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1.
目的采用快速膜乳化-溶剂挥发法制备不含载体辅料的阿立哌唑微粒,并对其体外释药行为进行评价。方法采用快速膜乳化-溶剂挥发法制备阿立哌唑微粒,将主药于室温条件下超声溶解于有机溶剂中作为油相。将聚乙烯醇(PVA)于磁力搅拌且加热的条件下溶解于去离子水中,并趁热用0.45 μm的微孔滤膜真空抽滤,得续滤液,作为水相。油相与水相经磁力搅拌混合均匀后得初乳液,将初乳液倒入快速不锈钢膜乳化装置,氮气加压,过膜,收集乳液。将乳液与固化液混合后固化至无有机溶剂气味,离心洗涤,冷冻干燥即得到阿立哌唑微粒冻干粉。以微粒粒径、跨距及表观形态为指标,采用单因素考察法对有机溶剂、水相PVA浓度、阿立哌唑质量浓度、油水相体积比、固化液pH值、过膜次数、固化方式进行考察,并初步确定最优制备条件;采用直接释药法测定并比较阿立哌唑原料药与微粒在不同时间点的累积释放率,并对其释放行为进行数学模型拟合。结果经过单因素考察,确定阿立哌唑微粒的制备工艺条件为:有机溶剂二氯甲烷,水相PVA浓度3%,药物质量浓度7 mg/mL,油水相体积比1:1,固化液3% PVA溶液(pH 8.5),四级串联不锈钢膜乳化器过膜1次,机械搅拌固化。阿立哌唑微粒平均D10、D50、D90及跨距分别为2.03、4.38、8.09 μm、1.39;扫描电镜下呈现较为均匀的薄片状;差示扫描量热法显示其结晶程度降低;平均药物质量分数为99.27%。阿立哌唑微粒在48 h时累积释放率可达100.17%,体外释放符合Logistic方程,而原料药在48 h时仅释放47.17%,释放符合一级方程。结论快速膜乳化法可用于提高难溶性药物的溶出速度,具有广阔的应用前景。 相似文献
2.
目的 制备聚乙烯醇(PVA)/海藻酸钠(SA)-聚乙烯醇(PVA)/壳聚糖(CS)双层(PAPCS)水凝胶膜伤口敷料,并进行质量评价。方法 将PVA与SA以质量比2∶1混合,配制PVA/SA混合溶液;将PVA与CS分别以质量比1∶1、2∶1、3∶1、4∶1、5∶1混合,配制不同质量比的PVA/CS混合溶液;采用涂布法制备PAPCS双层水凝胶膜伤口敷料。通过水蒸气透过率、溶胀性能、保水性、力学性能、体外凝血性能和血液相容性考察对水凝胶膜的性能进行评价、筛选PVA与CS质量比;通过傅里叶变换红外光谱检测(FTIR)和扫描电子显微镜(SEM)对PAPCS水凝胶膜的结构和形貌进行表征;通过抑菌实验比较PAPCS以及PAPCS复合载碘交联环糊精金属有机骨架(I2@COF@PAPCS)的体外抗菌性能。结果 PVA与CS质量比为2∶1时,PAPCS水凝胶膜综合性能较好。PAPCS水凝胶膜为多孔结构,具有良好的溶胀性能、保水性以及力学性能;PAPCS水凝胶膜的水蒸气透过率为(2 643.76±91.62)g·m-2·d-1,接近理想范围;与PVA/SA相比,PAPCS的凝血指数显著降低(P<0.01),为(72.93±3.58)%,溶血率小于5%,具有促进血液凝固的能力且血液相容性良好;与PVA/SA相比,PAPCS对于金黄色葡萄球菌、大肠埃希菌均有明显抑制作用,抑菌圈直径分别为(11.89±0.22)、(12.28±0.25) mm;I2@COF@PAPCS对金黄色葡萄球菌、大肠埃希菌的抑菌圈直径分别为(21.95±1.47)、(18.89±0.81)mm,抑菌效果显著优于PAPCS(P<0.001)。结论 采用涂布法可成功制备双层PAPCS水凝胶膜敷料,其各项性能指标良好,具有明显的凝血、抑菌效果,与I2@COF复合使用,抑菌作用进一步增强。 相似文献
3.
