Development and characterization of amoxicillin loaded floating microballoons for the treatment of Helicobacter pylori induced gastric ulcer

The current communication reports in vitro characterization of the optimized hollow floating microballoons of amoxicillin on the basis of micromeritic properties and in vitro minimum inhibitory concentration(MIC).Amoxicillin loaded hollow microballoons were prepared by emulsion solvent diffusion method.The morphological characterization was done on the basis of scanning electron microscopy(SEM).Fourier Transformed Infrared Spectroscopy(FTIR)was used to investigate drugepolymer interactions.The correlation between the in vitro buoyancy of microballoons and their physical properties,e.g.density and porosity were elucidated.The results of FTIR spectroscopy revealed the absence of any drugepolymer interactions.The porosity values of more than 69%and diameter to thickness ratio greater than 2.90,proved a high cavity volume within the microballoons in all size ranges.The spherical shape of microballoons with hollow internal cavity was confirmed from SEM photomicrographs.The in vitro MIC results showed a sustained drug effect from the microballoons.In conclusion,it can be said that the developed microballoons can be used for the effective treatment of Helicobacter pylori induced gastric ulcer.

Distinct patterns of mucosal apoptosis in H pylori-associated gastric ulcer are associated with altered FasL and perforin cytotoxic pathways

AIM: To analyze the level of apoptosis in different mucosal compartments and the differential expression of Fas/Fas-ligand and perforin in H pylori-associated gastric ulcer. METHODS: Antral specimens from patients with H pylori-related active gastric ulcer (GU), H pylori-related gastritis, and non-infected controls were analysed for densities and distribution of apoptotic cells determined by the TdT-mediated dUDP-biotin nick-end-labelling method. GU patients were submitted to eradication therapy with follow-up biopsy after 60 d. Fas, FasL, and perforin-expressing cells were assessed by immunoper- oxidase, and with anti-CD3, anti-CD20 and anti-CD68 by double immunofluorescence and confocal microscopy. Quantitative analysis was performed using a computer- assisted image analyser. RESULTS: H pylori-infected antrum showed greater surface epithelial apoptosis which decreased after eradi- cation therapy. In the lamina propria, higher rates of mononuclear cell apoptosis were observed in H pylori- gastritis. Co-expression of Fas with T-cell and macro- phage markers was reduced in GU. FasL- and perforin-expressing cells were increased in H pylori-infection and correlated with epithelial apoptosis. Perforin-expressing cells were also increased in GU compared with H pylori- gastritis. CONCLUSION: Epithelial apoptosis is increased in H pylori-infection and correlates to FasL- and perforin- expression by T cells. Expression of perforin is correlated with the tissue damage, and may represent the enhance- ment of a distinct cytotoxic pathway in GU. Increased expression of FasL not paralleled by Fas on T-cells and macrophages may indicate a reduced susceptibility to the Fas/FasL-mediated apoptosis of lymphoid cells in H pylori-infection.

H pylori infection and other risk factors associated with peptic ulcers in Turkish patients: A retrospective study

AIM: To identify and evaluate the relative impact of H pylori infection and other risk factors on the occurrence of gastric ulcer (GU), duodenal ulcer (DU) and gastritis in Turkish patients. METHODS: A total of 4471 patients (48.3% female) out of 4863 attended the Samatya hospital in Istanbul (June 1999 - October 2003) were included. The records of H pylori status (CLO-test), endoscopic f indings of GU, DU and gastritis, personal habits (smoking, alcohol intake) and medication [non-steroidal anti-inflammatory drugs (NSAIDs), aspirin intake] were analyzed using multi-way frequency analysis. RESULTS: We have found that GU in the presence of H pylori had significant association with aspirin (P = 0.0001), alcohol (P = 0.0090) and NSAIDs (P = 0.0372). DU on the other hand had significant association with aspirin/ smoking/NSAIDs (P = 0.0259), aspirin/alcohol (P = 0.0002) and aspirin/smoking (P = 0.0233), also in the presence of H pylori. In the absence of H pylori GU had significant association with alcohol/NSAIDs (P = 0.0431), and NSAIDs (P = 0.0436). While DU in the absence of H pylori had significant association with smoking/alcohol/ NSAIDs (P = 0.0013), aspirin/NSAIDs (P = 0.0334), aspirin/alcohol (P = 0.0360). CONCLUSION: In the presence of H pylori, aspirin, alcohol and NSAIDs intake act as an independent risk factors that had an augmenting impact on the occurrence of GU and only together on the occurrence of DU in Turkish patients.

