The dilemma of HER2 double-equivocal breast carcinomas: Genomic profiling and implications for treatment

Caterina Marchiò; Patrizia Dell'Orto; Laura Annaratone; Felipe C. Geyer; Tiziana Venesio; Enrico Berrino; Ludovica Verdun Di Cantogno; Andrea Garofoli; Nelson Rangel; Laura Casorzo; Carmine dell'Aglio; Patrizia Gugliotta; Elena Trisolini; Alessandra Beano; Francesca Pietribiasi; Renzo Orlassino; Paola Cassoni; Achille Pich; Filippo Montemurro; Marcella Mottolese; Anne Vincent-Salomon; Frédérique Penault-Llorca; Enzo Medico; Charlotte K.Y. Ng; Giuseppe Viale; Anna Sapino

doi:10.1097/PAS.0000000000001100

The dilemma of HER2 double-equivocal breast carcinomas: Genomic profiling and implications for treatment

Caterina Marchiò, Patrizia Dell'Orto, Laura Annaratone, Felipe C. Geyer, Tiziana Venesio, Enrico Berrino, Ludovica Verdun Di Cantogno, Andrea Garofoli, Nelson Rangel, Laura Casorzo, Carmine dell'Aglio, Patrizia Gugliotta, Elena Trisolini, Alessandra Beano, Francesca Pietribiasi, Renzo Orlassino, Paola Cassoni, Achille Pich, Filippo Montemurro, Marcella MottoleseAnne Vincent-Salomon, Frédérique Penault-Llorca, Enzo Medico, Charlotte K.Y. Ng, Giuseppe Viale, Anna Sapino

Producción: Contribución a una revista › Artículo › revisión exhaustiva

20 Citas (Scopus)

Resumen

The American Society of Clinical Oncology/College of American Pathologists (ASCO/CAP) 2013 guidelines for HER2 assessment have increased the number of HER2 equivocal breast carcinomas following in situ hybridization reflex testing, that is, HER2 "double equivocal" (equivocal protein expression and equivocal gene copy number). Forty-five double-equivocal carcinomas were subjected to Prosigna analysis. Twenty-seven cases were investigated for the expression of genes found to be differentially expressed between estrogen receptor (ER)-positive/HER2-positive (N =22) and ER-positive/HER2-negative (N =22) control cases. Twenty-nine of the 45 cases were also analyzed by targeted sequencing using a panel of 14 genes. We then explored the pathologic complete response rates in an independent series of double-equivocal carcinoma patients treated with trastuzumab-containing chemotherapy. All cases were ER-positive, with a mean Ki67 of 28%. Double-equivocal carcinomas were predominantly luminal B (76%); 9 cases (20%) were luminal A, and 2 cases (4%) HER2-enriched. The majority (73%) showed a high risk of recurrence by Prosigna, even when the carcinomas were small (< 2 cm), node-negative/micrometastatic, and/or grade 2. Double-equivocal carcinomas showed TP53 (6/29, 20%), PIK3CA (3/29, 10%), HER2 (1/29, 3%), and MAP2K4 (1/29, 3%) mutations. Compared with grade-matched ER-positive/HER2-negative breast carcinomas from METABRIC, double-equivocal carcinomas harbored more frequently TP53 mutations and less frequently PIK3CA mutations (P < 0.05). No significant differences were observed with grade-matched ER-positive/HER2-positive carcinomas. Lower pathologic complete response rates were observed in double-equivocal compared with HER2-positive patients (10% vs. 60%, P= 0.009). Double-equivocal carcinomas are preferentially luminal B and show a high risk of recurrence. A subset of these tumors can be labeled as HER2-enriched by transcriptomic analysis. HER2 mutations can be identified in HER2 double-equivocal cases.

Idioma original	Inglés
Páginas (desde-hasta)	1190-1200
Número de páginas	11
Publicación	American Journal of Surgical Pathology
Volumen	42
N.º	9
DOI	https://doi.org/10.1097/PAS.0000000000001100
Estado	Publicada - 01 sep. 2018
Publicado de forma externa	Sí

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Marchiò, C., Dell'Orto, P., Annaratone, L., Geyer, F. C., Venesio, T., Berrino, E., Di Cantogno, L. V., Garofoli, A., Rangel, N., Casorzo, L., dell'Aglio, C., Gugliotta, P., Trisolini, E., Beano, A., Pietribiasi, F., Orlassino, R., Cassoni, P., Pich, A., Montemurro, F., ... Sapino, A. (2018). The dilemma of HER2 double-equivocal breast carcinomas: Genomic profiling and implications for treatment. American Journal of Surgical Pathology, 42(9), 1190-1200. https://doi.org/10.1097/PAS.0000000000001100

