Unravelling triple-negative breast cancer molecular heterogeneity using an integrative multiomic analysis

Barèche, Yacine; Venet, David; Ignatiadis, Michail; Aftimos, Philippe; Piccart, Martine; Rothé, Françoise; Sotiriou, Christos

doi:10.1093/annonc/mdy024

Cited by 266 publications

(282 citation statements)

References 22 publications

(32 reference statements)

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“…Moreover, our presentation of global copy number alterations highlights the specific characteristics of TNBC: 8q24 ( MYC ) focal gain, 1q, 10p gain and 8p, 5q loss . Some transcriptomic subtypes in this cohort harbored specific somatic mutations already described in other studies LAR subtype corresponds to the luminal repertoire of genomic alterations: the most frequent mutations are PIK3CA and AKT1 (40%, 2/5) and the less frequent mutations are TP53 (20%). BL1 and BL2 present a high percentage of TP53 mutations (55.5 and 75%, respectively).…”

Section: Discussionsupporting

confidence: 58%

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A large collection of integrated genomically characterized patient‐derived xenografts highlighting the heterogeneity of triple‐negative breast cancer

Coussy

Koning

Lavigne

et al. 2019

Intl Journal of Cancer

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Triple‐negative breast cancer (TNBC) represents 10% of all breast cancers and is a very heterogeneous disease. Globally, women with TNBC have a poor prognosis, and the development of effective targeted therapies remains a real challenge. Patient‐derived xenografts (PDX) are clinically relevant models that have emerged as important tools for the analysis of drug activity and predictive biomarker discovery. The purpose of this work was to analyze the molecular heterogeneity of a large panel of TNBC PDX (n = 61) in order to test targeted therapies and identify biomarkers of response. At the gene expression level, TNBC PDX represent all of the various TNBC subtypes identified by the Lehmann classification except for immunomodulatory subtype, which is underrepresented in PDX. NGS and copy number data showed a similar diversity of significantly mutated gene and somatic copy number alteration in PDX and the Cancer Genome Atlas TNBC patients. The genes most commonly altered were TP53 and oncogenes and tumor suppressors of the PI3K/AKT/mTOR and MAPK pathways. PDX showed similar morphology and immunohistochemistry markers to those of the original tumors. Efficacy experiments with PI3K and MAPK inhibitor monotherapy or combination therapy showed an antitumor activity in PDX carrying genomic mutations of PIK3CA and NRAS genes. TNBC PDX reproduce the molecular heterogeneity of TNBC patients. This large collection of PDX is a clinically relevant platform for drug testing, biomarker discovery and translational research.

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Section: Discussionsupporting

confidence: 58%

“…Transcriptomic classifications are not used in clinical practice, but stress the importance of selection of the TNBC subtype before prescribing targeted therapy. However, except for the LAR and mesenchymal subtypes, it is difficult to demonstrate a specific correlation between transcriptomic subtype and response to targeted therapy …”

Section: Discussionmentioning

confidence: 99%

A large collection of integrated genomically characterized patient‐derived xenografts highlighting the heterogeneity of triple‐negative breast cancer

Coussy

Koning

Lavigne

et al. 2019

Intl Journal of Cancer

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“…Nowadays, with improving understanding of biological complexity and diversity of TNBC, six different molecular subtypes were identified, which helped to develop molecular drivers that can be therapeutically targeted. In view of the limited clinical benefit with targeted agents in unselected TNBC patients of some trials, Bareche et al unraveled molecular heterogeneity of six subtypes by using an integrative genomic analysis. The researchers found specific differences in mutational and copy number profiles characterizing each subtype and offered novel therapeutic avenues for these patients .…”

Section: Discussionmentioning

confidence: 99%

“…In view of the limited clinical benefit with targeted agents in unselected TNBC patients of some trials, Bareche et al unraveled molecular heterogeneity of six subtypes by using an integrative genomic analysis. The researchers found specific differences in mutational and copy number profiles characterizing each subtype and offered novel therapeutic avenues for these patients . For example, basal‐like 1 (BL1) subset characterizing with high genomic instability for BRCA1/2 may be sensitive to PARP inhibitors while mesenchymal (M) subtype tumors with high level of EGFR mRNA expression may be potential candidates to anti‐VEGF inhibitors and EGFR inhibitors .…”

