CpG island methylator phenotype in adenocarcinomas from the digestive tract: Methods, conclusions, and controversies

doi:10.4251/wjgo.v9.i3.105

Advanced Search

BPG is committed to discovery and dissemination of knowledge

Home / Archive / Volume 9, Issue 3

This Article

Academic Content and Language Evaluation of This Article

CrossCheck and Google Search of This Article

Academic Rules and Norms of This Article

Citation of this article

Corresponding Author of This Article

Research Domain of This Article

Article-Type of This Article

Open-Access Policy of This Article

Times Cited Counts in Google of This Article

Number of Hits and Downloads for This Article

Total Article Views (8669)

All Articles published online

The chart showing PDF series, WORD series, HTML series, Figures (1-3) series, Tables (1-6) series.

Item

Count

PDF

557

WORD

411

HTML

4499

Figures (1-3)

330

Tables (1-6)

499

Sum=6296

Publishing Process of This Article

The chart showing Browse series, Download series.

Item

Count

Browse

1006

Download

1367

Sum=2373

Mar 15, 2017 (publication date) through Feb 18, 2025

Times Cited of This Article

Times Cited (10)

Journal Information of This Article

Publication Name

World Journal of Gastrointestinal Oncology

ISSN

1948-5204

Publisher of This Article

Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

Frontier

World J Gastrointest Oncol. Mar 15, 2017; 9(3): 105-120
Published online Mar 15, 2017. doi: 10.4251/wjgo.v9.i3.105

Table 1 Overview of previous studies of CpG island methylator phenotype in tumors from the gastrointestinal track

Year	Event	Ref.
1999	CIMP is first reported in a set of CRC patients	[5]
2004	Nature Reviews paper discussing CIMP in a variety of tumors besides CRC	[23]
2006	Refined molecular subtyping includes CIMP-low and CIMP-0 categories in CRC, with associations to KRAS mutations	[47]
	New insights are gained about the interplay between BRAF V600E mutations, MSI status, MLH1 promoter methylation and CIMP in CRC	[14]
2006-2012	High throughput DNA methylation arrays become widely available, enabling the use of larger gene panels for CIMP characterization	[45,46]
2014	TCGA marker paper on gastric cancer highlights the biological relevance of CIMP for molecular subtyping, exploring associations with EBV infection	[64]
	A better mechanistic understanding of CIMP in CRC is gained through elucidation of the role of MAFG in the context of MLH1 silencing and BRAF V600E mutations	[76]
2015	Pan-cancer stratification of solid tumors reveals similarities in CIMP across a wide variety of cancer types	[51]

CIMP: CpG island methylator phenotype; CRC: Colorectal cancer; MSI: Microsatellite instability; TCGA: The Cancer Genome Atlas.

Table 2 Gastrointestinal adenocarcinoma types, sample sizes, probe set sizes, and CpG island methylator phenotype status

Cancer type	Differentially methylated probes	Control samples	Tumor samples	CIMP-	CIMPi	CIMP+
EAC	6717	11	87	26	31	30
STAD	1110	2	260	109	95	56
COAD	2656	38	274	96	92	86
READ	1255	7	96	31	39	26

CIMP: CpG island methylator phenotype; CIMPi: CIMP intermediate; COAD: Colon adenocarcinoma; EAC: Esophageal adenocarcinoma; READ: Rectal adenocarcinoma; STAD: Stomach adenocarcinoma.

Table 3 Comparison between our CpG island methylator phenotype classification of stomach adenocarcinomas and the four subtypes defined by The Cancer Genome Atlas Research Network¹

	CIN	EBV+	GS	MSI	Total
CIMP+	²12 (26.6)	³13 (5.4)	²2 (11.3)	³27 (10.7)	-54
CIMPi	43 (45.75)	12 (9.4)	20 (19.5)	18 (18.4)	93
CIMP-	³67 (49.68)	²0 (10.2)	³30 (21.2)	²4 (20.0)	101
Total	122	25	52	49	248

¹Numbers outside parentheses correspond to actual sample counts, whereas numbers in parentheses show expected counts under the null model of independent classification;

²Indicates under-represented counts;

³Indicates cells with significantly over-represented counts (P < 0.05, based on Fisher’s exact test). CIMP: CpG island methylator phenotype; CIMPi: CIMP intermediate; CIN: Chromosomal instability; EBV+: Epstein-Barr virus positive; GS: Genomically stable; MSI: Microsatellite instability.

