环氧化酶-2在胃癌和胃炎中的表达及其与幽门螺杆菌感染的关系

目的探讨环氧化酶-2（Cyclooxygense-2，COX-2）在胃癌和胃炎中的表达及其与幽门螺杆菌（Helicobacter pylori，Hp）感染的关系，为胃癌的预防和治疗提供有价值的实验和理论依据。方法采用免疫组化技术检测COX-2、Hp在胃癌以及各型胃炎中的表达。结果胃癌和萎缩性胃炎伴不典型增生组织中COX-2的表达率明显高于浅表性胃炎（P〈0.05），COX-2在Hp感染阳性萎缩性胃炎伴不典型增生病人中的表达率明显高于Hp感染阴性组（P〈0．05），高、中分化胃癌COX-2表达率高于低分化胃癌（P〈0．05）。结论COX-2在胃癌组织中存在过表达，Hp感染可使萎缩性胃炎伴不典型增生组织中COX-2表达增强，COX-2表达与胃癌分化程度有关。     

幽门螺杆菌感染的萎缩性胃炎和胃癌组织中MIF的表达

目的检测幽门螺杆菌(Helicobacter pylori,H.pylori)阳性的萎缩性胃炎和胃癌组织中巨噬细胞移动抑制因子(macro-phage migration inhibitory factor,MIF)的表达,探讨MIF表达和H.pylori感染与萎缩性胃炎和胃癌发病机制的可能联系。方法收集萎缩性胃炎和胃癌组织各60例为实验组,正常胃黏膜25例为对照组,用快速尿素酶试验、Warthin-Starry银染色法和14C呼气试验检测两组患者的幽门螺杆菌感染,用免疫组化和原位杂交技术检测两组组织中MIF和MIF mRNA的表达。结果萎缩性胃炎H.pylori阳性41例,其中MIF和MIF mRNA表达阳性分别为38例和37例,阳性率分别为92.7%和90.2%。胃癌组织中H.pylori阳性55例,其中MIF和MIF mRNA表达阳性分别为52例和51例,阳性率分别为94.5%和92.7%,以上结果与对照组比较,存在显著性差异(P0.001)。结论 MIF表达和H.pylori感染可能与萎缩性胃炎和胃癌的发生有一定的联系。     

疣状胃炎、胃癌组织中幽门螺杆菌感染与p53、p21蛋白表达

目的 探讨疣状胃炎与幽门螺杆菌（HP）及胃癌的相关性.方法 对经胃镜确诊的疣状胃炎41例、慢性浅表性胃炎21例、胃癌20例患者进行p21、p53蛋白及HP检测.结果 疣状胃炎、胃癌组HP感染率分别为60.98%和60%（P＞0.05）,均高于慢性浅表性胃炎组28.57%（P＜0.05）;p21蛋白在胃癌及疣状胃炎组中的表达率分别为45%和39%（P＞0.05）,均高于慢性浅表性胃炎组0%（P＜0.05）;p53在胃癌及疣状胃炎组中的表达率为55%和24.4%（P＜0.05）,均高于慢性浅表性胃炎组0%（P＜0.05）;疣状胃炎组HP感染阳性者中p53、p21表达阳性率分别为40%和56%,均显著高于HP感染阴性组（P＜0.05）.结论 HP感染与疣状胃炎发病相关.HP感染、ras基因激活、野生型p53基因突变参与了疣状胃炎向胃癌转化的过程.     

