Breast Cancer Biomarkers

Primary carcinoma of the breast is the most common type of breast malignancy. Breast cancer is diagnosed by breast biopsy or excision and is then subsequently staged. Estrogen receptor (ER), progesterone receptor (PR), and human epidermal growth factor receptor 2 (HER2) biomarker testing is performed to establish hormone receptor status, which provides both prognostic and predictive value. Women with early-stage invasive breast cancer and known ER+/PR+/HER2- status may then benefit from prognostic biomarker panels that can provide information to guide decisions about adjuvant systemic therapy. Individuals suspected of hereditary cancer risk may also undergo testing for pathogenic variants (mutations) commonly associated with breast cancer, including variants in BRCA1 and BRCA2 genes.

Tabs Content

Clinical Overview

Quick Answers

What is the definition of estrogen receptor (ER) and progesterone receptor (PR) positivity?

According to the most recent American Society of Clinical Oncology (ASCO) and College of American Pathologists (CAP) guideline, breast cancer tumors are considered estrogen receptor (ER) and/or progesterone receptor (PR) positive if ≥1% of tumor cell nuclei are immunoreactive.

What is the definition of human epidermal growth factor receptor 2 (HER2) positivity? How is HER2 status determined?

There are currently two approved methods for determining human epidermal growth factor receptor 2 (HER2) status in breast cancer: immunohistochemistry (IHC) and in situ hybridization (ISH). Breast cancer tumors are considered HER2+ if they are assigned a score of 3+ by an IHC method or demonstrate HER2 gene amplification by an ISH method. Equivocal results by IHC (considered IHC 2+) should be resolved by reflex testing using the ISH method on the same specimen or repeating tests if a new specimen is available. Equivocal results by an ISH assay must be confirmed by reflex testing using IHC methodology on the same specimen or by repeating tests if a new specimen is available.

When is gene expression signature testing useful in the management of breast cancer?

The results of gene expression signature testing may help a clinician determine if a patient would benefit from chemotherapy and may predict the likelihood of breast cancer recurrence. Oncotype DX, EndoPredict, and Prosigna are three representative multigene tests that are commercially available; refer to the Multiplexed Gene Expression Panels for Prognosis in Early Stage ER+ Breast Cancer table below for more information.

Are serum markers useful in managing breast cancer?

No tumor markers are currently recommended for breast cancer screening. All markers have low sensitivity and specificity when used in a screening setting. However, some markers (eg, cancer antigen [CA] 15-3 and CA 27.29) may be used in monitoring metastatic breast cancer.

Who should be considered for hereditary breast cancer genetic testing?

Any individual suspected of being at risk for hereditary cancer should be offered genetic counseling in order to select appropriate candidates for genetic testing. Genetic testing should be considered in high-risk individuals when it would impact medical management of the tested individual and their at-risk family members. Genetic testing may involve single-gene testing for pathogenic variants (mutations) in genes such as BRCA1/2 or multigene panel testing for additional high- and moderate-penetrance genes associated with breast cancer. Genes that might be included in a panel include BRCA1/2, ATM, CHEK2, PALB2, and TP53.

Which markers are useful for monitoring metastatic breast cancer?

Circulating tumor markers, including cancer antigen (CA) 15-3, CA 27.29, and carcinoembryonic antigen (CEA), may be used for monitoring metastatic breast cancer along with clinical evaluation to determine treatment response. Single measurements are not informative; serial measurements are required, using the same marker sequentially. Circulating tumor cells are not recommended for monitoring cancer recurrence in nonmetastatic breast cancer.

Indications for Testing

Individuals with malignant histology compatible with breast cancer should undergo disease staging, hormone receptor testing, and possible genetic evaluation for prognostic and therapeutic reasons.

Laboratory Testing

Diagnosis and Staging

Diagnosis is established by surgical pathology. Grading and staging are based on histologic features, lymph node involvement, and metastasis. Interpretive guidelines have changed over the years; clinicians are advised to consult the most recent societal statements for recommendations.

Biomarker Testing for Prognosis and Therapy Decisions

Prognostic and therapeutic decisions are made using a combination of tumor features, including ER, PR, and HER2, or ERBB2 status, and, when appropriate, gene expression panels.

Tumor Hormone Receptor Status Testing

ER and PR status should be determined in all patients with invasive breast cancers and breast cancer recurrences. ER and PR expression are generally associated with improved outcomes when the patient is treated with an antiestrogen therapy. ER status is used to determine if a patient should or should not receive adjuvant endocrine therapy. PR status appears to be prognostic and independent of ER, and high levels are generally associated with a favorable outcome.

