JNK and AP-1 mediate apoptosis induced by bortezomib in HepG2 cells via FasL/caspase-8 and mitochondria-dependent pathways

Lauricella, Marianna; Emanuele, Sonia; D’Anneo, Antonella; Calvaruso, Giuseppe; Vassallo, B; Carlisi, Daniela; Portanova, Patrizia; Vento, Renza; Tesoriere, Giovanni

doi:10.1007/s10495-006-4689-y

Cited by 90 publications

(80 citation statements)

References 62 publications

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“…Some studies have shown that JNK regulates DR5 expression (6,41,42). Although PS-341 indeed induced JNK activation in our cell lines as shown previously (20,21), we found that the JNK inhibitor SP600125 only weakly attenuated PS-341-induced DR5 induction, 1 suggesting that other mechanism(s) beyond JNK may be involved in PS-341-induced DR5 expression in human NSCLC cells. Because PS-341 induces endoplasmic reticulum stress, including up-regulation of CHOP/ GADD153 (43,44), a transcriptional factor known to regulate DR5 expression (27,45), it remains to be determined whether PS-341 induces a CHOP-dependent up-regulation of DR5.…”

Section: Discussionsupporting

confidence: 79%

“…Many preclinical studies documented that PS-341 alone or in combination with other cancer therapeutic agents, including TRAIL, induces apoptosis in a variety of human cancer cells in vitro, including both hematologic and solid tumor malignancies, and inhibits the growth of tumor xenografts in vivo (16,17). However, the molecular mechanisms underlying PS-341-induced apoptosis and enhancement of apoptosis when combined with other agents, including TRAIL, particularly in human lung cancer cells, remain largely uncharacterized, although it seems to be associated with nuclear factor-nB inhibition (14,18,19), c-Jun NH 2 -terminal kinase (JNK) activation (19)(20)(21), or Bik and Bim accumulation (22,23) shown in certain types of cancer cells.…”

Section: Introductionmentioning

confidence: 99%

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The Proteasome Inhibitor PS-341 (Bortezomib) Up-Regulates DR5 Expression Leading to Induction of Apoptosis and Enhancement of TRAIL-Induced Apoptosis Despite Up-Regulation of c-FLIP and Survivin Expression in Human NSCLC Cells

et al. 2007

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The proteasome inhibitor PS-341 (bortezomib or Velcade), an approved drug for treatment of patients with multiple myeloma, is currently being tested in clinical trials against various malignancies, including lung cancer. Preclinical studies have shown that PS-341 induces apoptosis and enhances tumor necrosis factor-related apoptosis-inducing ligand (TRAIL)-induced apoptosis in human cancer cells with undefined mechanisms. In the present study, we show that PS-341 induced caspase-8-dependent apoptosis, cooperated with TRAIL to induce apoptosis, and up-regulated death receptor 5 (DR5) expression in human non-small cell lung cancer (NSCLC) cells. DR5 induction correlated with the ability of PS-341 to induce apoptosis. Blockage of PS-341-induced DR5 up-regulation using DR5 small interfering RNA (siRNA) rendered cells less sensitive to apoptosis induced by either PS-341 or its combination with TRAIL, indicating that DR5 upregulation mediates PS-341-induced apoptosis and enhancement of TRAIL-induced apoptosis in human NSCLC cells. We exclude the involvement of c-FLIP and survivin in mediating these events because c-FLIP (i.e., FLIP S ) and survivin protein levels were actually elevated on exposure to PS-341. Reduction of c-FLIP with c-FLIP siRNA sensitized cells to PS-341-induced apoptosis, suggesting that c-FLIP elevation protects cells from PS-341-induced apoptosis. Thus, the present study highlights the important role of DR5 up-regulation in PS-341-induced apoptosis and enhancement of TRAIL-induced apoptosis in human NSCLC cells. [Cancer Res 2007;67(10):4981-8]

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Section: Discussionsupporting

confidence: 79%

Section: Introductionmentioning

confidence: 99%

The Proteasome Inhibitor PS-341 (Bortezomib) Up-Regulates DR5 Expression Leading to Induction of Apoptosis and Enhancement of TRAIL-Induced Apoptosis Despite Up-Regulation of c-FLIP and Survivin Expression in Human NSCLC Cells

et al. 2007

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“…B, quantification of phospho-JNK1/2 expression in MM xenograft tumors. The relative intensity of phospho-JNK1/2 expression was quantified using ImageJ software; *, P < 0.05. mediating bortezomib-induced apoptosis (23,(35)(36)(37)(38). Because disruption of polyamine homeostasis augments JNK activity (39-41), we hypothesized that JNK would also mediate the combination effects of bortezomib and CGC-11093.…”

