Indirubin derivatives inhibit Stat3 signaling and induce apoptosis in human cancer cells

Nam, Sangkil; Buettner, Ralf; Turkson, James; Kim, Donghwa; Cheng, Jin Q.; Muehlbeyer, Stephan; Hippe, Frankie; Vatter, Sandra; Merz, Karl‐Heinz; Eisenbrand, Gerhard; Jove, Richard

doi:10.1073/pnas.0409467102

Cited by 271 publications

(264 citation statements)

References 32 publications

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“…MSC/IFN-β inhibits 4 T1 cell proliferation in vitro It has been reported that Stat3 inhibition can induce apoptosis [36,37]. However, in our previous studies [19,20], we did not detect apoptosis after either knockdown or inhibition of Stat3.…”

Section: Ifn-β Inactivatescontrasting

confidence: 82%

Mesenchymal Stem Cells Overexpressing IFN-β Inhibit Breast Cancer Growth and Metastases through Stat3 Signaling in a Syngeneic Tumor Model

Ling

Marini

Konopleva

et al. 2010

Cancer Microenvironment

110

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We previously demonstrated that mesenchymal stem/stromal cells (MSC) are recruited to tumors and that IFN-β produced by MSC inhibited tumor growth in xenograft models. Because of a deficient immune system, murine xenograft models cannot fully recapitulate tumor and immune cell interactions during progression. Therefore we investigated the capacity of MSC to migrate to and engraft into primary breast tumor sites and subsequently explore mechanisms of tumor inhibition by MSC-delivered IFN-β in a syngeneic, immunocompetent murine model. Herein we report that 1) systemically administrated MSC migrate to established 4 T1 breast cancer sites and localize among the tumor-stroma border and throughout the tumor mass; 2) high levels of IFN-β secreted by MSC are detectable in the tumor microenvironment but not in circulation; 3) intratumorally produced IFN-β inactivates constitutive phosphorylation of signal transducer activator transcription factor 3 (Stat3), Src, and Akt and down-regulates cMyc and MMP2 expression in 4 T1 cells, and 4) in mice with established breast cancer IFN-β expressing MSC administered systemically resulted in inhibition of primary cancer growth and in dramatic reduction of pulmonary and hepatic metastases. 5) MSC-IFN-β treated, but not control mice, maintained normal levels of splenic mature dendritic (DC), CD8+ T cells and CD4+/Foxp3+ regulatory T-cells (Treg). Our findings suggest that MSC are capable of migrating to tumor sites in an immunocompetent environment, that IFN-β produced by MSC suppresses breast cancer growth through inhibition of Stat3 signaling, and dramatically reduces pulmonary and hepatic metastases.

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Section: Ifn-β Inactivatescontrasting

confidence: 82%

Mesenchymal Stem Cells Overexpressing IFN-β Inhibit Breast Cancer Growth and Metastases through Stat3 Signaling in a Syngeneic Tumor Model

Ling

Marini

Konopleva

et al. 2010

Cancer Microenvironment

110

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“…As a matter of fact, STAT3-binding motifs are present in the promoter of Mcl-1 (Puthier et al, 1999). Other studies have reported decreased Mcl-1 expression and increased apoptosis after disruption of phospho-STAT3 signaling (Niu et al, 2002;Lee et al, 2004;Nam et al, 2005). However, we can exclude an involvement of the JAK/ STAT3 pathway in the regulation of Mcl-1 in the present study, as LNCaP-IL-6 þ cells have been previously shown to lack phosphorylated STAT3 (Steiner et al, 2003).…”

Section: Discussionmentioning

confidence: 57%

The antiapoptotic effect of IL-6 autocrine loop in a cellular model of advanced prostate cancer is mediated by Mcl-1

et al. 2006

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“…About 5 mM indirubin-3 0 -monoxime also inhibited the phosphorylation of ERK1/ 2, PLCg, STAT1 and STAT3 in KG-1a cells. Previously, certain indirubin deratives were reported to inhibit phosphorylation of STAT3 by inhibiting an upstream kinase, Src (Nam et al, 2005). However, 5 mM indirubin-3 0 -monoxime did not inhibit phosphorylation of Src in the KG-1a cells, indicating that phosphorylation of STAT3 in this case is a downstream event to phosphorylation of the FGFR1 kinase.…”