Section: Discussionmentioning

confidence: 99%

“…The researchers found specific differences in mutational and copy number profiles characterizing each subtype and offered novel therapeutic avenues for these patients . For example, basal‐like 1 (BL1) subset characterizing with high genomic instability for BRCA1/2 may be sensitive to PARP inhibitors while mesenchymal (M) subtype tumors with high level of EGFR mRNA expression may be potential candidates to anti‐VEGF inhibitors and EGFR inhibitors . Thus, the application of a comprehensive genomic characterization may help to select the most appropriate treatment in TNBC and individualized treatment for TNBC patients may be extremely necessary .…”

Section: Discussionmentioning

confidence: 99%

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A Bayesian network meta‐analysis of the efficacy of targeted therapies and chemotherapy for treatment of triple‐negative breast cancer

et al. 2018

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Triple‐negative breast cancer (TNBC) is a heterogeneous disease with poorer prognosis than other subtypes, yet effective therapies are still not available. We aimed to compare the efficacy of various targeted therapies with chemotherapy (CT) in TNBC patients using a network meta‐analysis. A systematic literature search was performed in PubMed, EMBASE, and the Cochrane Library. A total of 27 randomized controlled trials (RCTs), involving 6924 TNBC patients, were included. Olaparib significantly improved PFS (0.43, 0.29‐0.64) and ORR (2.57, 1.31‐5.09) in comparison with CT. As for bevacizumab + CT, it showed a significant improvement of PFS (0.66, 0.55‐0.80) and ORR (2.15, 1.16‐4.05) compared with CT + placebo. It was also superior to CT alone in PFS (0.48, 0.35‐0.65) and pCR (1.30, 1.13‐1.49 for breast and axillary nodes and 1.26, 1.11‐1.44 for breast). Other targeted agents like iniparib, sorafenib, cetuximab, and ipatasertib combined with CT showed significant superiority in PFS compared with CT alone, and the HRs were 0.75 (0.62‐0.90), 0.44 (0.21‐0.91), 0.67 (0.47‐0.96), and 0.44 (0.24‐0.81), respectively, while some other agents such as sunitinib and cetuximab had the lowest SUCRA in OS, PFS, or ORR without any benefits. In conclusion, our results indicated that the addition of bevacizumab to CT was beneficial for TNBC patients, and olaparib had a great effect in PFS and ORR, especially for those with BRCA mutations. When combined with CT, targeted agents including iniparib, sorafenib, cetuximab, and ipatasertib may have better efficacies for treating TNBC.

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Identification and validation of a combined hypoxia and immune index for triple‐negative breast cancer

et al. 2020

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The interaction between hypoxia and immune status has been confirmed in various cancer settings, and corresponding treatments have been investigated. However, reliable biomarkers are needed for individual treatment, so we sought to develop a novel scoring system based on hypoxia and immune status. Prognostic hypoxia-immune status-related signatures of patients with triple-negative breast cancer (TNBC) were identified in The Cancer Genome Atlas (TCGA) (N = 158), Molecular Taxonomy of Breast Cancer International Consortium (METABRIC) (N = 297), and GSE58812 (N = 107). LASSO Cox regression was used for model construction. Hypoxia and immune status expression profiles were analyzed, and infiltrating immune cells were compared. Quantitative real-time PCR (qRT-PCR) was used for validation in the Sun Yat-sen University Cancer Center (SYSUCC) cohort, and immunofluorescence was applied for the detection of hypoxia and immune markers in cancer tissues. Ten cross-cohort prognostic hypoxia-immune signatures were included to construct the comprehensive index of hypoxia and immune (CIHI) in the METABRIC cohort. Two subgroups of patients with distinct hypoxia-immune status conditions were identified using CIHI: hypoxia high /immune low and hypoxia low /immune high , with a significantly better overall survival (OS) rate in the latter (P < 0.01). The prognostic value of CIHI was further validated in the TCGA, GSE58812, and SYSUCC cohorts (P < 0.01).

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Unravelling triple-negative breast cancer molecular heterogeneity using an integrative multiomic analysis

Cited by 266 publications

References 22 publications

A large collection of integrated genomically characterized patient‐derived xenografts highlighting the heterogeneity of triple‐negative breast cancer

A large collection of integrated genomically characterized patient‐derived xenografts highlighting the heterogeneity of triple‐negative breast cancer

A Bayesian network meta‐analysis of the efficacy of targeted therapies and chemotherapy for treatment of triple‐negative breast cancer

Identification and validation of a combined hypoxia and immune index for triple‐negative breast cancer

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