In vivo immunomodulatory profile of histamine receptors(H1,H2,H3 and H4):a comparative antagonists study

Objective:To delineate the comparative immunomodulatory roles of H1R-H4R in antibody generation profile in rabbit model.Methods:The cohort comprised of eight groups containing 18(9 male and 9 female) rabbits in each group.GroupⅠremained non-immunized and received only vehicle(sterile distilled water,1 mL/kg×b.i.d.) intramuscularly.GroupⅡreceived vehicle (1 mL/kg×b.i.d.) while GroupsⅢ-Ⅶ(drugs-treated) received subcutaneous histamine (100μg/kg×b.i.d.),and intramuscular H1R-antagonist(pheniramine,10 mg/kg×b.i.d.), H2R-antagonist(ranitidine,10 mg/kg×b.i.d.),H3R-antagonist(iodophenpropit,1μg/kg×b.i.d.) and H4R-antagonist(JNJ 7777120,10μg/kg×b.i.d.),and GroupⅧDMSO(1 mL/kg×b.i.d.),respectively for 10 days(starting from day 1).They were subsequendy immunized with intravenous injection of sheep red blood cells(SRBC) at day 3.The estimation of serum Igs,IgM and IgG were done by ELISA,and observed at day 0(pre-immunization),and 7,14,21,28 and 58(post-immunization).Results:It was shown that histamine and HRs-antagonists could influence a detectable antibody response to SRBC as early as day 7-post-immunization(post-Ⅰ), which lasted until day 58 post-Ⅰ.The results were found statistically significant(P【0.05,). Conclusions:This study suggests that histamine receptors play important roles in modulation of antibody generation in which H1R,H2R and H4R have immunosuppressive roles and conversely, H3R playes an immune enhancing role.The findings of this study may have clinical significance and provide the baseline information for future study.

H_1 and H_2 receptors in the locus ceruleus are involved in the intracere-broventricular histamine-induced carotid sinus baroreceptor reflex reset-ting in rats

Objective To investigate the role of H1 and H2 receptors in the locus ceruleus （LC） in carotid sinus baroreceptor reflex （CSR） resetting induced by intracerebroventricular （i.c.v.） injection of histamine （HA）. Methods The left and right carotid sinus regions were isolated from the systemic circulation in 18 male Sprague-Dawley rats anesthetized with pentobarbital sodium. The intracarotid sinus pressure （ISP） was altered in a stepwise manner in vivo. ISP-mean arterial pressure （MAP） relationship curve and its characteristic parameters were constructed by fitting to the logistic function with five parameters. The changes in CSR performance induced by i.c.v. HA and the effects of pretreatment with H1 or H2 receptors selective antagonist, chlorpheniramine （CHL） or cimetidine （CIM） into the LC, on the responses of CSR to HA were examined. Results I.c.v. HA （100 ng in 5 μl） significantly shifted the ISP-MAP relationship curve upwards （P 〈 0.05） and obviously decreased the value of the reflex parameters such as MAP range and maximum gain （P 〈 0.05）, but increased the threshold pressure, saturation pressure and ISP at maximum gain （P 〈 0.05）. The pretreatment with CHL （0.5 μg in 1 μl） or CIM （1.5 μg in 1 μl） into the LC could obviously attenuate the changes mentioned above in CSR performance induced by HA, but the alleviative effect of CIM was less remarkable than that of CHL （P 〈 0.05）. Respective microinjection of CHL or CIM alone into the LC with the corresponding dose and volume did not change CSR performance significantly （P 〉 0.05）. Conclusion Intracerebroventricular administration of HA results in a rapid resetting of CSR and a decrease in reflex sensitivity, and the responses of CSR to HA may be mediated, at least in part, by H1 and H2 receptors activities in the LC, especially by H1 receptors. Moreover, the effects of the central HA on CSR might be related to a histaminergic descending pathway from the hypothalamus to LC.