Section: Resultsmentioning

confidence: 99%

“…We focused on the role of JNK as a potential regulator of cell death induced by the CGC-11093/bortezomib combination as we and others have shown that JNK activation contributes to bortezomib-induced apoptosis (23,(35)(36)(37)(38). Furthermore, polyamines have been reported to control JNK activity (39)(40)(41), and thus, we hypothesized that CGC-11093 would augment JNK activity stimulated by bortezomib.…”

Section: Discussionmentioning

confidence: 99%

The Novel Polyamine Analogue CGC-11093 Enhances the Antimyeloma Activity of Bortezomib

Carew

Nawrocki²,

Reddy³

et al. 2008

Cancer Research

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“…The major stress-inducible isoform of the hsp70 family, hsp72, is expressed in human tumors, correlates with poor prognosis, and contributes to resistance to cancer therapy (29)(30)(31). Proteasome inhibitors seem to up-regulate hsp synthesis by increasing the amount of misfolded proteins as shown in breast tumor, hepatoma HepG 2 , myeloma, and B-lymphoma cells (32)(33)(34)(35)(36). Similar to these reports, in this study, hsp72 up-regulation occurred very early after the exposure of the two colorectal cancer cell lines, Caco-2 and HRT-18, to bortezomib.…”

Section: Discussionmentioning

confidence: 99%

Proteomic identification of aldo-keto reductase AKR1B10 induction after treatment of colorectal cancer cells with the proteasome inhibitor bortezomib

Löffler‐Ragg

Mueller

Gamerith

et al. 2009

Molecular Cancer Therapeutics

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Targeting the ubiquitin-proteasome pathway with the proteasome inhibitor bortezomib has emerged as a promising approach for the treatment of several malignancies. The cellular and molecular effects of this agent on colorectal cancer cells are poorly characterized. This study investigated the antiproliferative effect of bortezomib on colorectal cancer cell lines (Caco-2 and HRT-18). In order to define the proteins potentially involved in the mechanisms of action, proteome profiling was applied to detect the proteins altered by bortezomib. The in vitro efficacy of bortezomib as a single agent in colorectal cancer cell lines was confirmed. Proteome profiling with two-dimensional PAGE followed by mass spectrometry revealed the upregulation of the major inducible isoform of heat shock protein 70 (hsp72) and lactate dehydrogenase B in both cell lines, as well as the induction of aldo-keto reductase family 1 member B10 (AKR1B10) in HRT-18 cells. Both AKR1B10 and hsp72 exert cell-protective functions. This study shows for the first time a bortezomib-induced upregulation of AKR1B10. Small interfering RNA-mediated inhibition of this enzyme with known intracellular detoxification function sensitized HRT-18 cells to therapy with the proteasome inhibitor. To further characterize the relevance of AKR1B10 for colorectal tumors, immunohistochemical expression was shown in 23.2% of 125 tumor specimens. These findings indicate that AKR1B10 might be a target for combination therapy with bortezomib.

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JNK and AP-1 mediate apoptosis induced by bortezomib in HepG2 cells via FasL/caspase-8 and mitochondria-dependent pathways

Cited by 90 publications

References 62 publications

The Proteasome Inhibitor PS-341 (Bortezomib) Up-Regulates DR5 Expression Leading to Induction of Apoptosis and Enhancement of TRAIL-Induced Apoptosis Despite Up-Regulation of c-FLIP and Survivin Expression in Human NSCLC Cells

The Proteasome Inhibitor PS-341 (Bortezomib) Up-Regulates DR5 Expression Leading to Induction of Apoptosis and Enhancement of TRAIL-Induced Apoptosis Despite Up-Regulation of c-FLIP and Survivin Expression in Human NSCLC Cells

The Novel Polyamine Analogue CGC-11093 Enhances the Antimyeloma Activity of Bortezomib

Proteomic identification of aldo-keto reductase AKR1B10 induction after treatment of colorectal cancer cells with the proteasome inhibitor bortezomib

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