Method for quantification of prazosin in dog plasma and its application to pharmacokinetic study

A simple and sensitive high performance liquid chromatography method using fluorescence detection （HPLC- FLD） and a one-step single solvent extraction for the determination of prazosin（PZS） in dog plasma is developed and validated. After extraction with ether, the chromatographic separation of PZS is carried out using a reverse phase C18 column （ 150 mm ×4.6 mm, 5 μm） with a mobile phase of 30% acetonitrile and 70% acetic acid-sodium acetate buffer solution （pH = 3.6） and quantified by fluorescence detection operated with an excitation wavelength of 258 nm and an emission wavelength of 387 nm. The flow rate of the mobile phase is 1.0 mL/min and the retention time of PZS and the internal standard is found to be 4. 4 and 5. 8 rain, respectively. The calibration curve is linear within a concentration range from 1.0 to 1 000.0 ng/mL （ P 〉 0. 998）. The limit of detection is 0.4 ng/mL. The inter-day coefficient of variation （COV） of the calibration standards is below 5.0% and the mean accuracy is in the range from 92. 7% to 104. 2%. Moreover, by analyzing quality control plasma samples for three days, the results show that the method is precise and accurate, for the intra- and inter- day COV within 10% and the accuracy from 95.9% to 112.7%. The developed and validated method is successfully applied to phannacokinetic study for the preclinical evaluation of a new peroral PZS-sulfobutyl ether beta-cyclodextrin （PZS-SBE-β-CD） inclusion complex tablets （test preparation）, which demonstrates that the test preparation released PZS is conducted in a slow and controlled way, and the relative bioavailability of the test preparation is found to be 105.0%.

A Reevaluation of Prazosin Pharmacokinetics in a Two-Compartment Model, the Apparent Volume of Distribution and Comparative Simulations in the One-Compartment Model

Published clinical data of Prazosin were reevaluated pharmacokinetically using explicit solutions to drug concentration as a function of total time for IV bolus injection, intermittent intravenous infusion and oral routes of administration in an open two-compartment model. In a novel way, the apparent volume of distribution was estimated from a two-compartment model and found to be close to the total body water suggesting that Prazosin is distributed in all tissues both extracellularly and intracellularly. In addition, extracting the value of the apparent volume of distribution from a two-compartment model allowed comparative simulations in the one-compartment model. It is shown that dosage calculations of Prazosin intermittent infusion can be safely performed using the simpler one-compartment model equations. Lastly, several additional time-dependent pharmacokinetic parameters e.g., the peak time in the central and peripheral compartment and non-steady state and steady state peak concentration and AUC were determined using series equations for all three routes of administration, as a function of dose number and total time upon multiple drug administrations in the two-compartment model. It is also the first time that steady-state plasma drug concentration equations were derived in a two-compartment mammillary model.

Prazosin:a potential new management tool for iatrogenic autonomic dysreflexia in individuals with spinal cord injury?

Spinal cord injury （SCI） is a devastating condition that not only results in a loss of motor functions but also severe autonomic dysfunctions （Krassioukov and Claydon, 2006）. Autonomic dysreflexia （AD） is a life threatening episode of tran- sient hypertension that occurs up to 30x/day （1 Ix/day on average） in those with cervical or high thoracic SCI （Hubli et al., 2015）. Most common triggers of AD are from stimuli such as a full bowel and/or bladder, or sexual arousal （Teasell et al., 2000）. Penile vibrostimulation （PVS） is a clinical pro- cedure for sperm retrieval used for the purpose of family planning or fertility assessment that unfortunately iatrogenically induces episodes of AD （Elliott, 2006）. Recently, we published a clinical trial highlighting that prazosin may be a viable option for treating AD secondary to PVS （Phillips et al., 2014）.

