灯盏花素缓释制剂的药物代谢动力学研究
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摘要
灯盏花素是从菊科短葶飞蓬属植物短葶飞蓬Erigerm breviscapus(Vant.)Hand.-Mazz中提取出来的黄酮类有效成分,主要为灯盏甲素和乙素的混合物,其中灯盏乙素含量占95%以上。作为一种新型的活血化瘀中药,灯盏花素具有疗效好、用途广、不良反应少等优点,临床上主要用于治疗脑梗死、冠心病、心绞痛等。
本论文以灯盏花素为研究对象,建立了紫外分光光度法用于灯盏花素基本性质以及灯盏花素制剂含量的测定,并对其基本的理化性质进行了考察;建立了高效液相色谱法(HPLC)用于灯盏花素稳定性的研究,发现温度、pH值对其稳定性有显著影响;还建立了动物血浆中灯盏乙素浓度的HPLC测定方法,用于体内药代动力学的研究。
为了满足预防和治疗心脑血管性疾病长期用药的临床需求,达到减少服药次数、降低毒副作用和提高生物利用度的目的,将灯盏花素制成了肠溶缓释胶囊。为检查研制的药品质量,选择了目前中药质量控制中常用的高效液相色谱法建立了该药物的质量标准,包括鉴别、检查、含量测定和体外释放度测定等多项指标。
在分别静脉给予灯盏花素,灌胃给予灯盏花素普通片和灯盏花素肠溶缓释胶囊后,研究了犬血浆中灯盏乙素的血药浓度变化及药代动力学过程。灯盏花素肠溶缓释胶囊和灯盏花素片的血药浓度-时间曲线符合双室开放模型。在测定的时间范围内灯盏花素肠溶缓释胶囊的药时曲线较普通片剂的血药浓度变化平稳,达峰时间和半衰期均延长,具有明显的缓释特性。与静脉给药比较,灯盏花素肠溶缓释胶囊的绝对生物利用度达到76.79%,灯盏花素片的绝对生物利用度为50.38%;与普通片比较相对生物利用度达到152.95%,自制缓释胶囊的生物利用度明显高于参比制剂(市售普通片)。体内外相关性研究表明灯盏花素肠溶缓释胶囊的体内吸收与体外释放度有很好的相关性,可以用体外的释放度数据表征其体内的吸收。
同时,本论文还对灯盏花素的代谢产物进行了初步研究,将灯盏花素原料药分别在家犬的胃液和肠液中进行温孵;同时将其在碱性条件下进行水解。采用液相色谱-离子阱质谱技术检测灯盏花素在体液温孵条件下的代谢产物和碱性条件下的水解产物。体液中的酶水解产物和碱液中的化学水解产物的色谱和质谱行为一致,证明体内外代谢具有相关性,得到相同的代谢产物。灯盏乙素主要代谢途径为野黄芩苷脱去糖分子变为苷元。
Breviscapine were the flavonoids extracted from Erigeron breviscapus (Vant.) Hand-Mazz. Breviscapine were mainly the mixture of 4'-hydroxy- β-D-pyangluconate methyl ester and scutellarin and the content of the latter was about 95 percent. As a new type of Chinese proprietary medicines, which can promote blood circulation to remove blood stasis, breviscapine showed characteristics of good curative effects, wide uses and less side-effects. Breviscapine is efficacious in the treatment of cerebral infraction, coronary heart disease, angina pectoris.
In this paper, the study on breviscapine was reported. Ultraviolet spectrophotometry method was established for the study of physic chemical properties and drug content. The physiochemical properties were observed. High performance liquid chromatography with vv detection was established for studying the stability of breviscapine. Results demonstrated that temperature and PH value had significant influence on its stability. A reversed-phase high performance liquid chromatography method was established for determination if scutellarin in animals plasma which was used for the pharmacokinetics study.
To meet clinical need for long time use of drugs for prevent and treatment of cardiovascular disease and cerebrovascular disease, to attain the aim of reducing times of administration and side-effects, briviscapine sustained-release capsules dissolved in intestines were prepared through the technique of sustained-release microgranules. The HPLC method was developed to control the quality of sustained-release pellets.