蒙古沙土鼠幽门螺杆菌感染性胃炎和胃癌模型

幽门杆菌（Ｈｐ）感染蒙古沙土鼠胃炎模型的病理改变可出现萎缩、肠化、溃疡和异型增生,与其他动物模型相比其与人的慢性胃炎更相似,近年来单独用Ｈｐ感染诱发胃癌成功,是Ｈｐ研究史上的重大事件。本综述造模条件、影响因素及模型胃的组织学特点。     

胃癌中幽门螺杆菌感染与癌基因蛋白表达及凋亡

目的　研究幽门螺杆菌 (Hp)感染的胃癌 (GC)发展过程中c met蛋白表达与细胞凋亡的关系及对胃癌预后的意义。方法　对 14 5例经病理证实的不同胃粘膜病变采用免疫组化法检测c met基因表达及Warthin starry法检测Hp感染。采用原位末端标记法 (TUNEL)检测细胞凋亡。结果　在浅表性胃炎 (CSG)、萎缩肠化生胃炎 (CAG +IM )、异型增生 (DYS)、早期GC和进展期GC中 ,c met基因表达率分别为 2 5 .5 3 %、5 1.2 8%、6 1.5 4%、6 6 .6 7%和 6 8.42 % ,CAG +IM、DYS、GC的c met基因表达率均显著高于CSG (P <0 .0 5 )。凋亡指数 (AI)分别为( 4 .5 5± 2 .33) %、( 6 .43± 5 .6 0 ) %、( 6 .45± 5 .12 ) %、( 6 .5 5± 4.80 ) %和 ( 8.84± 5 .6 3) % ,进展期GC显著高于CSG(P <0 .0 5 )。胃粘膜凋亡指数与c met表达强度密切相关 (P <0 .0 5 )。c met阳性表达与胃癌组织类型、浆膜浸润和淋巴结转移密切相关 ,而且BorrmannⅣ明显高于早期胃癌和BorrmannⅠ ,Ⅱ (P <0 .0 5 )。Hp阳性者 5年生存期显著短于Hp阴性者。 结论　Hp感染和c met表达与胃粘膜增殖和恶化有关 ,且与凋亡有相关性。Hp感染与胃癌预后有关。     

胃幽门螺杆菌感染与胃癌：胃癌低发和高发区胃镜调查对照

我们在胃癌低发区和广州和高发区兰州市各选一间医院，对同月接受胃镜检查的全部病人进行活检组织学，幽门螺杆菌尿素酶法检测。结果显示兰州市胃癌和胃溃疡检出率高，该地区慢性胃炎病人ＨＰ感染病高，感染年龄提前，胃炎的组织学模式也有特点，即胃炎多犯及全胃，胃粘膜萎缩发生率高。     

幽门螺杆菌感染相关胃炎

幽门螺杆菌感染相关胃炎陈希陶幽门螺杆菌（Ｈｅｌｉｃｏｂａｃｔｅｒｐｙｌｏｒｉ，Ｈｐ）感染人体胃粘膜后，引起胃及十二指肠粘膜炎症。Ｈｐ感染引起的胃炎是发病率最高的消化道疾病，在世界某些地区及发展中国家的人群中发病率尤高。西方某些发达国家的５０岁以上人群...     

环氧化酶-2在胃癌和胃炎中的表达及其与幽门螺杆菌感染的关系

目的探讨环氧化酶-2(COX-2)在胃癌和胃炎中的表达及其与幽门螺杆菌(Helicobater pylori,HP)感染的关系,为胃癌的预防和治疗提供有价值的实验和理论依据。方法2004年11月至2005年4月中国医科大学附属第一医院门诊胃镜活检标本共128例,采用免疫组化技术检测COX-2在胃癌以及各型胃炎中的表达情况。结果胃癌和萎缩性胃炎伴不典型增生组织中COX-2的表达率明显高于浅表性胃炎(P<0.05),COX-2在萎缩性胃炎伴不典型增生HP感染阳性患者中的表达率明显高于HP感染阴性患者(P<0.05),高、中分化胃癌COX-2表达率高于低分化胃癌(P<0.05)。结论COX-2在胃癌组织中存在过表达,HP感染可使萎缩性胃炎伴不典型增生组织中COX-2表达增强,COX-2表达与胃癌分化程度有关。     