Human Epidermal Growth Factor Receptor 2 Status

HER2 status should be determined in all patients with invasive breast cancer and first recurrences of breast cancer. HER2 overexpression confers an unfavorable prognosis in the absence of therapy in patients with pathologically node-positive and node-negative breast cancer. Immunohistochemistry (IHC) or in situ hybridization (ISH) methods may be used in the initial evaluation; equivocal results by IHC should be resolved by reflex testing using the ISH method on the same specimen or repeating tests if a new specimen is available. Equivocal results by an ISH assay must be confirmed by reflex testing using IHC methodology on the same specimen or by repeating tests if a new specimen is available.

Multiplexed Gene Expression Assays for Prognosis in Early-Stage, Estrogen Receptor-Positive Breast Cancer

The American Society of Clinical Oncology (ASCO) 2016 recommendations address prognostic biomarker panels that may be helpful in guiding decisions about adjuvant systemic therapy for women with early-stage invasive breast cancer and known ER+/PR+/HER2- status. The results of this testing may help a clinician determine if a patient would benefit from chemotherapy and may also predict the likelihood of breast cancer recurrence. Oncotype DX, EndoPredict, and Prosigna are three representative multigene tests that are commercially available; specifics about these tests are detailed in the table below.

Multiplexed Gene Expression Panels^a for Prognosis in Early-Stage, ER+ Breast Cancer
Marker	Description	Indications for Use	Recommended for HER2+ Breast Cancer	Utility in Late Recurrence
Oncotype DX Breast Recurrence Score (Genomic Health)	Measures expression of 21 genes (16 cancer-related genes and 5 reference genes) to quantify the risk of distant recurrence and the likelihood of chemotherapy benefit	Use to guide decisions for adjuvant systemic chemotherapy	No	No
EndoPredict (Myriad Genetics)	EPclin Risk Score algorithm integrates 12 gene molecular scores, tumor size, and nodal status to generate 10-yr breast cancer recurrence risk score	Use to guide decisions for adjuvant systemic chemotherapy	No	Yes
Prosigna^b Breast Cancer Prognostic Gene Signature Assay (NanoString Technologies)	Proprietary algorithm determines probability of distant recurrence within 10 yrs	Use to guide decisions for adjuvant systemic chemotherapy in conjunction with other clinicopathologic variables	No (U.S. only)	Yes
^aAll three tests are validated in stage N0 and N1 cancers. ^bUsed for prognosis only in ER+ breast cancer in the United States under FDA regulations, but available for use in all breast cancer cases outside the U.S. Refer to www.prosigna.com for more information. FDA, U.S. Food and Drug Administration; NCCN, National Comprehensive Cancer Network Sources: NCCN; Duffy; Harris, ASCO; Ohnstad; Dubsky

Familial Risk (Hereditary) Genetic Testing

Up to 10% of all breast cancers are due to specific pathogenic variants (mutations) in single genes passed down in a family. BRCA1 and BRCA2 are the best characterized and most prevalent breast cancer susceptibility genes, but others (eg, ATM, CDH1, CHEK2, NBN, NFI, PALB2, PTEN, STK11, TP53) are also implicated in conferring an increased susceptibility to breast cancer.

Major organizations agree that any individual suspected of hereditary cancer risk should be offered genetic counseling. The U.S. Preventive Services Task Force (USPSTF) recommends that primary care clinicians assess women with a personal or family history of breast, ovarian, tubal, or peritoneal cancer or who have an ancestry associated with breast cancer susceptibility 1 and 2 (BRCA1/2) gene mutations with an appropriate brief familial risk assessment tool. Women who screen positive should be offered genetic counseling, and if appropriate, BRCA testing. Routine testing is not recommended in women whose personal or family history or ancestry is not associated with an increased risk.

