Inflammatory mediators in breast cancer: Coordinated expression of TNFα &amp; IL-1β with CCL2 &amp; CCL5 and effects on epithelial-to-mesenchymal transition

Soria, Gali; Ofri-Shahak, Maya; Haas, Ilana; Yaal-Hahoshen, Neora; Leider-Trejo, Leonor; Leibovich-Rivkin, Tal; Weitzenfeld, Polina; Meshel, Tsipi; Shabtai, Esther; Gutman, Mordechai; Ben‐Baruch, Adit

doi:10.1186/1471-2407-11-130

Cited by 245 publications

(238 citation statements)

References 74 publications

Supporting

Mentioning

220

Contrasting

Unclassified

Order By: Relevance

“…All these cytokines have been implicated in breast cancer progression previously. [46][47][48] To test the effect of these cytokines on PKCl/i activation, we treated MDA-MB-231 cells with different cytokines and tested phosphorylation of PKCl/i. Intriguingly, we found that both TGFb1 and IL1b, individually and in combination, induced PKCl/i phosphorylation in MDA-MB-231 cells (Figure 6a and Supplementary Figure S8a).…”

Section: Resultsmentioning

confidence: 99%

PKCλ/ι signaling promotes triple-negative breast cancer growth and metastasis

et al. 2014

View full text Add to dashboard Cite

Triple-negative breast cancer (TNBC) is a distinct breast cancer subtype defined by the absence of estrogen receptor (ER), progesterone receptor (PR) and epidermal growth factor receptor 2 (HER2/neu), and the patients with TNBC are often diagnosed with higher rates of recurrence and metastasis. Because of the absence of ER, PR and HER2/neu expressions, TNBC patients are insensitive to HER2-directed and endocrine therapies available for breast cancer treatment. Here, we report that expression of atypical protein kinase C isoform, PKCk/i, significantly increased and activated in all invasive breast cancer (invasive ductal carcinoma or IDC) subtypes including the TNBC subtype. Because of the lack of targeted therapies for TNBC, we choose to study PKCk/i signaling as a potential therapeutic target for TNBC. Our observations indicated that PKCk/i signaling is highly active during breast cancer invasive progression, and metastatic breast cancers, the advanced stages of breast cancer disease that developed more frequently in TNBC patients, are also characterized with high levels of PKCk/i expression and activation. Functional analysis in experimental mouse models revealed that depletion of PKCk/i significantly reduces TNBC growth as well as lung metastatic colonization. Furthermore, we have identified a PKCk/i-regulated gene signature consisting of 110 genes, which are significantly associated with indolent to invasive progression of human breast cancer and poor prognosis. Mechanistically, cytokines such as TGFb and IL1b could activate PKCk/i signaling in TNBC cells and depletion of PKCk/i impairs NF-jB p65 (RelA) nuclear localization. We observed that cytokine-PKCk/i-RelA signaling axis, at least in part, involved in modulating gene expression to regulate invasion of TNBC cells. Overall, our results indicate that induction and activation of PKCk/i promote TNBC growth, invasion and metastasis. Thus, targeting PKCk/i signaling could be a therapeutic option for breast cancer, including the TNBC subtype.

show abstract

Section: Resultsmentioning

confidence: 99%

PKCλ/ι signaling promotes triple-negative breast cancer growth and metastasis

et al. 2014

View full text Add to dashboard Cite

show abstract

“…Interestingly, from the coculture of EC and MC versus simultaneously MC alone and EC alone, 17 genes from the 27 known differentially expressed genes were linked to migratory and/or embryonic/cancer stem cell properties: nine overexpressed genes: CCL2, ICAM1, SELE, IL6, TRAF1, SERPINB2, CXCL6, PDGFB and EVX1, and eight underexpressed genes: CFDP1, BLID, RGNEF, MALT1, RANBP9, UPF1, PLAA and ZXDC. More specifically, these genes have demonstrated properties linked to (i) cancer cell migration: CCL2 [26,27], ICAM1 [28], IL6 [29], RGNEF [30] and RANBP9 [31]; (ii) cancer progression and metastasis: CCL2 [26,27,32], ICAM1 [33,34], SELE [35,36], TRAF1 [37], IL6 [29], SERPINB2 [38], CXCL6 [39], BLID [40], MALT1 [41], UPF1 [42], PLAA [43], RGNEF [44], ZXDC [45]; (iii) EMT: CCL2 [46] and IL6 [29] ; and (iv) embryonic and/or cancer stem cell properties: CCL2 [46][47][48] , PDGFB [49] , EVX1 [50], CFDP1 [51] and RANBP9 [52] . Furthermore, the 15 most significantly enriched functional groups analyzed by IPA included: development, cell movement, cancer, and embryonic development.…”