蒙古沙土鼠幽门螺杆菌感染性胃炎和胃癌模型

幽门螺杆菌(Hp)感染蒙古沙土鼠胃炎模型的病理改变可出现萎缩、肠化、溃疡和异型增生,与其他动物模型相比其与人的慢性胃炎更相似,近年来单独用Hp感染诱发胃癌成功,是Hp研究史上的重大事件。本文综述造模条件、影响因素及模型胃的组织学特点。     

幽门螺杆菌感染与慢性胃炎及胃癌关系研究进展

胡伏莲教授从幽门螺杆菌 (ｈｅｌｉｃｏｂａｃｔｅｒｐｙ ｌｏｒｉ,Ｈｐ)的发现至现在已超过 17年的历史 ,Ｈｐ的研究一直是胃肠病工作者的热门课题。有关Ｈｐ与上胃肠道疾病之间关系受到消化界和微生物学家的极大关注。Ｈｐ的出现使慢性胃炎和消化性溃疡面临着一场发病学和治疗学上的革命。目前已经确认Ｈｐ与上胃肠道疾病中的4种疾病密切相关 :①慢性胃炎 ;②消化性溃疡 ;③胃癌 ;④胃粘膜相关淋巴样组织 (ＭＡＬＴ)恶性淋巴瘤。而Ｈｐ与胃癌关系的研究则是热点中的重点。世界卫生组织已将Ｈｐ列入Ⅰ类致癌因子 ,因而关于Ｈｐ与胃癌的研究…     

Histological analysis of gastritis and Helicobacter pylori infection in patients with early gastric cancer: a case-control study

BACKGROUND AND AIMS: Infection with Helicobacter pylori is associated with an increased risk of gastric adenocarcinoma. However, most patients with H. pylori infection will not develop gastric cancer. The aims of the present study were to examine which histological features, including H. pylori infection, would increase the risk of gastric cancer using a case-control study. METHODS: Three gastric biopsy specimens were taken from 72 patients with early gastric cancer and 72 age- and sex-matched control subjects. The grade of gastritis was examined according to the updated Sydney System. The presence of H. pylori infection was determined by serology and histology. Odds ratio (OR) of developing gastric cancer was calculated for H. pylori positivity and histological features using conditional logistic regression. For patients with H. pylori infection, histological features in cancer patients and control subjects were compared. RESULTS: The OR of the presence of mononuclear cell infiltration in the corpus and intestinal metaplasia in the angulus were significantly elevated. The grade of mononuclear cell infiltration in the corpus and antrum was significantly higher in both types of cancer patients than controls. Glandular atrophy and intestinal metaplasia were increased in patients with intestinal-type cancer in the angulus and antrum. Bacterial density in the corpus and polymorphonuclear cell infiltration in the antrum were increased in patients with diffuse-type cancer. CONCLUSIONS: Severe chronic gastritis induced by H. pylori infection seems to be associated with diffuse-type gastric cancer. Glandular atrophy and intestinal metaplasia, which occur in gastric mucosa with chronic inflammation, are significantly associated with intestinal-type cancer.     

Helicobacter pylori infection and gastric function in patients with fundic atrophic gastritis

In the present study we evaluated the relation among histology, H. pylori, IgG to H. pylori, gastric emptying, and acid secretion in 43 patients with fundic atrophic gastritis. On the basis of gastric acid secretion, patients were divided into three subgroups: patients with preserved acid secretion (Group 1), patients with hypochlorhydria (Group 2), and patients with achlorhydria (Group 3). Fundic glandular atrophy was more severe in hypoachlorhydric patients than in those with preserved acid secretion (P < 0.05 vs Group 2, P < 0.005 vs Group 3). H. pylori colonization was found in 94% of patients in Group 1, in 61% of patients in Group 2, and in only 8% of patients in Group 3 (P < 0.001 vs Group 1, P < 0.05 vs Group 2). Conversely, serological positivity to H. pylori was high in all three subgroups of patients (100% in Group 1, 77% in Group 2, 92% in Group 3). Gastric emptying was delayed in atrophic patients, particularly in those with hypoachlorhydria. Our data suggest that fundic atrophic gastritis represents a possible end stage of H. pylori infection, characterized by a progressive disappearance of the bacterium and a progressive deterioration of gastric functions.     

