PDE9A基因多态性与冠心病患者阿托伐他汀调脂疗效的关系研究

doi:10.3760/cma.j.cn441417-20250428-19006

国际医药卫生导报 ›› 2025, Vol. 31 ›› Issue (19): 3196-3201.DOI: 10.3760/cma.j.cn441417-20250428-19006

PDE9A基因多态性与冠心病患者阿托伐他汀调脂疗效的关系研究

王粉¹ 何克强² 张树远³ 冯旭阳¹

¹咸阳市第一人民医院心血管内科，咸阳 712000；²延安大学咸阳医院心血管内科五病区，咸阳 712000；³延安大学咸阳医院心血管内科三病区，咸阳 712000

收稿日期:2025-04-28 出版日期:2025-10-01 发布日期:2025-10-24
通讯作者: 何克强，Email：514298711@qq.com
基金资助:
陕西省自然科学基础研究计划一般项目（2022JM-520）

Study on the relationship between PDE9A gene polymorphism and the lipid-regulating efficacy of atorvastatin in patients with coronary heart disease

Wang Fen¹, He Keqiang², Zhang Shuyuan³, Feng Xuyang¹

¹Department of Cardiovascular Medicine, Xianyang First People's Hospital, Xianyang 712000, China; ²Ward 5, Department of Cardiovascular Medicine, Yan'an University Xianyang Hospital, Xianyang 712000, China; ³Ward 3, Department of Cardiovascular Medicine, Yan'an University Xianyang Hospital, Xianyang 712000, China

Received:2025-04-28 Online:2025-10-01 Published:2025-10-24
Contact: He Keqiang, Email: 514298711@qq.com
Supported by:
Shaanxi Provincial Natural Science Basic Research Program General Project (2022JM-520)

摘要/Abstract

摘要：

目的　研究磷酸二酯酶9A（recombinant phosphodiesterase 9A，PDE9A）基因多态性及其表达水平对阿托伐他汀调脂的冠心病（coronary heart disease，CHD）患者疗效影响。方法　回顾性队列研究。选取2022年5月至2023年5月咸阳市第一人民医院及延安大学咸阳医院收治的186例CHD患者，其中男115例，女71例，年龄（47.85±6.42）岁，体重指数（BMI）（22.27±2.53）kg/m²，均接受3个月阿托伐他汀治疗（口服，起始剂量为10 mg/次，每日一次，每4周复查血脂进行个体化调整，最大剂量为80 mg/次）；另选取同期100例体检健康者作为对照组，其中男52例，女48例，年龄（47.62±6.34）岁，BMI（22.15±2.60）kg/m²。比较对照组与CHD组PDE9A表达水平；CHD患者依据PDE9A基因型分为3组，CC（58例）、CT（86例）与TT（42例）。测定186例CHD患者PDE9A等位基因与基因型频率分布；检测不同基因型CHD患者治疗前后总胆固醇（total cholesterol，TC）、甘油三酯（triglyceride，TG）、低密度脂蛋白胆固醇（LDL-C）、高密度脂蛋白胆固醇（high-density lipoprotein cholesterol，HDL-C）水平及变化率［血脂变化率=（治疗前血脂水平-治疗后血脂水平）/治疗前血脂水平×100%］。采用独立样本t检验、单因素方差分析、LSD检验、Kruskal-Wallis H检验、χ²检验进行统计学分析。结果　CHD患者PDE9A表达水平较对照组上调［（1.06±0.08）比（0.87±0.13）］，差异有统计学意义（t=15.276，P<0.001）。3种基因型CHD患者性别、年龄、BMI、空腹血糖、收缩压、舒张压、丙氨酸氨基转移酶（alanine aminotransferase，ALT）、天门冬氨酸氨基转移酶（aspartate aminotransferase，AST）、血尿素氮（blood urea nitrogen，BUN）、血肌酐（serum creatinine，Scr）水平对比，差异均无统计学意义（均P>0.05）。PDE9A基因rs2250870位点各基因型在186例CHD患者中的分布符合Hardy-Weinberg遗传平衡定律（χ²=0.870，P>0.05）。治疗前，3组CHD患者血脂水平对比，差异均无统计学意义（均P>0.05）；与治疗前相比，3组患者治疗后TC、TG、LDL-C水平降低，HDL-C水平升高（均P<0.05）；治疗后，3组患者TG水平对比差异无统计学意义（P>0.05），但CC型TC、LDL-C水平低于CT、TT型，HDL-C水平高于CT、TT型，CT型LDL-C水平低于TT型（均P<0.05）。CC型TC、LDL-C、HDL-C水平变化率高于CT、TT型，差异均有统计学意义（H=3.568、16.984、11.718，均P<0.05）；3组TG水平变化率对比，差异无统计学意义（P>0.05）。结论　PDE9A基因多态性与阿托伐他汀调脂疗效存在相关性，rs2250870位点不同基因型对阿托伐他汀疗效有差异化影响，CC型患者治疗后TC、LDL-C下降幅度及HDL-C升高幅度大于CT、TT型，该位点可能通过显性遗传模式影响药物反应。