Changes in hippocampal histamine receptors in rats after treatment with Trimeresurus albolabris venom

BACKGROUND： It has been demonstrated that histamine and its receptors in the hippocampus play an important role in memory and/or learning behaviors.OBJECTIVE： To investigate the expression levels of the histamine receptor gene and protein in the hippocampi of rats prior to and after administration of Trimeresurus albolabris venom using reverse transcription-polymerase chain reaction （RT-PCR） and Western blot techniques. DESIGN, TIME AND SETTING： A controlled observation based on cellular protein level was performed in the College of Life Sciences, Chongqing Normal University between March 2005 and April 2007. MATERIALS： Eighty adult male Sprague-Dawley rats were provided by the Laboratory Animal Center of the Third Military Medical University of Chinese PLA. The lyophilized powder of Trimeresurus albolabris venom was collected from Jin-Hu-Shan in Chongqing, China. METHODS： Twenty rats were randomly and evenly divided into an experimental group and a control group The experimental group was subcutaneously injected with 0.65 mg/mL Trimeresurus albolabris venom, 0.5 mL for each rat. The control group was subcutaneously injected with an equal amount of 0.9% physiological saline. Prior to and after injection, rats from these two groups were placed in the Morris Water Maze for recording of path length and escape latency. The remaining 60 rats were randomly allocated to another experimental group （n = 50） and another control group （n = 10）. Rats were correspondingly injected as described above. At different time points （0.1, 0.5, 1, 2, and 3 hours after injection）, rats were decapitated and bilateral hippocampal tissues were dissociated （approximately 100 mg for each sample）. Then, the acquired hippocampal tissue was immediately preserved at -70 ℃ for subsequent experiments. MAIN OUTCOME MEASURES： （1） The levels of histamine receptor （including H1R, H2R, and H3R） mRNA and protein in the hippocampi of rats were measured prior to and after injection of Trimeresurus albolabris venom using RT-PCR and Western Blot techniques. （2） Escape latency （namely, time to reach a platform） and path length were examined by Morris Water Maze testing. RESULTS： All 80 rats were included in the final analysis. In the experimental group, the level of mRNA for H3R receptor in rat hippocampi was just slightly changed, but the level of H3R receptor protein was significantly down-regulated compared with that in the control group （P 〈 0.05）. Both mRNA and protein levels for H1R receptor were initially downregulated and then recovered to normal levels. Expression of H2R receptor mRNA was initially upregulated, then downregulated, and finally restored to the control level. The level of H2R receptor protein showed a tendency for downregulation. In the Morris Water Maze testing, escape latency and path length were significantly longer in the experimental group than in the control group （P 〈 0.05）. CONCLUSION： Within three hours of injection with Trimeresurus albolabris venom, mRNA and protein levels of most histamine receptors in rat hippocampi were downregulated. Such changes possibly contribute to an impairment of memory and/or learning behaviors in rats following injection of Trimeresurus albolabris venom.

Role of Histamine H1 Receptors in Vestibular Nucleus in Motion Sickness

Objectives To investigate the expression of histamine H1 receptors （H1R） in the vestibular nucleus of brainstem in rats and the role of H1R in motion sickness （MS）. Methods A total of 24 healthy Sprague-Dawley rats were divided randomly into four groups （n=6 each） which determined if the animals would receive induction of MS or drug （promethazine） treatment： MS （ - ）/Drug （ - ）; MS（＋）/Drug （ - ）; MS （ - ）/Drug （ ＋ at 0.25 mg）; and MS （ ＋ ）/ Drug（＋）. MS was induced by complex motion stimulation and the conditioned taste aversion was used as a behavioral indicator of MS. The volume of 0.15% sodium saccharin solution （SS） intake within 45 minutes after motion stimulation was measured. H1R in the vestibular nucleus was examined by immunofluorescence staining. The expression of H 1R protein in brainstem tissue at vestibular nucleus level was detected by western blot. Results The mean SS intake volume in the MS （ ＋ ）/Drug （ - ） group （8.8 ml） was significantly less than that of the MS （ - ）/Drug （ - ） group （15.1 ml） （P 〈 0.01）. The mean SS intake volume of the MS （-）/Drug （＋） group （14.8 ml） was similar to that of the MS（-）/Drug（-） group. The mean SS intake volume （9.6 ml） of the MS（＋）/Drug（＋） group was more than that of the MS（＋）/Drug（-）group （P〈0.01）, but less than that of the MS（-）/Drug（-） group or MS（-）/Drug（＋） group （P 〈 0.01）. Immunofluorescence staining showed positive expression of H1R in the vestibular nucleus of brainstem and the expression was enhanced by motion stimulation. Western blot analysis showed that H1R protein expressed in the brainstem tissue at vestibular nucleus level and the expression also increased significantly after motion stimulation. The MS-induced increase of H1R was not affected significantly by promethazine. Conclusions H1Rs exist in the vestibular nucleus in rats and H 1R expression is up-regulated by motion stimulation, but not affected by promethazine. The findings indicate that the histaminergic system is involved in MS. Promethazine, as an H1R blocker, may play its anti-MS role by competing the binding site on H1Rs with histamine rather than inhibiting H1R expression.

