Retracted: <i>In vitro</i> and <i>in vivo</i> molecular evidence of genistein action in augmenting the efficacy of cisplatin in pancreatic cancer

Banerjee, Sanjeev; Zhang, Yuxiang; Wang, Zhiwei; Che, Mingxin; Chiao, Paul J.; Abbruzzese, James L.; Sarkar, Fazlul H.

doi:10.1002/ijc.22332

Cited by 78 publications

(68 citation statements)

References 43 publications

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“…We also found that piperlongumine downregulated the constitutive activation of NF-kB in pancreatic cancer cell lines. These results on downregulation of NF-kB activation by piperlongumine are consistent with previous reports that piperlongumine inhibited activation of NF-kB in other cancer cell lines (30,39) and with reports that resveratrol (45), genistein (46), dihydroartemisinin (44), zyflamend (47), g-tocotrienol (48), curcumin (49), shikonin (9), and 3,3 0 -Diindolylmethane (50), all present within piperlongumine, are associated with NF-kB inactivation.…”

Section: Discussionsupporting

confidence: 92%

Piperlongumine Suppresses Growth and Sensitizes Pancreatic Tumors to Gemcitabine in a Xenograft Mouse Model by Modulating the NF-kappa B Pathway

Wang

Zhou

et al. 2016

Cancer Prevention Research

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Pancreatic cancer is an aggressive malignancy, which generally respond poorly to chemotherapy. Hence, novel agents that are safe and effective are highly needed. The aim of this study was to investigate whether piperlongumine, a natural product isolated from the fruit of the pepper Piper longum, has any efficacy against human pancreatic cancer when used either alone or in combination with gemcitabine in vitro and in a xenograft mouse model. In vitro, piperlongumine inhibited the proliferation of pancreatic cancer cell lines, potentiated the apoptotic effects of gemcitabine, inhibited the constitutive and inducible activation of NF-kB, and suppressed the NF-kB-regulated expression of c-Myc, cyclin D1, Bcl-2, Bcl-xL, Survivin, XIAP, VEGF, and matrix metalloproteinase-9 (MMP-9). Furthermore, in an in vivo xenograft model, we found piperlongumine alone significantly suppressed tumor growth and enhanced the antitumor properties of gemcitabine. These results were consistent with the downregulation of NF-kB activity and its target genes, decreased proliferation (PCNA and Ki-67), decreased microvessel density (CD31), and increased apoptosis (TUNEL) in tumor remnants. Collectively, our results suggest that piperlongumine alone exhibits significant antitumor effects against human pancreatic cancer and it further enhances the therapeutic effects of gemcitabine, possibly through the modulation of NF-kB-and NF-kB-regulated gene products.Cancer Prev Res; 9(3); 234-44. Ó2015 AACR.

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Section: Discussionsupporting

confidence: 92%

Piperlongumine Suppresses Growth and Sensitizes Pancreatic Tumors to Gemcitabine in a Xenograft Mouse Model by Modulating the NF-kappa B Pathway

Wang

Zhou

et al. 2016

Cancer Prevention Research

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“…This later result might be surprising, since genistein was earlier reported to enhance the toxicity of cisplatin in other tumor cell types. 22,47 Nonetheless, the inability of genistein to increase apoptosis induction by drugs other than ATO in U937 cells seems to be consistent with its failure to inhibit Akt phosphorylation and NF-jB activation, since Akt and NF-jB are protective factors against multiple stressing treatments. Of note, our results only indicate that Akt and NF-jB do not play a main regulatory role under the present experimental conditions, but do not prejudge the capacity of genistein to modulate Akt/NF-jB in leukemia cells in other conditions, nor necessarily contradicts earlier observations in other cell types.…”

Section: Discussionmentioning

confidence: 87%

Genistein selectively potentiates arsenic trioxide‐induced apoptosis in human leukemia cells via reactive oxygen species generation and activation of reactive oxygen species‐inducible protein kinases (p38‐MAPK, AMPK)

