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Stromal integrin α11 regulates PDGFRβ signaling and promotes breast cancer progression
Irina Primac, … , Donald Gullberg, Agnès Noel
Irina Primac, … , Donald Gullberg, Agnès Noel
Published July 9, 2019
Citation Information: J Clin Invest. 2019;129(11):4609-4628. https://doi.org/10.1172/JCI125890.
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Research Article Cell biology Oncology Article has an altmetric score of 15

Stromal integrin α11 regulates PDGFRβ signaling and promotes breast cancer progression

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Abstract

Cancer-associated fibroblasts (CAFs) are key actors in modulating the progression of many solid tumors, such as breast cancer (BC). Herein, we identify an integrin α11/PDGFRβ–positive CAF subset displaying tumor-promoting features in BC. In the preclinical MMTV-PyMT mouse model, integrin α11 deficiency led to a drastic reduction of tumor progression and metastasis. A clear association between integrin α11 and PDGFRβ was found at both transcriptional and histological levels in BC specimens. High stromal integrin α11/PDGFRβ expression was associated with high grades and poorer clinical outcome in human BC patients. Functional assays using 5 CAF subpopulations (1 murine, 4 human) revealed that integrin α11 promotes CAF invasion and CAF-induced tumor cell invasion upon PDGF-BB stimulation. Mechanistically, the proinvasive activity of integrin α11 relies on its ability to interact with PDGFRβ in a ligand-dependent manner and to promote its downstream JNK activation, leading to the production of tenascin C, a proinvasive matricellular protein. Pharmacological inhibition of PDGFRβ and JNK impaired tumor cell invasion induced by integrin α11+ CAFs. Collectively, our study uncovers an integrin α11+ subset of protumoral CAFs that exploits the PDGFRβ/JNK signaling axis to promote tumor invasiveness in BC.

Authors

Irina Primac, Erik Maquoi, Silvia Blacher, Ritva Heljasvaara, Jan Van Deun, Hilde Y.H. Smeland, Annalisa Canale, Thomas Louis, Linda Stuhr, Nor Eddine Sounni, Didier Cataldo, Taina Pihlajaniemi, Christel Pequeux, Olivier De Wever, Donald Gullberg, Agnès Noel

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Figure 4

Integrin α11 expression is increased in human breast cancers.

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Integrin α11 expression is increased in human breast cancers.
(A) Meta-a...
(A) Meta-analysis data of integrin α11 differential expression in BCs versus breast normal tissues. Oncomine microarray database was used to analyze ITGA11 mRNA expression, and meta-analysis was performed on 12 analyses from 7 microarray data sets (2375 patients). Data are shown as median rank of ITGA11 expression through each data set analysis. P value for ITGA11 was determined using the median-ranked analysis of BC versus normal tissues. (B–H) Differential expressions of ITGA11 mRNA in the 7 data sets included in the meta-analysis (Normal, normal adjacent breast tissue; IC, invasive breast carcinoma; IDC, invasive ductal breast carcinoma; IDC-L, mixed lobular and ductal breast carcinoma; IDC-T, invasive ductal breast carcinoma–tubular type; ILC, invasive lobular breast carcinoma). Median and interquartile range (10th and 90th percentiles). Two-sided t test for 2-class differential expression analyses and Pearson’s correlation for multiclass analyses. FDR-corrected P values. (I and J) Kaplan-Meier plots showing the overall survival (I) and distant metastasis–free survival (J) for ITGA11 expression (probe: 23335_at). Log-rank P values calculated with the Kaplan-Meier plotter website.

Copyright © 2025 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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