Helicobacter pylori and gastric cancer

Abstract This review focuses on the similarities between the epidemiology of gastric cancer and the epidemiology of Helicobacter pylori. Their demographic patterns and the results of studies regarding familial and environmental risk factors are described. The association of gastric cancer and H. pylori infection with both gastric ulcer and chronic atrophic gastritis is also characterized and the possibility that a H. pylori infection could lead to gastric cancer is discussed.     

慢性萎缩性胃炎黏膜上皮中P53和C-erbB-2表达的临床意义

目的:探讨慢性萎缩性胃炎(CAG)黏膜上皮中P53及C-erbB-2的表达及意义．方法:用免疫组化技术(SP法)检测正常胃黏膜56例、慢性萎缩性胃炎429例(腺体囊性扩张61例,大肠型化生73例,轻、中、重度不典型增生各120、91和84例)和早期胃癌57例中P53和C-erbB-2的表达,分析P53和C-erbB-2表达及其与CAG胃黏膜病变类型的关系．结果:正常胃黏膜,囊性扩张腺体,轻、中度不典型增生,大肠型化生,重度不典型增生,早期胃癌P53和C-erbB-2表达的阳性率呈上升趋势．前三组间表达率差异无统计学意义(P>0．05);正常胃黏膜与中度不典型增生、大肠型化生、重度不典型增生及胃癌组P53和C-erbB-2的表达差异有统计学意义(P<0．01)．Spearman等级相关分析显示P53和C-efbB-2表达呈正相关(r=0．867,P<0．05)．年龄<40岁和≥40岁组间、性别组间P53表达阳性率差异有统计学意义(x2=12．393,P<0．01;x2=8．799, P<0．01)．C-erbB-2的表达在上述年龄组间差异有统计学意义(x2=7．706,P<0．01),而在性别组间无统计学意义(P>0．05)．结论:检测慢性萎缩性胃炎中P53和C-erbB-2的表达,有助于监测CAG癌前病变的进展及胃癌的早期发现．     

C-erbB-2蛋白和缝隙连接蛋白43在胃癌组织中的表达及意义

目的探讨C-erbB-2癌蛋白和缝隙连接蛋白43（connexin,Cx43）在腺型胃癌中的表达并分析其临床意义。方法应用免疫组织化学SP法分别检测C-erbB-2癌蛋白、Cx43在48例腺型胃癌和26例胃炎组织中的表达,并分析其与临床病理参数的关系。结果C-erbB-2癌蛋白、Cx43阳性呈棕黄色颗粒定位于细胞膜或细胞质;C-erbB-2癌蛋白在胃癌中的阳性表达率（50.0%）显著高于胃炎黏膜组织的阳性率（2χ=6.70,P〈0.05）;Cx43在胃癌中阳性率（43.8%）显著低于胃炎黏膜组织的阳性率（χ2=23.03,P〈0.05）;C-erbB-2癌蛋白的表达与胃癌的大小、分化程度及淋巴结转移呈显著相关（2χ=6.00、9.41、5.49,P值均〈0.05）;Cx43蛋白表达降低或缺失同样与胃癌的分化程度及淋巴结转移呈显著相关（χ2=7.49、6.86,P值均〈0.05）;C-erbB-2癌蛋白和Cx43蛋白呈负相关（χ2=0.01,r=-0.378,P〈0.05）。结论C-erbB-2癌蛋白的高表达、Cx43表达降低或缺失与胃癌分化程度、浸润转移密切相关,联合检测C-erbB-2和Cx43有助于判断胃癌的生物学行为。     

Risk of gastric cancer in Helicobacter pylori infection in a 15-year follow-up

Objective: We investigated the risk of gastric cancer among men with Helicobacter pylori (H. pylori) infection or atrophic gastritis (AG) in a 15-year follow-up.

