| Literature DB >> 25932641 |
Wei-Min Ho1, Chiung-Mei Chen2, Yun-Shien Lee3, Kuo-Hsuan Chang2, Huei-Wen Chen2, Sien-Tsong Chen2, Yi-Chun Chen2.
Abstract
BACKGROUND: Spontaneous deep intracerebral hemorrhage (SDICH) is a devastating stroke subtype. The causes of SDICH are heterogeneous. Matrix metalloproteinase-9 (MMP-9, Gelantinase B) has been shown to relate to stroke and the development of aneurysm and may increase risks of intracerebral hemorrhage. MMP activities are modulated by their endogenous inhibitors, tissue inhibitors of metalloproteinases (TIMPs). We analyzed the genetic variants of MMP-9 and TIMP-1 and SDICH susceptibility.Entities:
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Year: 2015 PMID: 25932641 PMCID: PMC4416754 DOI: 10.1371/journal.pone.0125397
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Primers used for amplification and mini-sequencing reaction with MALDI-TOF-based mini-sequencing genotyping method.
| MMP-9 | rs3918242 |
|
| MMP-9 | rs17576 |
|
| MMP-9 | rs3787268 |
|
| MMP-9 | rs2250889 |
|
| TIMP-1 | rs4898 |
|
F: forward primer; R: reverse primer; MSP: Mini-sequencing primer
Demographic data in patients with spontaneous deep intracerebral hemorrhage and controls.
| Males (n = 441) | Females (n = 324) | |||||
|---|---|---|---|---|---|---|
| SDICH | Controls | P-Value | SDICH | Controls | P-Value | |
| n = 229 | n = 212 | n = 97 | n = 227 | |||
| Age (years) | 57.0 ± 12.9 | 59.3 ± 13.0 | 0.07 | 64.2 ± 11.9 | 62.9 ± 10.9 | 0.33 |
| Hypertension (%) | 90.4 | 48.1 | <0.0001 | 92.8 | 51.1 | <0.0001 |
| Diabetes mellitus (%) | 15.4 | 14.8 | 0.86 | 27.1 | 13.6 | 0.002 |
| Alcohol use (%) | 41.5 | 19.8 | <0.0001 | 5.2 | 1.8 | 0.09 |
| Smoke (%) | 58.5 | 34.0 | <0.0001 | 5.2 | 1.8 | 0.09 |
| Body mass index (kg/m2) | 25.2 ± 4.1 | 25.7 ± 3.4 | 0.21 | 24.7 ± 3.7 | 25.3 ±3.8 | 0.17 |
| Total cholesterol (mg/dL) | 170.6 ± 43.6 | 165.5 ± 56.5 | 0.29 | 179.9 ± 48.5 | 174.8 ±60.6 | 0.46 |
| Triglyceride (mg/dL) | 143.6 ± 94.7 | 147.1 ± 101.9 | 0.73 | 136.0 ± 68.7 | 144.1 ± 73.0 | 0.37 |
Data are expressed as percentage or mean ± SE. Comparisons between controls and SDICH cases were analyzed by χ2 test or t-test where appropriate. To convert mg/dL to mmol/L, multiply cholesterol values by 0.02586 and triglycerides by 0.011.
aSDICH: spontaneous deep intracerebral hemorrhage.
Frequencies and associations of the genotypes in patients with spontaneous deep intracerebral hemorrhage and controls.
| Males | Females | All | |||||
|---|---|---|---|---|---|---|---|
| SDICH | Controls (%) | P-Value, OR | SDICH | Controls (%) | P-Value | P-Value, OR(95% CI) | |
|
| n = 63 | n = 75 | n = 50 | n = 108 | |||
|
| |||||||
| rs3918242 CC/CT+TT | 76.2/23.8 | 85.1/14.9 | NS | 72.0/28.0 | 79.3/20.7 | NS | NS |
| rs17576 GG/GA+AA | 58.7/41.3 | 60.9/39.1 | NS | 56.0/44.0 | 61.7/38.3 | NS | NS |
| rs3787268 GG/GA+AA | 38.1/61.9 | 25.7/74.3 | 0.019, 0.35(0.14,0.84) | 34.0/66.0 | 25.9/74.1 | NS | 0.01, 0.48(0.27,0.86) |
| rs2250889 CC/CG+GG | 64.5/35.5 | 67.6/32.4 | NS | 64.0/36.0 | 68.5/31.5 | NS | NS |
|
| |||||||
| rs4898 TT/CT+CC | 66.1/33.9 | 45.9/54.1 | 0.015, 0.35(0.15,0.81) | 22/78 | 27.1/72.9 | NS | NS |
|
| n = 166 | n = 137 | n = 47 | n = 119 | |||
|
| |||||||
| rs3918242 CC/CT+TT | 78.2/21.8 | 81.6/18.4 | NS | 84.4/15.6 | 76.5/23.5 | NS | NS |
| rs17576 GG/GA+AA | 55.8/44.2 | 48.9/51.1 | 0.05, 0.6(0.32,1.00) | 60.0/40.0 | 58.8/41.2 | NS | NS |
| rs3787268 GG/GA+AA | 33.9/66.1 | 40.2/59.8 | NS | 29.8/70.2 | 35.3/64.7 | NS | NS |
| rs2250889 CC/CG+GG | 63.6/36.4 | 51.5/48.5 | 0.01, 0.48(0.27,0.84) | 61.4/38.6 | 63.0/37.0 | NS | NS |
|
| |||||||
| rs4898 TT/CT+CC | 58.3/41.7 | 60.3/39.7 | NS | 31.9/68.1 | 33.6/66.4 | NS | NS |
Analysis was performed by logistic regression under dominant genetic model and adjust for age, sex, hypertension, DM, alcohol drinking, smoking, and total cholesterol level.
aSDICH: spontaneous deep intracerebral hemorrhage,
bOR: Odds ratio,
cCI: confidence interval,
dNS: non-significant.
