miRNA-30 Family Members Inhibit Breast Cancer Invasion, Osteomimicry, and Bone Destruction by Directly Targeting Multiple Bone Metastasis–Associated Genes

Martine Croset; Francesco Pantano; Casina W.S. Kan; Edith Bonnelye; Françoise Descôtes; Catherine Alix‐Panabières; Charles‐Henri Lecellier; Richard Bachelier; Nathalie Allioli; Saw-See Hong; Kai Bartkowiak; Klaus Pantel; Philippe Clézardin

doi:10.1158/0008-5472.can-17-3058

miRNA-30 Family Members Inhibit Breast Cancer Invasion, Osteomimicry, and Bone Destruction by Directly Targeting Multiple Bone Metastasis–Associated Genes

Martine Croset(Université Claude Bernard Lyon 1), Francesco Pantano(Université Claude Bernard Lyon 1), Casina W.S. Kan(Université Claude Bernard Lyon 1), Edith Bonnelye(Université Claude Bernard Lyon 1), Françoise Descôtes(Hospices Civils de Lyon), Catherine Alix‐Panabières(Institut de Recherche pour le Développement), Charles‐Henri Lecellier(Université de Montpellier), Richard Bachelier(Université Claude Bernard Lyon 1), Nathalie Allioli(Université Claude Bernard Lyon 1), Saw-See Hong(Université Claude Bernard Lyon 1), Kai Bartkowiak(Universität Hamburg), Klaus Pantel(Universität Hamburg), Philippe Clézardin(Université Claude Bernard Lyon 1)

Cancer Research

July 24, 2018

10.1158/0008-5472.can-17-3058

Cited by 193Open Access

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Abstract

Abstract miRNAs are master regulators of gene expression that play key roles in cancer metastasis. During bone metastasis, metastatic tumor cells must rewire their biology and express genes that are normally expressed by bone cells (a process called osteomimicry), which endow tumor cells with full competence for outgrowth in the bone marrow. Here, we establish miR-30 family members miR-30a, miR-30b, miR-30c, miR-30d, and miR-30e as suppressors of breast cancer bone metastasis that regulate multiple pathways, including osteomimicry. Low expression of miR-30 in primary tumors from patients with breast cancer were associated with poor relapse-free survival. In addition, estrogen receptor (ER)-negative/progesterone receptor (PR)-negative breast cancer cells expressed lower miR-30 levels than their ER/PR-positive counterparts. Overexpression of miR-30 in ER/PR-negative breast cancer cells resulted in the reduction of bone metastasis burden in vivo. In vitro, miR-30 did not affect tumor cell proliferation, but did inhibit tumor cell invasion. Furthermore, overexpression of miR-30 restored bone homeostasis by reversing the effects of tumor cell–conditioned medium on osteoclastogenesis and osteoblastogenesis. A number of genes associated with osteoclastogenesis stimulation (IL8, IL11), osteoblastogenesis inhibition (DKK-1), tumor cell osteomimicry (RUNX2, CDH11), and invasiveness (CTGF, ITGA5, ITGB3) were identified as targets for repression by miR-30. Among these genes, silencing CDH11 or ITGA5 in ER-/PR-negative breast cancer cells recapitulated inhibitory effects of miR-30 on skeletal tumor burden in vivo. Overall, our findings provide evidence that miR-30 family members employ multiple mechanisms to impede breast cancer bone metastasis and may represent attractive targets for therapeutic intervention. Significance: These findings suggest miR-30 family members may serve as an effective means to therapeutically attenuate metastasis in triple-negative breast cancer. Cancer Res; 78(18); 5259–73. ©2018 AACR.

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