关键词:

冠心病, 阿托伐他汀, PDE9A, 基因多态性, 低密度脂蛋白胆固醇

Abstract:

Objective　To investigate the influence of the gene polymorphism and expression level of recombinant phosphodiesterase 9A (PDE9A) on the lipid-regulating efficacy of atorvastatin in patients with coronary heart disease (CHD). Methods　It was a retrospective cohort study. A total of 186 patients with CHD who were admitted to Xianyang First People's Hospital and Yan'an University Xianyang Hospital from May 2022 to May 2023 were selected. Among them, there were 115 males and 71 females, with an age of (47.85±6.42) years old and a body mass index (BMI) of (22.27±2.53) kg/m². All the patients received 3-month atorvastatin treatment (oral administration, starting dose of 10 mg per time, once a day, and the lipid levels were rechecked every 4 weeks for individualized adjustment, with the maximum dose of 80 mg per time). Another 100 healthy individuals who underwent physical examinations during the same period were selected as the control group. Among them, there were 52 males and 48 females, with an age of (47.62±6.34) years old and a BMI of (22.15±2.60) kg/m². The expression level of PDE9A was compared between the control group and the CHD group. Based on the PDE9A genotype distribution of the CHD patients, they were divided into 3 groups: CC type (58 cases), CT type (86 cases), and TT type (42 cases). The frequency distribution of PDE9A alleles and genotypes were determined in the 186 CHD patients. The levels of total cholesterol (TC), triglyceride (TG), low-density lipoprotein cholesterol (LDL-C), and high-density lipoprotein cholesterol (HDL-C) in the CHD patients with different genotypes were measured before and after treatment, and their change rates were calculated [lipid change rate = (lipid level before treatment - lipid level after treatment) / lipid level before treatment × 100%]. Statistical analysis was conducted using the independent sample t-test, one-way analysis of variance, LSD test, Kruskal-Wallis H test, and χ² test. Results　The expression level of PDE9A in the CHD patients was significantly upregulated compared with that in the control group [(1.06±0.08) vs. (0.87±0.13)], with a statistically significant difference (t=15.276, P<0.001). There were no statistically significant differences in the levels of gender, age, BMI, fasting blood glucose, systolic blood pressure, diastolic blood pressure, alanine aminotransferase (ALT), aspartate aminotransferase (AST), blood urea nitrogen (BUN), and serum creatinine (Scr) among the three genotypes of the CHD patients (all P>0.05). The distribution of each genotype at the rs2250870 locus of the PDE9A gene in 186 CHD patients conformed to the Hardy-Weinberg genetic equilibrium law (χ²=0.870, P>0.05). Before treatment, there was no statistically significant difference in the blood lipid levels among the three groups of CHD patients (all P>0.05); compared with those before treatment, the levels of TC, TG, and LDL-C in the three groups decreased after treatment, while the level of HDL-C increased (all P<0.05); after treatment, there was no statistically significant difference in the TG level among the three groups (P>0.05), but the levels of TC and LDL-C of CC type were lower than those of CT and TT types, the level of HDL-C was higher than those of CT and TT types, and the level of LDL-C of CT type was lower than that of TT type (all P<0.05). The change rates of TC, LDL-C, and HDL-C levels of CC type were higher than those of CT and TT types, with statistically significant differences (H=3.568, 16.984, and 11.718, all P<0.05); there was no statistically significant difference in the change rate of TG level among the three groups (P>0.05). Conclusions　The polymorphism of the PDE9A gene is correlated with the lipid-regulating efficacy of atorvastatin. Different genotypes at the rs2250870 locus have differential effects on the efficacy of atorvastatin. The reductions in TC and LDL-C and the increase in HDL-C in patients with the CC genotype after treatment are greater than those in patients with the CT and TT genotypes. This locus may affect the drug response through the dominant inheritance pattern.

