Growth inhibition and apoptosis in human Philadelphia chromosome-positive lymphoblastic leukemia cell lines by treatment with the dual PPARα/γ ligand TZD18

Liu, Hongyu; Zang, Chuanbing; Fenner, Martin; Liu, Dachuan; Possinger, K.; Koeffler, H. Phillip; Elstner, E

doi:10.1182/blood-2005-05-2103

Cited by 56 publications

(54 citation statements)

References 81 publications

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“…Our observations are in accordance with the previous reports that have also suggested that the antitumor activity of PPARa agonists may involve unknown pathways that are independent of blocking PPARa transcriptional activity and have been described as 'off-target' effects. 15,17,20 Cyclin D1 overexpression is a hallmark of MCL cells. It has been recently reported that inhibition of cyclin D1 in MCL cells Effects of fenofibrate on mantle cell lymphoma Z Zak et al blocks cell proliferation but is not sufficient to induce cell death in these cells.…”

Section: Minomentioning

confidence: 99%

“…Furthermore, it is well documented that activation of mouse and human PPARa often results in opposite physiological effects in the liver. 12,14 In humans, PPARa-specific agonists have been recently reported to have antitumor effects in a number of various cancer types such as acute myeloid leukemia, [15][16] chronic lymphocytic leukemia 17 and malignant tumors of the ovary, 18 liver, 19 skin, breast and lung. 20 Recently, fenofibrate was found to be the most potent drug among all of the fibrates in inhibiting the growth of various cell lines derived from melanoma, lung carcinoma, glioblastoma and fibrosarcoma in a xenograft mouse model.…”

Section: Introductionmentioning

confidence: 99%

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Fenofibrate induces effective apoptosis in mantle cell lymphoma by inhibiting the TNFα/NF-κB signaling axis

2010

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Mantle cell lymphoma (MCL) is a type of aggressive B-cell non-Hodgkin's lymphoma characterized by frequent resistance to conventional chemotherapy. In this study we provided evidence that fenofibrate, which is widely known as an agonist for peroxisome proliferator-activated receptor-a (PPARa), can induce effective apoptosis in treating MCL cells. Addition of fenofibrate to MCL cell lines significantly decreased the number of viable cells by 50% at approximately 20 lM at 72 h. This decrease in cell growth was due to apoptosis, as evidenced by the cleavage of caspase 3 and poly(ADP-ribose) polymerase. The fenofibrate-mediated effects were not significantly affected by GW6471, a specific PPARa antagonist. Using an apoptosis pathway-specific oligonucleotide array, we found that fenofibrate significantly downregulated several pro-survival genes, including tumor necrosis factor-a (TNFa). Importantly, addition of recombinant TNF-a conferred partial protection against fenofibrate-induced apoptosis. Fenofibrate also decreased the nuclear translocation of nuclear factor (NF)-jB-p65 and significantly inhibited the DNA binding of NF-jB in a dose-dependent manner. To conclude, fenofibrate shows efficacy against MCL, and the mechanism can be attributed to its inhibitory effects on the TNF-a/NF-jB signaling axis. In view of the documented safety of fenofibrate in humans, it may provide a valuable therapeutic option for MCL patients.

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Section: Minomentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Fenofibrate induces effective apoptosis in mantle cell lymphoma by inhibiting the TNFα/NF-κB signaling axis

2010

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“…Western blot analysis was performed as described previously. 38 Antibodies against p-AKT (S473), p-AKT (T308) and AKT were from Cell Signaling Technology (New England Biolabs, Frankfurt am Main, Germany); antibody against ß-Actin was from Santa Cruz Biotechnology (Heidelberg, Germany).…”

