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Epidermal Growth Factor Receptor Status in Breast Cancer
Metastases to the Central Nervous System. Comparison With HER-2/neu
Status
Nichon L. Grupka, MD, Kelly C. Lear-Kaul, MD, Bette K.
Kleinschmidt-DeMasters, MD, and Meenakshi Singh, MD
From the Department of Pathology, University of Colorado
Health Sciences Center, Denver (Drs Grupka, Kleinschmidt-DeMasters, and Singh);
and the Office of the Medical Investigator, University of New Mexico,
Albuquerque (Dr Lear-Kaul). Reprints: Meenakshi Singh, MD, Department of
Pathology, Box B216, 4200 E 9th Ave, University of Colorado Health Sciences
Center, Denver, CO 80262 (E-mail: meenakshi.singh@uchsc.edu). Accepted
May 7, 2004.
Context. The development of drug
therapies (ZD1839) targeting epidermal growth factor receptor (EGFR) offers a
pragmatic reason for exploring expression of EGFR in breast cancer, particularly
metastatic breast cancer.
There is a reported synergistic relationship between trastuzumab and ZD1839
therapy in patients with breast cancer.
Although EGFR is the preferred dimerization partner for HER-2, it is unclear
whether expression of these 2 interrelated receptors in a given patient with
breast cancer would be parallel or mutually exclusive.
Objectives. To assess EGFR status in primary breast carcinoma versus
metastatic central nervous system (CNS) sites and to compare results with HER-2/neu
status in the same tumor.
Design. Central nervous system metastases (n = 51) from 33 patients
and corresponding primary breast cancer specimens, when available (n = 11), were
immunohistochemically stained for EGFR using a monoclonal mouse anti-EGFR
antibody (clone 31G7) that recognizes both the wild-type form and the 145-kd
variant III form of EGFR.
The sections were evaluated by visual and image analysis techniques, and results
were compared to previously assessed HER-2/neu status.
Results. Epidermal growth factor receptor expression was found in
CNS metastases from 39% of patients, with 82% concordance between the EGFR
status of the primary breast and metastatic sites, and 92% concordance between
the EGFR status among multiple CNS metastases in a given patient.
Epidermal growth factor receptor and HER-2/neu status were concordant at
the primary site in only 45% of patients.
Additionally, EGFR and HER-2/neu status were concordant among multiple
CNS metastases per individual case in only 45% of patients.
Conclusion. Thirty-nine percent of patients with metastatic breast
cancer express EGFR, with parallel expression between metastatic sites and the
primary neoplasm in 82% of the cases.
The discordance in 18% of the cases, however, suggests that anti-EGFR agents
might not show equal efficacy against metastatic tumor deposits and the primary
tumor within a given patient.
An additional corollary for pathologists based on this nonhomogeneity of
receptor expression is that both the primary breast and multiple metastatic
tumor deposits may need to be individually assessed for EGFR status.
In our study, most metastatic tumor deposits showed expression for either EGFR
or HER-2/neu, and less often for both, implying that drug therapies could
be individualized for patients based on test results for both receptors.
Presented in part at the Ninth Annual Breast Multidisciplinary
Symposium, Amelia Island, Fla, February 12–15, 2004.
© Copyright by College of American
Pathologists 2004
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