A prospective randomized trial of lafutidine vs rabeprazole on post-ESD gastric ulcers

AIM:To compare the effects of rabeprazole and lafutidine on post-endoscopic submucosal dissection(ESD) gastric ulcers.METHODS:Patients with gastric tumors indicated for ESD were prospectively studied.After ESD,all patients were treated with intravenous omeprazole for the first 3 d.Patients were then randomly assigned to oral lafutidine or rabeprazole.Ulcer size,ulcer size reduction rate,and ulcer stage were evaluated 4 wk later.Occurrence of complication was monitored throughout the 4-wk period.RESULTS:Sixty five patients were enrolled in the study,and 60 patients were subjected to the final analysis.In the lafutidine group(30 lesions in 29 patients),initial and 4-wk post-ESD ulcer sizes were 33.3 ± 9.2 and 10.5 ± 4.8 mm,respectively.In the rabeprazole group(34 lesions in 31 patients),the values were 34.7 ± 11.3 and 11.8 ± 6.7 mm,respectively.Ulcer size reduction rates in lafutidine and rabeprazole groups were 32.3% and 33.5%,respectively(P=0.974).Ulcer stage 4 wk post-ESD did not differ significantly between the two groups(P=0.868).Two cases in the rabeprazole group and no cases in the lafutidine group developed ulcer bleeding during the oral dose period,although the difference of bleeding rate between the two groups was not statistically significant(P=0.157).CONCLUSION:Lafutidine and rabeprazole have equivalent therapeutic effects on post-ESD gastric ulcers.

维胃方对胃溃疡大鼠胃黏膜MPO、H^+-K^+-ATP酶活性的影响

[目的]观察维胃方对胃溃疡大鼠胃黏膜髓过氧化物酶(MPO)和H+-K+-ATP酶的影响,探讨维胃方治疗胃黏膜损伤的可能机制。[方法]采用乙酸烧灼法,建立胃溃疡模型,用比色法测定胃黏膜MPO和H+-K+-ATP酶活性,并观察胃黏膜组织病理学变化。[结果]从胃黏膜大体标本、切片观察,维胃方中剂量组疗效最佳。与自愈组和模型组比较,维胃方各组胃黏膜MPO活性显著降低(P<0.01或P<0.05),其中以维胃方中剂量组值最小。维胃方各剂量组的H+-K+-ATP酶活性均高于自愈组(P<0.01或P<0.05),接近正常组(P>0.05),表明维胃方能恢复其活性。[结论]维胃方对大鼠实验性胃溃疡具有明显的保护作用,其机制可能是通过降低大鼠胃黏膜MPO活性,进而减轻炎症介质对胃黏膜的损伤。同时其能修复已损伤的胃黏膜,故能恢复H+-K+-ATP酶活性。

