Comparative Study
doi: 10.1111/j.1365-2613.2008.00583.x.
Epub 2008 Apr 17.
Expression of inhibitors of apoptosis family protein in 7,12-dimethylbenz[a]anthracene-induced hamster buccal-pouch squamous-cell carcinogenesis is associated with mutant p53 accumulation and epigenetic changes
Affiliations
- PMID: 18422599
- PMCID: PMC2613981
- DOI: 10.1111/j.1365-2613.2008.00583.x
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Comparative Study
Expression of inhibitors of apoptosis family protein in 7,12-dimethylbenz[a]anthracene-induced hamster buccal-pouch squamous-cell carcinogenesis is associated with mutant p53 accumulation and epigenetic changes
Int J Exp Pathol.
2008 Oct.
Abstract
Fifty outbred Syrian golden hamsters were equally divided into three experimental groups and two control groups. The pouches of the experimental groups were painted bilaterally with a 0.5% 7,12-dimethylbenz[a]anthracene (DMBA) solution thrice a week for 3, 7 and 14 weeks. One of the control groups was applied with mineral oil while another control group remained untreated throughout the experiment. Neither survivin nor cIAP2 could be detected in any of the control tissues, whereas survivin and cIAP2 were found to be significantly increased in 3-, 7- and 14-week DMBA-treated pouches compared with the control pouches. Expression of XIAP, cIAP1 and NAIP were noted for both the control and 3-, 7- and 14-week DMBA-treated pouches, but levels were found to be significantly elevated in the experimental groups compared with the control pouches. p53 was not detected in any control tissues, but was significantly increased in 3-, 7- and 14-week DMBA-treated pouches. Direct sequencing revealed a point mutation (C-->G) of p53 for pouch tissues treated with DMBA for 3 and 7 weeks, and there was a wide variation in the p53 sequence of the 14-week DMBA-treated pouch tissues, as compared with the control tissues. The control tissues had a survivin- and cIAP2-methylated allele, whereas the DMBA-treated tissues showed no evidence of survivin- and cIAP2-methylation. Neither the control nor DMBA-treated pouches showed evidence of XIAP-, cIAP1- or NAIP-methylation. Our results suggest that the expression of inhibitors of apoptosis family in DMBA-induced hamster buccal-pouch squamous-cell carcinogenesis may be modulated by both genetic (mutant p53) and epigenetic mechanisms.
Figures
cIAP2 staining was not detected in untreated hamster pouch tissue specimen (a, ABC stain ×100). Cytoplasmic staining of cIAP2 proteins was detected in the whole epithelial layer (except the basal layer) of a representative 3-week 7,12-dimethylbenz[a]anthracene (DMBA)-treated pouch tissue sample (b, ABC stain ×200). Patchy cytoplasmic staining was detected in the whole layer of a representative specimen of 7-week DMBA-treated pouch tissue (c, ABC stain ×100). Cytoplasmic cIAP2 staining was shown in a representative specimen of hamster pouch tissue treated with DMBA for 14 weeks (d, ABC stain ×100). A similar staining pattern is also observed for survivin immunostaining.
cIAP1 staining was located in the outermost keratinized layer of an untreated pouch tissue specimen (a, ABC stain ×200), as well as a representative 3-week 7,12-dimethylbenz[a]anthracene (DMBA)-treated pouch tissue (b, ABC stain ×100). Patchy cytoplasmic staining was detected in the whole layer of a representative specimen of 7-week DMBA-treated pouch tissue (c, ABC stain ×100). A representative specimen of pouch tissue treated with DMBA for 14 weeks demonstrated cytoplasmic cIAP1 staining (d) (ABC stain ×100). A similar immunostaining pattern is also observed for XIAP and NAIP proteins.
Negative p53 staining was observed for an untreated pouch tissue specimen (a, ABC stain ×100). Nuclear staining of p53 was noted in representative samples from 3-week (b, ABC stain ×200), 7-week (c, ABC stain ×100) and 14-week (d, ABC stain ×100) 7,12-dimethylbenz[a]anthracene-treated pouch tissue.
Upon RT-PCR, bands corresponding to mRNA of cIAP1 (354 bp), cIAP2 (328 bp), NAIP (446 bp), XIAP (360 bp), survivin (200 bp) and p53 (370 bp) were evident in all of the hamster buccal-pouch tissue specimens treated with 7,12-dimethylbenz[a]anthracene (DMBA) for 14 weeks (lanes 1–10). All samples (lanes 1–10), except the negative control samples (lane N), revealed bands of β-actin (350 bp). Similar results were observed for hamster pouch tissue treated with DMBA for 3 and 7 weeks. Lane M: molecular weight markers.
For all of the untreated samples (lanes 1–10), upon RT-PCR, bands corresponding to mRNA of cIAP1 (354 bp), NAIP (446 bp) and XIAP (360 bp) were detectable, whereas no bands for cIAP2, survivin and p53 were detected. All samples (lanes 1–10), except the negative control samples (lane N), revealed bands of β-actin (350 bp). Similar results were observed for mineral oil-treated pouch tissues. Lane M: molecular weight markers.
Upon direct sequencing of the PCR product of p53 (370 bp), a point mutation of C to G was noted for the hamster buccal-pouch tissue specimens treated with 7,12-dimethylbenz[a]anthracene (DMBA) for 3 and 7 weeks, as compared with the untreated tissue specimens (arrow). A great variation of the sequence of p53 for hamster buccal-pouch tissue specimens treated with DMBA for 14 weeks as compared with the untreated pouch tissue specimens was found.
Representative results of RT-PCR-based methylation assay of cIAP1, cIAP2, NAIP, XIAP and survivin genes for 3-, 7- and 14-week 7,12-dimethylbenz[a]anthracene-treated, untreated and mineral-oil treated hamster buccal-pouch tissues. Lane 1: PCR products for non-digested DNA samples without C → T conversion; lane 2: PCR products for digested DNA samples without C → T conversion; lane 3: PCR products for non-digested DNA samples with C → T conversion; lane 4: PCR products for digested DNA samples with C → T conversion; lane M: molecular weight markers.
Hypothesis of the genetic and epigenetic regulation of inhibitors of apoptosis (IAP) family members for 7,12-dimethylbenz[a]anthracene-induced hamster buccal-pouch squamous-cell carcinogenesis (brown line: interactions amongst the IAP family members remain unclear; purple double-head horizontal arrow: exact interrelationship between mutant p53 mechanism and epigenetic alteration is still uncertain; grey single-head vertical arrow: induction; orange single-head vertical arrow: overexpression of IAP members; brown asterisk: possibly partially regulated by epigenetic changes).
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