The NCCN recommends that individuals from a family with a known deleterious BRCA1/2 pathogenic variant consider testing. In individuals without a known pathogenic variant, testing should be considered if an individual has a personal history of breast cancer and meets one or more of the following criteria:

Ashkenazi Jewish ancestry
Diagnosed at 45 years of age or younger
Diagnosed with at least two breast cancer primaries, the first at 50 years of age or younger
Diagnosed at 46-50 years of age with any of the following
- One or more close blood relatives with breast cancer at any age
- One or more close blood relatives with high-grade prostate cancer
- An unknown or limited family history
Diagnosed with triple-negative breast cancer at 60 years of age or younger
Diagnosed at any age with one or more close blood relatives with any of the following
- Breast cancer diagnosed at 50 years of age or younger
- Ovarian cancer
- Male breast cancer
- Metastatic prostate cancer
- Pancreatic cancer
Diagnosed at any age with two or more additional diagnoses (in patient and/or close blood relatives) of breast cancer at any age

Additionally, other personal and/or family history meet NCCN BRCA1/2 testing criteria:

Personal history of
- Ovarian cancer
- Male breast cancer
- Metastatic prostate cancer
- High-grade prostate cancer at any age with any of the following
  - One or more close blood relatives with ovarian carcinoma, pancreatic cancer, metastatic prostate cancer at any age, or breast cancer diagnosed before 50 years of age
  - Two or more close blood relatives with breast or prostate cancer (any grade) at any age
  - Ashkenazi Jewish ancestry
- BRCA1/2 pathogenic/likely pathogenic variant detected by tumor profiling of any tumor type in the absence of germline analysis
Regardless of family history, some individuals with a BRCA-related cancer may benefit from genetic testing related to targeted treatments
An individual who does not meet any of the above criteria but has at least one first- or second-degree blood relative who does may also benefit from testing (limitations of testing unaffected individuals should be discussed)

Other Testing

Liquid biopsy and circulating tumor DNA (ctDNA) analysis in breast cancer are emerging areas of research interest, but are not currently recommended as part of the standard of care by societal guidelines.

Monitoring

Cancer antigen (CA) 15-3, CA 27.29, and carcinoembryonic antigen (CEA) may be used to monitor metastatic disease in conjunction with diagnostic imaging, history, and physical examination. Single measurements are uninformative; instead, serial measurements are required, using the same marker sequentially. Increasing values of these markers are concerning for tumor progression, but may also be seen in the setting of responding disease.

The most recent NCCN guidelines do not include recommendations regarding detection of circulating tumor cells in the management of patients with breast cancer. ASCO recommends that clinicians not use circulating tumor cells to guide decisions about adjuvant systemic therapy.

Pharmacogenetics

Many pharmacogenes are associated with drug response and optimal dosing. For example, the drug metabolizing enzyme encoded by CYP2D6 is involved in the conversion of tamoxifen, an antiestrogen drug used in the treatment of ER+ breast cancer, to the active metabolite endoxifen. Neither the NCCN nor ASCO recommend CYP2D6 genotyping to determine optimal adjuvant endocrine strategy. However, gene-based dosing guidelines are available for tamoxifen and many other drugs commonly used in treating patients with breast cancer through the Clinical Pharmacogenetics Implementation Consortium and the Dutch Pharmacogenomics Working Group. In addition to the gene-based dose guidelines, it is important to be aware of common drug-drug interactions. For example, patients who are prescribed tamoxifen should avoid strong CYP2D6 inhibitors, such as most antidepressant drugs.

Refer to the ARUP Consult Germline Pharmacogenetics topic for more information on pharmacogenetics, and the ARUP Laboratories test directory for access to the complete menu of pharmacogenetic tests available at ARUP.

ARUP Lab Tests

ER and PR Testing

Prognostic and predictive testing

Estrogen/Progesterone Receptor with Interpretation by Immunohistochemistry 0049210

Method: Immunohistochemistry

Estrogen Receptor (ER) by Immunohistochemistry 2004516

Method: Immunohistochemistry

Progesterone Receptor (PR) by Immunohistochemistry 2004525

Method: Immunohistochemistry

HER2 Testing

Prognostic and predictive testing

Includes reflex testing in case of equivocal result

ERBB2 (HER2/neu) (HercepTest) by Immunohistochemistry, Tissue with Reflex to FISH if 2+ 0049178

Method: Immunohistochemistry

Prognostic and predictive testing

Alternate test to confirm equivocal fluorescence in situ hybridization (FISH) result

ERBB2 (HER2/neu) (HercepTest) with Interpretation by Immunohistochemistry, Tissue 0049174