Section: Discussionmentioning

confidence: 99%

Pilot Study on “Pericytic Mimicry” and Potential Embryonic/Stem Cell Properties of Angiotropic Melanoma Cells Interacting with the Abluminal Vascular Surface

Lugassy

Wadehra

et al. 2012

Cancer Microenvironment

View full text Add to dashboard Cite

The interaction of tumor cells with the tumor vasculature is mainly studied for its role in tumor angiogenesis and intravascular metastasis of circulating tumor cells. In addition, a specific interaction of tumor cells with the abluminal surfaces of vessels, or angiotropism, may promote the migration of angiotropic tumor cells along the abluminal vascular surfaces in a pericytic location. This process has been termed extravascular migratory metastasis.The abluminal vascular surface may also provide a vascular niche inducing or sustaining stemness to angiotropic tumor cells. This pilot study investigated if angiotropic melanoma cells might represent a subset population with pericytic and embryonic or stem cell properties. Through microarray analysis, we showed that the interaction between melanoma cells and the abluminal surface of endothelial cells triggers significant differential expression of several genes. The most significantly differentially expressed genes have demonstrated properties linked to cancer cell migration (CCL2, ICAM1 and IL6), cancer progression (CCL2, ICAM1, SELE, TRAF1, IL6, SERPINB2 and CXCL6), epithelial to mesenchymal transition (CCL2 and IL6), embryonic/stem cell properties (CCL2, PDGFB, EVX1 and CFDP1) and pericytic recruitment (PDGFB). In addition, bioinformatics-based analysis of the differentially expressed genes has shown that the most significantly enriched functional groups included development, cell movement, cancer, and embryonic development. Finally, the investigation of pericyte/mesenchymal stem cells markers via immunostaining of human melanoma samples revealed expression of PDGFRB, NG2 and CD146 by angiotropic melanoma cells. Taken together, these preliminary data are supportive of the "pericytic mimicry" by angiotropic melanoma cells, and suggest that the interaction between melanoma cells and the abluminal vascular surface induce differential expression of genes linked to cancer migration and embryonic/ stem cell properties.

show abstract

“…The expression of CCL2 and CCL5 in the IDC-with-relapse group was associated with further elevated expression of IL1b and TNF-a. 35 In human breast tumor cells, CCL5-containing vesicles on microtubules traffic from the endoplasmic reticulum to the post-Golgi stage before CCL5 is released, and this process is controlled by the stiffness of the actin cytoskeleton in a manner dependent on the (43)TRKN(46) sequence of the 40 s loop of CCL5.…”

Section: Ccl5 and Human Breast Cancer (Bc)mentioning

confidence: 99%

CCL5 as a potential immunotherapeutic target in triple-negative breast cancer

Zhang

Kim

et al. 2013

Cell Mol Immunol

View full text Add to dashboard Cite

Breast cancer (BC) is a leading cause of mortality among women in the world. To date, a number of molecules have been established as disease status indicators and therapeutic targets. The best known among them are estrogen receptor-a (ER-a), progesterone receptor (PR) and HER-2/neu. About 15%-20% BC patients do not respond effectively to therapies targeting these classes of tumor-promoting factors. Thus, additional targets are strongly and urgently sought after in therapy for human BCs negative for ER, PR and HER-2, the so-called triple-negative BC (TNBC). Recent clinical work has revealed that CC chemokine ligand 5 (CCL5) is strongly associated with the progression of BC, particularly TNBC. How CCL5 contributes to the development of TNBC is not well understood. Experimental animal studies have begun to address the mechanistic issue. In this article, we will review the clinical and laboratory work in this area that has led to our own hypothesis that targeting CCL5 in TNBCs will have favorable therapeutic outcomes with minimal adverse impact on the general physiology.

show abstract

Inflammatory mediators in breast cancer: Coordinated expression of TNFα & IL-1β with CCL2 & CCL5 and effects on epithelial-to-mesenchymal transition

Cited by 245 publications

References 74 publications

PKCλ/ι signaling promotes triple-negative breast cancer growth and metastasis

PKCλ/ι signaling promotes triple-negative breast cancer growth and metastasis

Pilot Study on “Pericytic Mimicry” and Potential Embryonic/Stem Cell Properties of Angiotropic Melanoma Cells Interacting with the Abluminal Vascular Surface

CCL5 as a potential immunotherapeutic target in triple-negative breast cancer

Contact Info

Product

Resources

About