Table 4 Somatic mutations found in the tumor suppressor gene MLH1 in gastrointestinal adenocarcinoma samples

Sample	Cancer type	CIMP class	Mutation	Mutation type	AA pos.	Aff. AAs	VEST score¹
TCGA-A6-6780-01	COAD	CIMP+	chr3:37038192.G>A	Missense substitution	67	1	0.994
TCGA-CA-6719-01	COAD	CIMP+	chr3:37067243.G>A	Missense substitution	385	1	0.701
TCGA-CM-6171-01	COAD	CIMP+	chr3:37070349.C>-	Frameshift deletion	495	262	-
TCGA-EI-6917-01	READ	CIMP+	chr3:37058999.C>T	Missense substitution	265	1	0.981
TCGA-BR-6452-01	STAD	CIMP+	chr3:37107356.A>G	3' UTR	-	-	-
TCGA-FP-A4BE-01	STAD	CIMP+	chr3:37090086.C>T	Nonsense substitution	659	98	-
TCGA-A6-6138-01	COAD	CIMPi	chr3:37035084.G>A	Missense substitution	16	1	0.901
TCGA-AD-6889-01	COAD	CIMPi	chr3:37053348.->A	Frameshift insertion	195	562	-
TCGA-AZ-6601-01	COAD	CIMPi	chr3:37067242.C>T	Missense substitution	385	1	0.952
TCGA-CM-4746-01	COAD	CIMPi	chr3:37059062.A>-	Frameshift deletion	286	471	-
TCGA-EI-6884-01	READ	CIMPi	chr3:37058995.A>G	Acceptor splice site	264	493	-
TCGA-BR-6802-01	STAD	CIMPi	chr3:37053348.A>-	Frameshift deletion	195	562	-
TCGA-F1-6874-01	STAD	CIMPi	chr3:37050312.ACCTTTTTTACAACATAGCC>-	Frameshift deletion	154	603	-
TCGA-A6-6781-01	COAD	CIMP-	chr3:37053348.A>-	Frameshift deletion	195	562	-
TCGA-CM-6674-01	COAD	CIMP-	chr3:37058999.C>-	Frameshift deletion	265	492	-
TCGA-F4-6856-01	COAD	CIMP-	chr3:37089123.GAA>-	In-frame deletion	615	1	-
TCGA-R6-A6KZ-01	EAC	CIMP-	chr3:37034874.T>C	5’ UTR	-	-	-
TCGA-CG-5723-01	STAD	CIMP-	chr3:37053550.G>-	Frameshift deletion	213	544	-

¹Computed using the VEST tool[100], which evaluates only the effect of missense substitutions. AA pos.: Amino acid position; Aff. AAs: Number of affected amino acids (the MLH1 protein contains 756 residues); CIMP: CpG island methylator phenotype; CIMPi: CIMP intermediate; COAD: Colon adenocarcinoma; EAC: Esophageal adenocarcinoma; READ: Rectal adenocarcinoma; STAD: Stomach adenocarcinoma; VEST: Variant effect scoring tool.

Table 5 Association between methylation and gene expression in tumor suppressor genes with significantly hypermethylated promoters in CpG island methylator phenotype + samples across four gastrointestinal adenocarcinoma types¹