Method: Immunohistochemistry

Prognostic and predictive testing

Alternate test to confirm equivocal IHC result

ERBB2 (HER2/neu) Gene Amplification by FISH with Reflex, Tissue 2008603

Method: Fluorescence in situ Hybridization

Prognostic and predictive testing

ERBB2 (HER2) (HercepTest) by Immunohistochemistry 2007332

Method: Immunohistochemistry

Hereditary Genetic Testing

Recommended test to confirm hereditary breast and ovarian cancer (HBOC) syndrome

Includes only BRCA1/BRCA2 genes

Breast and Ovarian Hereditary Cancer Syndrome (BRCA1 and BRCA2) Sequencing and Deletion/Duplication 2011949

Method: Polymerase Chain Reaction/Sequencing/Multiplex Ligation-dependent Probe Amplification

Acceptable test to confirm HBOC syndrome

Includes only BRCA1/BRCA2 genes

Breast and Ovarian Hereditary Cancer Syndrome (BRCA1 and BRCA2) Sequencing 2011954

Method: Polymerase Chain Reaction/ Sequencing

Recommended test to confirm diagnosis of hereditary breast and/or ovarian cancer in individuals with a personal or family history of breast and/or ovarian cancer

Refer to Test Fact Sheet for full list of genes tested

Hereditary Breast and Ovarian Cancer Panel, Sequencing and Deletion/Duplication 2012026

Method: Massively Parallel Sequencing/Exonic Oligonucleotide-based CGH Microarray

Recommended test to confirm diagnosis of hereditary cancer syndrome in individuals with a personal or family history consistent with features of more than one cancer syndrome

Refer to Test Fact Sheet for full list of genes tested

Hereditary Cancer Panel, Sequencing and Deletion/Duplication 2012032

Method: Massively Parallel Sequencing/Exonic Oligonucleotide-based CGH Microarray

Recommended test if there is a known familial sequence variant previously identified in a family member

Familial Mutation, Targeted Sequencing 2001961

Method: Polymerase Chain Reaction/Sequencing

Monitoring

Monitor therapy and identify disease recurrence in metastatic breast cancer

Cancer Antigen-Breast (CA 15-3) 0080464

Method: Quantitative Electrochemiluminescent Immunoassay

Cancer Antigen 27.29 0080392

Method: Quantitative Chemiluminescent Immunoassay

Carcinoembryonic Antigen 0080080

Method: Quantitative Electrochemiluminescent Immunoassay

HER2/neu Quantitative by ELISA 2004672

Method: Quantitative Enzyme-Linked Immunosorbent Assay

Test Fact Sheet(s)

Hereditary Breast and Ovarian Cancer

Hereditary Cancer Panel

Medical Experts

Bernard, Philip S., MD, Medical Director, Molecular Oncology at ARUP Laboratories; Associate Professor of Anatomic Pathology, University of Utah

McMillin, Gwendolyn A., PhD, Medical Director, Toxicology; Medical Director, Pharmacogenetics; and Scientific Director, Mass Spectrometry, at ARUP Laboratories; Professor of Clinical Pathology, University of Utah

Wiley, Samantha, MS, LCGC, Genetic Counselor, Molecular Genetics, at ARUP Laboratories