Materials and methods: Study population consists of 12,016 men aged 50–65 years at the beginning of the follow-up in 1994–1996. Serum levels of pepsinogen I (SPGI) and antibodies (IgG) to H. pylori (HpAb) were assayed from serums collected in 1994–1996. Incidence of gastric cancer in the study population was assessed in follow-up from 1994 to 2011 by data from the nationwide cancer registry. Based on SPGI and HpAb values, standardized incidence ratios (SIRs) of gastric cancer were calculated in three subgroups, that is, in those with a healthy stomach, those with H. pylori infection but without AG and those with AG. Risk ratios (RR) of gastric cancer were calculated using SIR of subgroups.

Results: During 15 years, seven gastric cancers appeared per 79,928 person years among men with healthy stomachs, 50 cancers per 92,533 person years in men with H. pylori infection but without AG, and 8 per 8658 person years in men with AG. Risk ratio (RR) of stomach cancer in men with H. pylori infection was 5.8 (95%CI: 2.7–15.3) compared to men with healthy stomachs, and 9.1 (95%CI: 2.9–30.0) in men with AG. There were no differences in cancer risk between cardia and distal stomach.

Conclusions: Risk of gastric cancer is low in men with healthy stomachs. It is significantly increased in those with H. pylori infection and more in those with AG.     

Helicobacter pylori infection, glandular atrophy and intestinal metaplasia in superficial gastritis, gastric erosion, erosive gastritis, gastric ulcer and early gastric cancer

AIM: To evaluate the histological features of gastric mucosa, including Helicobacter pylori infection in patients with early gastric cancer and endoscopically found superficial gastritis, gastric erosion, erosive gastritis, gastric ulcer. METHODS: The biopsy specimens were taken from the antrum, corpus and upper angulus of all the patients. Giemsa staining, improved toluidine-blue staining, and Hpylori-specific antibody immune staining were performed as appropriate for the histological diagnosis of H pylori infection. Hematoxylin-eosin staining was used for the histological diagnosis of gastric mucosa inflammation, gastric glandular atrophy and intestinal metaplasia and scored into four grades according to the Updated Sydney System. RESULTS: The overall prevalence of H pylori infection in superficial gastritis was 28.7%, in erosive gastritis 57.7%, in gastric erosion 63.3%, in gastric ulcer 80.8%, in early gastric cancer 52.4%. There was significant difference (P<0.05), except for the difference between early gastric cancer and erosive gastritis. H pylori infection rate in antrum, corpus, angulus of patients with superficial gastritis was 25.9%, 26.2%, 25.2%, respectively; in patients with erosive gastritis 46.9%, 53.5%, 49.0%, respectively; in patients with gastric erosion 52.4%, 61.5%, 52.4%, respectively; in patients with gastric ulcer 52.4%, 61.5%, 52.4%, respectively; in patients with early gastric cancer 35.0%, 50.7%, 34.6%, respectively. No significant difference was found among the different site biopsies in superficial gastritis, but in the other diseases the detected rates were higher in corpus biopsy (P<0.05). The grades of mononuclear cell infiltration and polymorphonuclear cell infiltration, in early gastric cancer patients, were significantly higher than that in superficial gastritis patients, lower than that in gastric erosion and gastric ulcer patients (P<0.01); however, there was no significant difference compared with erosive gastritis. The grades of mucosa glandular atrophy and intestinal metaplasia were significantly highest in early gastric cancer, lower in gastric ulcer, the next were erosive gastritis, gastric erosion, the lowest in superficial gastritis (P<0.01). Furthermore, 53.3% and 51.4% showed glandular atrophy and intestinal metaplasia in angular biopsy specimens, respectively; but only 40.3% and 39.9% were identified in antral biopsy, and 14.1% and 13.6% in corpus biopsy; therefore, the angulus was more reliable for the diagnosis of glandular atrophy and intestinal metaplasia compared with antrum and corpus (P<0.01). The positivity rate of glandular atrophy and intestinal metaplasia of superficial gastritis with H pyloripositivity was 50.7%, 34.1%; of erosive gastritis 76.1%, 63.0%; of gastric erosion 84.8%, 87.8%; of gastric ulcer 80.6%, 90.9%; and of early gastric cancer 85.5%, 85.3%, respectively. The positivity rate of glandular atrophy and intestinal metaplasia of superficial gastritis with H pylorinegativity was 9.9%, 6.9%; of erosive gastritis 42.5%, 42.1%; of gastric erosion 51.1%, 61.9%; of gastric ulcer 29.8%, 25.5%; and of early gastric cancer 84.0%, 86.0%, respectively. The positivity rate of glandular atrophy and intestinal metaplasia of superficial gastritis, erosive gastritis, gastric erosion, and gastric ulcer patients with H pylon positivity was significantly higher than those with H pylori negativity (P<0.01); however, there was no significant difference in patients with early gastric cancer with or without H pylori infection. CONCLUSION: The progression of the gastric pre-cancerous lesions, glandular atrophy and intestinal metaplasia in superficial gastritis, gastric erosion, erosive gastritis and gastric ulcer was strongly related to H pylori infection. In depth studies are needed to evaluate whether eradication of H pylori infection will really diminish the risk of gastric cancer.     