目的 制备托伐普坦纳米结构脂质载体(Tol-NLCs),以提高托伐普坦(Tol)的口服生物利用度。方法 根据溶解度对辅料进行筛选,包括固体脂质(双硬脂酸甘油酯、山嵛酸甘油酯、聚乙二醇-8山嵛酸甘油酯、单硬脂酸甘油酯和单亚油酸甘油酯)、液体脂质(油酸聚乙二醇甘油酯、单油酸甘油酯、月桂酸聚乙二醇甘油酯和单辛酸丙二醇酯)和表面活性剂(聚山梨酯80、聚氧乙烯蓖麻油、聚乙二醇-15羟基硬脂酸酯和泊洛沙姆188),采用乳化超声-低温固化法制备TolNLCs,并使用Box-Behankn效应面法优化处方;分别采用电镜(TEM)观察、粒径分布及Zeta电位测定、差示扫描量热法(DSC)对制备的Tol-NLCs进行表征,同时比较Tol原料药和Tol-NLCs体外药物释放特点、跨膜转运特征;比较Tol混悬液和Tol-NLCs经大鼠ig给药后的体内药动学特征。结果 根据溶解度确定以山嵛酸甘油酯作为固体脂质,单油酸甘油酯作为液体脂质,聚乙二醇-15羟基硬脂酸酯作为表面活性剂,通过优化得到Tol-NLCs的最佳处方:总脂质质量浓度为40.0 mg·mL-1,表面活性剂质量浓度为25.0 mg·mL-1,超声时间为6 min。在透射电镜下可观察到制备的Tol-NLCs呈类球状,分布均匀;Tol-NLCs的平均粒径为(106.2±14.7)nm,PDI为(0.196±0.004),Zeta电位为(-26.6±0.6)mV;药物在Tol-NLCs中以非结晶形式存在。Tol-NLCs在pH 6.8磷酸盐缓冲液中表现为前期药物释放较快,后期药物释放平缓。Caco-2细胞跨膜转运结果显示,Tol-NLCs的Papp(AP→BL)值为(11.16±0.58)×10-6 cm·s-1,Papp(BL→AP)值为(4.51±0.46)×10-6 cm·s-1,与Tol溶液相比,Papp(AP→BL)表现出明显增加趋势,Papp(BL→AP)表现出明显降低趋势,说明Tol包裹在NLCs中促进了药物吸收,抑制了P-糖蛋白(P-gp)的外排作用。与Tol混悬液相比,大鼠ig Tol-NLCs后,Tol生物利用度提高了2.5倍。结论 按优化处方制备的Tol-NLCs,能够显著提高药物的生物利用度。 相似文献
4.
目的 制备他达拉非片并考察其体内外释药特性。方法 以溶出度为评价指标,筛选他达拉非片各辅料用量及包衣增重。用相似因子(f2)法比较自制制剂与参比制剂在0.5% SDS溶液、含0.5% SDS的0.1 mol/L的盐酸溶液、含0.5% SDS的pH 4.5醋酸钠缓冲液、含0.5% SDS的pH 6.8磷酸盐缓冲液中溶出曲线的相似性。比较二者在Beagle犬体内的药动学特征。结果 他达拉非片处方为他达拉非20 mg、乳糖50M 227.625 mg、羟丙基纤维素L 10.5 mg、交联羧甲基纤维素钠19.6 mg、SDS 0.525 mg、微晶纤维素M102 70 mg、硬脂酸镁1.75 mg,包衣增质量范围2%~4%。自制与参比制剂在4种溶出介质中的f2均大于65,二者体外溶出行为相似。2种制剂在Beagle体内的药动学参数AUC0~t、Cmax、tmax均无显著性差异,自制他达拉非片的相对生物利用度为(101.67±8.99)%。结论 成功制备他达拉非片,其体外溶出和体内药动学行为与参比制剂相似。 相似文献
5.
氟伐他汀钠缓释片的制备及其Beagle犬体内药动学研究 总被引:1,自引:1,他引:0
目的 制备氟伐他汀钠缓释片,进行体外释放特性以及Beagle犬体内药动学研究。方法 以羟丙甲纤维素为缓释材料制备氟伐他汀钠缓释片,测定其体外释放度和Beagle犬口服单剂量及多剂量后的血药浓度,推算药动学参数。结果 制备的氟伐他汀钠缓释片体外释放行为相似,口服单剂量和多剂量药动学参数Cmax分别为(3 304.23±1 043.30)μg·L-1和(3 760.86±754.77)μg·L-1,T1/2分别为(7.37±4.09)h和(6.04±2.63)h,AUC(0-t)分别为(15 052.91±3 878.01)μg·L-1和(15 374.91±2 712.20)μg·h·L-1。结论 制备的氟伐他汀钠缓释片具有较明显的缓释效果,多次给药未出现明显的蓄积现象,表现出良好的安全性。 相似文献
6.