Section: Measurement Of Chemokines With Elisamentioning

confidence: 99%

Targeting multiple tyrosine kinase receptors with Dovitinib blocks invasion and the interaction between tumor cells and cancer-associated fibroblasts in breast cancer

et al. 2015

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A constitutive and dynamic interaction between tumor cells and their surrounding stroma is a prerequisite for tumor invasion and metastasis. Fibroblasts and myofibroblasts (collectively called cancer associated fibroblasts, CAFs) often represent the major cellular components of tumor stroma. Tumor cells secret different growth factors which induce CAFs proliferation and differentiation, and, consequently, CAFs secrete different chemokines, cytokines or growth factors which induce tumor cell invasion and metastasis. In this study we showed here that CAFs from breast cancer surgical specimens significantly induced the invasion of breast cancer cells in vitro. Most interestingly, the novel multiple tyrosine kinase inhibitor Dovitinib significantly blocked the CAFs-induced invasion of breast cancer cells by, at least in part, inhibition of the expression and secretion of CCL2, CCL5 and VEGF in CAFs. Inhibition of PI3K/Akt/mTOR signaling could be responsible for the effects of Dovitinib, since Dovitinib antagonized the promoted phosphorylated Akt after treatment with PDGF, FGF or breast cancer cell-conditioned media. Treatment with Dovitinib in combination with PI3K/Akt/mTOR signaling inhibitors Ly294002 or RAD001 resulted in additive inhibition of cell invasion. This is the first in vitro study to show that the multiple tyrosine kinase inhibitor has therapeutic activities against breast cancer metastasis by targeting both tumor cells and CAFs.

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“…One is the extrinsic pathway that is triggered by ligation of cell death receptors leading to activation of Caspase 8. The other is the intrinsic pathway in which the bcl-2 superfamily and mitochondria are involved (Liu et al, 2006). In this case, decrease in the expression of antiapoptotic Bcl-2 protein or an increase in the level of proapoptotic Bax protein disrupts the mitochondrial membranes and releases proapoptotic proteins leading to activation of Caspase 9, as we have observed in cervical epithelium of RXRa mutant mice (Fig.…”

Section: Discussionmentioning

confidence: 84%

“…As we mentioned, Bcl-2 promotes cell survival, whereas Bax promotes cell death (Adams and Cory, 1998), and it is known that the ratio of Bcl-2 to Bax determines survival or death following an apoptotic stimulus (Adams and Cory, 1998;Liu et al, 2006;Thomas et al, 1996). Thus, the increase in bax gene expression and the decrease in bcl-2 gene expression observed after RXRa ablation should dramatically increase cell death.…”

Section: Discussionmentioning

confidence: 93%

Impaired cervical homeostasis upon selective ablation of RXRα in epithelial cells

Ocadiz-Delgado

Castañeda-Saucedo

Indra

et al. 2008

Genesis

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Summary: Retinoids play critical regulatory roles in the maintenance of mammalian epithelia and exert pleiotropic effects through nuclear receptors. RXRa, which is a ligand-dependent transcription factor, is the most abundant RXR isotype expressed in cervical epithelia, and may play a crucial role in cervix development and homeostasis. We have previously described a mouse model to induce the temporally controlled epithelia-specific somatic mutagenesis of RXRa alleles in epidermis. To study the role of RXRa in cervical homeostasis, we ablated RXRa in cervix epithelial cells of adult mice. We found that such mutant mice develop ectocervical atrophy with moderate epidermoid metaplasia. In addition, we report a simultaneous increase of cell proliferation and apoptosis levels accompanied by alteration in the expression of genes involved in both processes. genesis 46:19-28,

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Growth inhibition and apoptosis in human Philadelphia chromosome-positive lymphoblastic leukemia cell lines by treatment with the dual PPARα/γ ligand TZD18

Cited by 56 publications

References 81 publications

Fenofibrate induces effective apoptosis in mantle cell lymphoma by inhibiting the TNFα/NF-κB signaling axis

Fenofibrate induces effective apoptosis in mantle cell lymphoma by inhibiting the TNFα/NF-κB signaling axis

Targeting multiple tyrosine kinase receptors with Dovitinib blocks invasion and the interaction between tumor cells and cancer-associated fibroblasts in breast cancer

Impaired cervical homeostasis upon selective ablation of RXRα in epithelial cells

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