The plasma concentrations and pharmacokinetic parameters compared after vein administration of breviscapine and oral administration of normal tablet and sustained-release capsules dissolved in intestines respectively. The results showed that plasma concentration-time profile after coral administration of normal tablet and sustained-released capsules were both fitted in with two compartment model. The absolute bioavailability of sustained-release capsules dissoloved in intestine were calculated to be 76.79% and that of
common tablets were 50.38%. Compared with the normal tablet, the eliminative speed of capsules reduced more slowly. The relative bioavailability was 152.95%. The result showed that breviscapine sustained-release capsules dissolved in intestines was not bioequivalent with the reference preparation (normal tablet). At the same time, metabolites of breviscapine were researched. The breviscapine was incubated in dogs' gastric juice and intestinal juice respectively. The sample was examined by means of HPLC/MS and found the main metabolic product. Two-phase hydrolysis method was used to determined the hydrolysates of breviscapine in vitro. The two kind of product got from different method were the same. The decomposed course of breviscapine in vivo was consistent with that in vitro.
本论文以灯盏花素为研究对象,建立了紫外分光光度法用于灯盏花素基本性质以及灯盏花素制剂含量的测定,并对其基本的理化性质进行了考察;建立了高效液相色谱法(HPLC)用于灯盏花素稳定性的研究,发现温度、pH值对其稳定性有显著影响;还建立了动物血浆中灯盏乙素浓度的HPLC测定方法,用于体内药代动力学的研究。
为了满足预防和治疗心脑血管性疾病长期用药的临床需求,达到减少服药次数、降低毒副作用和提高生物利用度的目的,将灯盏花素制成了肠溶缓释胶囊。为检查研制的药品质量,选择了目前中药质量控制中常用的高效液相色谱法建立了该药物的质量标准,包括鉴别、检查、含量测定和体外释放度测定等多项指标。
在分别静脉给予灯盏花素,灌胃给予灯盏花素普通片和灯盏花素肠溶缓释胶囊后,研究了犬血浆中灯盏乙素的血药浓度变化及药代动力学过程。灯盏花素肠溶缓释胶囊和灯盏花素片的血药浓度-时间曲线符合双室开放模型。在测定的时间范围内灯盏花素肠溶缓释胶囊的药时曲线较普通片剂的血药浓度变化平稳,达峰时间和半衰期均延长,具有明显的缓释特性。与静脉给药比较,灯盏花素肠溶缓释胶囊的绝对生物利用度达到76.79%,灯盏花素片的绝对生物利用度为50.38%;与普通片比较相对生物利用度达到152.95%,自制缓释胶囊的生物利用度明显高于参比制剂(市售普通片)。体内外相关性研究表明灯盏花素肠溶缓释胶囊的体内吸收与体外释放度有很好的相关性,可以用体外的释放度数据表征其体内的吸收。
同时,本论文还对灯盏花素的代谢产物进行了初步研究,将灯盏花素原料药分别在家犬的胃液和肠液中进行温孵;同时将其在碱性条件下进行水解。采用液相色谱-离子阱质谱技术检测灯盏花素在体液温孵条件下的代谢产物和碱性条件下的水解产物。体液中的酶水解产物和碱液中的化学水解产物的色谱和质谱行为一致,证明体内外代谢具有相关性,得到相同的代谢产物。灯盏乙素主要代谢途径为野黄芩苷脱去糖分子变为苷元。
Breviscapine were the flavonoids extracted from Erigeron breviscapus (Vant.) Hand-Mazz. Breviscapine were mainly the mixture of 4'-hydroxy- β-D-pyangluconate methyl ester and scutellarin and the content of the latter was about 95 percent. As a new type of Chinese proprietary medicines, which can promote blood circulation to remove blood stasis, breviscapine showed characteristics of good curative effects, wide uses and less side-effects. Breviscapine is efficacious in the treatment of cerebral infraction, coronary heart disease, angina pectoris.