盐酸阿霉素聚乳酸纳米粒的制备及大鼠体内药动学研究 总被引:1,自引:1,他引:0
目的 优化盐酸阿霉素聚乳酸纳米粒(DOX-PLA-NPs)的制备工艺,并对其理化性质、体外释放及大鼠体内药动学进行研究。方法 采用改良的复乳-溶剂挥发法制备DOX-PLA-NPs,正交设计优化其处方工艺,对其纳米粒形态、粒径、Zeta电位、包封率与载药量进行测定。以DOX原药为对照组,考察DOX-PLA-NPs的体外释药特性及大鼠尾静脉给药后的体内药动学参数。结果 DOX-PLA-NPs外观圆整,平均粒径为(125.67±3.80) nm、Zeta电位为(-35.97±1.58) mV、包封率和载药量分别为(81.23±1.46)%,(10.29±0.63)%。体外释放结果显示,DOX经纳米粒包裹后,具明显的缓释作用。DOX原药和纳米粒的体内药动学过程均符合开放式二室模型,t1/2β分别为(1.15±0.175) h、(6.43±2.12) h,CL分别为(174.76±47.22) h·L-1、(30.68±11.86) h·L-1,AUC0→t分别为(6.01±1.61)μg·h·L-1、(36.04±13.72)μg·h·L-1。结论 制备的盐酸阿霉素聚乳酸纳米粒粒径较小、包封率较高,具明显的缓释作用,并能提高药物的生物利用度。 相似文献
7.
摘 要 目的: 建立他达拉非片含量测定及有关物质检查的方法。 方法: 采用高效液相色谱法。色谱柱:安捷伦ZORBAX Eclipse XDB C8(250 mm×4.6 mm,5 μm) ;流动相:0.1% 三氟乙酸溶液-乙腈(65∶35);流速:1.0 ml·min-1;柱温:35℃;检测波长:285 nm,进样量20 μl。结果:在选定的色谱条件下,主成分与各杂质峰分离度良好。他达拉非质量浓度在20.13~201.30 μg·ml-1范围内与峰面积有良好的线性关系(r=0.999 3);平均回收率为99.5%(RSD=1.1%,n=9) ;检出限为0.6 ng,定量限为2 ng。结论: 该方法专属性强、灵敏度高,可用于他达拉非片含量和有关物质测定。 相似文献
8.
目的 制备左乙拉西坦缓释片,进行体外释放特性以及Beagle犬体内药动学研究。方法 按照筛选处方制备左乙拉西坦缓释片,以市售左乙拉西坦缓释片(Keppra-XR)为参比制剂,采用相似因子(f2)法进行体外释放行为相似度评价;并将自制左乙拉西坦缓释片与市售普通片进行Beagle犬体内药动学参数比较。结果 自制左乙拉西坦缓释片与市售左乙拉西坦缓释片体外释放行为相似。市售左乙拉西坦普通片和自制左乙拉西坦缓释片的药动学参数Tmax分别为(1.75±0.50)和(5.50±1.00)h,Cmax分别为(30.33±2.00)和(17.29±3.56)mg·L-1,AUC0-t分别为(186.88±8.83)和(202.50±34.20)mg·L-1·h。结论 自制的左乙拉西坦缓释片具有缓释效果。 相似文献
9.
