Downregulation of Bcl-2, FLIP or IAPs (XIAP and survivin) by siRNAs sensitizes resistant melanoma cells to Apo2L/TRAIL-induced apoptosis

Chawla‐Sarkar, Mamta; Bae, Sohyun; Reu, Frederic J.; Jacobs, Barbara; Lindner, Daniel J.; Borden, Ernest C.

doi:10.1038/sj.cdd.4401416

Cited by 325 publications

(264 citation statements)

References 47 publications

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“…The TYR gene associated with melanoma pathogenesis and significantly upregulated in this study is expressed at various levels in human melanoma cells and is considered an important biochemical marker of melanocytes Parkhurst et al, 1998;Overwijk et al, 1999), while the RAB28 gene, also overexpressed in this study, is expressed in melanocytes and is involved in melanosomal transport and docking (Jager et al, 2000) as well as in the proper sorting of tyrosinase-related protein 1 (TYRP1). The increased transcription of anti-apoptotic genes in this study, including BCL-2 that is elevated in a range of human cancers including melanomas, prostate carcinoma and gliomas (LaCasse et al, 1998;Altieri, 2003;Chawla-Sarkar et al, 2004), demonstrates further the similarity in the modulation of gene expression in Sinclair swine and human cancers.…”

Section: Discussionsupporting

confidence: 60%

Gene expression in Sinclair swine with malignant melanoma

Okomo-Adhiambo

Rink

Rauw

et al. 2012

Animal

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Sinclair swine develop an aggressive form of melanoma, which, in many cases, spontaneously regresses after a complete metastatic phase. We used Affymetrix GeneChip R Porcine Genome Arrays consisting of 24 123 probe sets to compare gene expression in white blood cells (WBCs) and various tissues including the liver, lungs, inguinal lymph nodes and spleen harvested from a Sinclair piglet afflicted by melanoma at birth and exhibiting metastatic lesions at weaning (6 weeks) with those from a full-sibling piglet that showed no incidence of melanoma at birth and weaning. The highest number (3489; ,14%) of significantly upregulated transcripts (fold change in gene expression >2.0 and t-test P-value r0.05) was observed in the liver, while the spleen exhibited the lowest number of upregulated transcripts (528; ,2%). Among significantly downregulated genes, the highest numbers were observed in the inguinal lymph nodes (3651; ,15%) and the least in WBCs (730; ,3%). Differentially expressed transcripts included genes involved in melanoma pathogenesis including SILV, TYR and RAB28. SILV was over-expressed 784-, 430-and 164-fold, while TYR was over-expressed 138-, 81-and 28-fold in the liver, lungs and inguinal lymph nodes, respectively. Quantitative real-time RT-PCR (qRT-PCR) confirmed the microarray data of 12 selected differentially expressed sequences. These results suggest that significant changes in gene expression occur during metastasis of malignant melanoma in the Sinclair swine model. In addition, qRT-PCR analysis of the above 12 differentially expressed sequences was carried out on liver samples collected from 22 pigs (12 of which had melanoma during the first 6 weeks of life), and an ANOVA test contrasting absolute RNA expression between pigs with regressing, progressing and without tumors was significant for TYR, TACSTD1, MATP, GPNMB and CYP4A22, with P-values of 0.034, 0.015, 0.007, 0.050 and 0.022, respectively.

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Section: Discussionsupporting

confidence: 60%

Gene expression in Sinclair swine with malignant melanoma

Okomo-Adhiambo

Rink

Rauw

et al. 2012

Animal

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“…Real-time RT-PCR (Table 1) and immunoblotting (data not shown) also identified cellspecific induction of XAF1 by IFNs, markedly in SK-MEL-28 but less in SK-MEL-3. XAF1 interacts with an inhibitor of apoptosis (XIAP) that may function as a competitive inhibitor of caspases to play a critical role in TRAIL-induced apoptosis (Deveraux et al, 1997;Liston et al, 2001;Leaman et al, 2002;Chawla-Sarkar et al, 2004). XAF1 has been silenced by DNA methylation in gastric cancer and is frequently reduced in expression in melanoma (Byun et al, 2003;Ng et al, 2004;Reu et al, 2006a).…”

