发布者: 华静 发布时间: 2021-09-15 浏览次数: 273
联系方式
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电子邮箱:angelina_ai@163.com
办公地址:桂林市育才路15号国重楼
简介
艾纯芝,博士,副研究员,硕士生导师,广西师范大学教师,省部共建国家重点实验室研究员,大连理工大学外聘教师,从事生物信息学与药学研究,主要基于药物的ADME/T性质,开展药物研发与个体化用药研究。在中科院化物所课题组工作多年,作为生物信息学与药学项目小组的负责人,在项目申请、组织实施、探索新的研究方向、研究生指导以及实验室管理等方面积累了丰富的经验。作为项目主持人及重要参与人主持及参与了国家自然基金、“重大新药创制”科技重大专项、国家973 计划等近10项重大科研项目。在生物信息学、药物研发、药代动力学研究、个体化用药指导等领域具有良好的工作基础。先后荣获第二届亚太药代国际会议(2nd Asian PacificRegional ISSX Meeting,2008年5月,上海)等多项奖励。已在国内外学术期刊如《J Comput Chem》、《Curr Drug Metab》、《Bioorg Med Chem Lett.》等发表论文40余篇,参与编撰中文著作两部;获得授权国家发明专利1件。
主要研究方向
1、药物研发
2、生物信息学
3、个体化用药研究
4、成药性研究
讲授课程
制药工艺学、制药设备与工艺设计
主要代表性论文:
1. Zhou QH , SongYQ, Que YF, He QQ, Tu DZ, Zeng HR , Qin WW,*, Ai CZ,*,Ge GB *. Methylophiopogonanone A is a naturally occurring broad-spectruminhibitor against human UDP-glucuronosyltransferases: inhibition behaviors and implicationin herb-drug interactions. Basic & Clinical Pharmacology & Toxicology. Accepted,2019.(IF:3.6; JCR:Q2)
2. Ai CZ, Chen DC, Saeed Y Liu Y Jiang YZ. Regioselectivityfor Bioactivation of Thiophene-contained Compounds be Determined duringSubstrate Oxidation by Cytochrome P450. J Biol Inorg Chem. 2019;24 (7):OCT 1023-1033.(IF:3.6; JCR:Q2)
3. Ai CZ1,Man HZ1,Chen DC, Saeed Y, Wang LH, Jiang YZ.Computational Insight into Crucial Binding Features for Metabolic Specificityof Cytochrome P450 17A1. Informatics in Medicine Unlocked. 2019;15: 100172.
4. Ai CZ, Liu Y,Li W, Chen DM, Zhu XX, Yan YW, Chen DC, Jiang YZ. Computational explanation for bioactivation . mechanismof targeted anticancer agents mediated by cytochrome P450s: a case of Erlotinib.PLoS One.2017;12(6):e0179333.(IF:3.1; JCR:Q1)
5. Dai ZR1, Ai CZ1, Ge GB, He YQ, Wu JJ, Wang JY, Man HZ, Jia Y and Yang L. A Mechanism-Based Model for the Prediction of theMetabolic Sites of Steroids Mediated by Cytochrome P450 3A4. Int.J. Mol. Sci. 2015 Jun 30, 16, 14677-14694.(1共同第一作者)(IF:3.1; JCR:Q2)
6. Ge GB1, Ai CZ1,Hu WB, Hou J, Zhu LL, He GY, Fang ZZ, Liang SC, Wang FY, Yang L., Wang F, YangL. The role of serum albumin in the metabolism of Boc5: molecularidentification, species differences and contribution to plasma metabolism. Eur J Pharm Sci.2013 23; 48(1-2):360-9.(1共同第一作者)(IF:3.4 ; JCR:Q2)
7. Ai CZ, Li Y, Wang YH, Li W, Dong PP, Ge GB, Yang L. Investigation of binding features:effects on the interaction between CYP2A6 and inhibitors. J Comput Chem.2010; 31(9):1822-31. (IF:4.3; JCR:Q1)
8. Ai CZ, Li Y, Wang YH, Chen YD, Yang L. Insight intothe effects of chiral isomers quinidine and quinine on CYP2D6 inhibition. BioorgMed Chem Lett. 2009, 19(3):803-806. (IF:2.6; JCR:Q2)
