Promoting genetics in non-alcoholic fatty liver disease: Combined risk score through polymorphisms and clinical variables

Non-alcoholic fatty liver disease(NAFLD) has a prevalence of approximately 30% in western countries, and is emerging as the first cause of liver cirrhosis and hepatocellular carcinoma(HCC). Therefore, risk stratification emerges as fundamental in order to optimize human and economic resources, and genetics displays intrinsic characteristics suitable to fulfill this task. According to the available data, heritability estimates for hepatic fat content range from 20% to 70%, and an almost 80% of shared heritability has been found between hepatic fat content and fibrosis. The rs738409 single nucleotide polymorphism(SNP) in patatin-like phospholipase domain-containing protein 3 gene and the rs58542926 SNP in transmembrane 6 superfamily member 2 gene have been robustly associated with NAFLD and with its progression, but promising results have been obtained with many other SNPs. Moreover, there has been proof of the additive role of the different SNPs in determining liver damage, and there have been preliminary experiences in which risk scores created through a few genetic variants, alone or in combination with clinical variables, were associated with a strongly potentiated risk of NAFLD, non-alcoholic steatohepatitis(NASH), NASH fibrosis or NAFLD-HCC. However, to date, clinical translation of genetics in the field of NAFLD has been poor or absent. Fortunately, the research we have done seems to have placed us on the right path: We should rely on longitudinal rather than on cross-sectional studies; we should focus on relevant outcomes rather than on simple liver fat accumulation; and we should put together the genetic and clinical information. The hope is that combined genetic/clinical scores, derived from longitudinal studies and built on a few strong genetic variants and relevant clinical variables, will reach a significant predictive power, such as to have clinical utility for risk stratification at the single patient level and even to esteem the impact of intervention on the risk of disease-related outcomes. Well-structured future studies would demonstrate if this vision can become a reality.

脂蛋白相关磷脂酶A2基因多态性与子痫前期和妊娠期高血压的相关性

目的探讨脂蛋白相关磷脂酶A2(Lp-PLA2)基因多态性位点在子痫前期、妊高症人群的分布及其与子痫前期、妊高症的关系。方法292例住院待产的孕妇分为轻度子痫前期组(mPE组,n=68)、重度子痫前期组(sPE组,n=60)、妊娠期高血压组(HDCP组,n=32)及对照组(n=132),均于入院时测量血压、并收集24 h尿液进行24 h尿蛋白定量检测,采集外周血检测血清空腹血糖(FPG)、胰岛素(INS)、甘油三脂(TG)、总胆固醇(TC)、高密度脂蛋白(HDLC)、低密度脂蛋白(LDLC)水平及血细胞Lp-PLA2水平;提取全血DNA检测Lp-PLA 2基因rs1051931、rs1421378、rs1805017位点的多态性,分析Lp-PLA 2基因型在各组间的分布差异。结果mPE组、sPE组、对照组孕妇入院时的收缩压及舒张压低于HDCP组(P<0.05),mPE组、sPE组、HDCP组孕妇TC、TG、LDLC高于对照组、HDLC低于对照组(P<0.05),mPE组、sPE组、HDLC组血细胞Lp-PLA2水平和24 h蛋白尿含量高于对照组(P<0.05),mPE组血细胞Lp-PLA2水平和24 h尿蛋白含量低于sPE组(P<0.05);Lp-PLA 2基因rs 1051931、rs 1421378、rs 1805017位点基因型AA、AG、GG频率分布在4组孕妇间比较差异无统计学意义(χ2=0.790、2.058、4.701,P=0.914、0.992、0.583),Lp-PLA 2基因rs 16874954位点基因型CC、AC在mPE组和对照组比较差异有统计学意义(χ^(2)=4.86,P=0.03),携带CC型基因孕妇发生妊娠期子痫和高血压疾病风险高于AC型(OR=2.139,95%CI为1.024~4.458),rs 1805017位点AG+AA基因型患者HDLC水平明显低于GG基因型患者,TG水平高于GG基因型患者(P<0.05);rs 16874954位点CC基因型患者TG、Lp-PLA2水平高于AC型患者(P<0.05);HDLC水平低于AC型,其余血脂水平在不同基因型孕妇间比较,差异无统计学意义(P>0.05)。结论Lp-PLA 2基因rs 16874954位点多态性位点与子痫前期、妊高症的发生有关。

PLCL2基因多态性与大动脉粥样硬化型缺血性卒中的关系研究

目的探讨磷脂酶C样蛋白2(PLCL2)基因rs4535211、rs75885714、rs7653834位点单核苷酸多态性与大动脉粥样硬化(LAA)型缺血性卒中的相关性。方法选取2021年7月至2022年7月新疆医科大学第二附属医院就诊的105例新发LAA型缺血性卒中患者作为观察组,选取同期该院性别、年龄相匹配的103例体检者作为对照组。收集并比较两组临床资料及血清炎症指标,同时检测两组PLCL2基因rs4535211、rs75885714、rs7653834位点的基因型,并计算基因型和等位基因频率。结果观察组C反应蛋白(CRP)、白细胞介素-6(IL-6)、中性粒细胞与淋巴细胞比值(NLR)、单核细胞与高密度脂蛋白-胆固醇比值(MHR)、血小板与淋巴细胞比值(PLR)、D-二聚体水平高于对照组,高密度脂蛋白-胆固醇(HDL-C)水平低于对照组(P<0.05)。rs7653834位点为C/C、C/T、T/T基因型,两组比较差异有统计学意义(P<0.05)。两组rs7653834位点C/C、T/C、T/T基因型NLR、PLR水平比较,差异有统计学意义(P<0.05)。共显性模型、显性模型、超显性模型分析结果显示,两组rs7653834位点基因型比较,差异有统计学意义(P<0.05)。结论PLCL2基因rs7653834位点多态性与LAA型缺血性卒中可能存在潜在关联。