Distinct Expression Profiles and Functions of Kindlins in Breast Cancer

Overview

Journal J Exp Clin Cancer Res

Publisher Biomed Central

Specialty Oncology

Date 2018 Nov 28

PMID 30477537

Citations 14

Authors

Paula Azorin

Florian Bonin

Ahmad Moukachar

Aurelie Ponceau

Sophie Vacher

Ivan Bieche

Elisabetta Marangoni

Laetitia Fuhrmann

Anne Vincent-Salomon

Rosette Lidereau

Keltouma Driouch

Affiliations

Soon will be listed here.

Abstract

Background: Kindlin-1, - 2, and - 3 are the three members of the Kindlin family. They are best known as regulators of integrin functions, contributing to fundamental biological processes such as cell survival, adhesion and migration. Their deregulation leads to diverse pathologies including a broad range of cancers in which both, tumor-promoting and tumor-inhibiting functions have been described.

Methods: To better characterize Kindlins implication in breast cancer, in vitro experiments were performed in a series of cancer cell lines. We first assessed their expression profiles and subcellular distributions. Then, their involvement in breast cancer cell morphology, migration and invasion was verified by examining phenotypic changes induced by the depletion of either isoforms using RNA interference. An expression study was performed in a series of breast cancer patient derived xenografts (n = 58) to define the epithelial and stromal contribution of each Kindlin. Finally, we analyzed the expression levels of the three Kindlins in a large series of human breast tumors, at the RNA (n = 438) and protein (n = 129) levels and we evaluated their correlation with the clinical outcome.

Results: We determined that Kindlin-1 and Kindlin-2, but not Kindlin-3, were expressed in breast tumor cells. We uncovered the compensatory roles of Kindlin-1 and -2 in focal adhesion dynamics and cell motility. Remarkably, Kindlin-2 had a predominant effect on cell spreading and Kindlin-1 on cell invasion. In line with these experimental observations, Kindlin-1 overexpression was associated with a worse patients' outcome. Notably, Kindlin-3, expressed by tumor infiltrating leukocytes, also correlated with a poor prognosis of breast cancer patients.

Conclusion: This study demonstrates that each one of the Kindlin family members has a different expression profile emphasizing their redundant and complementary roles in breast tumor cells. We highlight the specific link between Kindlin-1 and breast cancer progression. In addition, Kindlin-3 overexpression in the tumor microenvironment is associated with more aggressive breast tumors. These results suggest that Kindlins play distinctive roles in breast cancer. Kindlins may be useful in identifying breast cancer patients with a worst prognosis and may offer new avenues for therapeutic intervention against cancer progression.

Citing Articles

Kindlin-1 promotes gastric cancer cell motility through the Wnt/β-catenin signaling pathway.

Jang J, Jung J, Kang H, Kim W, Kim W, Lee H Sci Rep. 2025; 15(1):2481.

PMID: 39833319 PMC: 11756408. DOI: 10.1038/s41598-025-86220-7.

Involvement of Kindlin-1 in cutaneous squamous cell carcinoma.

Carrasco G, Stavrou I, Treanor-Taylor M, Beetham H, Lee M, Masalmeh R Oncogenesis. 2024; 13(1):24.

PMID: 38982038 PMC: 11233684. DOI: 10.1038/s41389-024-00526-1.

Pan-cancer analyses suggest kindlin-associated global mechanochemical alterations.

Chowdhury D, Mistry A, Maity D, Bhatia R, Priyadarshi S, Wadan S Commun Biol. 2024; 7(1):372.

PMID: 38548811 PMC: 10978987. DOI: 10.1038/s42003-024-06044-5.

Kindlin-1 regulates IL-6 secretion and modulates the immune environment in breast cancer models.

Webb E, Dodd G, Noskova M, Bullock E, Muir M, Frame M Elife. 2023; 12.

PMID: 36883731 PMC: 10023156. DOI: 10.7554/eLife.85739.

Kindlins as modulators of breast cancer progression.

Plow E, Pluskota E, Bialkowska K J Breast Cancer Res. 2022; 1(2):20-29.

PMID: 35936112 PMC: 9352049.

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