Imetit Dihydrobromide and Thioperamide Medication in Cough Hypersensitivity Model—The Role of H3 Receptors

Chronic cough is a troublesome problem and it is frequently associated with diseases such as gastroesophageal reflux, asthma and upper airway diseases—so called diagnostic triade. The magnitude and severity of cough is strongly associated with the ongoing nasal inflammation in subjects with rhinosinusitis and treatment of nasal inflammation leads to the down regulation of pathologically up-regulated cough. Histamine plays a key role in the inflammation of the upper airways of different aetiologies;therefore histamine receptors seem to be promising targets. The aim of our study was to ascertain the effect of H3R agonist imetit and H3R antagonist thioperamide on cough and symptoms of allergic rhinitis (AR) in an animal model of upper airway cough syndrome in ovalbumin sensitized guinea pigs. OVA sensitized guinea pigs (n = 10) were repeatedly challenged with i.n. allergen-OVA to induce allergic rhinitis and to enhance cough reflex according to the validated model of experimental allergic rhinitis. Animals were pre-treated by i.p. administration of imetit (1 mg/kg and 2 mg/kg of body weight) and thioperamide 30 min. prior i.n. OVA administration. Rhinitis evaluation was based on the occurrence of typical symptoms. The effect on cough was assessed from the response to inhalation of citric acid (0.4 M, 10 min), final cough count and cough latency were analysed from the airflow traces, cough motor pattern and the cough sound. AR up-regulated the cough response from 9 ± 2 to 16 ± 1 cough per provocation, med ± IQR, p < 0.05 and shortened cough latency. Imetit (1 mg/kg) suppressed nasal symptoms and decreased number of cough from 16 ± 1 to 12 ± 1;however the data did not reach significance. Imetit (2 mg/kg) significantly suppressed the nasal symptoms, and number of coughs from 16 ± 1 to 6 ± 2, med ± IQR, p < 0.05. Thioperamide (5 mg/kg of body weight) did not have expected effects on tested parameters. H3R agonist imetit, unlike H3R antagonist thioperamide has antitussive potential and ability to suppress nasal symptoms in animal model of allergic rhinitis.

雷公藤多苷联合他克莫司及激素治疗难治性肾病综合征的效果及对血清sTNF-R1、IGFBP-2、CFH水平的影响

目的 探讨雷公藤多苷联合他克莫司及激素治疗难治性肾病综合征(RNS)的疗效对血清可溶性肿瘤坏死因子受体1(s TNF-R1)、胰岛素样生长因子结合蛋白-2(IGFBP-2)、补体因子H(CFH)水平的影响。方法 研究对象为2018年8月至2021年8月于江南大学附属医院治疗的RNS患者102例,以随机数字表法分为对照组(n=51,采取甲泼尼龙片加他克莫司胶囊治疗)和观察组(n=51,在对照组基础上给予雷公藤多苷片治疗)。评估两组的治疗效果、血清相关指标,统计两组的不良反应。结果 观察组治疗总有效率(96.08%)高于对照组(80.39%)(χ^(2)=6.044,P=0.014);治疗后,观察组患者血清白蛋白、CFH水平[分别为(36.54±8.11) g·L^(-1)、(586.20±100.72)μg·m L^(-1)],高于对照组[分别为(32.58±6.12) g·L^(-1)、(540.11±100.47)μg·m L^(-1)],差异均有统计学意义(t=2.783,P=0.006;t=2.314,P=0.023);观察组患者24 h尿蛋白、肌酐、s TNF-R1、IGFBP-2水平[分别为(2.67±0.69) g、(82.25±16.13)μmol·L^(-1)、(1.56±0.45) ng·m L^(-1)、(51.34±10.44) ng·m L^(-1)],低于对照组[分别为(3.24±1.02) g、(92.68±17.35)μmol·L^(-1)、(1.91±0.58) ng·m L^(-1)、(57.79±12.58) ng·m L^(-1)],差异均有统计学意义(t=3.306,P=0.001;t=3.135,P=0.002;t=3.405,P=0.001;t=2.820,P=0.005);观察组复发率(1.96%)低于对照组(13.73%)(χ^(2)=4.883,P=0.027)。结论 公藤多苷联合他克莫司及激素治疗RNS效果佳,降低复发率,改善肾功能,减轻炎症,有望作为辅助治疗RNS的药物。

