| Literature DB >> 22461898 |
Xiaopan Wu1, Jia Wu, Zhenhui Xin, Huifen Wang, Xilin Zhu, Liping Pan, Zhuo Li, Hui Li, Ying Liu.
Abstract
BACKGROUND: Accumulated evidences indicate that single nucleotide polymorphisms (SNP) in angiogenesis and tumorigenesis related genes are associated with risk of Hepatocellular carcinoma (HCC). COL18A1 encodes the precursor of endostatin, which is a broad-spectrum angiogenesis inhibitor, and we speculate that SNPs in COL18A1 may be associated with susceptibility to HCC. METHODS ANDEntities:
Mesh:
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Year: 2012 PMID: 22461898 PMCID: PMC3312886 DOI: 10.1371/journal.pone.0033855
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Clinical features of the subjects included in the study.
| 302_Beijing | Youan_Beijing | Guangxi | |||||||
| HCC | CHB | P | HCC | CHB | P | HCC | CHB | P | |
| Number | 169 | 203 | 326 | 522 | 313 | 342 | |||
| Age, | 50 (42, 55) | 49 (38, 57) | 0.37 | 52 (45, 58) | 40 (34, 49) | <0.001 | 43 (37, 51) | 41 (35, 52) | 0.10 |
| Gender (male/female) | 143/26 | 158/45 | 0.10 | 270/56 | 379/143 | <0.001 | 280/33 | 283/59 | 0.01 |
| Smoking (Yes/No) | 84/85 | 64/139 | <0.001 | 135/159 | 103/378 | <0.001 | 128/185 | 141/201 | 0.93 |
| Drinking (Yes/No) | 93/76 | 71/132 | <0.001 | 141/153 | 113/366 | <0.001 | 95/218 | 97/245 | 0.58 |
| Family history of HBV (Yes/No) | 98/71 | 133/70 | 0.14 | 141/172 | 333/169 | <0.001 | |||
| Family history of HCC (Yes/No) | 52/261 | 16/326 | <0.001 | ||||||
| HbeAg (+/−) | 65/104 | 131/72 | <0.001 | 128/198 | 356/166 | <0.001 | |||
| ALT (IU/L) | 218 (67, 227) | 227 (113, 268) | <0.001 | 129 (109, 142) | 131 (122, 143) | 0.01 | |||
| AST (IU/L) | 158 (72, 230) | 160 (96, 245) | 0.03 | 124 (108, 165) | 125 (109, 162) | 0.88 | |||
| TBil (µmol/L) | 36 (19, 49) | 34 (21, 50) | 0.08 | 49 (28, 61) | 39 (22, 54) | <0.001a | |||
| DBil (µmol/L) | 28 (15, 35) | 29 (15, 36) | 0.89 | 33 (16, 50) | 27 (11, 35) | <0.001 | |||
| Log HBV-DNA (copy/mL) | 5.9 (4.6, 6.2) | 6.7 (5.5, 7.2) | <0.001 | 5.4 (4.6, 6.0) | 5.6 (4.7, 6.1) | <0.001 |
Age, ALT, AST, TBil, DBil, and HBV-DNA as median (25-percentile, 75-percentile).
HCC: hepatocellular carcinoma.
CHB: chronic hepatitis B.
Mann-Whitney U test.
Chi-square test.
Genotype distributions of 4 SNPs in COL18A1 gene of the 302_Beijing samples.