Section: Role Of Trail In Sensitization To Ifns By 5-azadcmentioning

confidence: 99%

Reversal of methylation silencing of Apo2L/TRAIL receptor 1 (DR4) expression overcomes resistance of SK-MEL-3 and SK-MEL-28 melanoma cells to interferons (IFNs) or Apo2L/TRAIL

et al. 2007

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Human melanoma cell lines, SK-MEL-3 and SK-MEL-28, despite induction of the proapoptotic cytokine, Apo2L/TRAIL, did not undergo apoptosis in response to interferons . Postulating that genes important for apoptosis induction by IFNs might be silenced by methylation, the DNA demethylating agent 5-aza-2 0 -deoxycytidine (5-AZAdC) was assessed. DR4 (TRAIL-R1) was identified as one of the genes reactivated by 5-AZAdC with a >3-fold increase in 8 of 10 melanoma cell lines. Pretreatment with 5-AZAdC sensitized SK-MEL-3 and SK-MEL-28 cells to apoptosis induced by IFN-a2b and IFN-b; methylation-specific PCR and bisulfite sequencing confirmed demethylation of 5 0 CpG islands of DR4 and flow cytometry showed an increase in DR4 protein on the cell surface. In cells with reactivated DR4, neutralizing mAB to TRAIL reduced apoptosis in response to IFN-b or Apo2L/TRAIL. To further confirm the role of DR4, it was expressed by retroviral vector in SK-MEL-3 and SK-MEL-28 cells with reversal of resistance to IFN-b and Apo2L/TRAIL. Thus, reexpressing DR4 by 5-AZAdC or retroviral transfection in melanoma cell in which promoter methylation had suppressed its expression, potentiated apoptosis by IFNa2b, IFN-b and Apo2L/TRAIL. Reactivation of silenced proapoptotic genes by inhibitors of DNA methylation may enhance clinical response to IFNs or Apo2L/TRAIL.

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“…26,27 In the case of FLIP, FLIP L and FLIP S isoforms, as well as a 43 kDa cleavage fragment (FLIP 43 ), bind to the DISC and block caspase-8 cleavage and hence activation of the apoptotic cascade. 28 Since CHX sensitized NHU and 253J cells to TRAILinduced apoptosis, we investigated the effects of CHX on FLIP, IAP-2 and XIAP expression.…”

Section: Effects Of Trail On Antiapoptotic Protein Expressionmentioning

confidence: 99%

“…Therefore, to determine whether FLIP specifically protects against TRAIL-induced apoptosis in resistant urothelial cells, we used siRNA technology to knockdown FLIP L expression. We used two small interfering RNAs (siRNAs) previously shown to knockdown FLIP L expression, 26,34 as detailed in Materials and Methods. FLIP L siRNA F1 did not reduce FLIP L protein expression (Figure 7a) and had no effect on TRAIL-mediated apoptosis (Figure 7b).…”

Section: Effect Of Flip L Knockdown On Trail-induced Apoptosismentioning

confidence: 99%

Differential susceptibility to TRAIL of normal versus malignant human urothelial cells

et al. 2006

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Comparing normal human urothelial (NHU) cells to a panel of six representative urothelial cell carcinoma (UCC)-derived cell lines, we showed that while TRAIL receptor expression patterns were similar, susceptibility to soluble recombinant crosslinked TRAIL fell into three categories. 4/6 carcinoma lines were sensitive, undergoing rapid and extensive death; NHU and 253J cells were partially resistant and HT1376 cells, like normal fibroblasts, were refractory. Both normal and malignant urothelial cells underwent apoptosis via the same caspase-8/9-mediated mechanism. Rapid receptor downregulation was a mechanism for evasion by some UCC cells. TRAIL resistance in malignant urothelial cells was partially dependent on FLIP L and was differentially mediated by p38 MAPK , whereas in normal cells, resistance was mediated by NF-jB. Importantly, extensive killing of UCC cells could be induced using noncrosslinked TRAIL after prolonged exposure, with no damage to their homologous, normal urothelial cell counterparts.

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Downregulation of Bcl-2, FLIP or IAPs (XIAP and survivin) by siRNAs sensitizes resistant melanoma cells to Apo2L/TRAIL-induced apoptosis

Cited by 325 publications

References 47 publications

Gene expression in Sinclair swine with malignant melanoma

Gene expression in Sinclair swine with malignant melanoma

Reversal of methylation silencing of Apo2L/TRAIL receptor 1 (DR4) expression overcomes resistance of SK-MEL-3 and SK-MEL-28 melanoma cells to interferons (IFNs) or Apo2L/TRAIL

Differential susceptibility to TRAIL of normal versus malignant human urothelial cells

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