Plasminogen Activator Inhibitor 1 (PAI1) Promotes Actin Cytoskeleton Reorganization and Glycolytic Metabolism in Triple-Negative Breast Cancer

Humphries, Brock A.; Buschhaus, Johanna M.; Chen, Yu‐Chih; Haley, Henry; Qyli, Tonela; Chiang, Benjamin N.; Shen, Nathan; Rajendran, Shrila; Cutter, Alyssa C.; Cheng, Yu; Chen, Yuting; Cong, Jason; Spinosa, Phillip C.; Yoon, Euisik; Luker, Gary D.

doi:10.1158/1541-7786.mcr-18-0836

Cited by 49 publications

(48 citation statements)

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“…Moreover, in triple negative breast cancer (TNBC), PAI-1-secreted by TNBC cells could stimulate the expression and secretion of CCL5 from endothelial cells, which then enhanced TNBC cells migration, invasion, and metastasis [44]. Overexpression of PAI-1 in TNBC cells further promoted alignment of collagen perpendicular to the margin of tumor, suggesting PAI-1 might exert roles in surrounding tumor microenvironment in orthotopic breast cancer [48]. Interestingly, our present study indicated breast cancer cells secreted PAI-1 led to the activation of PLOD2 expression in adipocytes microenvironment, while the addition of tiplaxtinin further abrogated PLOD2 activation in CAAs (Fig.…”

Section: Discussionmentioning

confidence: 99%

Tumor-secreted PAI-1 promotes breast cancer metastasis via the induction of adipocyte-derived collagen remodeling

Wei

et al. 2019

Cell Commun Signal

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Background: Breast cancer cells recruit surrounding stromal cells, such as cancer-associated fibroblasts (CAFs), to remodel collagen and promote tumor metastasis. Adipocytes are the most abundant stromal partners in breast tissue, local invasion of breast cancer leads to the proximity of cancer cells and adipocytes, which respond to generate cancer-associated adipocytes (CAAs). These cells exhibit enhanced secretion of extracellular matrix related proteins, including collagens. However, the role of adipocyte-derived collagen on breast cancer progression still remains unclear. Methods: Adipocytes were cocultured with breast cancer cells for 3D collagen invasion and collagen organization exploration. Breast cancer cells and adipose tissue co-implanted mouse model, clinical breast cancer samples analysis were used to study the crosstalk between adipose and breast cancer cells in vivo. A combination of proteomics, enzyme-linked immunosorbent assay, loss of function assay, qPCR, western blot, database analysis and chromatin immunoprecipitation assays were performed to study the mechanism mediated the activation of PLOD2 in adipocytes. Results: It was found that CAAs remodeled collagen alignment during crosstalk with breast cancer cells in vitro and in vivo, which further promoted breast cancer metastasis. Tumor-derived PAI-1 was required to activate the expression of the intracellular enzyme procollagen-lysine, 2-oxoglutarate 5-dioxygenase 2 (PLOD2) in CAAs. Pharmacologic blockade of PAI-1 or PLOD2 disrupted the collagen reorganization in CAAs. Mechanistically, it was observed that PI3K/AKT pathway was activated in adipocytes upon co-culturing with breast cancer cells or treatment with recombinant PAI-1, which could promote the translocation of transcription factor FOXP1 into the nucleus and further enhanced the promoter activity of PLOD2 in CAAs. In addition, collagen reorganization at the tumor-adipose periphery, as well as the positive relevance between PAI-1 and PLOD2 in invasive breast carcinoma were confirmed in clinical specimens of breast cancer. Conclusion: In summary, our findings revealed a new stromal collagen network that favors tumor invasion and metastasis establish between breast cancer cells and surrounding adipocytes at the tumor invasive front, and identified PLOD2 as a therapeutic target for metastatic breast cancer treatment.

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Section: Discussionmentioning

confidence: 99%

Tumor-secreted PAI-1 promotes breast cancer metastasis via the induction of adipocyte-derived collagen remodeling

Wei

et al. 2019

Cell Commun Signal

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“…MMP-1 COLI Regulated to facilitate melanoma cell growth and invasion [227,228] COLIV Regulated to foster breast cancer cell invasion in response to prolactin [229] MMP-2 COLI Modulating MMP-2 activation in osteosarcoma [230] COL4A2 Modulating MMP-2 activation and activity in liver cancer [231] COLI and COLIV Regulated by the knockdown of MMP-2 to induce cancer metastases [232,233] Collagen organization Regulated to enhance malignant glioma recurrence and resistance to vemurafenib [234,235] MMP carcinoma [166,167]. TACS-3 was shown to be driven by increased plasminogen activator inhibitor 1 via ERK signaling and promoted the migration of triple-negative breast cancer cells [168]. The elevated density and depth of collagen deposition showed high proliferation and invasion of cancer cells [169,170].…”

