Epigenetic-Genetic Interactions in the<i>APC/WNT, RAS/RAF</i>, and<i>P53</i>Pathways in Colorectal Carcinoma

Suehiro, Yutaka; Wong, Chi Wai; Chirieac, Lucian R.; Kondo, Yutaka; Shen, Lanlan; Webb, C. Renee; Chan, Yeewai; Chan, Alan K. L.; Chan, Tsun Leung; Wu, Tsung Teh; Rashid, Asif; Hamanaka, Yuichiro; Hinoda, Yuji; Shannon, Rhonda L.; Wang, Xuemei; Morris, Jeffrey S.; Issa, Jean–Pierre J.; Yuen, Siu Tsan; Leung, Suet Yi; Hamilton, Stanley R.

doi:10.1158/1078-0432.ccr-07-1802

Cited by 95 publications

(63 citation statements)

References 58 publications

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“…16 Our reported frequency of K-ras overexpression and mutations (48.9% and 41.1%, respectively), together with the significant correlation with reduced OS, was comparable to that reported in some previous studies. In this context, Bazan et al, 16 Suehiro et al, 46 and Pajkos et al 47 reported a significant correlation between K-ras codon 12 mutations and aggressive forms of disease with reduced survival rates. In contrast, Akkiprik et al 7 and Bouzourene et al 15 demonstrated that the presence or absence of K-ras mutations was not correlated with prognosis in patients with stage II CRC.…”

Section: Discussionmentioning

confidence: 98%

The prognostic value of c‐Kit, K‐ras codon 12, and p53 codon 72 mutations in Egyptian patients with stage II colorectal cancer

El-Serafi

Bahnassy

Ali

et al. 2010

Cancer

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BACKGROUND:The prognosis for patients with colorectal cancer (CRC) depends mainly on standard clinicopathologic factors. However, patients with similar disease characteristics exhibit various outcomes, especially in stage II. Therefore, the identification of molecular prognostic markers is needed to predict patient outcomes. METHODS: The authors assessed the prognostic value of c-Kit (also called cluster of differentiation 117 [CD117] or KIT), cyclooxygenase-2 (COX-2), tumor protein 53 (p53), and Kirsten rat sarcoma viral oncogene homolog (K-ras) aberrations in 90 patients with stage II CRC using immunohistochemistry and molecular techniques. The results were correlated with standard clinicopathologic prognostic factors, overall survival (OS), and disease-free survival (DFS). RESULTS: COX2 and c-Kit overexpression was detected in 54.6% and 59.3% of patients, respectively. Overexpression of p53 was detected in 47 patients, including 29 who had mutations, and a unique mutation pattern was detected with 3 hotspots at codons 72, 245, and 273. Overexpression of ras was detected in 44 patients, including 37 who had mutations. On multivariate analysis, c-Kit overexpression, p53 codon 72 mutations, perforation, and performance status were independent prognostic factors for DFS (P ¼ .054, P ¼ .015, P < .0001, and P ¼ .043, respectively); whereas codon 12 K-ras mutation, performance status, and perforation were independent prognostic factors for OS (P ¼ .033, P ¼ .006, and P < .0001, respectively). CONCLUSIONS: The current results provide evidence for the prognostic value of c-Kit overexpression in patients with stage II CRC. The high p53 mutation rate and the unique hotspot in codon 72 have not been reported previously in CRC. This may be related to environmental or racial features that are unique to the studied population. Cancer 2010;116:4954-64.

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Section: Discussionmentioning

confidence: 98%

The prognostic value of c‐Kit, K‐ras codon 12, and p53 codon 72 mutations in Egyptian patients with stage II colorectal cancer

El-Serafi

Bahnassy

Ali

et al. 2010

Cancer

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“…BRAF acts as direct effector of RAS and through the activation of MEK, promotes tumourogenesis (Sclafani et al, 2013). The BRAF pV600E (c.1799T > A) mutation occurs in 15-20% of CRCs and has important genetic, prognostic, and therapeutic implications (Koinuma et al, 2004;Suehiro et al, 2008). A recent literature review and meta-analysis indicates the incidence of BRAF mutation in sporadic MLH1 MSI CRC to be 63.50% (95% CI: 46.98% -78.53%) (Parsons et al, 2012) Likewise most CRCs containing activated BRAF mutation have CIMP, whereas CIMP and the BRAF mutation are uncommon in Lynch syndrome-associated cancers (≤1%) (Lagerstedt Robinson et al, 2007).…”

