苗药痛风停汤对人肾小管上皮细胞hUAT、hURAT1基因表达的影响

目的:观察不同浓度苗药痛风停汤兔含药血清对人肾小管上皮细胞尿酸盐转运体(h UAT)mRNA和尿酸盐阴离子转运体1(h URAT1)mRNA表达的影响。方法:建立肾小管上皮细胞模型,分为苗药痛风停汤高、中、低剂量组和苯溴马隆组、空白组;采用清洁级新西兰制备含药血清家兔,以高、中、低剂量苗药痛风停汤兔含药血清、苯溴马隆兔含药血清、0.9%氯化钠注射液兔含药血清干预,采用实时荧光定量PCR检测HK-2细胞中h UAT、h URAT1 mRNA的相对表达量(双标准曲线法)。结果:与空白组比较,苗药痛风停汤高、中、低剂量组h UATmRNA表达水平均增高,h URAT1mRNA表达水平均下降,差异均有统计学意义(P<0.05)。结论:苗药痛风停汤对体外培养的HK-2细胞h UAT、h URAT1mRNA的表达有调控作用,在mRNA水平上上调h UAT、下调h UART1的表达可能是苗药痛风停降尿酸的作用机制之一。

高血压心衰合并高尿酸血症患者hURAT1(T6092C)基因多态性对氯沙坦降尿酸疗效的影响

目的探讨hURAT1(T6092C)基因多态性对高血压心衰合并高尿酸血症患者服用氯沙坦疗效的影响。方法方便选取2014年1月—2018年8月该院急诊科收治的高血压性心脏病、心功能不全合并高尿酸血症患者146例为研究对象,应用多聚酶链-限制性片段长度多态性(PCR-RFLP)方法检测146例患者的hURAT1(T6092C)基因多态性,同时观察不同基因组服用氯沙坦后尿酸值下降幅度的差异。结果患者TT、TC、CC 3组基因型服用氯沙坦后尿酸值下降幅度差异有统计学意义(P<0.05),TT基因型个体血尿酸下降幅度为(132.3±62.7)μmol/L,高于TC(7.3±12.4)μmol/L和CC基因型个体(2.0±13.9)μmol/L。结论氯沙坦对hURAT1(T6092C)基因突变的高血压性心脏病、心功能不全合并高尿酸血症患者疗效降低,应该注意联合用药提高疗效。

Single Nucleotide Polymorphisms (SNPs) of URAT1 (rs7932775) and ABCG2 (rs3825016) on Chronic Kidney Disease Patients with Hyperuricemia

Background: More and more chronic kidney disease (CKD) patients are accompanied with hyperuricaemia. As is known, hyperuricaemia is an independent hazard of both cardiovascular diseases (CVD) and chronic kidney diseases. We aim at identifying Single Nucleotide Polymorphism (SNP) difference of hURAT1 (rs7932775) and ABCG2 (rs3825016) on CKD patient with hyperuricemia and/or gout. Methods: All forty-two CKD patients were divided into two groups: hyperuricemia, and control group. 24 hours urine sample and serum were prepared for testing biochemistry parameters. The polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) method is used to analyze hURAT1 and ABCG2 single nucleotide polymorphisms in different groups. Results: 17 patients have CT SNP of hURAT1 (rs7932775) and 13 patients have CT SNP of ABCG2 (rs3825016) in hyperuricemia group, while only 5 persons and 6 persons have the same mutations in control group respectively. 7 patients have CT SNP of both hURAT1 (rs7932775) and ABCG2 (rs3825016) in hyperuricemia group, while only 2 persons have the same mutations in control group. CT mutation rates of hURAT1 (rs7932775) and ABCG2 (rs3825016) in hyperuricemia group were 60.7% (17/28) and 50% (13/28) respectively, higher than that of control group (35.7% (5/14) and 42.8% (6/14)). What is more, Double SNP mutations in both hURAT1 (rs7932775) and ABCG2 (rs3825016) in hyperuricemia group were 25% (7/28), higher than that of control group (14.2%, 2/14). Conclusion: There are higher mutation rates of CT SNP in hURAT1 (rs7932775) and/or ABCG2 (rs3825016) in hyperuricemia group. We can conclude that hyperuricemia is a high risk factor in progress of CKD, which is necessary to take measures of decreasing serum uric acid to delay CKD progress.