Histamine Excites Rat GABAergic Ventral Pallidum Neurons via Co-activation of H1 and H2 Receptors

The ventral pallidum(VP) is a crucial component of the limbic loop of the basal ganglia and participates in the regulation of reward, motivation, and emotion.Although the VP receives afferent inputs from the central histaminergic system, little is known about the effect of histamine on the VP and the underlying receptor mechanism. Here, we showed that histamine, a hypothalamicderived neuromodulator, directly depolarized and excited the GABAergic VP neurons which comprise a major cell type in the VP and are responsible for encoding cues of incentive salience and reward hedonics. Both postsynaptic histamine H1 and H2 receptors were found to be expressed in the GABAergic VP neurons and co-mediate the excitatory effect of histamine. These results suggested that the central histaminergic system may actively participate in VP-mediated motivational and emotional behaviors via direct modulation of the GABAergic VP neurons. Our findings also have implications for the role of histamine and the central histaminergic system in psychiatric disorders.

组胺H 1受体激动剂通过Akt/NF-κB通路抑制脂多糖诱导的星形胶质细胞炎症反应

目的探讨组胺H 1受体(histamine H 1 receptor,H 1R)对脂多糖(lipopolysaccharide,LPS)诱导的星形胶质细胞炎症反应的影响及其调控机制。方法采用LPS建立体外星形胶质细胞炎症模型,随机将大鼠原代星形胶质细胞分为对照组、LPS组、LPS+H 1R激动剂组(2-pyridylethlamine,Pyri)和H 1R激动剂组。对照组仅加入培养液,LPS+H 1R激动剂组提前在培养液中加入100μmol·L-1的Pyri,1 h后再加入终浓度为100μg·L-1的LPS。CCK-8法检测细胞活性;免疫荧光法检测活化标记物GFAP和H 1R的表达;倒置相差显微镜下观察星形胶质细胞的形态变化;ELISA法检测细胞上清中炎症因子TNF-α和IL-6水平;Western blot检测p-Akt、Akt、p-NF-κB p65、NF-κB p65的蛋白表达。结果与对照组比较,LPS组星形胶质细胞分支和辐射状突起减少,GFAP表达增加,细胞表面H 1R表达下调,上清液中TNF-α和IL-6含量增加,Akt和NF-κB p65的磷酸化水平明显增加;与LPS组相比,LPS+H 1R激动剂组激活态星形胶质细胞减少,GFAP表达降低,培养基上清中TNF-α和IL-6的含量明显下降,Akt和NF-κB p65的磷酸化表达明显降低。结论H 1R激动剂能够抑制LPS诱导的星形胶质细胞活化和炎症因子的表达,且Akt/NF-κB通路可能是H 1R参与星形胶质细胞免疫调节的重要途径。

Stimulation by nizatidine,a histamine H_2-receptor antagonist,of duodenal HCO_3^-secretion in rats:relation to anti-cholinesterase activity