Screening of atrophic gastritis and gastric cancer by serum pepsinogen, gastrin-17 and Helicobacter pylori immunoglobulin G antibodies

OBJECTIVE: Currently the screening and diagnosis of gastric cancer and atrophic gastritis are mainly made by endoscopy and biopsy. The aim of this study was to evaluate the use of serum tests: serum pepsinogen I (PGI pepsinogen I/II ratio (PGR), gastrin‐17 (G‐17) and H. pylori‐immunoglobulin G (IgG) antibodies to screen atrophic gastritis and gastric cancer. METHODS: A total of 458 patients were recruited, and each underwent endoscopy with biopsies before the serum tests were performed. These patients were divided into five groups based on the endoscopic and histological findings: 92 patients in the atrophic gastritis group, 58 in the gastric ulcer group, 90 in the duodenal ulcer group, 141 in the gastric cancer group (40 early gastric cancer and 101 advanced gastric cancer) and 77 (including mild non‐atrophic gastritis) served as a control group. Serum samples for PGI and II, G‐17, and H. pylori‐IgG antibodies estimation were analyzed by ELISA. RESULTS: PGI and PGR values decreased significantly both in atrophic gastritis and gastric cancer groups (P < 0.01). For the best discrimination of atrophic gastritis, the cut‐off values of PGI and PGR were 82.3 µg/L and 6.05, respectively. The PGI, PGR and G‐17 values were related significantly with the grades and/or sites of atrophic gastritis (P < 0.01). Patients with atrophic corpus gastritis had low PGI and PGR values and high G‐17 level, and patients with atrophic antral gastritis had low G‐17 level. G‐17 increased significantly in the gastric cancer group (P < 0.01). PGI and PGR values were significantly lower in patients with advanced gastric cancer than in patients with early gastric cancer, while there was no difference in G‐17 level between them. The positivity rate of H. pylori‐IgG antibodies was 54.55% in the control group. The PGI level was higher in H. pylori positive patients than in H. pylori negative ones (P < 0.001), while there was no difference in G‐17 level between them. The positivity rates of H. pylori‐IgG antibodies were over 85% in all other four groups. CONCLUSIONS: Low serum PGI, PGR and G‐17 values are biomarkers of atrophic antral gastritis. Atrophic corpus gastritis can be screened by lower serum PGI, PGR and high G‐17 values. [Correction added after online publication on 2 February 2007: the preceding sentence has replaced one that read ‘Atrophic be screened by serum PGI and PGR values’]. Gastric cancer can be screened on the basis of increased serum G‐17 and remarkedly low serum PGI and PGR values. The H. pylori infection is related to the change of PG level.