Key words:

Coronary heart disease, Atorvastatin, PDE9A, Gene polymorphism, Low density lipoprotein cholesterol

王粉何克强张树远冯旭阳.

PDE9A基因多态性与冠心病患者阿托伐他汀调脂疗效的关系研究 [J]. 国际医药卫生导报, 2025, 31(19): 3196-3201.

Wang Fen, He Keqiang, Zhang Shuyuan, Feng Xuyang.

Study on the relationship between PDE9A gene polymorphism and the lipid-regulating efficacy of atorvastatin in patients with coronary heart disease [J]. International Medicine and Health Guidance News, 2025, 31(19): 3196-3201.

参考文献

[1] Smith TW. Intimate relationships and coronary heart disease: implications for risk, prevention, and patient management[J]. Curr Cardiol Rep, 2022, 24(6):761-774. DOI: 10.1007/s11886-022-01695-4.
[2] Shaya GE, Leucker TM, Jones SR, et al. Coronary heart disease risk: low-density lipoprotein and beyond[J]. Trends Cardiovasc Med, 2022, 32(4):181-194. DOI: 10.1016/j.tcm.2021.04.002.
[3] Lee YJ, Hong SJ, Kang WC, et al. Rosuvastatin versus atorvastatin treatment in adults with coronary artery disease: secondary analysis of the randomised LODESTAR trial[J]. BMJ, 2023, 383:e075837. DOI: 10.1136/bmj-2023-075837.
[4] 聂斌,张宽心,潘漩,等. 瑞舒伐他汀与阿托伐他汀对动脉钙化抑制作用的比较[J]. 中华实验外科杂志,2024,41(9):1992-1995. DOI:10.3760/cma.j.cn421213-20230926-00196.
[5] Dheyaa Aziz N, Abbood SH, Al-Mayali AH, et al. Association of solute carrier organic anion transporter 1B1 gene polymorphism with response to atorvastatin and associated myopathy in Iraqi dyslipidemia patients[J]. Pol Merkur Lekarski, 2023,51(5):496-503. DOI: 10.36740/Merkur202305108.
[6] Sivkov A, Chernus N, Gorenkov R, et al. Relationship between genetic polymorphism of drug transporters and the efficacy of Rosuvastatin, atorvastatin and simvastatin in patients with hyperlipidemia[J]. Lipids Health Dis, 2021, 20(1):157. DOI: 10.1186/s12944-021-01586-7.
[7] Calamera G, Moltzau LR, Levy FO, et al. Phosphodiesterases and compartmentation of cAMP and cGMP signaling in regulation of cardiac contractility in normal and failing hearts[J]. Int J Mol Sci, 2022, 23(4):2145. DOI: 10.3390/ijms23042145.
[8] Wahlang B, McClain C, Barve S, et al. Role of cAMP and phosphodiesterase signaling in liver health and disease[J]. Cell Signal, 2018, 49:105-115. DOI: 10.1016/j.cellsig.2018.06.005.
[9] Postmus I, Verschuren JJ, de Craen AJ, et al. Pharmacogenetics of statins: achievements, whole-genome analyses and future perspectives[J]. Pharmacogenomics, 2012, 13(7):831-840. DOI: 10.2217/pgs.12.25.
[10] Fopiano KA, Zhazykbayeva S, El-Battrawy I, et al. PDE9A inhibition improves coronary microvascular rarefaction and left ventricular diastolic dysfunction in the ZSF1 rat model of HFpEF[J]. Microcirculation, 2024, 31(8):e12888. DOI: 10.1111/micc.12888.