AIM To examine whether nizatidine stimulates duodenal HCO_3^- secretion in rats by inhibiting AChE activity. METHODS Under pentobarbital anesthesia,a proximal duodenal loop was perfused with saline,and the HCO_3 secretion was measured at pH 7.0 using a pH-stat method and by adding 10mM HCI.Nizatidine,neostigmine,carbachol or famotidine was administered i.v.as a single injection. RESULTS Intravenous administration of nizatidine(3-30 mg/kg)dose-dependently increased duodenal HCO_3^- secretion,and the effect at 10mg/kg was equivalent to that obtained by carbachol at 0.01 mg/kg.This nizatidine action was observed at the same dose range that inhibited acid secretion and enhanced gastric motility,mimicked by i.v.injection of neostigmine(0.03 mg/kg),and significantly attenuated by bilateral vagotomy and prior s.c. administration of atropine but not by indomethacin,a cyclooxygenase inhibitor,or N^G-nitro-L-arginine methyl ester,a NO synthase inhibitor.The HCO_3^- secretory response to acetylcholine(0.001 mg/kg)was significantly potentiated by the concurrent administration of nizatidine(3mg/kg,i.v.).The IC_(50)of nizatidine for AChE of rat erythrocytes was 1.4×10^(-6)M,about 12 times higher than that of neostigmine.Neither famotidine(>10^(-3)M, 30mg/kg,i.v.)nor cisapride(> 10^(-3)M, 3mg/kg,i.v.)had any influence on AChE activity or duodenal HCO_3^- secretion.Duodenal damage induced by acid perfusion(100 mM HCI for 4 h)in the presence of indomethacin was significantly prevented by nizatidine and neostigmine,at the doses that increased the HCO_3^- secretion. CONCLUSION Nizatidine stimulates duodenal HCO_3^- secretion,in both vagal-dependent and atropine-sensitive manners,and the action is associated with the anti-AChE activity of this agent.

紫外/过二硫酸盐对组胺H_(2)受体拮抗剂的降解特性及自由基模拟

研究了基于硫酸根的高级氧化技术UV/过二硫酸盐(UV/PDS)对水体中组胺H2受体拮抗剂(HRAs)的降解,并选取HRAs中的典型物质西咪替丁(CMTD)为目标污染物.采用竞争动力学方法得到了HRAs和·OH及SO_(4)^(−)反应的二级速率常数,k·OH/HRAs为(2.8—14.6)×10^(9)L·mol^(−1)·s^(−1),kSO_(4)^(−)/HRAs为(0.81—8.10)×10^(9)L·mol^(−1)·s^(−1).研究在实验基础上建立了UV/PDS的自由基拟稳态模型,模拟结果表明,UV/PDS对污染物的降解,其间接光解起主要作用,体系中·OH和SO_(4)^(−)是间接光解的主导自由基.在(0.1—0.5)mmol·L^(−1)PDS投加量下,·OH和SO_(4)^(−)的浓度分别为(3.85—5.16)×10^(−16)mol·L^(−1),(1.21—1.68)×10^(−13)mol·L^(−1),SO_(4)^(−)对污染物的降解起主导作用.酸性条件下自由基浓度相对更高,从而促进了CMTD的去除.水体基质(Cl^(−)、HCO_(3)^(−)和NOM)存在条件下,CMTD的降解受到一定的抑制,模拟结果表明自由基浓度显著降低;但是模拟结果与实验结果有一定偏差,主要是基质存在下生成了衍生自由基,由于衍生自由基的复杂性而未计入模型计算中导致.在实际水样中应用的研究表明,UV/PDS可以有效降解地表水(SW)和实际废水(WW)中的CMTD,具有良好的应用前景.

Effects of splice sites on the intron retention in histamine H_3 receptors from rats and mice

In the alternative splicing, intron retention, of histamine H3 receptors in rats and mice, the short transcript isoforms that are excised alternatively spliced introns are easily detected in a very low level in rats and are undetectable in mice using the regular PCR protocol. The retained introns have common 5＇ splice site and different 3＇ splice sites. The detailed mechanism for the special alternative splicing remains largely unclear. In this study, we developed a minigene splicing system to recapitulate natural alternative splicing of the receptors and investigated the effects of 5＇ and 3＇ splice sites on intron retention in HeLa cells. Mutating weak 5＇ and 3＇ splice sites of the alternatively spliced introns toward the canonical consensus sequences promoted the splicing of the corresponding introns in rat and mouse minigenes. The effect of splice site strength was context-dependent and much more sigiaificant for the 3＇ splice site of the longer alternative intron than for the 3＇ splice site of the shorter alternative intron and the common 5＇ splice sites; it was also more significant in the rat minigene than in the mouse minigene. Mutating the 3＇ splice site of the longer alternative intron resulted in almost complete splicing of the intron and made the corresponding isoform to become the nearly exclusive transcript in the rat minigene.