		Differential methylation				Correlation with expression
Gene symbol	Promoter probes	Significant probes per cancer type				EAC		STAD		COAD		READ
		COAD	EAC	READ	STAD	cor	p-val	cor	p-val	cor	p-val	cor	p-val
TP73	24	18	3	2	23	-0.34	4.E-01	-0.24	1.E-01	-0.10	1.E+00	-0.20	1.E+00
MAL	8	6	5	2	7	-0.37	3.E-01	-0.46	2.E-07	-0.47	7.E-09	-0.45	3.E-02
C2orf40	8	5	3	1	7	-0.51	2.E-03	-0.57	5.E-13	-0.39	2.E-05	-0.24	6.E-01
TMEFF2	7	7	7	7	7	-0.54	2.E-03	-0.49	2.E-08	-0.41	2.E-03	-0.32	5.E-01
ERBB4	6	7	7	2	7	-0.26	5.E-01	-0.15	5.E-01	NA	1.E+00	-0.30	6.E-01
TWIST2	5	5	4	1	4	-0.26	3.E-01	-0.33	3.E-04	-0.38	2.E-06	-0.37	3.E-02
LRRC3B	13	9	7	1	12	-0.36	5.E-01	-0.38	2.E-04	-0.41	4.E-03	-0.11	1.E+00
HTRA3	10	6	3	1	6	0.02	1.E+00	-0.03	1.E+00	-0.10	1.E+00	-0.07	1.E+00
UNC5C	13	13	13	8	13	-0.38	7.E-02	-0.34	5.E-04	-0.43	4.E-08	-0.40	3.E-02
FAT4	13	13	9	2	13	-0.33	2.E-01	-0.44	4.E-07	-0.34	4.E-05	-0.28	4.E-01
IRX1	5	3	4	3	4	-0.37	2.E-01	-0.37	3.E-04	NA	1.E+00	NA	1.E+00
SCGB3A1	9	9	4	2	9	-0.27	4.E-01	-0.37	3.E-05	-0.22	3.E-01	-0.12	1.E+00
AKAP12	10	9	5	1	10	-0.19	1.E+00	-0.42	1.E-06	-0.42	7.E-08	-0.27	6.E-01
DFNA5	12	10	8	1	9	-0.75	0.E+00	-0.56	1.E-12	-0.36	1.E-05	-0.34	1.E-01
TFPI2	15	22	14	19	22	-0.49	3.E-03	-0.54	2.E-11	-0.38	4.E-06	-0.22	1.E+00
NRCAM	7	6	1	1	6	-0.52	3.E-04	-0.47	2.E-08	-0.19	8.E-02	-0.17	1.E+00
CNTNAP2	14	14	11	1	14	-0.14	1.E+00	-0.27	2.E-02	-0.14	1.E+00	-0.12	1.E+00
PAX6	12	12	5	3	11	-0.22	1.E+00	-0.18	6.E-01	-0.04	1.E+00	-0.32	3.E-01
WT1	12	12	12	3	12	-0.25	1.E+00	-0.04	1.E+00	-0.26	8.E-03	-0.23	1.E+00
PHOX2A	11	11	6	5	11	-0.26	1.E+00	-0.13	1.E+00	-0.38	3.E-03	-0.26	1.E+00
WIF1	8	5	5	3	7	-0.57	2.E-03	-0.32	5.E-03	-0.44	9.E-07	-0.56	2.E-04
SLC5A8	9	11	10	4	12	-0.26	1.E+00	-0.28	2.E-01	-0.17	1.E+00	-0.33	9.E-01
TBX5	17	11	7	1	16	-0.32	5.E-01	-0.09	1.E+00	0.03	1.E+00	-0.16	1.E+00
ATP8A2	8	5	4	2	5	-0.28	1.E-01	-0.37	2.E-05	-0.24	5.E-03	-0.24	3.E-01
ADAMTS18	8	7	5	3	7	-0.27	3.E-01	-0.36	6.E-05	-0.34	5.E-05	-0.30	2.E-01
GALR1	29	27	5	8	27	-0.17	1.E+00	-0.47	2.E-04	0.00	1.E+00	-0.14	1.E+00
RASSF2	5	6	4	3	6	-0.52	5.E-04	-0.31	1.E-03	-0.41	1.E-07	-0.40	2.E-02
CDH4	3	2	2	2	4	-0.17	6.E-01	-0.09	8.E-01	-0.16	3.E-01	-0.32	1.E-01

¹Promoter regions were designated as 2-kb regions encompassing 1.5 kb upstream and 0.5 kb downstream of the transcription start site. For each cancer type, probes were considered significant if the P-value after a one-sided Mann-Whitney U test with Bonferroni correction for multiple testing was < 0.05. The total number of probes considered across all four cancer types was 395814. COAD: Colon adenocarcinoma; EAC: Esophageal adenocarcinoma; READ: Rectal adenocarcinoma; STAD: Stomach adenocarcinoma.