[11] Zheng L, Zhou ZZ. An overview of phosphodiesterase 9 inhibitors: insights from skeletal structure, pharmacophores, and therapeutic potential[J]. Eur J Med Chem, 2023, 259:115682. DOI: 10.1016/j.ejmech.2023.115682.
[12] 中国成人血脂异常防治指南修订联合委员会. 中国成人血脂异常防治指南(2016年修订版)[J]. 中国循环杂志,2016,31(10):937-950. DOI:10.3969/j.issn.1000-3614.2016.10.001.
[13] 李才信,马志强,马云珊,等. 血清残余脂蛋白胆固醇定量检测对动脉粥样硬化性心血管疾病诊断的临床价值研究[J]. 现代检验医学杂志,2023,38(4):16-21. DOI:10.3969/j.issn.1671-7414.2023.04.003.
[14] 王华,秦利,陈月. 健脾清化方对高脂饮食诱导肥胖小鼠胰岛细胞分化的影响[J]. 世界临床药物,2023,44(6):561-566. DOI:10.13683/j.wph.2023.06.008.
[15] 李婧,苏培,王琨,等. 阿托伐他汀和苯溴马隆联合使用对动脉粥样硬化合并高尿酸血症的影响[J]. 世界临床药物,2020,41(10):796-799,821. DOI:10.13683/j.wph.2020.10.008.
[16] Hong SJ, Lee YJ, Lee SJ, et al. Treat-to-target or high-intensity statin in patients with coronary artery disease: a randomized clinical trial[J]. JAMA, 2023, 329(13):1078-1087. DOI: 10.1001/jama.2023.2487.
[17] 朱扬媚,曹建刚,周玉生. 基因检测在降脂药物个体化治疗中的应用[J]. 中国药房,2023,34(9):1147-1152. DOI:10.6039/j.issn.1001-0408.2023.09.23.
[18] Gong F, Shi Q, Mou X, et al. Atorvastatin mitigates memory deficits and brain monocyte infiltration in chronic hypercholesterolemia[J]. Aging (Albany NY), 2023, 15(23):13669-13679. DOI: 10.18632/aging.205217.
[19] Feil R, Lehners M, Stehle D, et al. Visualising and understanding cGMP signals in the cardiovascular system[J]. Br J Pharmacol, 2022, 179(11):2394-2412. DOI: 10.1111/bph.15500.
[20] Meibom D, Micus S, Andreevski AL, et al. BAY-7081: a potent, selective, and orally bioavailable cyanopyridone-based PDE9A inhibitor[J]. J Med Chem, 2022, 65(24):16420-16431. DOI: 10.1021/acs.jmedchem.2c01267.
[21] García-Campa M, Flores-Ramírez R, Rojo-Garza S, et al. Atorvastatin before percutaneous coronary intervention: a systematic review and meta-analysis[J]. PLoS One, 2024, 19(1):e0293404. DOI: 10.1371/journal.pone.0293404.
[22] Mitani H, Suzuki K, Ako J, et al. Achievement rates for low-density lipoprotein cholesterol goals in patients at high risk of atherosclerotic cardiovascular disease in a real-world setting in Japan[J]. J Atheroscler Thromb, 2023, 30(11):1622-1634. DOI: 10.5551/jat.63940.
[23] Rahman F, Brates I, Aweeka F, et al. Evaluating the effect of atorvastatin exposure and vitamin D levels on lipid outcomes in people with HIV-1 with suppressed HIV-1 RNA and LDL cholesterol <130 mg/dL[J]. HIV Med, 2023, 24(6):749-753. DOI: 10.1111/hiv.13453.
[24] Essayan-Perez S, Südhof TC. Neuronal γ-secretase regulates lipid metabolism, linking cholesterol to synaptic dysfunction in Alzheimer's disease[J]. Neuron, 2023,111(20):3176-3194.e7. DOI: 10.1016/j.neuron.2023.07.005.