Section: Sporadic Colorectal Cancer With Msimentioning

confidence: 99%

The current value of determining the mismatch repair status of colorectal cancer: A rationale for routine testing

Ryan

Sheahan

Creavin

et al. 2017

Critical Reviews in Oncology/Hematology

113

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“…14 MGMT methylation or loss of MGMT protein expression is reportedly associated with an increased frequency of mutations in the KRAS oncogene and P53 tumour-suppressor gene in colorectal cancer, particularly G4A transitions, consistent with a causative function of G4A mutagenesis in tumourigenesis. 11,12,[15][16][17][18] However, other studies have found no specific associations with this sequence change, 19,20 or only a weak association with the presence of a G4A mutation within one of the four cancer-associated genes KRAS, P53, APC and b-catenin. 21 Association studies between MGMT methylation, CIMP and microsatellite stability (MSS) status in colorectal cancer have also reported inconsistent findings.…”

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confidence: 99%

“…21 Association studies between MGMT methylation, CIMP and microsatellite stability (MSS) status in colorectal cancer have also reported inconsistent findings. MGMT methylation has been correlated with MSS and low-level MSI, 17,20 though the existence of low-level MSI as an entity distinct from MSS remains controversial. Although MGMT methylation was initially included as one of the panel of markers to predict CIMP in some studies, [22][23][24][25] it has since been shown to be a poor marker for this epigenetic phenotype and may be independent of CIMP status altogether.…”

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confidence: 99%

MGMT methylation is associated primarily with the germline C>T SNP (rs16906252) in colorectal cancer and normal colonic mucosa

Hawkins¹,

Lee²,

Wong³

et al. 2009

Modern Pathology

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O6 -methylguanine DNA methyltransferase (MGMT) is a DNA repair protein that restores mutagenic O 6 -methylguanine to guanine. MGMT methylation is frequently observed in sporadic colorectal cancer and was recently correlated with the C4T allele at SNP rs16906252, within the transcriptional enhancer element of the promoter. MGMT methylation has also been associated with KRAS mutations, particularly G4A transitions. We studied 1123 colorectal carcinoma to define the molecular and clinicopathological profiles associated with MGMT methylation. Furthermore, we assessed factors contributing to MGMT methylation in the development of colorectal cancer by studying the allelic pattern of MGMT methylation using SNP rs16906252, and the methylation status of neighbouring genes within 10q26 in selected tumours and matched normal colonic mucosa. MGMT methylation was detected by combined bisulphite restriction analysis in 28% of tumours and was associated with a number of characteristics, including CDKN2A methylation, absent lymphovascular space invasion and KRAS mutations (but not specifically with KRAS G4A transitions). In a multivariate analysis adjusted for age and sex, MGMT methylation was associated with the T allele of SNP rs16906252 (Po0.0001, OR 5.5, 95% CI 3.8-7.9). Low-level methylation was detected by quantitative methylation-specific PCR in the normal colonic mucosa of cases, particularly those with a correspondingly methylated tumour, as well as controls without neoplasia, and this was also associated with the C4T SNP. We show that the T allele at SNP rs16906252 is a key determinant in the onset of MGMT methylation in colorectal cancer, whereas the association of methylation at MGMT and CDKN2A suggests that these loci may be targets of a common mechanism of epigenetic dysregulation.

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Epigenetic-Genetic Interactions in theAPC/WNT, RAS/RAF, andP53Pathways in Colorectal Carcinoma

Cited by 95 publications

References 58 publications

The prognostic value of c‐Kit, K‐ras codon 12, and p53 codon 72 mutations in Egyptian patients with stage II colorectal cancer

The prognostic value of c‐Kit, K‐ras codon 12, and p53 codon 72 mutations in Egyptian patients with stage II colorectal cancer

The current value of determining the mismatch repair status of colorectal cancer: A rationale for routine testing

MGMT methylation is associated primarily with the germline C>T SNP (rs16906252) in colorectal cancer and normal colonic mucosa

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