不同pH值对消化性溃疡并出血疗效的影响

目的：探讨不同ｐＨ值对消化性溃疡并出血疗效的影响，方法和结果：１临床和动物实验富血小板血浆（ＰＲＰ）中加入不同剂量的ＨＣｌ以改变其ｐＨ环境并测定其血小板聚集率。结果显示，随着ＨＣｌ量的增加，ｐＨ下降，血小板聚集率也降低，当ｐＨ＜６８时，血小板聚集率显著下降，用不同ｐＨ值的缓冲液冲洗大白鼠胃内活检伤口，测定其胃粘膜出血时间（ＧＭＢＴ），结果显示，当ｐＨ≥６０时，ＧＭＢＴ明显减少，约５７６±１８６秒。２胃内ｐＨ值监测连续４８小时监测胃内ｐＨ值，结果显示，甲氰米胍１６００ｍｇ静脉注射与奥美拉唑４０ｍｇ静脉注射，胃内ｐＨ值相仿，分别为５４±１３和５８±１３，逐步降低甲氰米胍用量，其ｐＨ值亦逐步下降，至８００ｍｇ时，胃内ｐＨ值为１５，基本无作用。３临床疗效观察回顾性分析３０３例应用雷尼替丁与３２６例应用奥美拉唑的溃疡出血病人，前者手术率与死亡率为７２８％和１９９％，后者为４９１％和１８４％。结论：ｐＨ值与血小板聚集率及ＧＭＢＴ密切相关，药物治疗溃疡出血成功的关键在于有效提高胃内ｐＨ值。

大鼠实验性胃溃疡自愈过程中HDC和H^+,K^+-ATP酶的表达

目的探讨胃黏膜内组氨酸脱羧酶(histidine decarboxylase,HDC)和H+,K+-ATP酶的表达与大鼠实验性胃溃疡自愈过程的关系。方法制备大鼠乙酸性胃体溃疡模型,采用逆转录聚合酶链反应和Western blot技术,观察溃疡自愈过程中大鼠胃黏膜内HDC和H+,K+-ATP酶mRNA及蛋白表达的动态变化。结果制模术后1d大鼠胃体出现明显溃疡,3d溃疡最为明显,12d溃疡基本愈合。HDC和H+,K+-ATP酶mRNA表达在制模术后1d即开始降低,术后9d恢复正常。HDC和H+,K+-ATP酶蛋白表达在制模术后也出现降低,术后6d达到最低,术后12d基本恢复正常。结论在胃溃疡自愈过程中,胃黏膜内HDC和H+,K+-ATP酶mRNA和蛋白表达下调,其作用是抑制胃酸分泌以促进溃疡愈合。

健脾活血中药对胃溃疡大鼠H^+,K^+-ATP酶及壁细胞胃泌素受体作用的影响

目的观察健脾活血中药对胃溃疡大鼠H+,K+-ATP酶及壁细胞胃泌素受体作用的影响。方法采用放射配基受体结合测定技术分别检测各组壁细胞胃泌素受体结合位点数,同时分别检测各组大鼠H+,K+-ATP酶活性及胃液总酸度。结果健脾活血组壁细胞胃泌素受体结合位点数低于正常大鼠(P<0.05),胃液总酸度及H+,K+-ATP酶活性升高(P<0.05);奥美拉唑组壁细胞胃泌素受体结合位点数明显高于正常大鼠(P<0.05),胃液总酸度及H+,K+-ATP酶活性明显降低(P<0.05);中西药组壁细胞胃泌素受体结合位点数、胃液总酸度及H+,K+-ATP酶活性与正常大鼠比较无显著性差异(P>0.05)。结论健脾活血中药平缓地抑制胃壁细胞的H+,K+-ATP酶活性,降低胃酸的分泌;同时,不影响胃泌素受体结合位点数,防止停药后反跳性过多泌酸。

大鼠乙酸性胃溃疡自愈过程中HDC和H^+、K^+-ATP酶的表达

目的探讨胃黏膜内组氨酸脱羧酶(HDC)和H+,K+-ATP酶的表达与大鼠乙酸性胃溃疡自愈过程的关系。方法制备大鼠乙酸性胃体溃疡模型,采用逆转录聚合酶链反应和免疫组化法,观察溃疡自愈过程中大鼠胃黏膜内HDC和H+,K+-ATP酶mRNA及蛋白表达的动态变化。结果制模术后1d大鼠胃体出现明显溃疡,3d溃疡最为明显,12d溃疡基本愈合。胃黏膜内HDC和H+,K+-ATP酶mRNA表达在制模术后1d即开始降低,术后9d恢复正常。胃黏膜内HDC和H+,K+-ATP酶阳性细胞率及胞质平均灰度值在制模术后也出现降低,术后6d达到最低,术后12d基本恢复正常。结论在胃溃疡自愈过程中,胃黏膜内HDC和H+,K+-ATP酶表达下调,其作用是抑制胃酸分泌以促进溃疡愈合。