In this paper, the study on breviscapine was reported. Ultraviolet spectrophotometry method was established for the study of physic chemical properties and drug content. The physiochemical properties were observed. High performance liquid chromatography with vv detection was established for studying the stability of breviscapine. Results demonstrated that temperature and PH value had significant influence on its stability. A reversed-phase high performance liquid chromatography method was established for determination if scutellarin in animals plasma which was used for the pharmacokinetics study.
To meet clinical need for long time use of drugs for prevent and treatment of cardiovascular disease and cerebrovascular disease, to attain the aim of reducing times of administration and side-effects, briviscapine sustained-release capsules dissolved in intestines were prepared through the technique of sustained-release microgranules. The HPLC method was developed to control the quality of sustained-release pellets.
The plasma concentrations and pharmacokinetic parameters compared after vein administration of breviscapine and oral administration of normal tablet and sustained-release capsules dissolved in intestines respectively. The results showed that plasma concentration-time profile after coral administration of normal tablet and sustained-released capsules were both fitted in with two compartment model. The absolute bioavailability of sustained-release capsules dissoloved in intestine were calculated to be 76.79% and that of
common tablets were 50.38%. Compared with the normal tablet, the eliminative speed of capsules reduced more slowly. The relative bioavailability was 152.95%. The result showed that breviscapine sustained-release capsules dissolved in intestines was not bioequivalent with the reference preparation (normal tablet). At the same time, metabolites of breviscapine were researched. The breviscapine was incubated in dogs' gastric juice and intestinal juice respectively. The sample was examined by means of HPLC/MS and found the main metabolic product. Two-phase hydrolysis method was used to determined the hydrolysates of breviscapine in vitro. The two kind of product got from different method were the same. The decomposed course of breviscapine in vivo was consistent with that in vitro.
引文
[1] 甄志亚主编.中国医学史.北京:人民卫生出版社,1991
[2] 中国药材公司编著.中国中药资源.北京:中国医药科技出版社,1995
[3] 王宝琴主编.中成药质量标准与标准物质研究.北京:中国医药科技出版社,1991:464-468
[4] 陈可翼.中医中药研究的现状与展望.中国中医药科技,1997,4(1):1-3
[5] 李连达,靖雨珍.中药现代化与走向世界.中国中医药信息杂志,1997,4(11):3-5
[6] 郭涛.传统中药向现代化中药转变的思路.中国中药杂志,1998,23(8):508-510
[7] 孙瑞元,宋建国.以药效指标进行中药药动学研究.中药药理与临床,1988,4(1):3-6
[8] 李成韶,杜以兰.以药效指标进行中药药动学研究的思路和体会,1988,4(1):8-10
[9] 周丽玲,李瑞.青藤碱制剂药动学试验中药物积累法与血药浓度法相关性研究.中成药,1996,18(9):1-3