Sánchez

Amrán

Fernández

et al. 2008

Intl Journal of Cancer

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The observation that genistein may behave as a pro-oxidant agent lead us to examine the capacity of this isoflavone to modulate the toxicity of the oxidation-sensitive anti-leukemic agent arsenic trioxide (ATO), and for comparison other anti-tumor drugs. Cotreatment with genistein increased ATO-provoked apoptosis and activated apoptosis regulatory events (Bcl-X L down-regulation, cytochrome c and Omi/HtrA2 release from mitochondria, XIAP decrease and caspase-8/Bid and caspase-3 activation) in U937 promonocytes and other human leukemia cell lines (HL60, THP-1, Jurkat, RPMI-8866), but not in phytohemagglutinin-stimulated non-tumor peripheral blood lymphocytes (PBLs). Genistein, alone and with ATO, stimulated reactive oxygen species generation, and apoptosis was attenuated by N-acetyl-L-cysteine and butylated hydroxyanisole. Addition of low H 2 O 2 concentrations mimicked the capacity of genistein to increase ATO-provoked apoptosis in leukemia cells, but not in PBLs. By contrast, co-treatment with genistein or H 2 O 2 failed to potentiate the toxicity of DNA-targeting agent cisplatin, the proteasome inhibitor MG-132 and the histone deacetylase inhibitor MS-275. Within the here used time-period (14 hr) genistein, alone or with ATO, did not significantly affect Akt phosphorylation and NF-jB binding activity, nor decreased intracellular GSH content. However, it elicited N-acetyl-L-cysteine-inhibitable phosphorylation of p38-MAPK and AMPK, and apoptosis was attenuated by pharmacologic inhibitors against these kinases. The pro-oxidant capacity of genistein might be exploited to improve the efficacy of ATO as anti-leukemic agent, and perhaps the efficacy of other oxidation-based therapeutic approaches.

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“…The constitutive activation of NF-κB is believed to promote inhibition of apoptosis and resistance to chemotherapy (Arlt and Schafer, 2002;Holocomb et al, 2008;Liptay et al, 2003). This notion is further supported by the fact that inactivation of NF-κB sensitizes cancer cells to conventional chemotherapies (Banerjee et al, 2005;Banerjee et al, 2007). Therefore, treating pancreatic cancer with NF-κB inhibitors can improve the outcomes of chemotherapy.…”

Section: Discussionmentioning

confidence: 99%

“…Previous reports have demonstrated that inhibition of spontaneous NF-κB activation can potentiate the anticancer effect of various chemotherapeutic agents (Banerjee et al, 2007). Thus, we treated the cell with evodiamine in the presence of SN50, a specific NFκBp65 inhibitor and cell death was measured by live/ dead assay and apoptosis assay.…”

Section: Discussionmentioning

confidence: 99%

Evodiamine induces apoptosis in pancreatic carcinoma PANC-1 cells via NF κB inhibition

Khan

Qazi

Rasul

et al. 2013

Bangladesh J Pharmacol

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Retracted: In vitro and in vivo molecular evidence of genistein action in augmenting the efficacy of cisplatin in pancreatic cancer

Cited by 78 publications

References 43 publications

Piperlongumine Suppresses Growth and Sensitizes Pancreatic Tumors to Gemcitabine in a Xenograft Mouse Model by Modulating the NF-kappa B Pathway

Piperlongumine Suppresses Growth and Sensitizes Pancreatic Tumors to Gemcitabine in a Xenograft Mouse Model by Modulating the NF-kappa B Pathway

Genistein selectively potentiates arsenic trioxide‐induced apoptosis in human leukemia cells via reactive oxygen species generation and activation of reactive oxygen species‐inducible protein kinases (p38‐MAPK, AMPK)

Evodiamine induces apoptosis in pancreatic carcinoma PANC-1 cells via NF κB inhibition

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