Disease as a Risk Factor for Breast Cancer: A Systematic Review and Meta-Analysis Protocol.. Iranian journal of medical sciences. 2018; 43 (1): p.1-8.
Choe AI, Kasales C, Mack J, Al-Nuaimi M, Karamchandani DM. Fibrocystic Changes of the Breast: Radiologic–Pathologic Correlation of MRI. J of Breast Imaging. 2021; 4 (1): p.48-55.doi: 10.1093/jbi/wbab071 . | Open in Read by QxMD
Visscher DW, Nassar A, Degnim AC, et al. Sclerosing adenosis and risk of breast cancer.. Breast Cancer Res Treat. 2014; 144 (1): p.205-12.doi: 10.1007/s10549-014-2862-5 . | Open in Read by QxMD
Salzman B, Collins E, Hersh L. Common Breast Problems. Am Fam Physician. 2019; 99 (8): p.505-514.
Goldbach AR, Tuite CM, Ross E. Clustered Microcysts at Breast US: Outcomes and Updates for Appropriate Management Recommendations. Radiology. 2020; 295 (1): p.44-51.doi: 10.1148/radiol.2020191505 . | Open in Read by QxMD
Rinaldi P, Ierardi C, Costantini M, et al. Cystic Breast Lesions. J Ultrasound Med. 2010; 29 (11): p.1617-1626.doi: 10.7863/jum.2010.29.11.1617 . | Open in Read by QxMD
Maimone S, Ocal IT, Robinson KA, Wasserman MC, Maxwell RW. Characteristics and Management of Male Breast Parenchymal Cysts. J Breast Imaging. 2020; 2 (4): p.330-335.doi: 10.1093/jbi/wbaa035 . | Open in Read by QxMD
Cho SH, Park SH. Mimickers of Breast Malignancy on Breast Sonography. Journal Ultrasound Med. 2013; 32 (11): p.2029-2036.doi: 10.7863/ultra.32.11.2029 . | Open in Read by QxMD
Choe J, Chikarmane SA, Giess CS. Nonmass Findings at Breast US: Definition, Classifications, and Differential Diagnosis. RadioGraphics. 2020; 40 (2): p.326-335.doi: 10.1148/rg.2020190125 . | Open in Read by QxMD
Cheung H, Parker EU, Yu M, Kilgore MR, Lam DL. Radiologic and Pathologic Correlation for Benign Breast Processes. Curr Breast Cancer Rep. 2021; 13 (4): p.381-397.doi: 10.1007/s12609-021-00438-8 . | Open in Read by QxMD
Moy L, Heller SL, Bailey L, et al. ACR Appropriateness Criteria ® Palpable Breast Masses. J Am Coll Radiol. 2017; 14 (5): p.S203-S224.doi: 10.1016/j.jacr.2017.02.033 . | Open in Read by QxMD
$Contributor Disclosures - Fibrocystic breast changes. None of the individuals in control of the content for this article reported relevant financial relationships with ineligible companies. For details, please review our full conflict of interest (COI) policy:.

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