[10] 张志蓉,胡晓颖,蒋大义,等.银黄冲剂中黄芩苷在家兔体内的代谢动力学研究.中成药,1996,18(6):1-4
[11] 周艳文,李梅,赵素荣.丁公藤注射液在家兔体内的药代动力学研究.中国中药杂志,1997,22(3):179-181
[12] 王淑丽,陈济民.苏子油乳剂亚麻酸的药物动力学与生物利用度.沈阳药科大学学报,1998,15(3):160-163
[13] 郭济贤,潘伟坚,杨瑞萍,等.中药灯盏花及其同属部分植物的研究概况.中成药研究,1987,9(8):31-33
[14] 云南省药物研究所.灯盏细辛化学成分的研究(第一报).中草药通讯,1976,7(11):11-13
[15] 宫碧琴.治疗瘫痪新药灯盏花素鉴定会在昆明召开.中草药,1980,11(10):480-483
[16] 胡昌奇,张德成,华云,等.灯盏花化学成分的研究Ⅱ.中草药,1985,16(10):12-14
[17] 张人伟,张元玲,王杰生,等.灯盏花黄酮类成分的分离鉴定.中草药,1988,19(5):7-11
[18] Yue JM Lin ZW Sun HD et al, A Sesquiterpene and other constituents from Erigeron Breviscapuls[J]. Phytochemistry, 1994,36(3):717-722
[19] Yue JM Lin ZW Sun HD. A New Caffeoyl Conjugate from Erigeron Breviscapus. Chinese Chemical Letters[J], 1994, 6(3): 225-260
[20] 岳建民,赵勤实,林中文,等.灯盏细辛中酚类化合物的研究.植物学报,2000,42(3):311-315
[21] Zhang WD Kong DY Li HT et al, A New Glycoside from Erigeron Breviscapus. Chinese Chemical Letters[J], 1998,10(2): 125-128
[22] 张卫东,孔德云,李惠庭,等.灯盏花的化学成分研究(Ⅱ).中国医药工业杂志,1998,29(12):554-556
[13] 张卫东,陈万生,孔德云,李惠庭,等.中药灯盏细辛化学成分的研究(Ⅰ).第二军医大学学报,2000,21(2):143-147
[14] 张卫东,陈万生,孔德云,李惠庭,等。中药灯盏细辛化学成分的研究(Ⅱ).第二军医大学学报,2000,21(10):914-918
[25] 灯盏花素片质量标准.卫生部中药标准,WS3-B-2516-97
[26] 灯盏花素注射液质量标准.卫生部中药标准,WS3-B-3822-98
[27] 杨晖.灯盏细辛胶囊的检测方法.中成药,1997,19(7):37-38
[28] 李守拙,李沈明,范书铎,等.黄芩茎中野黄芩苷含量测定.中草药,2000,31,(12):910-913
[29] 华捷,陈超,许桢灿.HPLC法测定灯盏花素片含量.海峡药学,2002,14(1):30-32
[30] 何永志,刘新元.灯盏花滴丸含量测定研究.中草药,2002,33(6):519-521
[31] 杨文宇,张艺,段俊国.高效液相色谱法测定灯盏细辛中灯盏乙素的含量.成都中医药大学学报,2001,24(3):37-39
[32] 张世轩,牛玉娟,吕浩然,鞠秀兰.HPLC法测定灯盏花索注射液中野黄芩苷.中成药,2002,24(2):95
[33] 饶毅,魏惠珍,王义明,罗国安.高效毛细管电泳法测定灯盏花素系列制剂的含量.中成药,2002,24(8):584
[34] 曲峻,王义明,罗国安,等.LC/MS/MS的多反应监测方法定量测定灯盏乙素.药学学报,2000,35(2):139-141
[35] 帅杰,董为伟.PKC抑制剂灯盏花素对缺血/再灌流脑损害的作用研究.中国药理学通报,1998,14(1):75-77
[36] 陈一岳,王胜涛,曾文珊,等.灯盏花素对大鼠主动脉肌环的松弛作用.中药新药与临床药理,1994,5(2):15-19
[37] 沈志强,吴兰欧,陈植和,等.灯盏细辛有效部位对中性粒白细胞与血小板之间粘附和聚集的影响.天然产物研究与开发,2000,13(1):60-63
[38] 李文凡,白娟,王立荣.灯盏花对实验性肝纤维化大鼠血清和肝匀浆中透明质酸和层粘蛋白含量的影响.兰州医学院学报,1999,25(6):28-30
[39] 贾莉君,刘忠浩,罗学港.青光康注射液对急性实验性高眼压大鼠视网膜节细胞代谢的作用.中华眼科杂志,1995,13(2):129-132
[40] 岳建民.二咖啡酰氧基奎宁酸在制药中的应用.中国专利:1136434,1996-11-26
[41] 孙汉董.焦袂康酸及其葡萄苷(飞蓬苷)在制药中的应用.中国专利:1136435,1996-11-26
[42] 李铁军,郑杰民,等.灯盏花中咖啡酰化合物对溶血磷脂酰胆碱致牛脑微血管内皮细胞损伤的保护作用.第二军医大学学报,2001,22(3):255-258
[43] 李卫东,李江桃,龙建新.灯盏花注射液治疗脑梗塞的临床与实验研究.实用医学杂志,1998,11(2):10-14
[44] 闫农,刘卓,张树新,等.云南灯盏花注射液治疗缺血性心脏病120例临床研究.中国急救医
学,1997,17(6):26-29
[45] 马春蓉.灯盏花注射液治疗高粘滞综合症51例疗效观察.川北医学院学报,1999,14(1):70
[46] 张杰,王兰琼,李永平.灯盏细辛及其相关产品应用近况.中国民族民间医药杂志,2001,51:197-201
[47] 蒋学华,李素华,兰轲,等.灯盏华素在家犬体内的药代动力学.药学学报,2003,38(5):371-373
[48] 张铁军.中药新药研究的科研思路初探.中草药,1999,30(增):28-30
[49] 盛宝英,王海超,杨立波,等.灯盏花素治疗急性脑梗死的研究.黑龙江医药科学,2001,24(3):45-46
[50] 谢淑英,朱凤真,张锐,等.灯盏花素治疗心绞痛45例.辽宁中医杂志,1997,24(1):21-22
[51] 柳玉瑾.灯盏花素片治疗老年痴呆35例临床观察.辽宁中医杂志,1997,24(6):263-264
[52] 张品雅.灯盏花素片治疗中风后遗症32例临床分析.中成药,1998,20(1):36-37.