Section: Indirubin-3 0 -Monoxime Inhibits Fgfr1mentioning

confidence: 69%

“…Furthermore, indirubin-3 0 -monoxime, but not indirubin, was able to inhibit CDK9 in a cell-free kinase assay and to inhibit replication of HIV-1 in blood mononuclear cells and macrophages (Heredia et al, 2005). Additionally, it was recently reported that indirubin derivatives were able to block Stat3 signaling by inhibiting the Src kinase activity and in this way induce apoptosis in human cancer cells (Nam et al, 2005), and also, bind to and inhibit glycogen synthetase kinase-3 (Leclerc et al, 2001;Polychronopoulos et al, 2004), aryl hydrocarbon receptor (Adachi et al, 2001), muscle glycogen phosphorylase b (Kosmopoulou et al, 2004) and c-Jun NH2-terminal kinase (JNK) (Xie et al, 2004). More recently, indirubin-3 0 -monoxime was found to inhibit the activation of nuclear factor-kB resulting in enhancement of apoptosis induced by tumor necrosis factors in human leukemic cells (Sethi et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

Indirubin-3′-monoxime inhibits autophosphorylation of FGFR1 and stimulates ERK1/2 activity via p38 MAPK

et al. 2007

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Indirubin-3 0 -monoxime is a derivative of the bis-indole alkaloid indirubin, an active ingredient of a traditional Chinese medical preparation that exhibits anti-inflammatory and anti-leukemic activities. Indirubin-3 0 -monoxime is mainly recognized as an inhibitor of cyclin-dependent kinases (CDKs) and glycogen synthase kinase-3. It inhibits proliferation of cultured cells, mainly through arresting the cells in the G1/S or G2/M phase of the cell cycle. Here, we report that indirubin-3 0 -monoxime is able to inhibit proliferation of NIH/3T3 cells by specifically inhibiting autophosphorylation of fibroblast growth factor receptor 1 (FGFR1), blocking in this way the receptormediated cell signaling. Indirubin-3 0 -monoxime inhibits the activity of FGFR1 at a concentration lower than that required for inhibition of phosphorylation of CDK2 and retinoblastoma protein and cell proliferation stimulated by fetal calf serum. The ability of indirubin-3 0 -monoxime to inhibit FGFR1 signaling was similar to that of the FGFR1 inhibitor SU5402. In addition, we found that indirubin-3 0 -monoxime activates long-term p38 mitogen-activated protein kinase activity, which stimulates extracellular signal-regulated kinase 1/2 in a way unrelated to the activity of FGFR1. Furthermore, we show that indirubin-3 0 -monoxime can inhibit proliferation of the myeloid leukemia cell line KG-1a through inhibition of the activity of the FGFR1 tyrosine kinase. The data presented here demonstrate previously unknown activities of indirubin-3 0 -monoxime that may have clinical implications.

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Indirubin derivatives inhibit Stat3 signaling and induce apoptosis in human cancer cells

Cited by 271 publications

References 32 publications

Mesenchymal Stem Cells Overexpressing IFN-β Inhibit Breast Cancer Growth and Metastases through Stat3 Signaling in a Syngeneic Tumor Model

Mesenchymal Stem Cells Overexpressing IFN-β Inhibit Breast Cancer Growth and Metastases through Stat3 Signaling in a Syngeneic Tumor Model

The antiapoptotic effect of IL-6 autocrine loop in a cellular model of advanced prostate cancer is mediated by Mcl-1

Indirubin-3′-monoxime inhibits autophosphorylation of FGFR1 and stimulates ERK1/2 activity via p38 MAPK

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