Activity Induced by a Naphthalene-Prazosin Derivative on Ischemia/Reperfusion Injury in Rats

In this study, a new naphthalene-prazosin derivative (compound 5) was synthetized with the objective of evaluating its activity on ischemia/reperfusion injury. The Langendorff technique was used to evaluate the effect of the compound 5 on ischemia/reperfusion injury. Additionally, the mechanism of action involved in the activity exerted by the compound 5 on perfusion pressure and coronary resistance was evaluated by measuring left ventricular pressure in absence or presence of following compounds;prazosin, metoprolol, indomethacin and nifedipine. The results showed that the compound 5 reduced infarct size compared with the control conditions. Other results showed that the compound 5 significantly increases (p = 0.05) the perfusion pressure and coronary resistance in isolated rat heart. In addition, other data indicate that the compound 5 increases left ventricular pressure in a dose-dependent manner (0.001 to 100 nM);however, this phenomenon was significantly inhibited by nifedipine at a dose of 1 nM (p = 0.05) and this effect was independent of cAMP levels. In conclusion, these data suggest that the naphthalene-prazosin derivative exerts a cardio protective effect via the calcium channels activation and consequently induces changes in the left ventricular pressure levels. This phenomenon results in a decrease of myocardial necrosis after ischemia and reperfusion.

哌唑嗪(Prazosin)合成新工艺

由邻二甲氧基苯(Ⅰ)经硝化成4-硝基-1,2-二甲氧基苯(Ⅱ),还原成3,4-二甲氧基苯胺(Ⅲ),与光气反应得异氰酸-3,4-二甲氧基苯酯(Ⅳ)与氰胺缩合成N-3,4-二甲氧基苯基-N′-氰基代脲(Ⅴ)再用PCl_5/POCl_3闭环成2-氯-4-氨基-6,7-二甲氧基喹唑磷酸酰胺酯(Ⅵ)及水解成盐酸盐(Ⅶ)再碱化等八步反应合成哌唑嗪的药效关键结构2-氯-4-氨基-6,7-二甲氧基喹唑(Ⅷ),总产率按邻二甲氧基苯计为38.2％。其另一片段糠甲酰基哌嗪(Ⅸ)用哌嗪单盐酸盐代替单氢溴酸盐与糠甲酰氯反应获同样结果。

Different Effects of Topical Prazosin and Pilocarpine on Uveoscleral Outflow in Rabbit Eyes

Purpose: To investigate the effects of topical prazosin and pilocarpine on uveoscleral outflow(Fu) in rabbits.Methods: Sixteen rabbits were randomly divided into the control group (5 rabbits, only topical application of normal saline in the right eye of each rabbit), Prazosin (PZ) treated group (6 rabbits, only 0.1% Prazosin eyedrop 0.1% in the right eye of each one) and Pilocarpine (PC) treated group (5 rabbits, 1% Pilocarpine eye drop in each right eye).Intraocular pressure (IOP)of bilateral eyes of each rabbit was measured before and 1 h after topical application of the eye drop.And the bilateral eyes were perfused with Fluorescein-isothiocyanate bovine serum albumin (FITC-BSA) as the tracer into the anterior chamber of each rabbit for 30 min at 90 min after topical treatment. Then the rabbits were killed for Fu measurement.Results: IOP of PZ-treated eyes decreased [ (0.71 +0.07)kPa ] in 1 hour after PZ application.IOP of PC-treated eyes decreased [(0.70+0.08)kPa] in 1 hour after PC application. The average value of Fu was (0.176+0.048)μl/min in control eyes. The average value of Fu in PZ-treated eyes was (0.339+0.018)μl/min. The average value of Fu in PC-treated eye was(0.123+0.022) μl/min.Conclusion: Both of PZ and PC can decrease IOP in rabbits following topical application.Topical PZ can increase Fu in rabbits and this is one of the mechanisms of PZ-induced IOP decrease.Topical PC can prevent Fu. PC decreases IOP not through uveoscleral pathway.This study demonstrates that uveoscleral pathway plays an important role in aqueous humor drainage. PZ may be a novel drug for decreasing IOP. FITC-BSA is an effective tracer for studying uveoscleral pathway.