[53] 杨汝德.生物药物分析与检验.广州:华南理工大学出版社,2002
[54] 何华,曾经泽.生物药物分析.北京:化学工业出版社,2003
[55] 中国药典(一部).2000年
[56] 魏树礼主编.生物药剂学与药物动力学.北京:北京医科大学-中国协和医科大学联合出版社,1997
[57] Laurene X Y, Lipka E, Crison J R. Transport approaches to the biopharmaceutical design of oral drug delivery system: prediction of intestinal absorption. Adv Drug Del Rev. 1996,19(3):359-369
[58] Morrison R A, Kpipalani K J, Marino A M. Intestinal absorption of captopril and the thioester analogs in rats and dogs. Biopharm Drug Dispos, 1997,18(2):25-39
[59] Matsuda K, Yuasa H, Watanake J. Fractinal absorption of L-carnitine after oral administration in rats: Bio Pharm Bull, 1998, 21(7): 752-755
[60] L 拉赫曼,HA 利伯曼,JL 卡凡希主编.北京医学院药学系译.工艺药剂学理论与实践.北京:化学工业出版社,1984
[61] 洪诤,邓海星.黄酮类药物的药代动力学研究近况.中药药理与临床,1998,14(6):46-49
[62] 丁江生,张均寿.灯盏花素大鼠小肠吸收特性的研究.中国药科大学学报,2003,34(1):65-69
[63] 肖崇厚主编.中药化学.上海:上海科学技术出版社,1997
[64] 车庆明,黄立新,李艳梅,等.黄芩苷的药物代谢产物研究.中国中药杂志,2001,26(11):89-91
[65] Y S Zhou, Q M Che, S X Xul. Metabolites of Baicalin in Human Urine. Pharmazic, 2000, 55(8): 626-629
[66] 钟大放.药物代谢.北京:中国医药科技出版社,1996
[2] 中国药材公司编著.中国中药资源.北京:中国医药科技出版社,1995
[3] 王宝琴主编.中成药质量标准与标准物质研究.北京:中国医药科技出版社,1991:464-468
[4] 陈可翼.中医中药研究的现状与展望.中国中医药科技,1997,4(1):1-3
[5] 李连达,靖雨珍.中药现代化与走向世界.中国中医药信息杂志,1997,4(11):3-5
[6] 郭涛.传统中药向现代化中药转变的思路.中国中药杂志,1998,23(8):508-510
[7] 孙瑞元,宋建国.以药效指标进行中药药动学研究.中药药理与临床,1988,4(1):3-6
[8] 李成韶,杜以兰.以药效指标进行中药药动学研究的思路和体会,1988,4(1):8-10
[9] 周丽玲,李瑞.青藤碱制剂药动学试验中药物积累法与血药浓度法相关性研究.中成药,1996,18(9):1-3
[10] 张志蓉,胡晓颖,蒋大义,等.银黄冲剂中黄芩苷在家兔体内的代谢动力学研究.中成药,1996,18(6):1-4
[11] 周艳文,李梅,赵素荣.丁公藤注射液在家兔体内的药代动力学研究.中国中药杂志,1997,22(3):179-181
[12] 王淑丽,陈济民.苏子油乳剂亚麻酸的药物动力学与生物利用度.沈阳药科大学学报,1998,15(3):160-163
[13] 郭济贤,潘伟坚,杨瑞萍,等.中药灯盏花及其同属部分植物的研究概况.中成药研究,1987,9(8):31-33
[14] 云南省药物研究所.灯盏细辛化学成分的研究(第一报).中草药通讯,1976,7(11):11-13