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title = "The dilemma of HER2 double-equivocal breast carcinomas: Genomic profiling and implications for treatment",

abstract = "The American Society of Clinical Oncology/College of American Pathologists (ASCO/CAP) 2013 guidelines for HER2 assessment have increased the number of HER2 equivocal breast carcinomas following in situ hybridization reflex testing, that is, HER2 {"}double equivocal{"} (equivocal protein expression and equivocal gene copy number). Forty-five double-equivocal carcinomas were subjected to Prosigna analysis. Twenty-seven cases were investigated for the expression of genes found to be differentially expressed between estrogen receptor (ER)-positive/HER2-positive (N =22) and ER-positive/HER2-negative (N =22) control cases. Twenty-nine of the 45 cases were also analyzed by targeted sequencing using a panel of 14 genes. We then explored the pathologic complete response rates in an independent series of double-equivocal carcinoma patients treated with trastuzumab-containing chemotherapy. All cases were ER-positive, with a mean Ki67 of 28%. Double-equivocal carcinomas were predominantly luminal B (76%); 9 cases (20%) were luminal A, and 2 cases (4%) HER2-enriched. The majority (73%) showed a high risk of recurrence by Prosigna, even when the carcinomas were small (< 2 cm), node-negative/micrometastatic, and/or grade 2. Double-equivocal carcinomas showed TP53 (6/29, 20%), PIK3CA (3/29, 10%), HER2 (1/29, 3%), and MAP2K4 (1/29, 3%) mutations. Compared with grade-matched ER-positive/HER2-negative breast carcinomas from METABRIC, double-equivocal carcinomas harbored more frequently TP53 mutations and less frequently PIK3CA mutations (P < 0.05). No significant differences were observed with grade-matched ER-positive/HER2-positive carcinomas. Lower pathologic complete response rates were observed in double-equivocal compared with HER2-positive patients (10% vs. 60%, P= 0.009). Double-equivocal carcinomas are preferentially luminal B and show a high risk of recurrence. A subset of these tumors can be labeled as HER2-enriched by transcriptomic analysis. HER2 mutations can be identified in HER2 double-equivocal cases.",

keywords = "Breast carcinoma, Equivocal result, HER2, Molecular subtype, Mutations, Risk of recurrence",

author = "Caterina Marchi{\`o} and Patrizia Dell'Orto and Laura Annaratone and Geyer, {Felipe C.} and Tiziana Venesio and Enrico Berrino and {Di Cantogno}, {Ludovica Verdun} and Andrea Garofoli and Nelson Rangel and Laura Casorzo and Carmine dell'Aglio and Patrizia Gugliotta and Elena Trisolini and Alessandra Beano and Francesca Pietribiasi and Renzo Orlassino and Paola Cassoni and Achille Pich and Filippo Montemurro and Marcella Mottolese and Anne Vincent-Salomon and Fr{\'e}d{\'e}rique Penault-Llorca and Enzo Medico and Ng, {Charlotte K.Y.} and Giuseppe Viale and Anna Sapino",

year = "2018",

month = sep,

day = "1",

doi = "10.1097/PAS.0000000000001100",

language = "English",

volume = "42",

pages = "1190--1200",

journal = "American Journal of Surgical Pathology",

issn = "0147-5185",

publisher = "Wolters Kluwer Health",

number = "9",

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Marchiò, C, Dell'Orto, P, Annaratone, L, Geyer, FC, Venesio, T, Berrino, E, Di Cantogno, LV, Garofoli, A, Rangel, N, Casorzo, L, dell'Aglio, C, Gugliotta, P, Trisolini, E, Beano, A, Pietribiasi, F, Orlassino, R, Cassoni, P, Pich, A, Montemurro, F, Mottolese, M, Vincent-Salomon, A, Penault-Llorca, F, Medico, E, Ng, CKY, Viale, G & Sapino, A 2018, 'The dilemma of HER2 double-equivocal breast carcinomas: Genomic profiling and implications for treatment', American Journal of Surgical Pathology, vol. 42, n.º 9, pp. 1190-1200. https://doi.org/10.1097/PAS.0000000000001100

TY - JOUR

T1 - The dilemma of HER2 double-equivocal breast carcinomas

T2 - Genomic profiling and implications for treatment

AU - Marchiò, Caterina

AU - Dell'Orto, Patrizia

AU - Annaratone, Laura

AU - Geyer, Felipe C.

AU - Venesio, Tiziana

AU - Berrino, Enrico

AU - Di Cantogno, Ludovica Verdun

AU - Garofoli, Andrea

AU - Rangel, Nelson

AU - Casorzo, Laura

AU - dell'Aglio, Carmine

AU - Gugliotta, Patrizia

AU - Trisolini, Elena

AU - Beano, Alessandra

AU - Pietribiasi, Francesca

AU - Orlassino, Renzo

AU - Cassoni, Paola

AU - Pich, Achille

AU - Montemurro, Filippo

AU - Mottolese, Marcella

AU - Vincent-Salomon, Anne

AU - Penault-Llorca, Frédérique

AU - Medico, Enzo

AU - Ng, Charlotte K.Y.