| Allele, n (%) | Genotype, n (%) | Cochran Armitage trend test | logistic regression | ||||||
| 1/2 | 1 | 2 | P/OR (95% CI) | 11 | 12 | 22 | P | P/OR (95% CI) | |
| rs2183589 | C/T | ||||||||
| HCC (n = 169) | 306 (90.5%) | 32 (9.5%) | 0.18 | 139 (82.2%) | 28 (16.6%) | 2 (1.2%) | 0.18 | 0.20 | |
| CHB (n = 203) | 355 (87.4%) | 51 (12.6%) | 1.37 (0.86–2.19) | 155 (76.4%) | 45 (22.2%) | 3 (1.5%) | 1.37 (0.85–2.22) | ||
| rs2230688 | G/T | ||||||||
| HCC (n = 169) | 223 (66.0%) | 115 (34.0%) | 0.43 | 72 (42.6%) | 79 (46.7%) | 18 (10.7%) | 0.43 | 0.41 | |
| CHB (n = 203) | 279 (68.7%) | 127 (31.3%) | 0.88 (0.65–1.20) | 99 (48.8%) | 81 (39.9%) | 23 (11.3%) | 0.88 (0.64–1.20) | ||
| rs11702425 | T/C | ||||||||
| HCC (n = 169) | 262 (77.5%) | 76 (22.5%) | 0.98 | 104 (61.5%) | 54 (32.0%) | 11 (6.5%) | 0.98 | 0.73 | |
| CHB (n = 203) | 315 (77.6%) | 91 (22.4%) | 0.99 (0.70–1.41) | 127 (62.6%) | 61 (30.0%) | 15 (7.4%) | 0.94 (0.67–1.32) | ||
| rs7499 | C/T | ||||||||
| HCC (n = 169) | 153 (45.3%) | 185 (54.7%) | 0.006 | 29 (17.2%) | 95 (56.2%) | 45 (26.6%) | 0.005 | 0.009 | |
| CHB (n = 203) | 225 (55.4%) | 181 (44.6%) | 0.67 (0.50–0.89) | 63 (31.0%) | 99 (48.8%) | 41 (20.2%) | 0.66 (0.48–0.90) |
P values were adjusted for age, gender, smoking and drinking by binary logistic regression.
Common haplotypes constructed with SNPs rs2183589, rs2230688, rs11702425 and rs7499 in COL18A1 gene of the 302_Beijing samples.
| Haplotypes | HCC (n = 169) | CHB (n = 203) | P | OR (95%CI) |
| C-G-C-T | 42.84 (12.7%) | 24.33 (6.0%) | 0.003 | 2.20 (1.31–3.71) |
| C-G-T-C | 77.97 (23.1%) | 113.98 (28.1%) | 0.06 | 0.73 (0.52–1.02) |
| C-G-T-T | 63.69 (18.8%) | 76.35 (18.8%) | 0.82 | 0.96 (0.66–1.39) |
| C-T-T-C | 24.70 (7.3%) | 51.37 (12.7%) | 0.01 | 0.52 (0.31–0.86) |
| C-T-T-T | 68.67 (20.3%) | 40.61 (10.0%) | 0.0002 | 2.22 (1.46–3.39) |
| others | 60.13 (17.8%) | 99.36 (24.5%) |
Association results for rs7499 in replication studies.
| Allele, n (%) | Genotype, n (%) | Cochran Armitage trend test | logistic regression | |||||
| C | T | P/OR (95% CI) | CC | CT | TT | P | P/OR (95% CI) | |
| Youan_Beijing | ||||||||
| HCC (n = 326) | 297 (45.6%) | 355 (54.4%) | 0.003 | 63 (19.3%) | 171 (52.5%) | 92 (28.2%) | 0.003 | 0.29 |
| CHB (n = 522) | 552 (52.9%) | 492 (47.1%) | 0.75 (0.61–0.91) | 151 (28.9%) | 250 (47.9%) | 121 (23.2%) | 0.88 (0.70–1.11) | |
| Guangxi | ||||||||
| HCC (n = 313) | 237 (37.9%) | 389 (62.1%) | 0.01 | 41 (13.1%) | 155 (49.5%) | 117 (37.4%) | 0.01 | 0.01 |
| CHB (n = 342) | 307 (44.9%) | 377 (55.1%) | 0.75 (0.60–0.93) | 70 (20.5%) | 167 (48.8%) | 105 (30.7%) | 0.75 (0.60–0.94) | |
| Combined | ||||||||
| HCC (n = 808) | 687 (42.5%) | 929 (57.5%) | 5e-7 | 133 (16.5%) | 421 (52.1%) | 254 (31.4%) | 4e-7 | 0.00001 |
| CHB (n = 1067) | 1084 (50.8%) | 1050 (49.2%) | 0.72 (0.63–0.82) | 284 (26.6%) | 516 (48.4%) | 267 (25.0%) | 0.73 (0.64–0.84) |
P values were adjusted for age, gender, smoking and drinking by binary logistic regression.
Combination of 3 case-control samples from 302_Beijing, Youan_Beijing and Guangxi.
Figure 1Quantification of COL18A1 mRNA expression by real-time PCR.
GAPDH was used as an internal control gene. Final abundance figures were adjusted to yield an arbitrary value of 1 for HCC patients. Each experiment was performed in triplicate assay. Data are means±SD. A. COL18A1 mRNA expression in HCC, CHB, and healthy individuals. B. COL18A1 mRNA expression in CHB patients, among different genotypes of rs7499.