Section: Subtype Of Mmps Associated Collagen Pathological Functions Omentioning

confidence: 99%

The role of collagen in cancer: from bench to bedside

et al. 2019

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Collagen is the major component of the tumor microenvironment and participates in cancer fibrosis. Collagen biosynthesis can be regulated by cancer cells through mutated genes, transcription factors, signaling pathways and receptors; furthermore, collagen can influence tumor cell behavior through integrins, discoidin domain receptors, tyrosine kinase receptors, and some signaling pathways. Exosomes and microRNAs are closely associated with collagen in cancer. Hypoxia, which is common in collagen-rich conditions, intensifies cancer progression, and other substances in the extracellular matrix, such as fibronectin, hyaluronic acid, laminin, and matrix metalloproteinases, interact with collagen to influence cancer cell activity. Macrophages, lymphocytes, and fibroblasts play a role with collagen in cancer immunity and progression. Microscopic changes in collagen content within cancer cells and matrix cells and in other molecules ultimately contribute to the mutual feedback loop that influences prognosis, recurrence, and resistance in cancer. Nanoparticles, nanoplatforms, and nanoenzymes exhibit the expected gratifying properties. The pathophysiological functions of collagen in diverse cancers illustrate the dual roles of collagen and provide promising therapeutic options that can be readily translated from bench to bedside. The emerging understanding of the structural properties and functions of collagen in cancer will guide the development of new strategies for anticancer therapy.

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“…To identify the activity of ERK and Akt, we used the kinase translocation reporter (KTR) for ERK and Akt as previously described [17,18]. This KTR construct contains H2B fused to mCherry (H2B-mCherry), the Akt-KTR reporter (Aquamarine), the ERK-KTR reporter (mCitrine), and a puromycin selection marker all separated by P2A linker sequences cloned into the Piggyback transposon vector as described previously (pHAEP) [18].…”

Section: Vectors and Cell Linesmentioning

confidence: 99%

Enhanced mitochondrial fission suppresses signaling and metastasis in triple-negative breast cancer

et al. 2020

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Background: Mitochondrial dynamics underlies malignant transformation, cancer progression, and response to treatment. Current research presents conflicting evidence for functions of mitochondrial fission and fusion in tumor progression. Here, we investigated how mitochondrial fission and fusion states regulate underlying processes of cancer progression and metastasis in triple-negative breast cancer (TNBC). Methods: We enforced mitochondrial fission and fusion states through chemical or genetic approaches and measured migration and invasion of TNBC cells in 2D and 3D in vitro models. We also utilized kinase translocation reporters (KTRs) to identify single cell effects of mitochondrial state on signaling cascades, PI3K/Akt/mTOR and Ras/ Raf/MEK/ERK, commonly activated in TNBC. Furthermore, we determined effects of fission and fusion states on metastasis, bone destruction, and signaling in mouse models of breast cancer. Results: Enforcing mitochondrial fission through chemical or genetic approaches inhibited migration, invasion, and metastasis in TNBC. Breast cancer cells with predominantly fissioned mitochondria exhibited reduced activation of Akt and ERK both in vitro and in mouse models of breast cancer. Treatment with leflunomide, a potent activator of mitochondrial fusion proteins, overcame inhibitory effects of fission on migration, signaling, and metastasis. Mining existing datasets for breast cancer revealed that increased expression of genes associated with mitochondrial fission correlated with improved survival in human breast cancer. Conclusions: In TNBC, mitochondrial fission inhibits cellular processes and signaling pathways associated with cancer progression and metastasis. These data suggest that therapies driving mitochondrial fission may benefit patients with breast cancer.

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Plasminogen Activator Inhibitor 1 (PAI1) Promotes Actin Cytoskeleton Reorganization and Glycolytic Metabolism in Triple-Negative Breast Cancer

Cited by 49 publications

References 48 publications

Tumor-secreted PAI-1 promotes breast cancer metastasis via the induction of adipocyte-derived collagen remodeling

Tumor-secreted PAI-1 promotes breast cancer metastasis via the induction of adipocyte-derived collagen remodeling

The role of collagen in cancer: from bench to bedside

Enhanced mitochondrial fission suppresses signaling and metastasis in triple-negative breast cancer

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