目的 以聚乳酸-羟基乙酸共聚物(PLGA)作为纳米制剂载体材料将葫芦素B制备成纳米粒,并考察其对HepG2肝癌细胞的抑制效果。方法 使用乳化溶剂蒸发法制备葫芦素B-PLGA载药纳米粒,以PLGA浓度(X1)、PVA浓度(X2)和药物浓度(X3)作为考察因素,以载药纳米粒的粒径大小(Y1)和包封率(Y2)作为评价指标,应用中心复合设计-效应面法优化葫芦素B-PLGA载药纳米粒处方;测定了纳米粒的粒径分布和Zeta电位值,通过透射电镜观察其微观形态,并考察了葫芦素B-PLGA载药纳米粒的体外药物释放特性;比较了葫芦素B与葫芦素B-PLGA载药纳米粒对HepG2肝癌细胞的抑制效果。结果 葫芦素B-PLGA载药纳米粒的最优处方组成为:PLGA浓度为9.0%,PVA浓度为2.0%,药物浓度为4.5%,制备的纳米粒粒径为(145.4±15.8) nm,Zeta电位值为(-7.6±0.8) mV;透射电镜下可观察到纳米粒表面光滑,分布均匀;葫芦素B-PLGA载药纳米粒释药前期出现突释,后期平缓,48 h药物释放达到86%;葫芦素B-PLGA载药纳米粒对HepG2肝癌细胞的抑制作用显著高于葫芦素B。结论 葫芦素B-PLGA载药纳米粒可延缓药物释放,提高对HepG2肝癌细胞的抑制活性,为进一步临床研究奠定实验基础。 相似文献
10.
目的 建立高效液相色谱法测定依达拉奉注射液的有关物质。方法 采用Agilent SB-C18(4.6 mm×250 mm,5 μm)色谱柱,流动相A为0.05 mol·L-1磷酸二氢钾溶液(用三乙胺调节pH值至7.0),流动相B为甲醇,梯度洗脱,流速为1.0 mL﹒min-1,检测波长为243 nm,柱温30 ℃。结果 依达拉奉及各杂质均能有效分离,在相应的浓度范围峰面积与浓度呈良好的线性关系,相关系数均大于0.999,平均回收率在95%~105%范围内。结论 该方法专属性强,简便可靠、灵敏、准确,适用于依达拉奉注射液中的有关物质的测定。 相似文献
11.
New 2,6-piperidinediones 2a–g and 4a–d were prepared by initial condensation of aromatic aldehydes or cycloalkanones with cyanoacetamide to give α-cyanocinnamides
la–g or cycloalkylidenes 3a,b which underwent Michae1 addition with ethyl cyanoacetate or diethylmalonate. Compounds 4a–d were alkylated by various alkyl halides to produce the N-alkylated 2,6-piperidinedione derivatives 5a–m.
Some new selected compounds 2a–c,f, 4a–d & 5e,h,j were pharmacologically evaluated for potential anticonvulsant, sedative and analgesic activities. These compounds exhibited
significant anticonvulsant and analgesic effects after a single I.P. administration 100 mg/kg b.wt. . On the other hand all
the investigated compounds induced hypnotic activity and prolonged the phenobarbital sodium- induced sleep as compared with
the control group and the most potent compound was found to be 2f. 相似文献
12.
EFFECT OF POLICOSANOL SUCCESSIVE DOSE INCREASES ON PLATELET AGGREGATION IN HEALTHY VOLUNTEERS 《Pharmacological research》1996,34(5-6)
Policosanol is a cholesterol-lowering drug with hypocholesterolemic effects demonstrated in experimental models, healthy volunteers and type II hypercholesterolemic patients. In addition, antiplatelet effects of policosanol have been shown in experimental models and healthy volunteers. The effect of successively increasing doses of policosanol on platelet aggregation was investigated in a randomized, placebo-controlled, double-blind study conducted in 37 healthy volunteers. The volunteers were on a placebo-baseline period (two tablets per day) for 7 days and thereafter they received randomly, under double-blind conditions, placebo or policosanol (10mgday−1) for 7 days. After this period dosage was doubled to 20mgday−1for the next 7 days and then again doubled to 40mgday−1, while the control group received placebo tablets all the time. Platelet aggregation as well as coagulation time was measured at baseline and after each dosing step. Results showed that antiplatelet effects of policosanol were successfully enhanced throughout the study, thus suggesting a dose-dependent relationship. No significant effect was reached during the first dosing period, but significant reductions of epinephrine and ADP-induced platelet aggregation were observed after the second one. Finally, a significant inhibition of platelet aggregation induced by all the agonists was observed at the last dosing step. Coagulation time remained unchanged during the trial. 相似文献
13.