[15] 宫碧琴.治疗瘫痪新药灯盏花素鉴定会在昆明召开.中草药,1980,11(10):480-483
[16] 胡昌奇,张德成,华云,等.灯盏花化学成分的研究Ⅱ.中草药,1985,16(10):12-14
[17] 张人伟,张元玲,王杰生,等.灯盏花黄酮类成分的分离鉴定.中草药,1988,19(5):7-11
[18] Yue JM Lin ZW Sun HD et al, A Sesquiterpene and other constituents from Erigeron Breviscapuls[J]. Phytochemistry, 1994,36(3):717-722
[19] Yue JM Lin ZW Sun HD. A New Caffeoyl Conjugate from Erigeron Breviscapus. Chinese Chemical Letters[J], 1994, 6(3): 225-260
[20] 岳建民,赵勤实,林中文,等.灯盏细辛中酚类化合物的研究.植物学报,2000,42(3):311-315
[21] Zhang WD Kong DY Li HT et al, A New Glycoside from Erigeron Breviscapus. Chinese Chemical Letters[J], 1998,10(2): 125-128
[22] 张卫东,孔德云,李惠庭,等.灯盏花的化学成分研究(Ⅱ).中国医药工业杂志,1998,29(12):554-556
[13] 张卫东,陈万生,孔德云,李惠庭,等.中药灯盏细辛化学成分的研究(Ⅰ).第二军医大学学报,2000,21(2):143-147
[14] 张卫东,陈万生,孔德云,李惠庭,等。中药灯盏细辛化学成分的研究(Ⅱ).第二军医大学学报,2000,21(10):914-918
[25] 灯盏花素片质量标准.卫生部中药标准,WS3-B-2516-97
[26] 灯盏花素注射液质量标准.卫生部中药标准,WS3-B-3822-98
[27] 杨晖.灯盏细辛胶囊的检测方法.中成药,1997,19(7):37-38
[28] 李守拙,李沈明,范书铎,等.黄芩茎中野黄芩苷含量测定.中草药,2000,31,(12):910-913
[29] 华捷,陈超,许桢灿.HPLC法测定灯盏花素片含量.海峡药学,2002,14(1):30-32
[30] 何永志,刘新元.灯盏花滴丸含量测定研究.中草药,2002,33(6):519-521
[31] 杨文宇,张艺,段俊国.高效液相色谱法测定灯盏细辛中灯盏乙素的含量.成都中医药大学学报,2001,24(3):37-39
[32] 张世轩,牛玉娟,吕浩然,鞠秀兰.HPLC法测定灯盏花索注射液中野黄芩苷.中成药,2002,24(2):95
[33] 饶毅,魏惠珍,王义明,罗国安.高效毛细管电泳法测定灯盏花素系列制剂的含量.中成药,2002,24(8):584
[34] 曲峻,王义明,罗国安,等.LC/MS/MS的多反应监测方法定量测定灯盏乙素.药学学报,2000,35(2):139-141
[35] 帅杰,董为伟.PKC抑制剂灯盏花素对缺血/再灌流脑损害的作用研究.中国药理学通报,1998,14(1):75-77
[36] 陈一岳,王胜涛,曾文珊,等.灯盏花素对大鼠主动脉肌环的松弛作用.中药新药与临床药理,1994,5(2):15-19
[37] 沈志强,吴兰欧,陈植和,等.灯盏细辛有效部位对中性粒白细胞与血小板之间粘附和聚集的影响.天然产物研究与开发,2000,13(1):60-63
[38] 李文凡,白娟,王立荣.灯盏花对实验性肝纤维化大鼠血清和肝匀浆中透明质酸和层粘蛋白含量的影响.兰州医学院学报,1999,25(6):28-30
[39] 贾莉君,刘忠浩,罗学港.青光康注射液对急性实验性高眼压大鼠视网膜节细胞代谢的作用.中华眼科杂志,1995,13(2):129-132
[40] 岳建民.二咖啡酰氧基奎宁酸在制药中的应用.中国专利:1136434,1996-11-26