References

Hammond EH, Hayes DF, Dowsett M, Allred C, Hagerty KL, Badve S, Fitzgibbons PL, Francis G, Goldstein NS, Hayes M, Hicks DG, Lester S, Love R, Mangu PB, McShane L, Miller K, Osborne K, Paik S, Perlmutter J, Rhodes A, Sasano H, Schwartz JN, Sweep FC, Taube S, Torlakovic EE, Valenstein P, Viale G, Visscher D, Wheeler T, Williams B, Wittliff JL, Wolff AC, American Society of Clinical Oncology, College of American Pathologists. American Society of Clinical Oncology/College of American Pathologists guideline recommendations for immunohistochemical testing of estrogen and progesterone receptors in breast cancer (unabridged version). Arch Pathol Lab Med. 2010; 134(7): e48-72. PubMed
NCCN Clinical Practice Guidelines in Oncology, Breast Cancer. Version 4.2018. National Comprehensive Cancer Network. Fort Washington, PA [Accessed: Mar 2019]
Wolff AC, Hammond EH, Allison KH, Harvey BE, Mangu PB, Bartlett JM, Bilous M, Ellis IO, Fitzgibbons P, Hanna W, Jenkins RB, Press MF, Spears PA, Vance GH, Viale G, McShane LM, Dowsett M. Human Epidermal Growth Factor Receptor 2 Testing in Breast Cancer: American Society of Clinical Oncology/College of American Pathologists Clinical Practice Guideline Focused Update. J Clin Oncol. 2018; 36(20): 2105-2122. PubMed
Harris L, Fritsche H, Mennel R, Norton L, Ravdin P, Taube S, Somerfield MR, Hayes DF, Bast RC, American Society of Clinical Oncology. American Society of Clinical Oncology 2007 update of recommendations for the use of tumor markers in breast cancer. J Clin Oncol. 2007; 25(33): 5287-312. PubMed
NCCN Genetic/Familial high-risk assessment Breast and Ovarian Version 3.2019. National Comprehensive Cancer Network. Fort Washington, PA [Accessed: Mar 2019]
U.S. Preventive Services Task Force. BRCA-Related Cancer: Risk Assessment, Genetic Counseling, and Genetic Testing. Rockville, MD [Accessed: Aug 2019]
Van Poznak C, Somerfield MR, Bast RC, Cristofanilli M, Goetz MP, Gonzalez-Angulo AM, Hicks DG, Hill EG, Liu MC, Lucas W, Mayer IA, Mennel RG, Symmans WF, Hayes DF, Harris LN. Use of Biomarkers to Guide Decisions on Systemic Therapy for Women With Metastatic Breast Cancer: American Society of Clinical Oncology Clinical Practice Guideline. J Clin Oncol. 2015; 33(24): 2695-704. PubMed
Duffy MJ, Walsh S, McDermott EW, Crown J. Biomarkers in breast cancer: where are we and where are we going? Adv Clin Chem. 2015; 71: 1-23. PubMed
Harris LN, Ismaila N, McShane LM, Andre F, Collyar DE, Gonzalez-Angulo AM, Hammond EH, Kuderer NM, Liu MC, Mennel RG, Van Poznak C, Bast RC, Hayes DF. Use of Biomarkers to Guide Decisions on Adjuvant Systemic Therapy for Women With Early-Stage Invasive Breast Cancer: American Society of Clinical Oncology Clinical Practice Guideline. J Clin Oncol. 2016; 34(10): 1134-50. PubMed
Ohnstad HO, Borgen E, Falk RS, Lien TG, Aaserud M, Sveli MA, Kyte JA, Kristensen VN, Geitvik GA, Schlichting E, Wist EA, Sørlie T, Russnes HG, Naume B. Prognostic value of PAM50 and risk of recurrence score in patients with early-stage breast cancer with long-term follow-up. Breast Cancer Res. 2017; 19(1): 120. PubMed
Dubsky P, Brase JC, Jakesz R, Rudas M, Singer CF, Greil R, Dietze O, Luisser I, Klug E, Sedivy R, Bachner M, Mayr D, Schmidt M, Gehrmann MC, Petry C, Weber KE, Fisch K, Kronenwett R, Gnant M, Filipits M, Austrian Breast and Colorectal Cancer Study Group (ABCSG). The EndoPredict score provides prognostic information on late distant metastases in ER+/HER2- breast cancer patients. Br J Cancer. 2013; 109(12): 2959-64. PubMed

Additional Resources

Cardoso F, Senkus E, Costa A, Papadopoulos E, Aapro M, André F, Harbeck N, Lopez A, Barrios CH, Bergh J, Biganzoli L, Boers-Doets CB, Cardoso MJ, Carey LA, Cortés J, Curigliano G, Diéras V, Saghir NS, Eniu A, Fallowfield L, Francis PA, Gelmon K, Johnston SR, Kaufman B, Koppikar S, Krop IE, Mayer M, Nakigudde G, Offersen BV, Ohno S, Pagani O, Paluch-Shimon S, Penault-Llorca F, Prat A, Rugo HS, Sledge GW, Spence D, Thomssen C, Vorobiof DA, Xu B, Norton L, Winer EP. 4th ESO-ESMO International Consensus Guidelines for Advanced Breast Cancer (ABC 4)†. Ann Oncol. 2018; 29(8): 1634-1657. PubMed

Qaseem A, Lin JS, Mustafa RA, Horwitch CA, Wilt TJ, for the Clinical Guidelines Committee of the American College of Physicians. Screening for Breast Cancer in Average-Risk Women: A Guidance Statement From the American College of Physicians.. Ann Intern Med. [Epub ahead of print: Apr 2019; Accessed: Apr 2019]