用~3H-prazosin与~3H-rauwolscine的结合实验来研究狗大隐静脉平滑肌细胞膜α受体亚型的特征

用~3H-prazosin 与~3H-rauwolscine 结合从狗大隐静脉分离出富含质膜的微粒体部分来研究突触后α受体亚型。Bmax,~3H-rauwolscine 4倍高于~3H-prazosin。两放射性配体Kα值,在饱和实验中与动力学实验中相一致。竞争实验显示两种不同的结合部位。α_1受体激动剂 phenylephrine 与两放射性配体有相同亲和力,而α_2受体激动剂 B-HT920示不同亲和力。本文表明狗大隐静脉质膜上存在两类α受体拮抗剂的结合部位。

The fate of prazosin and levonorgestrel after electrochemical degradation process: Monitoring by-products using LC-TOF/MS

Prazosin（PRZ） and levonorgestrel（LNG） are widely used as an anti-disease drugs due to their biological activity in the human body. The frequent detection of these compounds in water samples requires alternative technologies for the removal of both compounds. After electrochemical degradation of PRZ and LNG, the parent compounds could be completely removed after treatment, but the identification and characterization of by-products are necessary as well. In this study, the effects of NaCl concentration and applied voltage were investigated during the electrochemical degradation process. The results revealed that the increase of NaCl concentration and applied voltage could promote the generation of hypochlorite OCl-and then enhance the degradation of PRZ and LNG. After initial study, 6 V and 0.2 g NaCl were selected for further experiments（96% and 99% removal of PRZ and LNG after 40 min, respectively）. Energy consumption was also evaluated and calculated for PRZ and LNG at 3, 6 and 8 V. Solid phase extraction（SPE） method plays an important role in enhancing the detection limit of by-products. Furthermore, characterization and identification of chlorinated and non-chlorinated by-products were conducted using an accurate liquid chromatography-time of flight/mass spectrometry LC-TOF/MS instrument. The monitoring of products during the electrochemical degradation process was performed at6 V and 0.2 g NaCl in a 50 m L solution. The results indicated that two chlorinated products were formed during the electrochemical process. The toxicity of by-products toward E. coli bacteria was investigated at 37°C and 20 hr incubation time.

Adra1a调节LPS诱导的Lbp^(-/-)小鼠原代肝细胞炎症反应

目的探究Adra1a调节LPS诱导的LBP敲除小鼠(Lbp^(-/-))原代肝细胞炎症反应。方法利用二步灌流法提取WT型、Lbp^(-/-)型小鼠原代肝细胞,构建由LPS诱发的原代肝细胞原发炎症模型;采用加入抑制剂哌唑嗪、转染siRNA来下调LBP敲除小鼠原代肝细胞Adra1a的表达;抑制剂法将原代肝细胞分为3组分别是对照组A、LPS组A、抑制剂哌唑嗪组,转染siRNA主要是对原代肝细胞进行分组,包括对照组B、LPS组B、si-NC组、si-Adra1a组;将WT型小鼠的原代肝细胞分为两组分别为对照组(空白对照)、LPS组(LPS刺激12 h)。本研究以WT型、Lbp^(-/-)型小鼠原代肝细胞为研究对象利用Western blot方法验证Adra1a在LPS刺激下的变化情况,采用CCK-8、qRT-PCR、Western blot等实验方法验证哌唑嗪及si-Adra1a对Lbp^(-/-)小鼠的原代肝细胞的炎症及存活率的改善情况。结果在LPS刺激下Lbp^(-/-)小鼠的原代肝细胞Adra1a蛋白表达显著升高(P<0.01),而野生型没有显著变化;抑制剂哌唑嗪组及干扰组的细胞存活率显著升高(P<0.01,P<0.05);抑制剂哌唑嗪组及si-Adra1a组的TNF-α、IL-1β炎症因子表达情况显著降低(P<0.01),与细胞损伤及炎症相关的蛋白p-p38、p-ERK、p-JNK的表达量也显著降低(P<0.01)。结论LPS刺激Lbp^(-/-)小鼠原代肝细胞后Adra1a表达上调、炎症信号因子上调,使用哌唑嗪与si-Adra1a特异性降低Adra1a表达后使LPS相关的Lbp^(-/-)小鼠原代肝细胞炎症因子明显下降,可验证敲除LBP导致Adra1a在LPS诱导的炎症调节中参与反应。