目的 建立鼻渊净胶囊的高效液相色谱(HPLC)指纹图谱。方法 采用Agilent SB-C18(4.6 mm×250 mm,5 μm)色谱柱,乙腈-水为流动相、以1.0 ml/min流速行梯度洗脱,检测波长210 nm,柱温30 ℃,洗脱时间为80 min。采用中药色谱指纹图谱相似度评价系统(2004A版)对检测出色谱进行指纹图谱相似度评价。结果 建立了鼻渊净胶囊的HPLC指纹图谱,确定了20个共有峰,15个峰归属到各药材,其中5个峰确认了化学成分;10批样品的指纹图谱的整体相似度与对照图谱比较,均在90%以上。结论 所建立的鼻渊净胶囊指纹图谱有助于从整体上控制该制剂的质量。 相似文献
14.
NEURAMIDE STIMULATES ADRENOCORTICOTROPIN BUT NOT PROLACTIN RELEASE FROM RAT PITUITARY 《Pharmacological research》1996,34(5-6)
Neuramide (NMD), a substance found in crude preparations of porcine stomach extract, is a viral inhibitor that also has putative immunostimulatory effects. The effects of NMD on stress-hormone (ACTH and prolactin—PRL) release were assessed inin vivoandin vitrostudies. In the former, blood levels of corticosterone and PRL were measured in NMD-treated male rats.In vitroexperiments were performed to evaluate the effects of NMD and three of its fractions (obtained with high performance liquid chromatography) on ACTH and PRL release from perfused rat pituitary slices. NMD increased plasma corticosterone levelsin vivoand produced dose-dependent increases inin vitropituitary release of ACTH. No effects on PRL secretion were observedin vivoorin vitro. The stimulatory effects on ACTH release were caused by the NMD fraction with a molecular weight of >5000<10000Da. 相似文献
15.
In this study, the antibiotic susceptibilities to tigecycline and tetracycline of 35 selected Bacteroides fragilis group strains were determined by Etest, and the presence of tetQ, tetX, tetX1 and ermF genes was investigated by polymerase chain reaction (PCR). tetQ was detected in all 12 B. fragilis group isolates (100%) exhibiting elevated tigecycline minimum inhibitory concentrations (MICs) (≥8 μg/mL) as well as the 8 strains (100%) with a tigecycline MIC of 4 μg/mL, whilst tetX and tetX1 were present in 15% and 75% of these strains, respectively. All of these strains were fully resistant to tetracycline (MIC ≥ 16 μg/mL). On the other hand, amongst the group of strains with tigecycline MICs < 4 μg/mL (15 isolates), tetQ, tetX and tetX1 were found less frequently (73.3%, 13.3% and 46.7%, respectively). All but two strains harbouring the tetQ gene in this group were non-susceptible to tetracycline, with a MIC > 4 μg/mL. These data suggest that in most cases tigecycline overcomes the tetracycline resistance mechanisms frequently observed in Bacteroides strains. However, the presence of tetX and tetX1 genes in some of the strains exhibiting elevated MICs for tigecycline draws attention to the possible development and spread of resistance to this antibiotic agent amongst Bacteroides strains. The common occurrence of ermF, tetX, tetX1 and tetQ genes together predicted the presence of the CTnDOT-like Bacteroides conjugative transposon in this collection of Bacteroides strains. 相似文献
16.
《Pharmacological research》1996,34(5-6)
Inhibitory effects of the class III antiarrhythmic compound
/
-sotalol on acetylcholinesterase (AChE; EC 3.1.1.7) isoenzymes of both erythrocytes and the human caudate nucleus and on serum cholinesterase (ChE; EC 3.1.1.8) were studiedin vitrousing a spectrophotometric kinetic assay with acetylthiocholine (ASCh) as substrate. Sotalol concentrations in the assays varied from 0.32 to 3.2m
. All isoenzymes studied were inhibited by
/
-sotalol in a reversible and concentration-dependent manner. Double reciprocal plots of the reaction velocity against varying ASCh concentrations revealed that
/
-sotalol reduced substrate affinity (apparent Michaelis constant, KM, increased) of serum ChE, but did not change the enzyme's maximal rate of ASCh hydrolysis (Vmax). Thus,
/
-sotalol inhibition of serum ChE was of the competitive type (rate constant for reversible competitive inhibition: Ki=0.51m
). In contrast,
/
sotalol reduced the maximal reaction velocity of the AChE isoenzyme from the central nervous system (caudate nucleus), but had no influence on substrate affinity of the enzyme (KMwith ASCh unchanged) indicating purely non-competitive inhibition kinetics (rate constant of reversible non-competitive inhibition: Ki′=0.44m
).