Histamine H2 receptor deletion in glutamatergic neurons causes schizophrenia-like pheno⁃ types

OBJECTIVE Genetic variation in histamine H2 receptor(H2R)and H2R ligands are linked to schizophrenia,however little is known about how H2R contributes to pathogenesis of schizophrenia.Here,we detected a decreased expression of H2R in medial prefrontal cortex(mPFC)glutamatergic neurons in schizophrenia patients.METHODS AND RESULTS Selective knockout of H2R gene(Hrh2)in glutamatergic neurons induced schizophrenia-like behaviors including sensorimotor gating deficit,increased locomotor activity,social withdrawal and anhedo⁃nia in behavior tests,as well as reduced sponta⁃neous firing of mPFC glutamatergic neurons in electrophysiological tests.Selective deletion of the Hrh2 in mPFC glutamatergic neurons but not hippocampus glutamatergic neurons also induced such schizophrenia-like behaviors.Patch-clamp electrophysiology establishes that H2R deficiency reduced the intrinsic excitability of glutamatergic neurons by up-regulation of hyperpolarization activated cyclic nucleotide-gated channels.Fur⁃thermore,either overexpression of H2R in gluta⁃matergic neurons or activation of H2R in the mPFC reversed the MK-801-induced schizophrenia-like symptoms.CONCLUSION H2R can serve as a novel drug target given that functional deficiency of this receptor in mPFC glutamatergic neurons may be crucial for the pathogenesis of schizo⁃phrenia.H2R agonists can be viewed as drug candidates for the treatment of schizophrenia.

Histamine_2-receptor antagonists: Rapid development of tachyphylaxis with repeat dosing

Histamine_2-receptor antagonists(H_2RAs) are availableover-the-counter (OTC) for the treatment and prevention of heartburn, but more than occasional, singledose use can lead to rapid development of tachyphylaxis. The aim of this review is to assess the publishedevidence regarding the development of tachyphylaxiswith repeat usage of H_2RAs. PubMed and SCOPUS were searched across all years to identify clinical studies thatexamined the development of tachyphylaxis with repeated dosing of H_2RAs. Although a single (first) doseof an H_2RA can be effective for controlling gastric acidand preventing or relieving food-related heartburn, numerous studies confirm that tachyphylaxis, also knownas tolerance, is consistently detected at the first timepoint assessed after the first dose, including the second day and/or second dose. Even if symptom relief isachieved with an H_2RA, it may be due to desensitizationof the esophagus to acid exposure, potentially providingsymptom relief without significantly decreasing esophageal acid exposure. When recommending OTC drugsfor treatment of frequent heartburn, clinicians shouldbe aware of the potential for rapid development oftachyphylaxis in patients who use H_2RAs for 2 or more consecutive days. Even if symptom relief is achieved, it may be due to desensitization of the esophagus to acid by the H_2RA, potentially providing symptom relief without significantly decreasing esophageal acid exposure. Other strategies, such as an OTC proton pump inhibitor, may be needed to optimize management of frequent heartburn.

质子泵抑制剂和H_2受体阻滞剂预防应激性溃疡的系统评价再评价

目的对质子泵抑制剂和H_2受体阻滞剂预防应激性溃疡的有效性和安全性系统评价进行再评价。方法计算机检索Cochrane图书馆、Pub Med、Embase、Web of Sciene、中国知网(CNKI)、中国科技期刊全文数据库(VIP)、中国生物医学文献数据库(CBM)和万方医学数据库,检索时限均从建库至2016年5月。根据纳入排除标准,筛选符合纳入排除标准的系统评价和Meta分析,使用AMSTAR量表评价所纳入系统评价的方法学质量,Grade系统评价结局指标的证据质量,提取原始研究用Rev Man 5.3软件进行Meta分析。结果共纳入7个系统评价/Meta分析,方法学质量评分>7分者仅占41.86%;对21个单个结局指标分别进行质量评价,14个(67.77%)的证据质量均为低或极低。对36个研究(3 820例)数据进行再分析,PPI在预防应激性溃疡出血、临床大出血和显性出血方面优于H_2RA(P<0.001),但是在肺炎发生率、死亡率和ICU住院天数方面,PPI和H_2RA比较差异无统计学意义(P>0.05)。结论 PPI预防ICU的危重患者的应激性溃疡出血优于H_2RA,但原始研究质量不高,仍需后续更多的高质量、结局指标设计全面的前瞻性研究。