褪黑激素对青霉素所致癎样发作的预防作用(英文)

以往报道表明 ,褪黑激素 (melatonin ,MEL)对癫活动有作用 ,但结果并不一致。有实验表明MEL有抗作用 ,也有证据支持MEL有促作用。本文用海马内微量注射的方法 ,观察了MEL对青霉素所致样发作 (penicillin inducedseizures ,PIS)的影响 ,并对其与受体的可能作用作了探讨。发现 ,预先给予MEL对PIS有抑制作用 ,且该效应具有剂量依赖性。褪黑激素的作用可被Ⅰ型受体拮抗剂luzindole部分阻断 ,而Ⅱ型受体拮抗剂prazosine对此无影响。结果表明 ,MEL对PIS有预防作用 。

非甾体抗炎药酮咯酸的脊髓镇痛作用

采用小鼠温浴法研究非甾体抗炎药（ＮＳＡＩＤ）酮咯酸氨了三醇的脊髓镇痛作用及其机制，发现脊髓内注射酮咯酸氨了三醇０．４ｍｇ·ｋｇ－１有明显镇痛作用，但全身给药（ｉｐ）需８ｍｇ·ｋｇ－１才能达到同样镇痛效果，脊髓与腹腔注射有效剂量比为１：２０，证实酮咯酸具有脊髓镇痛作用，该作用可被ｓｃ利血平、呱唑嗪或育亨宾取消，表明酮咯酸脊髓镇痛作用机制与内源镇痛系统中的去甲肾上腺素能神经有密切关系。本文研究结果为了解ＮＳＡＩＤｓ的中枢镇痛作用及其机制提供了新资料。

甲基莲心碱降低血压及松弛血管作用的分析

甲基莲心碱(neferine,Nef)对自发性高血压大鼠有明显的降压作用,ig给药降压作用可维持3h以上。对由高钾去极化引起的兔主动脉环收缩的抑制作用为维拉帕米(verapamil,Ver)的1/792,使CaCl_2及甲氧明(methoxamine,Met)的量效曲线平行右移,最大反应前者压低、后者不变,pD_2及pA_2值分别为5.4及6.3。还抑制由去甲肾上腺素(norepinephrine,NE)引起的依内钙收缩反应,提示Nef对α_1肾上腺素受体有阻断作用及较弱的钙拮抗作用。

3,15-二乙酰苯甲酰乌头宁镇痛作用与中枢去甲肾上腺素能系统的关系

大鼠电刺激法及小鼠醋酸扭体法测痛表明,利血平,二乙基二硫代氨基甲酸钠(DDC),酚苄明和育亨宾均可使3,15-二乙酰苯甲酰乌头宁(DABA)镇痛作用减弱或消失,哌唑嗪及普萘洛尔对其作用无明显影响,结果提示DABA的镇痛作用可能与中枢去甲肾上腺素能系统的α_2受体有关.