9. Ai CZ, Li Y, Wang YH, Li YH, Dong PH, Ge GB, YangL.A 3-D QSAR Studyof Catechol-O-Methyltransferase Inhibitors Using CoMFA and CoMSIA. QSARComb Sci. 2008, 27 (10): 1183-1192.(IF:2.9; JCR:Q2)
10. 艾纯芝,孙仁安,王长生,马琳,正己烷催化异构反应中氢溢流机理的理论研究,高等学校化学学报, 2008,29(1): 182-86。 (IF:0.8)
11. Ai CZ,Sun RA,Wang CS.DFT Studies on Hydrogen OverfallMechanism for Catalyzed Hydroisomerization of Pentane. Chinese J StrucChem. 2007, 26(2): 239-247. (IF:0.7; JCR:Q4)
12. Ai CZ,Sun RA,Yan J.TheoreticalStudy of Decomposition Pathways for Rare-gas-containing Compounds HRgX (Rg =He, Ne, Ar, Kr; X = Cl, Br). Chinese J. Struct. Chem. 2005,24(12): 1445-1451. (IF:0.7; JCR:Q4)
13. Liu XY1, Lv X1, Wang P1, Ai CZ, Zhou QH, Finel M, Fan B,Cao YF, Tang H, Ge GB. Inhibition of UGT1A1 by natural and syntheticflavonoids. Int J Biol Macromol. 2019 Apr 1; 126:653-661. (IF:3.9; JCR:Q1)
14. Shen L, Ai CZ, SongYC, Wang FW, Jiao RH, Zhang AH, Man HZ, Tan RX. Cytotoxic TrichotheceneMacrolides Produced by the Endophytic Myrothecium roridum. J Nat Prod. 2019 Jun 28;82(6):1503-1509. (IF:; JCR:)
15. Liao, K; Liu, Y; Ai, CZ;Yu, X; Li, W. The association between CYP2C9/2C19 polymorphisms and phenytoinmaintenance doses in Asian epileptic patients: A systematic review andmeta-analysis.IntJ Clin Pharmacol Ther. 2018 Jul, 56 ( 7):337-346.(IF:1.1; JCR:Q4)
16. LvX1, Feng L1, AiCZ, Hou J, Wang P, Zou LW, Cheng J, Ge GB, Cui JN, and Yang L. Apractical and high-affinity fluorescent probe for uridine diphosphateglucuronosyltransferase 1A1: a good surrogate for bilirubin. J.Med. Chem.,2017. 60(23):9664-9675. (IF:6.3; JCR:Q1)
17. Zhu XX, Yan YW,Ai CZ, Jiang S, Xu SS, Niu M,Wang XZ, Zhong GS, Lu XF, Xue Y, Tian S, Li G, Tang S, Jiang YZ..Jarid2 is essential for the maintenanceof tumor initiating cells in bladder cancer.Oncotarget. 2017 Apr 11;8(15):24483-24490. (IF:6.4; JCR:Q1)
18. Zhu XX, Yan YW, Chen D, Ai CZ, Lu X, Xu SS, Jiang S, Zhong GS, Chen DB, Jiang YZ..Long non-coding RNA HoxA-AS3 interacts with EZH2 to regulate lineage commitmentof mesenchymal stem cells. Oncotarget. 2016;7(39):63561-63570. (IF:6.4; JCR:Q1)
19. Wang Y, Wu MW, Ai CZ, Wang YH. Insight into the Structural Determinants of ImidazoleScaffold-Based Derivatives as TNF-α Release Inhibitors by in SilicoExplorations. Int J Mol Sci. 2015;16(9):20118-38.(IF:2.9; JCR:Q2)
