Gene-expression Profiling of Microdissected Breast Cancer Microvasculature Identifies Distinct Tumor Vascular Subtypes

Overview

Journal Breast Cancer Res

Specialty Oncology

Date 2012 Aug 22

PMID 22906178

Citations 19

Authors

Francois Pepin

Nicholas Bertos

Julie Laferriere

Svetlana Sadekova

Margarita Souleimanova

Hong Zhao

Greg Finak

Sarkis Meterissian

Michael T Hallett

Morag Park

Affiliations

Soon will be listed here.

Abstract

Introduction: Angiogenesis represents a potential therapeutic target in breast cancer. However, responses to targeted antiangiogenic therapies have been reported to vary among patients. This suggests that the tumor vasculature may be heterogeneous and that an appropriate choice of treatment would require an understanding of these differences.

Methods: To investigate whether and how the breast tumor vasculature varies between individuals, we isolated tumor-associated and matched normal vasculature from 17 breast carcinomas by laser-capture microdissection, and generated gene-expression profiles. Because microvessel density has previously been associated with disease course, tumors with low (n = 9) or high (n = 8) microvessel density were selected for analysis to maximize heterogeneity for this feature.

Results: We identified differences between tumor and normal vasculature, and we describe two subtypes present within tumor vasculature. These subtypes exhibit distinct gene-expression signatures that reflect features including hallmarks of vessel maturity. Potential therapeutic targets (MET, ITGAV, and PDGFRβ) are differentially expressed between subtypes. Taking these subtypes into account has allowed us to derive a vascular signature associated with disease outcome.

Conclusions: Our results further support a role for tumor microvasculature in determining disease progression. Overall, this study provides a deeper molecular understanding of the heterogeneity existing within the breast tumor vasculature and opens new avenues toward the improved design and targeting of antiangiogenic therapies.

Citing Articles

Meta-Analysis of Microdissected Breast Tumors Reveals Genes Regulated in the Stroma but Hidden in Bulk Analysis.

Savino A, De Marzo N, Provero P, Poli V Cancers (Basel). 2021; 13(13).

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Dynamic Contrast Enhanced MRI and Intravoxel Incoherent Motion to Identify Molecular Subtypes of Breast Cancer with Different Vascular Normalization Gene Expression.

Tsai W, Chang K, Kao K Korean J Radiol. 2021; 22(7):1021-1033.

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Identification of disease-promoting stromal components by comparative proteomic and transcriptomic profiling of canine mammary tumors using laser-capture microdissected FFPE tissue.

Poschel A, Beebe E, Kunz L, Amini P, Guscetti F, Malbon A Neoplasia. 2021; 23(4):400-412.

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Study of Gene Expression Profiles of Breast Cancers in Indian Women.

Malvia S, Bagadi S, Pradhan D, Chintamani C, Bhatnagar A, Arora D Sci Rep. 2019; 9(1):10018.

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