HPLC-MS/ESI 法同时测定人血浆中盐酸特拉唑嗪盐酸哌唑嗪和甲磺酸多沙唑嗪

目的:建立同时测定血浆中盐酸特拉唑嗪、盐酸哌唑嗪和甲磺酸多沙唑嗪的 HPLC-MS/ESI 方法。方法:血浆样品0.5mL,加入10 ng·mL^(-1)二盐酸氟哌噻吨内标液50 μL,经饱和碳酸钠200 μL碱化和1.25 mL 正已烷-叔丁基甲醚(1:1)萃取;以Hypersil GOLD C_(18)柱(100 mm×2.1 mm,5 μm)为固定相,20 mmol·L^(-1)醋酸铵(0.05%甲酸,pH 4.2)-乙腈-甲醇为流动相,梯度洗脱分离,流速为0.2 mL·min^(-1);采用 HPLC-MS,选择离子检测(SIM)法测定盐酸特拉唑嗪([M+H]^+,m/z 388)、盐酸哌唑嗪([M+H]^+,m/z 384)、盐酸多沙唑嗪([M+H]^+,m/z 452和内标氟哌噻吨([M+H]^+,m/z 435)的血药浓度。结果:线性范围为1～100 ng·mL^(-1),r>0.9930(n=7);萃取回收率大于83.0%;方法回收率大于97.0%;日内、日间精密度 RSD 均小于10.0%。结论:该方法灵敏、专属、快速,适用于3种药物的血药浓度监测,以及药代动力学和生物等效性的研究。

鞘内注射哌唑嗪对氯胺酮抗伤害作用的影响

目的 探讨脊髓α1 受体和氯胺酮(Ket, 37. 5mg·kg-1,ip)抗伤害作用的关系。方法 用热水甩尾法观察大鼠鞘内预先注射α1 受体拮抗剂哌唑嗪(Pra, 10, 30μg)对Ket抗伤害作用的影响。并用c fos基因免疫组织化学技术,观察Ket对痛刺激诱发的大鼠脊髓c- fos表达的调节作用及鞘内预先注射Pra(30μg)对Ket调节作用的影响。结果 鞘内单独注射各剂量Pra对动物痛阈均无明显影响(P>0 .05), 鞘内预注Pra(10μg)对Ket抗伤害作用无明显影响(P>0 .05)。而鞘内预注Pra(30μg)则可明显减弱Ket抗伤害作用(P<0 .05)。痛刺激前给予Ket明显减少背角各层Fos免疫阳性神经元的数量(P<0 .05),Ket对痛刺激诱发的脊髓ⅠⅣ层c fos表达的抑制作用可被鞘内预注Pra所减弱(P<0 .05)。结论 脊髓α1 受体参与Ket抗伤害作用。

酮洛芬的脊髓镇痛作用及其机制

目的研究酮洛芬的脊髓镇痛作用及作用机制。方法采用温浴法、热板法观察动物痛阈变化。结果鞘内注射（ｉｔｈ）酮洛芬１．６～３．２ｍｇ·ｋｇ－１具有明显镇痛作用，全身用药需１６ｍｇ·ｋｇ－１才具有同等镇痛效应。ｉｔｈ与ｉｐ药物有效剂量比为１∶１０。ｉｔｈ用药，作用可被ｉｐ利血平、ｓｃ哌唑嗪、育亨宾阻滞。结论酮洛芬具有脊髓镇痛作用。

大鼠侧脑室注射神经降压素对血压的作用

雄性ＳｐｒａｇｕｅＤａｗｌｅｙ大鼠，用乌拉坦（１２ｇ／ｋｇ）腹腔麻醉。在侧脑室注射（ｉｃｖ）神经降压素（ＮＴ）（１０，２０μｇ）可引起血压升高或降低，心率减慢。预先ｉｃｖα１受体阻断剂哌唑嗪（１５μｇ／３μｌ），可阻断ＮＴ的中枢升压反应；预先ｉｃｖＭ受体阻断剂硫酸阿托品（２５μｇ／３μｌ），可阻断ＮＴ的中枢降压反应；预先ｉｃｖＨ１受体阻断剂扑尔敏（５０μｇ／３μｌ）或Ｈ２受体阻断剂甲氰咪胍（２５０μｇ／３μｌ），对ＮＴ的中枢心血管效应均无明显影响。实验结果表明：脑中ＮＴ升高可使血压升高或降低；在ＮＴ引起升压反应的中枢环节中，有肾上腺素能α１受体活动的参与；在ＮＴ引起降压反应的中枢环节中，有胆碱能Ｍ受体活动的参与。可以设想，ＮＴ与儿茶酚胺及乙酰胆碱三者一起参与中枢对血压的调节。