PDE9A基因多态性与冠心病患者阿托伐他汀调脂疗效的关系研究

Study on the relationship between PDE9A gene polymorphism and the lipid-regulating efficacy of atorvastatin in patients with coronary heart disease

可视化

摘要/Abstract

引用本文

使用本文

参考文献

相关文章 15

编辑推荐

Metrics

[1]	怡文辉王凯悦陈霄. TyG指数、Hcy及叶酸代谢基因多态性与脑卒中的相关性 [J]. 国际医药卫生导报, 2025, 31(4): 674-679.
[2]	韩鑫盛杰鑫任琳子于杰. 预测冠心病患者心肌缺血事件的冠状动脉CT血管成像定量参数分析 [J]. 国际医药卫生导报, 2025, 31(3): 365-370.
[3]	刘功艳王琳李传波韩克丽. 尼可地尔联合胺碘酮对冠心病心绞痛患者临床症状及血清相关细胞因子水平的影响 [J]. 国际医药卫生导报, 2025, 31(3): 382-386.
[4]	张阿龙马晶莹米白冰. 血清Gas6、NETs水平与老年冠心病患者介入治疗预后的关系 [J]. 国际医药卫生导报, 2025, 31(19): 3174-3180.
[5]	刘伟平. PCI术后患者复发风险感知评分及相关因素调查 [J]. 国际医药卫生导报, 2025, 31(19): 3207-3211.
[6]	郝超凡叶发民. 某三甲医院冠心病重症监护室住院患者心功能现状及影响因素分析 [J]. 国际医药卫生导报, 2025, 31(15): 2515-2519.
[7]	杜晓艳闫会丽韩建伦余蒙蒙. 阿托伐他汀联合阿利西尤单抗注射液对冠心病患者血脂指标的影响 [J]. 国际医药卫生导报, 2025, 31(15): 2525-2529.
[8]	孟芳芳余丽娅康樱樱吴瑞欣朱青春王宁波. 个案管理模式的康复护理决策方案在冠心病伴心力衰竭患者中的应用效果 [J]. 国际医药卫生导报, 2025, 31(15): 2621-2625.
[9]	李红艳. 基于结构方程分析冠心病患者术后健康行为在正念水平与生活质量的中介效应及护理方案 [J]. 国际医药卫生导报, 2025, 31(15): 2630-2635.
[10]	刘谊韩宝华张悦. 黄芪宗气方治疗冠心病合并心力衰竭患者的效果及对血管内皮功能影响 [J]. 国际医药卫生导报, 2025, 31(11): 1770-1774.
[11]	金兴山杨莉. 地奥心血康胶囊联合地尔硫卓对冠心病心绞痛患者临床症状及血清相关细胞因子水平的影响分析 [J]. 国际医药卫生导报, 2025, 31(11): 1791-1795.
[12]	张红艳刘铭刘丽丽锁冬梅. 血清NGAL及sdLDL-C水平对老年T2DM患者MACCE的预测价值 [J]. 国际医药卫生导报, 2025, 31(10): 1632-1636.
[13]	杨星王秋茹周雪. 脂蛋白a和载脂蛋白B联合维生素D检测对冠心病严重程度及短期预后的评估价值 [J]. 国际医药卫生导报, 2024, 30(8): 1238-1242.
[14]	豆峰李丹丹张秋艳. Lp-PLA2基因多态性与高血压大动脉粥样硬化性脑梗死的风险关联 [J]. 国际医药卫生导报, 2024, 30(8): 1358-1362.
[15]	张展李杏莫琳勤苏严琳孙艳彬. 结局引导的双心服务在冠心病不稳定型心绞痛患者PCI围手术期中的应用 [J]. 国际医药卫生导报, 2024, 30(4): 641-646.