Effects of the myeloperoxidase 463 gene polymorphisms on development of atrophy in H pylori infected or noninfected gastroduodenal disease

AIM： To investigate the relationship between myeloperoxidase polymorphisms as a host-related factor and atrophy caused by H pylori. METHODS： Our study enrolled 77 patients. Biopsy materials obtained during gastrointestinal endoscopies were evaluated for the presence of H pylori. Polymerase chain reaction-restriction fragment length polymorphism assay was used to characterize myeloperoxidase genothpes. RESULTS： Forty four patients （57.1%） were lip （＋） and 33 （42.9%） were Hp （-）. Sixty six （85.7%） had GG genotype, 10 （12.9%） had GA genotype and 1 （1.29%） had AA genotype. The change in atrophy in relation to neutrophil infiltration was significant in Hp （＋） patients （P = 0.0001）. The change in atrophy in relation to neutrophil infiltration in patients with GG genotype was significant （P = 0.002）. However, the change in atrophy in relation to neutrophil infiltration was not significiant in patients with Hp （＋） GG genotype （r = 0.066, P = 0.63）. CONCLUSION： Myeloperoxidase genotype is critical for development of atrophy in relation to the severity of inflammation. However, it is interesting to note that, H pylori does not show any additive effect on development of atrophy.

消化性溃疡HP阴性和阳性状态下相关病因及胃粘膜组织学变化的研究

探讨消化性溃疡(PU)患者HP(-)及(+)状态下相关病因和胃粘膜组织病变。方法:139例内镜确诊的PU患者,胃溃疡48例,十二指肠溃疡79例,复合性溃疡12例。胃镜下取胃窦组织4块,分别作组织病理学检查和快速尿素酶检测。结果:122例(87.8％)HP(+),17例(12.2％)HP(-)。HP(+)PU HP感染仍为首要病因之一,因镜下粘膜病损多发生于胃角、小弯及球部,HP(-)PU病因则多达两个以上,内镜下病变亦较HP(+)者更为多样化。本组HP(-)PU病因依次:眼用NSAID(35.3％);伴随其他疾病(29.5％);曾服抗生素或H-2受体阻滞剂(29.4％);应激因素(5.8％)等。无论HP(-)或(+),PU患者病理组织学所表现的固有膜内淋巴细胞、单核细胞等慢性炎细胞浸润现象且无显著性差异。但胃窦粘膜的急性炎性反应Hp(+)者较HP(-)者有显著性差异(P<0.001)。结论:虽然HP(-)和PU(+)共同的发病机理仍为胃粘膜“保护性屏障”与“侵袭性”腔内因子之间的平衡失调,但两者在发病过程中的致病因子及组织形态学表现亦有差异。由此提示,对PU治疗的关键应在于针对不同病因选择相应的治疗方案。

Microbial Diversity in Patients with Gastroduodenal Diseases

H. pylori infection is mainly spread in the kind of gastroduodenal diseases: chronic gastritis, peptic ulcer disease, MALT-lymphoma, gastric cancer. According to certain literature, the mentioned bacterium causes diseases of other visceral organs of humans. Study of the aggravating impact of this infection is under the attention of the scientists. However, other infectious agents, including fungi, other bacteria, parasites, and viruses and their role in different gastroduodenal diseases are not studied enough. The aim of our study was to identify mucous (parietal) gastroduodenal microflora in patients with different diseases of this zone. 390 patients with chronic gastritis (CG), peptic ulcer diseases (PUD) and gastric cancer (GC) were included in the study. The resection materials and biopsy specimens were taken during the operation or endoscopy procedures. Identification of strains H. pylori, Candida spp and others was performed by established methods, on the basis of morphological, tinctorial, cultural and biochemical properties. Microflora of patients with different gastroduodenal diseases is diverse enough. It is represented by facultative, obligate anaerobes, microaeropilic bacteria. More frequently, there were H. pylori and Candida sp, as well as in associations and monocultures. The obtained results confirmed the wide distribution of H. pylori and Candida spp and their frequent coexistence in patients with gastric cancer, chronic gastritis and peptic ulcer disease. Microflora of patients with CG and GC was represented on 11 species. Microflora of patients with PUD-13 species was more diverse.