Resources from the ARUP Institute for Clinical and Experimental Pathology®

Bastien RR, Rodríguez-Lescure A, Ebbert MT, Prat A, Munárriz B, Rowe L, Miller P, Ruiz-Borrego M, Anderson D, Lyons B, Álvarez I, Dowell T, Wall D, Seguí M, Barley L, Boucher KM, Alba E, Pappas L, Davis CA, Aranda I, Fauron C, Stijleman IJ, Palacios J, Antón A, Carrasco E, Caballero R, Ellis MJ, Nielsen TO, Perou CM, Astill M, Bernard PS, Martín M. PAM50 breast cancer subtyping by RT-qPCR and concordance with standard clinical molecular markers. BMC Med Genomics. 2012; 5: 44. PubMed

Caan BJ, Sweeney C, Habel LA, Kwan ML, Kroenke CH, Weltzien EK, Quesenberry CP, Castillo A, Factor RE, Kushi LH, Bernard PS. Intrinsic subtypes from the PAM50 gene expression assay in a population-based breast cancer survivor cohort: prognostication of short- and long-term outcomes. Cancer Epidemiol Biomarkers Prev. 2014; 23(5): 725-34. PubMed

Carey LA, Rugo HS, Marcom K, Mayer EL, Esteva FJ, Ma CX, Liu MC, Storniolo AM, Rimawi MF, Forero-Torres A, Wolff AC, Hobday TJ, Ivanova A, Chiu W, Ferraro M, Burrows E, Bernard PS, Hoadley KA, Perou CM, Winer EP. TBCRC 001: randomized phase II study of cetuximab in combination with carboplatin in stage IV triple-negative breast cancer. J Clin Oncol. 2012; 30(21): 2615-23. PubMed

Cohen AL, Factor RE, Mooney K, Salama ME, Wade M, Serpico V, Ostrander E, Nelson E, Porretta J, Matsen C, Bernard P, Boucher K, Neumayer L. POWERPIINC (PreOperative Window of Endocrine TheRapy Provides Information to Increase Compliance) trial: Changes in tumor proliferation index and quality of life with 7 days of preoperative tamoxifen. Breast. 2017; 31: 219-223. PubMed

Factor RE, Schmidt RL, Chadwick BE, Witt BJ, Morgan M, Neumayer LA, Layfield LJ. Axillary lymph node FNA in women with breast cancer is a highly accurate procedure, so why are core biopsies being done? Diagn Cytopathol. 2015; 43(6): 510-2. PubMed

Geiersbach KB, Willmore-Payne C, Pasi AV, Paxton CN, Werner TL, Xu X, Wittwer CT, Gulbahce E, Downs-Kelly E. Genomic Copy Number Analysis of HER2-Equivocal Breast Cancers. Am J Clin Pathol. 2016; 146(4): 439-47. PubMed

Kallak K, Baumgart J, Evers S, Poromaa S, Moby L, Kask K, Norjavaara E, Kushnir MM, Bergquist J, Nilsson K. Higher than expected estradiol levels in aromatase inhibitor-treated, postmenopausal breast cancer patients. Climacteric. 2012; 15(5): 473-80. PubMed

Kroenke CH, Sweeney C, Kwan ML, Quesenberry CP, Weltzien EK, Habel LA, Castillo A, Bernard PS, Factor RE, Kushi LH, Caan BJ. Race and breast cancer survival by intrinsic subtype based on PAM50 gene expression. Breast Cancer Res Treat. 2014; 144(3): 689-99. PubMed

Kwan ML, Bernard PS, Kroenke CH, Factor RE, Habel LA, Weltzien EK, Castillo A, Gunderson EP, Maxfield KS, Stijleman IJ, Langholz BM, Quesenberry CP, Kushi LH, Sweeney C, Caan BJ. Breastfeeding, PAM50 tumor subtype, and breast cancer prognosis and survival. J Natl Cancer Inst. 2015; 107(7): PubMed

Kwan ML, Kroenke CH, Sweeney C, Bernard PS, Weltzien EK, Castillo A, Factor RE, Maxfield KS, Stijleman IJ, Kushi LH, Quesenberry CP, Habel LA, Caan BJ. Association of high obesity with PAM50 breast cancer intrinsic subtypes and gene expression. BMC Cancer. 2015; 15: 278. PubMed

Layfield LJ, Schmidt RL. HER2/neu gene amplification heterogeneity: the significance of cells with a 3:1 HER2/CEP17 ratio. Appl Immunohistochem Mol Morphol. 2012; 20(6): 543-9. PubMed