组胺H_3受体对垂体瘤AtT-20细胞分泌ACTH的调节作用

目的 观察组胺受体激动剂对 At T- 2 0细胞分泌ACTH的影响 ,并探讨 G蛋白在组胺 H3受体信号转导机制中的作用 .方法 选用文献报道的高表达组胺 H3受体的垂体细胞瘤 At T- 2 0作为观察系统 ,用放免分析法测定给予组胺受体激动剂后各时间点细胞上清液中 ACTH分泌量的变化 ,并观察药物对细胞增殖的影响 .结果 组胺 H3受体激动剂R- (α) - Me HA(0 .1μmol· L- 1 )作用 8h能明显促进 ACTH的释放 ,释放量为 192 0 μg· L- 1 ,与同时间对照组 (780 μg·L- 1 )相比 ,明显增高 (P<0 .0 1) ;H1 和 H2 激动剂则无此作用 .且 R- (α) - Me HA引起 ACTH分泌的效应能被 H3受体特异性拮抗剂 thioperamide所拮抗 ,而 H1 受体和 H2 受体拮抗剂均不影响 R- (α) - Me HA的效应 .R- (α) - Me HA作用 8和 2 4h,对细胞增殖无明显影响 .用 G蛋白失活剂 NEM预先处理细胞后 ,取消了 R- (α) - Me HA增强 At T- 2 0细胞 ACTH分泌的效应 .结论 特异性激动组胺 H3受体后能引起兴奋 -分泌耦联过程 ,其信号转导过程中有 G蛋白的参与 .

H_2受体拮抗剂用于抑制由化疗引起的恶心呕吐的临床研究

基于含铂或中度以上致呕肿瘤化疗方案 ,应用 5 HT3 受体拮抗剂为基础的止呕方法 ,对 12 6例病理学确诊为晚期恶性肿瘤患者按 2∶1信封法随机分组进行跟踪治疗 ,研究组加用H2 受体拮抗剂和安定 ,而对照组加用地塞米松 ,并从疗效、不良反应、耐受性及安全性等方面对两分组加以分析比较。研究组对抑制急性恶心呕吐有效率为91 2 % ( 73 / 80 ) ,迟缓性恶心呕吐有效率为 87 5 % ( 70 / 80 ) ,而对照组分别为 71 7% ( 3 3 / 46)及 60 9% ( 2 8/ 46) ,两分组相比差异有统计学意义 ,P值分别为 0 0 0 4及 0 0 0 1;加救援治疗后 ,研究组总完全控制率 10 0 % ( 80 / 80 ) ,对照组仅70 % ( 2 8/ 46) ,两组间差异也有统计学意义 ,P =0 0 0 0。初步研究结果提示 ,以 5 HT3 受体拮抗剂为基础加H2 受体拮抗剂和安定的止呕方法对由含铂或中度以上致呕肿瘤化疗方案所引起的恶心呕吐有明显的抑制作用 ,尤其是在迟缓性呕吐方面 ,有效率高 ,不良反应小 ,患者有良好的耐受性及安全性。