Frequencies and associations of the MMP-9 haplotypes carrier in patients with spontaneous deep intracerebral hemorrhage and controls.
| Males | Females | All | |||||
|---|---|---|---|---|---|---|---|
| SDICH | Controls | P-Value, OR | SDICH | Controls | P-Value, OR (95% CI) | P-Value, OR (95% CI) | |
| Age ≥65 y/o | n = 63 | n = 75 | n = 50 | n = 108 | |||
| Hap1 carrier | 61.9% | 72.6% | 0.025, 0.36 (0.15,0.88) | 65.3% | 74.1% | NS | 0.014, 0.48 (0.26,0.86) |
| Hap2 carrier | 58.7% | 54.8% | NS | 57.1% | 53.7% | NS | NS |
| Hap3 carrier | 34.9% | 30.1% | NS | 34.7% | 31.5% | NS | NS |
| Hap4 carrier | 7.9% | 8.2% | NS | 14.3% | 7.4% | NS | NS |
| Age <65 y/o | n = 166 | n = 137 | n = 47 | n = 119 | |||
| Hap1 carrier | 65.6% | 60.3% | NS | 70.2% | 64.7% | NS | NS |
| Hap2 carrier | 57.1% | 58.1% | NS | 61.7% | 55.5% | NS | NS |
| Hap3 carrier | 36.2% | 48.5% | 0.009, 0.47 (0.26,0.83) | 36.2% | 37.0% | NS | 0.04, 0.61 (0.38,0.97) |
| Hap4 carrier | 8.6% | 5.2% | NS | 2.1% | 7.6% | NS | NS |
Haplotype 1 (Hap1) carrying one or two copies of GAC, Hap2: GGC, Hap3: AGG, Hap4: AGC.
Analysis was performed by logistic regression model and adjust with age, sex, DM, HTN, Alcohol drinking, smoking, and total cholesterol level are adjusted.
aSDICH: spontaneous deep intracerebral hemorrhage,
bOR: Odds ratio,
cCI: confidence interval,
dNS: non-significant.
Fig 1Haploview disequilibrium coefficients (D’) of the pairwise loci in the Intracerebral hemorrhage group and control group.
Four SNPs in the genomic region of MMP-9 loci were analyzed by Haploview version 4.2 software. The D’ value of the pairwise loci were measured from the SDICH group and control group and are shown in Panel A and B, respectively. A D’ value of “1” indicates that the examined two loci exhibit complete linkage while a value of “0” demonstrates the independence of one another. While rs3918242 was weak linkage disequilibrium (LD) with the other 3 SNPs in the SDICH group (Panel A), the four polymorphisms showed strong LD with each other in control group (Panel B). In both group, strong LD was observed between rs17576, rs3787268, and rs2250889. Panel C and D represented levels of recombination between rs3918242 and the block in the SDICH group and control group, respectively. Alleles are displayed using 1 as major allele and 2 as minor allele of each SNPs. Frequencies are shown next to each haplotype and lines show the most common crossings from rs3918242 and the block, with thicker lines showing more common crossings than thinner lines. Shown beneath the crossing lines is multilocus D', which is a measure of the LD between rs3918242 and the block. The amount of historical recombination between the two blocks in SDICH (0.82) was greater than that in controls (0.96).
Fig 2Interaction between TIMP-1 rs4898 and MMP-9 haplotype 3 (Hap3) and SDICH susceptibility.
Interaction between TIMP-1 rs4898 and MMP-9 haplotypes was significant (P = 0.009) in ICH susceptibility among younger male subjects. In subjects carrying rs4898 major allele (T), SDICH risk was similar between Hap 3 carriers and non-carriers (P = 0.96). However, in subjects carrying rs4898 minor allele (C), Hap3 carriers had a significant protective effect from SDICH risk compared to non-Hap3 carriers (OR = 0.21, 95% CI 0.08 to 0.54, P = 0.001). Therefore, rs4898 minor allele and Hap3 had a significant additive protective effect from SDICH susceptibility.
Fig 3Interaction between MMP-9 haplotypes and environmental factors to SDICH susceptibility.
Interaction between MMP-9 haplotypes and alcohol consumption was significant (P = 0.004). Specifically, in alcohol-free subjects, SDICH risk was similar between carriers and non-carriers of haplotype 3 (Hap3, P = 0.53), whereas in subjects with alcohol consumption, Hap3 carriers had a significant protective effect than non-Hap3 carriers (OR = 0.06, 95% CI 0.01 to 0.27, P = 0.0002). Interaction between MMP-9 haplotype 2 (Hap2) and smoke was also significant (P = 0.007). In subjects with smoke, Hap2 carrier had a significant SDICH risk than non-Hap2 carriers (OR = 2.45, 95% CI 1.05 to 5.73, P = 0.04), while in smoke-free subjects, SDICH risk was similar between Hap2 carriers and non-carriers (P = 0.15).