AU - Viale, Giuseppe

AU - Sapino, Anna

PY - 2018/9/1

Y1 - 2018/9/1

N2 - The American Society of Clinical Oncology/College of American Pathologists (ASCO/CAP) 2013 guidelines for HER2 assessment have increased the number of HER2 equivocal breast carcinomas following in situ hybridization reflex testing, that is, HER2 "double equivocal" (equivocal protein expression and equivocal gene copy number). Forty-five double-equivocal carcinomas were subjected to Prosigna analysis. Twenty-seven cases were investigated for the expression of genes found to be differentially expressed between estrogen receptor (ER)-positive/HER2-positive (N =22) and ER-positive/HER2-negative (N =22) control cases. Twenty-nine of the 45 cases were also analyzed by targeted sequencing using a panel of 14 genes. We then explored the pathologic complete response rates in an independent series of double-equivocal carcinoma patients treated with trastuzumab-containing chemotherapy. All cases were ER-positive, with a mean Ki67 of 28%. Double-equivocal carcinomas were predominantly luminal B (76%); 9 cases (20%) were luminal A, and 2 cases (4%) HER2-enriched. The majority (73%) showed a high risk of recurrence by Prosigna, even when the carcinomas were small (< 2 cm), node-negative/micrometastatic, and/or grade 2. Double-equivocal carcinomas showed TP53 (6/29, 20%), PIK3CA (3/29, 10%), HER2 (1/29, 3%), and MAP2K4 (1/29, 3%) mutations. Compared with grade-matched ER-positive/HER2-negative breast carcinomas from METABRIC, double-equivocal carcinomas harbored more frequently TP53 mutations and less frequently PIK3CA mutations (P < 0.05). No significant differences were observed with grade-matched ER-positive/HER2-positive carcinomas. Lower pathologic complete response rates were observed in double-equivocal compared with HER2-positive patients (10% vs. 60%, P= 0.009). Double-equivocal carcinomas are preferentially luminal B and show a high risk of recurrence. A subset of these tumors can be labeled as HER2-enriched by transcriptomic analysis. HER2 mutations can be identified in HER2 double-equivocal cases.

AB - The American Society of Clinical Oncology/College of American Pathologists (ASCO/CAP) 2013 guidelines for HER2 assessment have increased the number of HER2 equivocal breast carcinomas following in situ hybridization reflex testing, that is, HER2 "double equivocal" (equivocal protein expression and equivocal gene copy number). Forty-five double-equivocal carcinomas were subjected to Prosigna analysis. Twenty-seven cases were investigated for the expression of genes found to be differentially expressed between estrogen receptor (ER)-positive/HER2-positive (N =22) and ER-positive/HER2-negative (N =22) control cases. Twenty-nine of the 45 cases were also analyzed by targeted sequencing using a panel of 14 genes. We then explored the pathologic complete response rates in an independent series of double-equivocal carcinoma patients treated with trastuzumab-containing chemotherapy. All cases were ER-positive, with a mean Ki67 of 28%. Double-equivocal carcinomas were predominantly luminal B (76%); 9 cases (20%) were luminal A, and 2 cases (4%) HER2-enriched. The majority (73%) showed a high risk of recurrence by Prosigna, even when the carcinomas were small (< 2 cm), node-negative/micrometastatic, and/or grade 2. Double-equivocal carcinomas showed TP53 (6/29, 20%), PIK3CA (3/29, 10%), HER2 (1/29, 3%), and MAP2K4 (1/29, 3%) mutations. Compared with grade-matched ER-positive/HER2-negative breast carcinomas from METABRIC, double-equivocal carcinomas harbored more frequently TP53 mutations and less frequently PIK3CA mutations (P < 0.05). No significant differences were observed with grade-matched ER-positive/HER2-positive carcinomas. Lower pathologic complete response rates were observed in double-equivocal compared with HER2-positive patients (10% vs. 60%, P= 0.009). Double-equivocal carcinomas are preferentially luminal B and show a high risk of recurrence. A subset of these tumors can be labeled as HER2-enriched by transcriptomic analysis. HER2 mutations can be identified in HER2 double-equivocal cases.

KW - Breast carcinoma

KW - Equivocal result

KW - HER2

KW - Molecular subtype

KW - Mutations

KW - Risk of recurrence

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U2 - 10.1097/PAS.0000000000001100

DO - 10.1097/PAS.0000000000001100

M3 - Article

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AN - SCOPUS:85052335445

SN - 0147-5185

VL - 42

SP - 1190

EP - 1200

JO - American Journal of Surgical Pathology

JF - American Journal of Surgical Pathology

IS - 9

ER -

The dilemma of HER2 double-equivocal breast carcinomas: Genomic profiling and implications for treatment

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