活动性胃溃疡及幽门螺杆菌与中医毒热证的关联研究

目的:探讨消痈溃得康颗粒对胃溃疡活动期患者幽门螺杆菌的影响,反证"毒热"为胃溃疡活动期的病因,幽门螺杆菌为"毒热"病因要素的生物学基础。方法:选取胃溃疡活动期符合中医胃毒热证患者300例,采用随机对照双盲双模拟试验研究方法,治疗组150例口服消痈溃得康颗粒加溃疡胶囊模拟剂,对照组150例口服溃疡胶囊加消痈溃得康颗粒模拟剂,6周后,采用快速尿素酶法试验测定幽门螺杆菌的根除率及中医症状积分变化,进行统计分析。结果:治疗组脱落8例,对照组脱落6例。治疗前后两组幽门螺杆菌的分级量化评分有统计学差异(P<0.01);胃脘灼痛,痛势较剧,泛酸嘈杂,口干及口苦记分两组治疗前比较,差异均无统计学意义(P>0.05);胃脘灼痛,痛势较剧,泛酸,嘈杂,口干及口苦的改善治疗后两组间记分差异有统计学意义,治疗组优于对照组(P<0.01)。综合疗效:符合方案集(PPS):治疗组临床痊愈率为45.1%(64/142),总有效率为99.3%(141/142);对照组分别为6.9%(10/144),91.0%(131/144),两组比较,差异有统计学意义(P<0.01);全分析集(FAS):治疗组临床痊愈率为42.7%(64/150),总有效率为94.0%(141/150);对照组分别为6.7%(10/150),87.3%(131/150),两组比较,差异有统计学意义(P<0.05)。结论:清热解毒、消痈生肌之消痈溃得康颗粒可以有效根除胃溃疡活动期患者幽门螺杆菌,显著改善中医症状,从而达到治疗胃溃疡的目的,且疗效优于对照组,以效测证,反证了"毒热"确为胃溃疡活动期的重要病因,幽门螺杆菌为"毒热"病因要素的重要生物学基础之一。

水浸束缚应激大鼠胃壁细胞形态和泌酸功能的研究

背景应激性溃疡(SU)是临床危重疾病的常见并发症,通常认为胃黏膜缺血是SU的主要发病机制,而胃酸则在此基础上起重要作用,但胃酸在SU发病中的确切作用尚未完全阐明。目的研究水浸束缚应激(WRS)大鼠胃壁细胞形态和泌酸功能的变化,以进一步阐明胃酸在SU发病中的作用。方法将15只Sprague鄄Dawley大鼠随机分为WRS2h组、WRS4h组和正常对照组,予相应处理后测定胃液pH值,处死大鼠,评估胃黏膜溃疡指数(UI),以免疫荧光技术标记H+/K+鄄ATP酶后用激光共聚焦扫描显微镜观察壁细胞形态并进行分类和计数。分析胃液pH值与胃黏膜UI和分泌期壁细胞数之间的关系。结果WRS2h组和WRS4h组的胃液pH值均较正常对照组显著降低(P<0.01),两组WRS组之间则无显著差异。WRS2h组和WRS4h组的胃黏膜UI和分泌期壁细胞(网格样细胞)数均显著高于正常对照组(P<0.01),其中WRS4h组显著高于WRS2h组(P<0.01)。正常对照组的胃液pH值与分泌期壁细胞数呈负相关(r=-0.81,P<0.05),WRS组的胃液pH值与胃黏膜UI和分泌期壁细胞数均呈负相关(r=-0.85,P<0.05;r=-0.89,P<0.05)。结论WRS大鼠的胃酸分泌与胃黏膜UI和分泌期壁细胞数呈正相关,从细胞学水平证明胃酸增高在SU的形成中起重要作用。