20. Gao X, Qu H, Ai CZ, Cao YF, Huang T, Chen JX,Zeng J, Sun XY, Hong M, Gonzalez FJ, Liu Z, Fang ZZ. Xenobiotica. Regulationprofile of phosphatidylcholines (PCs) and lysophosphatidylcholines (LPCs)components towards UDP-glucuronosyltransferases (UGTs) isoforms.Xenobiotica.2015;45(3):197-206.(IF:2.2; JCR:Q3)
21. MaHY, Sun DX, Cao YF, Ai CZ, QuYQ, Hu CM, Jiang C, Dong PP, Sun XY, Hong M, Tanaka N, Gonzalez FJ, Ma XC, FangZZ. Herb-drug interaction prediction based on the high specific inhibition ofandrographolide derivatives towards UDP-glucuronosyltransferase (UGT) 2B7. ToxicolAppl Pharmacol. 2014; 277(1):86-94.(IF:4.1)
22. Li Y, Han CX, Wang JH, Xiao W, Wang ZZ, Zhang JX, Yang YF, Zhang SW, Ai CZ. Investigation into themechanism of Eucommia ulmoides Oliv. based on a systems pharmacology approach. JEthnopharmacol. 2014,151(1),452-460.(IF:3.2; JCR:Q1)
23. Ge GB, Ning J, Hu LH, Dai ZR, Hou J, Cao YF,Yu ZW, Ai CZ, Gu JK, Ma XC, Yang L.. A highly selectiveprobe for human cytochrome P450 3A4: isoform selectivity, kineticcharacterization and its applications. ChemCommun. 2013; 49 ( 84): 9779-9781.(IF:6.8; JCR:Q1)
24. ZhouK, Ai CZ, Dong PP, Fan XR, Yang L. A novel model to predictO-glycosylation sites using a highly unbalanced dataset. Glycoconj J. 2012. 29 (7):551-564. (IF:2.2; JCR:Q4)
25. WuJJ, Ai CZ, Liu Y, Zhang YY, Jiang M, Lv AP, Yang L. Interactionsbetween Phytochemicals from Traditional Chinese Medicines and Human CytochromeP450 Enzymes. Curr Drug Metab. 2012, 13 (5): 599-614. (IF:4.3; JCR:Q1)
主要科研项目
1. 广西自然科学基金面上项目:基于细胞色素P450酶催化机制的药物生物激活位点预测研究【编号:2019JJA140609】2020.7.1-2023.6.30,在研。(项目负责人)
2. 国家自然科学基金面上项目:抗肿瘤药物酪氨酸激酶抑制剂发生生物激活的机理研究,【编号:81173124】,2012-2012,已结题。(项目负责人)
3. 中国博士后科学基金面上资助(第62批),2017M622784,RNA甲基化表观修饰酶的结构-功能研究与心血管药物发现,2017/12-2018/12,在研。(项目负责人)
4. 中国科学院大连化学物理研究所博士探索基金: CYPs酶催化多样性与特异性的机理的探索,【编号:S201106】,2011-2012,已结题。(项目负责人)
5. 国家自然科学基金面上项目:人源细胞色素P450s酶催化特异性与多样性的机理研究(2011-2013),【编号:81072698】,已结题。(第一参与人)
6. 2019年-2020年,深圳科技创新委-基础研究,项目名称:酶激活肿瘤血管靶向前体药物。项目经费50万。(第一参与人)
7. 国家自然基金面上项目:影响 UGT1A 底物选择性与催化效率的机理研究,【编号:81273590】,2013-2016,正在进行。(第二参与人)
8. 973计划: 基于中药性(气)味科学内涵假说的利水功效中药的药性理论研究,【编号:2013CB531800】,2013-2017,正在进行。(项目骨干)
9. 十二五新药创制国家重大专项:早期成药性评价关键技术,【编号:2012ZX09501001-002】,2012-2015,已结题。(技术攻关)
10.十二五新药创制国家重大专项:基于新型体内探针的药物反应个体间差异标记物及检测试剂盒关键技术研究,【编号:2012ZX09506001】,2012-2015,已结题。(技术攻关)
11.973计划:确有疗效的有毒中药科学应用关键问题的基础研究曙子课题名称:有毒中药毒代动力学特征及基于ADME决定因素和靶点的毒性作用机理研究,已结题。【编号:2009CB522808】。(技术攻关)
专著:
Ø 编委《中药药物代谢动力学研究思路与实践》(已出版), ISBN:9787030359674,2013.01.01;
Ø 编委《现代创新方法与中医药研究》 (已出版), ISBN:9787030309945,2011.06.01,
专利:
杨凌、艾纯芝、葛广波、于洋、夏杨柳、刘兆明。一种新型靶向性抗肿瘤药物的制备方法与应用,申请日期 2011年11月29日,专利号:ZL201110386523.0;授权日期:2015年6月17日。授权编号:1701396。