Liu J, Welm B, Boucher KM, Ebbert MT, Bernard PS. TRIM29 functions as a tumor suppressor in nontumorigenic breast cells and invasive ER+ breast cancer. Am J Pathol. 2012; 180(2): 839-47. PubMed

Martín M, Brase JC, Ruiz A, Prat A, Kronenwett R, Calvo L, Petry C, Bernard PS, Ruiz-Borrego M, Weber KE, Rodriguez CA, Alvarez IM, Segui MA, Perou CM, Casas M, Carrasco E, Caballero R, Rodríguez-Lescure A. Prognostic ability of EndoPredict compared to research-based versions of the PAM50 risk of recurrence (ROR) scores in node-positive, estrogen receptor-positive, and HER2-negative breast cancer. A GEICAM/9906 sub-study. Breast Cancer Res Treat. 2016; 156(1): 81-9. PubMed

Okal A, Matissek KJ, Matissek SJ, Price R, Salama ME, Janát-Amsbury MM, Lim CS. Re-engineered p53 activates apoptosis in vivo and causes primary tumor regression in a dominant negative breast cancer xenograft model. Gene Ther. 2014; 21(10): 903-12. PubMed

Prat A, Cheang MC, Martín M, Parker JS, Carrasco E, Caballero R, Tyldesley S, Gelmon K, Bernard PS, Nielsen TO, Perou CM. Prognostic significance of progesterone receptor-positive tumor cells within immunohistochemically defined luminal A breast cancer. J Clin Oncol. 2013; 31(2): 203-9. PubMed

Sheffield BS, Kos Z, Asleh-Aburaya K, Wang XQ, Leung S, Gao D, Won J, Chow C, Rachamadugu R, Stijleman I, Wolber R, Gilks B, Myles N, Thomson T, Hayes MM, Bernard PS, Nielsen TO, Chia SK. Molecular subtype profiling of invasive breast cancers weakly positive for estrogen receptor. Breast Cancer Res Treat. 2016; 155(3): 483-90. PubMed

Sweeney C, Bernard PS, Factor RE, Kwan ML, Habel LA, Quesenberry CP, Shakespear K, Weltzien EK, Stijleman IJ, Davis CA, Ebbert MT, Castillo A, Kushi LH, Caan BJ. Intrinsic subtypes from PAM50 gene expression assay in a population-based breast cancer cohort: differences by age, race, and tumor characteristics. Cancer Epidemiol Biomarkers Prev. 2014; 23(5): 714-24. PubMed

Thompson MD, Grubbs CJ, Bode AM, Reid JM, McGovern R, Bernard PS, Stijleman IJ, Green JE, Bennett C, Juliana M, Moeinpour F, Steele VE, Lubet RA. Lack of effect of metformin on mammary carcinogenesis in nondiabetic rat and mouse models. Cancer Prev Res (Phila). 2015; 8(3): 231-9. PubMed

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Won JR, Gao D, Chow C, Cheng J, Lau SY, Ellis MJ, Perou CM, Bernard PS, Nielsen TO. A survey of immunohistochemical biomarkers for basal-like breast cancer against a gene expression profile gold standard. Mod Pathol. 2013; 26(11): 1438-50. PubMed

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Breast Cancer Biomarkers

Quick Answers

What is the definition of estrogen receptor (ER) and progesterone receptor (PR) positivity?

What is the definition of human epidermal growth factor receptor 2 (HER2) positivity? How is HER2 status determined?

When is gene expression signature testing useful in the management of breast cancer?

Are serum markers useful in managing breast cancer?

Who should be considered for hereditary breast cancer genetic testing?

Which markers are useful for monitoring metastatic breast cancer?

Indications for Testing

Laboratory Testing

Diagnosis and Staging

Biomarker Testing for Prognosis and Therapy Decisions

Tumor Hormone Receptor Status Testing

Human Epidermal Growth Factor Receptor 2 Status

Multiplexed Gene Expression Assays for Prognosis in Early-Stage, Estrogen Receptor-Positive Breast Cancer

Familial Risk (Hereditary) Genetic Testing

Other Testing

Monitoring

Pharmacogenetics

ARUP Lab Tests

Test Fact Sheet(s)

Medical Experts

References

Additional Resources

Resources from the ARUP Institute for Clinical and Experimental Pathology®

ARUP Laboratories

ARUP Websites

ARUP Consult