选择性COX-2抑制剂对实验性大鼠胃溃疡愈合及胃酸分泌的影响

目的明确选择性环氧合酶-2(COX-2)抑制剂对实验性大鼠胃溃疡愈合的影响,并从胃酸分泌的角度探讨其延缓胃溃疡愈合的机制。方法以乙酸性大鼠胃溃疡模型为基础,观察选择性COX-2抑制剂塞来昔布对胃溃疡愈合的影响及其对胃液总酸度、H+,K+-ATP酶mRNA和蛋白表达及壁细胞形态的影响。结果制模术后第9日,生理盐水组和塞来昔布组的溃疡面积(mm2)分别为11.9±3.1和19.7±3.8(P<0.01);制模术后第6日和第9日,塞来昔布组胃液总酸度和H+,K+-ATP酶mRNA和蛋白表达水平均显著高于生理盐水组,而两组壁细胞的分泌小管和微绒毛数量则均无明显差异。结论选择性COX-2抑制剂能显著延缓实验性大鼠胃溃疡的愈合过程,其延缓胃溃疡愈合的机制之一可能是通过刺激壁细胞胃酸分泌,加强了对溃疡底部新生肉芽组织的消化作用。

幽门螺杆菌相关性胃溃疡与胃癌中NF-κB、TFF3的表达及意义

目的探讨核转录因子-κB(NF-κB)和三叶因子3(TFF3)在胃溃疡和胃癌中表达的意义,以及与幽门螺杆菌(H.pylori)感染的关系。方法胃溃疡组(GU)60例,胃癌组(GC)70例,应用免疫组化方法测定TFF3和NF-κBp65的表达,同时检测H.pylori感染情况。结果 GC中NF-κBp65和TFF3表达水平均高于GU(P<0.01)。GC中NF-κBp65表达与TFF3表达呈显著正相关(r=0.350,P=0.003)。GU中H.pylori阳性病例中NF-κBp65、TFF3表达显著高于H.pylori阴性病例(P均<0.05)。H.pylori感染病例中,GC组的NF-κBp65、TFF3表达水平均比GU组高(P均<0.05);H.pylori阴性病例中,GC组的NF-κBp65、TFF3表达水平亦均比GU组高(P均<0.01)。结论 NF-κBp65和TFF3的高表达与胃癌的发生发展有着密切的关系,二者可能存在协同作用。H.pylori感染可以上调宿主胃黏膜NF-κBp65和TFF3的表达,表达的差异与胃溃疡和胃癌两种不同疾病转归相关。

姜黄素对大鼠实验性胃溃疡作用的研究

目的探讨姜黄素对大鼠实验性胃溃疡的作用及机制。方法将40只大鼠随机分为4组,即正常对照组、溃疡模型组、姜黄素组、奥美拉唑组。采用水浸-束缚(WRS)方法建立大鼠胃溃疡模型,检测各组胃黏膜溃疡指数(UI)、胃液pH值、壁细胞H+,K+-ATP酶活性和mRNA基因表达,采用SPSS13.0软件进行统计学分析。结果与正常对照组相比,溃疡模型组UI明显升高(P<0.01),胃液pH值明显下降(P<0.01),壁细胞H+,K+-ATP酶活性和mRNA基因表达明显升高(P<0.01);与溃疡模型组相比,姜黄素组UI明显下降(P<0.01),胃液pH值明显上升(P<0.01),壁细胞H+,K+-ATP酶活性和mRNA基因表达明显下降(P<0.01);姜黄素组与奥美拉唑组相比差异无统计学意义(P>0.05)。结论姜黄素可有效抑制胃溃疡模型大鼠胃壁细胞H+,K+-ATP酶活性和mRNA基因表达,减少胃酸分泌,减轻胃黏膜损伤,对胃溃疡有良好的防治作用。