Table 6 Genes differentially mutated between CpG island methylator phenotype+ and CpG island methylator phenotype- gastrointestinal adenocarcinoma samples¹

Gene	Count CIMP+	% CIMP+	Count CIMP-	% CIMP-	P% Diff	P-value	FDR	Pathway
KMT2D	35	20.30%	10	4.30%	16.00%	6.22E-07	2.24E-05	Chromatin
ARID1A	60	34.90%	32	13.90%	21.00%	1.15E-06	2.24E-05	Chromatin
RNF43	42	24.40%	17	7.40%	17.10%	3.04E-06	3.79E-05	Wnt
CSF3R	19	11.00%	2	0.90%	10.20%	4.19E-06	3.79E-05	ERK
SOX7	14	8.10%	0	0.00%	8.10%	4.86E-06	3.79E-05	ERK
PIK3CA	48	27.90%	26	11.30%	16.70%	2.62E-05	1.70E-04	PI3K/RAS
PAX6	17	9.90%	2	0.90%	9.00%	3.96E-05	2.21E-04	Differentiation
ATM	37	21.50%	17	7.40%	14.20%	5.05E-05	2.46E-04	DNA damage
KRAS	52	30.20%	32	13.90%	16.40%	1.04E-04	4.53E-04	PI3K/RAS
EGR1	15	8.70%	2	0.90%	7.90%	1.63E-04	6.37E-04	Differentiation
GATA3	19	11.00%	5	2.20%	8.90%	2.22E-04	7.87E-04	NF-KB
KMT2C	38	22.10%	22	9.50%	12.60%	6.15E-04	2.00E-03	Chromatin
ALDH2	10	5.80%	1	0.40%	5.40%	1.18E-03	3.30E-03	Metabolic
CDK12	18	10.50%	6	2.60%	7.90%	1.18E-03	3.30E-03	PI3K/RAS
SAFB	15	8.70%	4	1.70%	7.00%	1.44E-03	3.73E-03	Chromatin
BCOR	19	11.00%	7	3.00%	8.00%	1.68E-03	4.09E-03	Chromatin
PTEN	24	14.00%	11	4.80%	9.20%	1.97E-03	4.32E-03	PI3K/RAS
AXIN2	21	12.20%	9	3.90%	8.30%	2.00E-03	4.32E-03	Wnt
CTCF	14	8.10%	4	1.70%	6.40%	2.73E-03	5.41E-03	Chromatin
PALB2	11	6.40%	2	0.90%	5.50%	2.77E-03	5.41E-03	DNA repair
ERBB3	18	10.50%	7	3.00%	7.40%	2.96E-03	5.49E-03	PI3K/RAS
ERBB4	29	16.90%	17	7.40%	9.50%	4.05E-03	6.97E-03	PI3K/RAS
FBXW7	32	18.60%	20	8.70%	9.90%	4.11E-03	6.97E-03	Notch
CIC	23	13.40%	12	5.20%	8.20%	6.55E-03	1.06E-02	Proliferation
HLA.A	17	9.90%	8	3.50%	6.40%	1.13E-02	1.71E-02	Immune
MSH6	19	11.00%	10	4.30%	6.70%	1.14E-02	1.71E-02	MMR
ERBB2	15	8.70%	8	3.50%	5.30%	2.98E-02	4.21E-02	PI3K/RAS
CASP8	13	7.60%	6	2.60%	5.00%	3.02E-02	4.21E-02	Apoptosis
SMAD4	27	15.70%	20	8.70%	7.00%	4.05E-02	5.45E-02	Wnt
TFE3	6	3.50%	1	0.40%	3.10%	4.53E-02	5.90E-02	Wnt
APC	82	47.70%	87	37.70%	10.00%	5.24E-02	6.60E-02	Wnt
NRAS	10	5.80%	5	2.20%	3.60%	6.55E-02	7.74E-02	PI3K/RAS
SMARCB1	10	5.80%	5	2.20%	3.60%	6.55E-02	7.74E-02	Chromatin
IGFBP7	3	1.70%	0	0.00%	1.70%	7.70E-02	8.65E-02	DNA Damage
TBL1XR1	6	3.50%	2	0.90%	2.60%	7.76E-02	8.65E-02	Wnt

¹Results are based on a combined set of 179 CIMP- and 154 CIMP+ gastrointestinal adenocarcinoma samples. P-values were computed using a two-tailed Fishers’ exact test. Only genes with FDR < 10% are shown. CIMP: CpG island methylator phenotype.

Citation: Sánchez-Vega F, Gotea V, Chen YC, Elnitski L. CpG island methylator phenotype in adenocarcinomas from the digestive tract: Methods, conclusions, and controversies. World J Gastrointest Oncol 2017; 9(3): 105-120
URL: https://www.wjgnet.com/1948-5204/full/v9/i3/105.htm
DOI: https://dx.doi.org/10.4251/wjgo.v9.i3.105