/
-sotalol inhibition of erythrocyte AChE was of mixed competitive/non-competitive type (Ki=0.31m
, Ki′=0.49m
). Non-competitive
/
-sotalol inhibition of caudate nucleus AChE and the non-competitive component of erythrocyte AChE inhibition cannot be overcome by increased concentrations of the cholinergic transmitter acetylcholine (ACh). Peak
/
-sotalol plasma levels as described in the literature for both humans (15μ
) and experimental animals (dogs: 18μ
; rats: 260μ
) as well as maximal myocardial concentrations of the substance (dogs: 46μ
; rats: 478μ
) are in the range of about 2% to 100% of the sotalol inhibition rate constants determined in the present paper for cholinesterase isoenzymesin vitro. Thus,
/
-sotalol inhibition of ACh hydrolysisin vivomay contribute to both the well known antiarrhythmic potential and proarrhythmic side effects of the compound. 相似文献
17.
AMELIORIATION OF CHEMICALLY-INDUCED HEPATOCYTE INJURY BY CYCLOSPORINE A 《Pharmacological research》1996,34(5-6)
Cyclosporine A, beside its current applications, possesses potential hepatoprotective effects. This study was directed to investigate the effect of Cyclosporine A pretreatment on hepatic injury due to carbon tetrachloride (CCl4) and
-galactosamine. Rats were injected by two successive doses of Cyclosporine A (5mgkg−1day−1). Six hours after the second dose, 1mlkg−1of CCl4was administered i.p. Effects associated with Cyclosporine A pretreatment were examined by using isolated hepatocytes and hepatocytes that were immobilized and continuously perfused.
-Galactosamine (5m
) was added directly to the perfusion medium. After isolation, hepatocytes were examined histologically by light and electron microscopy, immobilized and perfused for further metabolic functional activity evaluation. Cyclosporine A pretreatmentin vivoproduced hepatoameliorative effects of various degrees which were statistically significant as manifested by: (1) an increased trypan blue exclusion after CCl4; (2) an improved ureagenesis after CCl4; (3) a reduction in the lipid droplets accumulation in the cytoplasm produced by CCl4administration; (4) well preserved cytoplasmic organelles as mitochondria, endoplasmic reticulum ER, nuclear chromatin structures that were altered by CCl4; and (5) an increased hepatocytes survival in the agarose gel matrix, reduction of LD leakage and improvement of ureagenesis after
-galactosamine addition to the perfusion medium. The beneficial effect of Cyclosporine A pretreatment in modifying hepatotoxicity of chemical insults merits further studies. 相似文献
18.
喙果黑面神化学成分研究 总被引:2,自引:0,他引:2
目的研究大戟科植物喙果黑面神(Breynia rostrata Merr.)的化学成分。方法利用硅胶、凝胶等色谱技术分离纯化化学成分,根据化合物的理化性质和光谱数据进行结构鉴定。结果从喙果黑面神的正丁醇萃取部分分离得到4个化合物,分别鉴定为6-O-甲基丙酰基-α-D-吡喃葡糖(6-O-methylpropanoyl-α-D-glucopyranose,1);4″-苯酚基-6-O-甲基丙酰基-β-D-吡喃葡糖苷(4″-phenolic-6-O-methylpropanoyl-β-D-glucopyranoside,2);1-O-没食子酰基-β-D-吡喃葡糖苷(1-O-galloyl-β-D-glucopyranoside,3);熊果苷(arbutin,4)。结论化合物1和2为新化合物,3和4均为首次从该种植物分离得到。 相似文献
19.
EFFECTS OF -GUANIDINE--METHYLQUINAZOLINE ON GASTRIC ACID SECRETION IN RATS 《Pharmacological research》1996,34(5-6)
In this study 2-guanidine-4-methylquinazoline (2-GMQ) appeared to decrease basal and stimulated gastric acid secretion, while structurally related compounds as dimethyl- biguanide, cyanoguanidine and 2-cyanoamino-4-methylpyrymidine did not. Thus, there is an antisecretory effect when the biguanide group is associated with a lipophilic structure. The antisecretive effects exerted by 2-GMQ are associated with anti H2-histamine activity.The anti H2-histamine nature of the effects of 2-GMQ was confirmed by the capacity of this compound of depressing the chronotropic activity of the isolated guinea pig auricle increased by histamine, as well as relaxant activity in rat uterus contracted by histamine, since both preparations are rich in H2-histamine receptors. 相似文献