颅脑损伤大鼠胃壁细胞形态和泌酸功能的变化

目的研究颅脑损伤(braininjury,BI)大鼠胃壁细胞形态和泌酸功能的变化。方法采用液压打击法建立BI大鼠模型。大鼠随机分为对照组、BI4h及8h组,测定胃液pH值、胃溃疡指数(ulcerindex,UI),用免疫荧光技术标记H+/K+ATP酶后在激光共聚焦扫描显微镜下观察壁细胞形态并分类、计数,比较胃液pH与UI及分泌期壁细胞数的关系。结果BI4h组胃液pH值为1.71±0.18,显著低于对照组的2.60±0.31,BI8h组胃液pH值为2.16±0.17,与对照组差异显著,和BI4h组相比无显著差异;BI4h组UI为15.80±3.27,显著高于对照组,BI8h组UI达29.80±2.17,高于BI4h组;BI4h组分泌期壁细胞数(115.6±5.98)/200,BI8h组为(133±8.12)/200,均显著高于对照组的(86.2±7.23)/200,胃液pH值与胃UI及分泌期壁细胞数均无明显相关。结论BI后胃酸分泌增加,胃液pH值不能完全反映壁细胞泌酸功能。

幽门螺杆菌感染对延缓乙酸诱导大鼠胃溃疡愈合的实验研究

本工作旨在观察幽门螺秆菌（Ｈｅｌｉｃｏｂａｃｔｅｒｐｙｌｏｒｉ，ＨＰ）感染对大鼠乙酸性胃溃疡愈合的影响。实验发现，大鼠发生乙酸性溃疡后，一次性接种ＨＰ几乎使所有大鼠感染，并引起胃溃疡的自然愈合明显减慢；组织学和生化检测观察到ＨＰ组大鼠胃溃疡病灶处有更多炎症细胞浸润，以中性粒细胞为主，未受溃疡累及的胃窦和胃后壁粘膜也有炎症细胞浸润；免疫组化研究发现ＨＰ组胃粘膜出现较多的ＩＬ－８阳性细胞；此外发现ＨＰ组胃粘膜ＢｒｄＵ标记细胞显著减少，既粘膜上皮的再生减慢。结果提示，ＨＰ感染延缓乙酸性溃疡的愈合，后者与ＨＰ感染后增加ＩＬ－８表达所诱导更强的炎症反应和粘膜细胞再生减慢有关。

太白楤木总皂苷对无水乙醇致大鼠胃溃疡的预防作用

目的观察太白楤木总皂苷(TSAT)对无水乙醇诱导大鼠胃溃疡的预防作用。方法将36只SD大鼠随机分成空白组、模型组、胃康灵组以及低、中、高剂量TSAT组,每组6只。空白组和模型组大鼠均给予生理盐水灌胃,胃康灵组大鼠给予胃康灵胶囊(0. 5 g/kg)灌胃,低、中、高剂量TSAT组大鼠分别给予3、6、12 g/kg TSAT灌胃。末次给药1 h后,除空白组外,其余各组均予10 ml/kg无水乙醇灌胃造模。1 h后,观察各组大鼠胃黏膜大体形态及组织形态学,检测胃液pH值及胃黏膜组织中H^+-K^+-ATP酶活性。结果模型组大鼠胃黏膜呈深红色,肿胀,纵行皱襞可见条索样出血。各剂量TSAT组大鼠胃黏膜出血及损伤程度较模型组减轻。模型组胃液pH值高于空白组(P <0. 05),胃康灵组、中剂量及高剂量TSAT组胃液pH值均低于模型组(均P <0. 05)。模型组胃黏膜组织H^+-K^+-ATP酶活性低于空白组(P <0. 05),胃康灵组及各剂量TSAT组胃黏膜组织H^+-K^+-ATP酶活性均高于模型组(均P <0. 05)。结论 TSAT对无水乙醇致大鼠胃溃疡具有良好的预防作用,其黏膜保护作用可能与提高壁细胞膜H^+-K^+-ATP酶活性、恢复胃液pH值有关。