番石榴叶总黄酮对2型糖尿病模型小鼠肝糖异生ERRγ/CREBH信号通路相关因子的影响

目的:探讨番石榴叶总黄酮(GLTF)对2型糖尿病(T2DM)模型小鼠肝脏雌激素相关受体γ(ERRγ)/环磷酸腺苷应答元件结合蛋白H(CREBH)通路相关因子的影响,探讨其降血糖作用的具体机制。方法:取健康雄性ICR小鼠,采用高糖高脂饲料喂养联合多次腹腔注射小剂量链脲佐菌素的方法建立T2DM模型。将造模成功的小鼠按血糖值随机分为模型组、二甲双胍组(阳性对照,0.17 g/kg)、消渴降糖胶囊组(阳性对照,0.75 g/kg)和GLTF低、高剂量组(0.047、0.094 g/kg),每组12只;另选12只正常小鼠作为正常组。除正常组和模型组小鼠灌胃等体积水外,其余各组小鼠灌胃相应药物溶液10 mL/kg,qd,连续21 d。给药结束后,检测各组小鼠空腹血糖值、血清胰岛素水平,计算胰岛素敏感指数(ISI);采用苏木素-伊红染色法观察小鼠肝脏和胰腺组织病理学变化;采用免疫印迹法检测小鼠肝组织中ERRγ、CREBH的蛋白表达水平;采用实时定量聚合酶链式反应法检测小鼠肝组织中过氧化物酶体增殖物激活受体γ辅激活因子1α(PGC1α)、CREB调节转录辅激活因子2(TORC2)的mRNA表达水平。结果:与正常组比较,模型组小鼠空腹血糖和血清胰岛素水平均显著升高,ISI值显著降低(P<0.01);肝组织病变明显、可见大量空泡;胰腺组织中胰岛数目减少、体积变小,胰岛细胞呈轻度空泡病变;肝组织中ERRγ、CREBH的蛋白表达水平及PGC1α、TORC2的mRNA表达水平均显著升高(P<0.01)。与模型组比较,GLTF各剂量组小鼠上述血糖、胰岛素指标及病理学变化均明显改善;肝组织中ERRγ、CREBH的蛋白表达水平及PGC1α、TORC2的m RNA表达水平均显著降低(P<0.05或P<0.01)。结论:GLTF对T2DM模型小鼠具有明显降糖及肝、胰腺组织保护作用;其降血糖作用的机制可能与抑制肝脏ERRγ/CREBH信号通路有关。

质子泵抑制药和H2受体拮抗药预防应激性溃疡有效性和安全性的Meta分析

目的比较质子泵抑制药(proton pump inhibitors,PPI)和H2受体拮抗药(histamine-2-receptor antagonists,H2RAs)预防危重患者应激性溃疡的有效性和安全性。方法对Cochrane图书馆,Pub Med,Embase,Science Direct数据库,中国知网,中国生物医学文献数据库进行检索。只纳入PPI和H2RA预防应激性溃疡的随机对照(RCT)实验进行Meta分析,统计指标包括临床消化道大出血,明显上消化道出血,医源性肺炎,死亡率,ICU住院时间,艰难梭菌感染。结果纳入9篇文献,其中高质量文献3篇,共报道消化道大出血患者1151例,结果表明预防性应用PPI与H2RA相比,可以降低临床胃肠道大出血的风险(RR=0. 39;95%CI=0. 21-0. 71;P=0. 002;I^2=0%)。结论应用PPI预防应激性溃疡效果要优于H2RA,可以降低消化道大出血和明显上消化道出血的风险,同时未增加肺炎风险、死亡率和ICU住院时间。两药对艰难梭菌感染的影响尚不明确。

H_2受体拮抗剂预防低剂量阿司匹林相关上消化道损伤的研究

随着低剂量阿司匹林(LDA)在心脑血管疾病一级预防及二级预防中的广泛应用,LDA相关上消化道损伤的发病率逐年增加。质子泵抑制剂(PPI)能够有效预防LDA相关的上消化道损伤,但长期应用PPI的不良反应、价格及其与氯吡格雷的相互作用,使PPI的预防作用受到质疑。传统的抑酸药物H2受体拮抗剂(H2RA)再次受到关注。该文就H2RA对LDA相关上消化道损伤的预防效果及与PPI的疗效比较予以综述。

质子泵抑制剂及H2受体拮抗剂对胰腺癌发生风险的Meta分析

目的:探讨质子泵抑制剂(PPI)、组胺-2受体拮抗剂(H2RA)的使用与胰腺癌发生风险的关系。方法:检索2019年7月31日前公开发表的有关PPI及H2RA与胰腺癌发病风险有关的临床试验的相关文献。通过纳入和排除标准筛选后采用纽卡斯尔-渥太华量表进行质量评分,采用Stata12.0进行Meta分析。结果:最终纳入8篇文献共551137例患者,其中胰腺癌患者21015例,包括6个病例对照研究,2个队列研究。Meta分析结果显示:PPI及H2RA可增加胰腺癌发病风险,OR值分别为1.61(95%置信区间1.11-2.32)及1.26(95%置信区间1.02-1.57)。结论:使用PPI及H2RA可能增加胰腺癌发生风险,因此需严格按照适应症慎重开具处方,避免长时间、大剂量使用。