法尼醇 X 受体单核苷酸多态性对门脉高压性肝硬化失代偿和死亡的影响。
Impact of farnesoid X receptor single nucleotide polymorphisms on hepatic decompensation and mortality in cirrhotic patients with portal hypertension.
机构信息
Division of Gastroenterology and Hepatology, Department of Internal Medicine III, Medical University of Vienna, Vienna, Austria.
Vienna Hepatic Hemodynamic Lab, Medical University of Vienna, Vienna, Austria.
出版信息
J Gastroenterol Hepatol. 2019 Dec;34(12):2164-2172. doi: 10.1111/jgh.14700. Epub 2019 Jun 14.
BACKGROUND AND AIM
The nuclear farnesoid X receptor (FXR) regulates critical pathways of hepatic metabolism, inflammation, and gut mucosal barrier. Thus, we investigated the association of FXR-single nucleotide polymorphism (SNPs) with hepatic decompensation and liver-related mortality in patients with advanced chronic liver disease.
METHODS
Two FXR-SNPs (rs56163822 G > T and rs35724 G > C) were genotyped in a cohort of 402 prospectively characterized patients with hepatic venous pressure gradient (HVPG) ≥ 6 mmHg.
RESULTS
Only 19 patients (4.7%) harbored a rs56163822 T-allele and had less pronounced liver disease as indicated by lower Child-Pugh score (CPS, 6 ± 1 vs 7 ± 2 points, P = 0.034) and higher albumin levels (38.9 ± 4.9 vs 35.9 ± 5.9 g/L, P = 0.026). In contrast, n = 267 (66.4%) patients harbored minor rs35724 allele (G/C or C/C) and had more advanced liver disease, as indicated by a higher model of end-stage liver disease (11 ± 4 vs 10 ± 3, P = 0.016), while other baseline characteristics were similar across FXR-SNP genotypes. In compensated CPS-A patients, the rs35724 minor allele was independently protective for the development of ascites (adjusted hazard ratio [aHR] = 0.411, 95% confidence interval (95% CI): 0.191-0.885; P = 0.023) and tended to reduce the risk of hepatic decompensation (aHR = 0.625, 95% CI: 0.374-1.044, P = 0.072) in multivariate analyses. Of note, transplant-free survival was longer in patients with rs35724 minor allele and HVPG ≥ 10 mmHg (at 5 years: 68.2% vs 55.8%, P = 0.047) and those with HVPG ≥ 16 mmHg (63.3% vs 44.0%, P = 0.021). After adjusting for established risk factors, the rs35724 minor allele was independently associated with reduced liver-related mortality in the overall cohort (aHR = 0.658, 95% CI: 0.434-0.998, P = 0.049), in compensated CPS-A patients (aHR = 0.488, 95% CI: 0.252-0.946, P = 0.034), in patients with HVPG ≥ 10 mmHg (aHR = 0.547, 95% CI: 0.346-0.864, P = 0.010), and in patients with HVPG ≥ 16 mmHg (aHR = 0.519, 95% CI: 0.307-0.878, P = 0.014).
CONCLUSION
The FXR-SNP rs35724 was associated with a reduced risk for development of ascites and liver-related mortality in patients with advanced chronic liver disease.
背景与目的
核法尼醇 X 受体(FXR)调节肝脏代谢、炎症和肠道黏膜屏障的关键途径。因此,我们研究了 FXR 单核苷酸多态性(SNP)与晚期慢性肝病患者肝失代偿和与肝脏相关的死亡率之间的关系。
方法
在一组 402 例肝静脉压力梯度(HVPG)≥6mmHg 的前瞻性特征患者中,对 2 个 FXR-SNPs(rs56163822 G>T 和 rs35724 G>C)进行了基因分型。
结果
只有 19 名患者(4.7%)携带 rs56163822 T 等位基因,肝脏疾病程度较轻,Child-Pugh 评分(CPS)较低(6±1 与 7±2 分,P=0.034),白蛋白水平较高(38.9±4.9 与 35.9±5.9g/L,P=0.026)。相比之下,n=267(66.4%)患者携带 minor rs35724 等位基因(G/C 或 C/C),肝脏疾病更严重,模型终末期肝病评分(MELD)较高(11±4 与 10±3,P=0.016),而其他基线特征在 FXR-SNP 基因型之间相似。在代偿性 CPS-A 患者中,rs35724 次要等位基因独立地降低了腹水发生的风险(调整后的危险比[aHR]为 0.411,95%置信区间[95%CI]:0.191-0.885;P=0.023),并倾向于降低肝失代偿的风险(aHR 为 0.625,95%CI:0.374-1.044,P=0.072)。值得注意的是,在 HVPG≥10mmHg 的患者中(5 年:68.2%与 55.8%,P=0.047)和 HVPG≥16mmHg 的患者中(63.3%与 44.0%,P=0.021),携带 rs35724 次要等位基因的患者无肝移植生存率更长。在校正了既定的危险因素后,rs35724 次要等位基因与整个队列中与肝脏相关的死亡率降低独立相关(aHR 为 0.658,95%CI:0.434-0.998,P=0.049),在代偿性 CPS-A 患者中(aHR 为 0.488,95%CI:0.252-0.946,P=0.034),在 HVPG≥10mmHg 的患者中(aHR 为 0.547,95%CI:0.346-0.864,P=0.010),在 HVPG≥16mmHg 的患者中(aHR 为 0.519,95%CI:0.307-0.878,P=0.014)。
结论
FXR-SNP rs35724 与晚期慢性肝病患者腹水发生和与肝脏相关的死亡率降低风险相关。
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