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Clinicogenomic characterization of inflammatory breast cancer.
Priedigkeit, Nolan; Harrison, Beth; Shue, Robert; Hughes, Melissa; Li, Yvonne; Kirkner, Gregory J; Spurr, Liam F; Remolano, Marie Claire; Strauss, Sarah; Files, Janet; Feeney, Anne-Marie; Grant, Libby; Mohammed-Abreu, Ayesha; Garrido-Castro, Ana; Sousa, Romualdo Barroso; Bychkovsky, Brittany; Nakhlis, Faina; Bellon, Jennifer R; King, Tari A; Winer, Eric P; Lindeman, Neal; Johnson, Bruce E; Sholl, Lynette; Dillon, Deborah; Overmoyer, Beth; Tolaney, Sara M; Cherniack, Andrew; Lin, Nancy U; Lynce, Filipa.
Affiliation
  • Priedigkeit N; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Harrison B; Harvard Medical School, Boston, MA, USA.
  • Shue R; The Broad Institute of MIT & Harvard, Cambridge, MA, USA.
  • Hughes M; Harvard Medical School, Boston, MA, USA.
  • Li Y; Breast Oncology Program, Dana-Farber Brigham Cancer Center, Boston MA, USA.
  • Kirkner GJ; Department of Pathology, Brigham and Women's Hospital, Boston, MA, USA.
  • Spurr LF; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Remolano MC; The Broad Institute of MIT & Harvard, Cambridge, MA, USA.
  • Strauss S; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Files J; Breast Oncology Program, Dana-Farber Brigham Cancer Center, Boston MA, USA.
  • Feeney AM; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Grant L; The Broad Institute of MIT & Harvard, Cambridge, MA, USA.
  • Mohammed-Abreu A; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Garrido-Castro A; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Sousa RB; The Broad Institute of MIT & Harvard, Cambridge, MA, USA.
  • Bychkovsky B; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Nakhlis F; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Bellon JR; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • King TA; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Winer EP; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Lindeman N; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Johnson BE; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Sholl L; Harvard Medical School, Boston, MA, USA.
  • Dillon D; Breast Oncology Program, Dana-Farber Brigham Cancer Center, Boston MA, USA.
  • Overmoyer B; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Tolaney SM; Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, MA, USA.
  • Cherniack A; Harvard Medical School, Boston, MA, USA.
  • Lin NU; Breast Oncology Program, Dana-Farber Brigham Cancer Center, Boston MA, USA.
  • Lynce F; Division of Cancer Genetics and Prevention, Dana-Farber Cancer Institute, Boston, MA, USA.
bioRxiv ; 2024 May 10.
Article in En | MEDLINE | ID: mdl-38766070
ABSTRACT

Background:

Inflammatory breast cancer (IBC) is a rare and poorly characterized type of breast cancer with an aggressive clinical presentation. The biological mechanisms driving the IBC phenotype are relatively undefined-partially due to a lack of comprehensive, large-scale genomic studies and limited clinical cohorts. Patients and

Methods:

A retrospective analysis of 2457 patients with metastatic breast cancer who underwent targeted tumor-only DNA-sequencing was performed at Dana-Farber Cancer Institute. Clinicopathologic, single nucleotide variant (SNV), copy number variant (CNV) and tumor mutational burden (TMB) comparisons were made between clinically confirmed IBC cases within a dedicated IBC center versus non-IBC cases.

Results:

Clinicopathologic differences between IBC and non-IBC cases were consistent with prior reports-including IBC being associated with younger age at diagnosis, higher grade, and enrichment with hormone receptor (HR)-negative and HER2-positive tumors. The most frequent somatic alterations in IBC involved TP53 (72%), ERBB2 (32%), PIK3CA (24%), CCND1 (12%), MYC (9%), FGFR1 (8%) and GATA3 (8%). A multivariate logistic regression analysis revealed a significant enrichment in TP53 SNVs in IBC; particularly in HER2-positive and HR-positive disease which was associated with worse outcomes. Tumor mutational burden (TMB) did not differ substantially between IBC and non-IBC cases and a pathway analysis revealed an enrichment in NOTCH pathway alterations in HER2-positive disease.

Conclusion:

Taken together, this study provides a comprehensive, clinically informed landscape of somatic alterations in a large cohort of patients with IBC. Our data support higher frequency of TP53 mutations and a potential enrichment in NOTCH pathway activation-but overall; a lack of major genomic differences. These results both reinforce the importance of TP53 alterations in IBC pathogenesis as well as their influence on clinical outcomes; but also suggest additional analyses beyond somatic DNA-level changes are warranted.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: BioRxiv Year: 2024 Document type: Article Affiliation country: United States
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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: BioRxiv Year: 2024 Document type: Article Affiliation country: United States