甲磺酸多沙唑嗪片治疗轻中度原发性高血压的临床试验研究

目的探讨甲磺酸多沙唑嗪片在治疗轻中度原发性高血压中的临床效果。方法根据试验设计标准选择40例轻中度原发性高血压患者,随机分成试验组与对照组(n试验组=20,n对照组=20)。采用双盲对照的方法。试验组与对照组分别应用甲磺酸多沙唑嗪片和盐酸特拉唑嗪片,疗程均为8周,判断其疗效。结果入选双盲试验病例40例,完成39例(1例脱落)。两组用药前后收缩压、舒张压组间比较均无差异(P>0.05),而组内比较均有显著性差异(P<0.01)。试验组与对照组降压总有效率分别为95%与100%。试验组与对照组不良反应有头晕、头痛、轻度心动过速等,患者均能耐受。结论甲磺酸多沙唑嗪片与盐酸特拉唑嗪片疗效相似,是治疗轻中度原发性高血压安全、有效的药物。

去甲肾上腺素和哌唑嗪对自发性高血压大鼠动脉平滑肌细胞膜Ca^(2+)-ATPase活性和PMCA1 mRNA表达的影响

目的观察去甲肾上腺素及其α1肾上腺素能受体拮抗剂哌唑嗪对自发性高血压大鼠血管平滑肌细胞Ca2+-ATPasee活性及mRNA表达的影响。方法采用生化酶学法和逆转录聚合酶链反应技术观察不同浓度去甲肾上腺素和哌唑嗪对自发性高血压大鼠血管平滑肌细胞Ca2+-ATPase活性和mRNA表达的影响。结果与自发性高血压大鼠组比较,10-7mol/L去甲肾上腺素能减弱Ca2+-ATPase活性(P<0.01)及mRNA的表达(P<0.01),10-5mol/L和10-6mol/L哌唑嗪能减弱10-7mol/L去甲肾上腺素对Ca2+-ATPase活性的抑制作用(P<0.05)。10-6mol/L哌唑嗪可抑制10-7mol/L去甲肾上腺素对PMCA1mRNA表达的影响(P<0.05)。单用哌唑嗪对Ca2+-ATPase活性及mRNA表达水平无明显改变(P>0.05)。结论去甲肾上腺素抑制自发性高血压大鼠Ca2+-ATPase活性和下调PMCA1mRNA表达,可能是通过α1肾上腺素能受体途径介导基因转录的下调。哌唑嗪可通过阻断α1肾上腺素能受体途径抑制去甲肾上腺素对自发性高血压大鼠血管平滑肌细胞Ca2+-ATPase活性和PMCA1mRNA表达的影响。

氯沙坦对肾性高血压大鼠血管中ACE2 mRNA和蛋白质表达水平的影响

目的观察血管紧张素转换酶2(ACE2)在两肾一夹高血压大鼠(2K1C)血管中的表达以及氯沙坦对其干预后ACE2 mRNA和蛋白质表达水平的影响。方法建立两肾一夹高血压大鼠模型,用夹尾法测定血压。在实验结束时,使用磷酸盐缓冲溶液对大鼠进行灌注,再用4%多聚甲醛在体灌注,剪取胸主动脉,10%福尔马林中保存进行形态学分析。RT-PCR和Wester-blot分别测定血管组织中ACE2 mRNA及蛋白质表达水平。结果肾动脉狭窄大鼠血压较假手术大鼠明显升高(P<0.01),肾性高血压大鼠较正常大鼠ACE2显著降低(P<0.01)。氯沙坦能剂量依赖性的显著降低血压(P<0.05),减少大鼠主动脉管壁厚度(P<0.01),剂量依赖性地增加ACE2 mR-NA和蛋白质的表达(P<0.05)。结论氯沙坦降低血压和逆转高血压血管重构的机制可能与增加ACE2表达有关。