[41] 孙汉董.焦袂康酸及其葡萄苷(飞蓬苷)在制药中的应用.中国专利:1136435,1996-11-26
[42] 李铁军,郑杰民,等.灯盏花中咖啡酰化合物对溶血磷脂酰胆碱致牛脑微血管内皮细胞损伤的保护作用.第二军医大学学报,2001,22(3):255-258
[43] 李卫东,李江桃,龙建新.灯盏花注射液治疗脑梗塞的临床与实验研究.实用医学杂志,1998,11(2):10-14
[44] 闫农,刘卓,张树新,等.云南灯盏花注射液治疗缺血性心脏病120例临床研究.中国急救医
学,1997,17(6):26-29
[45] 马春蓉.灯盏花注射液治疗高粘滞综合症51例疗效观察.川北医学院学报,1999,14(1):70
[46] 张杰,王兰琼,李永平.灯盏细辛及其相关产品应用近况.中国民族民间医药杂志,2001,51:197-201
[47] 蒋学华,李素华,兰轲,等.灯盏华素在家犬体内的药代动力学.药学学报,2003,38(5):371-373
[48] 张铁军.中药新药研究的科研思路初探.中草药,1999,30(增):28-30
[49] 盛宝英,王海超,杨立波,等.灯盏花素治疗急性脑梗死的研究.黑龙江医药科学,2001,24(3):45-46
[50] 谢淑英,朱凤真,张锐,等.灯盏花素治疗心绞痛45例.辽宁中医杂志,1997,24(1):21-22
[51] 柳玉瑾.灯盏花素片治疗老年痴呆35例临床观察.辽宁中医杂志,1997,24(6):263-264
[52] 张品雅.灯盏花素片治疗中风后遗症32例临床分析.中成药,1998,20(1):36-37.
[53] 杨汝德.生物药物分析与检验.广州:华南理工大学出版社,2002
[54] 何华,曾经泽.生物药物分析.北京:化学工业出版社,2003
[55] 中国药典(一部).2000年
[56] 魏树礼主编.生物药剂学与药物动力学.北京:北京医科大学-中国协和医科大学联合出版社,1997
[57] Laurene X Y, Lipka E, Crison J R. Transport approaches to the biopharmaceutical design of oral drug delivery system: prediction of intestinal absorption. Adv Drug Del Rev. 1996,19(3):359-369
[58] Morrison R A, Kpipalani K J, Marino A M. Intestinal absorption of captopril and the thioester analogs in rats and dogs. Biopharm Drug Dispos, 1997,18(2):25-39
[59] Matsuda K, Yuasa H, Watanake J. Fractinal absorption of L-carnitine after oral administration in rats: Bio Pharm Bull, 1998, 21(7): 752-755
[60] L 拉赫曼,HA 利伯曼,JL 卡凡希主编.北京医学院药学系译.工艺药剂学理论与实践.北京:化学工业出版社,1984
[61] 洪诤,邓海星.黄酮类药物的药代动力学研究近况.中药药理与临床,1998,14(6):46-49
[62] 丁江生,张均寿.灯盏花素大鼠小肠吸收特性的研究.中国药科大学学报,2003,34(1):65-69
[63] 肖崇厚主编.中药化学.上海:上海科学技术出版社,1997
[64] 车庆明,黄立新,李艳梅,等.黄芩苷的药物代谢产物研究.中国中药杂志,2001,26(11):89-91
[65] Y S Zhou, Q M Che, S X Xul. Metabolites of Baicalin in Human Urine. Pharmazic, 2000, 55(8): 626-629
[66] 钟大放.药物代谢.北京:中国医药科技出版社,1996