抗H.pylori治疗对胆石症患者胆汁H.pylori DNA、PLA-2活性及免疫功能的影响

背景胆石症发病与胆道系统动力学、胆汁成分改变、幽门螺杆菌(Helicobacter pylori,H.pylori)感染等因素有关.H.pylori感染一方面能引起胆汁中磷脂酶A2(phospholipaseA-2,PLA-2)释放增加,可促进胆固醇沉淀,引发结石;另一方面,H.pylori感染可对机体免疫反应产生刺激作用,导致免疫功能下降.胆石症合并H.pylori感染抗H.pylori治疗,能否降低PLA-2活性、改善免疫功能,目前并不确切.本研究初步探讨抗H.pylori治疗与胆汁H.pylori DNA、PLA-2、免疫功能关系.目的探讨胆石症患者实施抗H.pylori治疗对其胆汁H.pyloriDNA、PLA-2活性以及免疫功能的影响.方法选取粤北人民医院2014-06/2018-03因胆石症行经内镜逆行性胰胆管造影术胆总管取石+鼻胆管引流术或外科胆管取石行T管引流术合并H.pylori感染患者80例.通过随机数字法分为两组,40例予以抗H.pylori治疗者为研究组,40例常规施予质子泵抑制剂治疗者为对照组.回顾性对比分析两组胆汁H.pylori DNA转阴率、PLA-2活性、免疫功能变化.结果研究组胆汁H.pylori DNA转阴率为92.50%,较对照组的67.50%高,差异有统计学意义(P<0.05);研究组治疗后PLA-2低于对照组,差异存在统计学意义(P<0.05);两组治疗后免疫球蛋白A、免疫球蛋白M差异无统计学意义(P>0.05);治疗后免疫球蛋白G较治疗前升高,差异有统计学意义(P<0.05),且两组免疫球蛋白G差异有统计学意义(P<0.05);研究组CD4+、CD8+水平优于对照组,差异有统计学意义(P<0.05).结论抗H.pylori治疗可通过提升H.pylori DNA转阴率、降低胆汁PLA-2水平,达到改善患者免疫功能.

幽门螺杆菌对胃癌细胞线粒体DNA编码的细胞色素氧化酶基因表达的影响

背景:既往研究表明胃黏膜细胞核基因组有线粒体DNA(mtDNA)片段整合,且这种整合与幽门螺杆菌(H.pylori)感染有关,并参与胃癌的发生。mtDNA片段与核基因整合后,是否会引起所编码基因表达的改变,这种改变是否与H.pylori感染有关尚不明确。目的:观察H.pylori作用于胃癌细胞后线粒体编码基因细胞色素氧化酶(COX)Ⅰ、COXⅡ和COXⅢmRNA表达的变化,探讨H.pylori致胃癌的分子机制。方法:将6μl/mlH.pylori培养滤液与胃癌细胞分别作用4h、8h和12h,收集细胞,提取RNA,应用逆转录聚合酶链反应(RT-PCR)检测各时间点COXⅠ、COXⅡ和COXⅢmRNA的表达。结果:H.pylori作用4h后,线粒体COXⅠ、COXⅡ和COXⅢmRNA的表达有所降低,8h时下降更明显,12h时段下降速度减缓;除COXⅡ4h时与对照组无差异外,其余各时间点的表达量均显著低于对照组(P<0.05)。结论:H.pylori可引起胃癌细胞线粒体编码基因COXⅠ、COXⅡ和COXⅢmRNA表达下调,影响线粒体的功能。

Effects of bile reflux on gastric mucosal lesions in patients with dyspepsia or chronic gastritis

AIM: To investigate the influences of bile reflux on profiles of gastric mucosal lesions in patients with dyspepsia or chronic gastritis.METHODS: A total of 49 patients diagnosed with dyspepsia and chronic gastritis underwent 24-h ambulatory andsimultaneous monitoring of intragastric bilirubin absorbance and pH values, and then they were divided into bile refluxpositive group and bile reflux negative group. Severity of pathological changes in gastric mucosa including activeinflammation, chronic inflammation, intestinal metaplasia, atrophy and dysplasia as well as Helicobacter pylori (H pylori) infection at the corpus, incisura and antrum were determined respectively according to update Sydney system criteria. The profiles of gastric mucosal lesions in the two groups were compared, and correlations between time-percentage of gastric bilirubin absorbance ＞0.14 and severity of gastric mucosal lesions as well as time-percentage of gastric pH ＞4 were analyzed respectively. RESULTS: Thirty-eight patients (21 men and 17 women, mean age 44.2 years, range 25-61 years) were found existing with bile reflux (gastric bilirubin absorbance ＞0.14) and 11 patients (7 men and 4 women, mean age 46.2 years,range 29-54 years) were bile reflux negative. In dyspepsia patients with bile reflux, the mucosal lesions such as active inflammation, chronic inflammation, intestinal metaplasia, atrophy or H pylori infection in the whole stomach, especially in the corpus and incisura, were significantly more severe than those in dyspepsia patients without bile reflux. Moreover, the bile reflux time was well correlated with the severity of pathological changes of gastric mucosa as well as H pylori colonization in the near-end stomach, especially in the corpus region. No relevance was found between the time of bile reflux and pH ＞4 in gastric cavity. CONCLUSION: Bile reflux contributes a lot to mucosal lesions in the whole stomach, may facilitate H pylori colonization in the corpus region, and has no influence on acid-exposing status of gastric mucosa in patients with dyspepsia or chronic gastritis.

合并幽门螺杆菌感染对儿童原发性胆汁反流性胃炎病情的影响

目的探讨儿童胆汁反流性胃炎(BRG)合并幽门螺杆菌(Hp)感染对病情的影响。方法 151例原发性BRG患儿根据13C尿素呼气试验(UBT)、胃窦黏膜组织Hp快速尿素酶试验(RUT)和病理组织学检查结果分Hp阳性组和Hp阴性组。比较2组临床症状分度、胃镜下胆汁反流分级、活检组织病理学表现及分级Dixon评分。结果 Hp阳性组与Hp阴性组在发病年龄和性别方面比较无显著差异。Hp阳性组就诊时临床症状总体上较Hp阴性组重,以中度以上表现为多见。Hp阳性组胃镜下胆汁反流程度重于Hp阴性组,且与临床症状呈正相关;2组胃黏膜炎症活动性、淋巴滤泡增生、胃小凹增生、黏膜浅层血管扩张方面比较有显著差异,而在炎症程度、间质水肿、固有膜内平滑肌纤维增生、肠化生、腺体萎缩等方面则无显著差异。结论 BRG患儿合并Hp感染时临床症状、胃镜下及组织学表现更重,且胆汁反流程度加重,二者在发病中有协同关系。

影响残胃泌酸功能的相关性因素分析

目的研究胃远端部分切除术后患者泌酸功能及其与黏膜病理改变、胆汁反流和幽门螺杆菌(Hp)感染的相关性。方法采用24hpH监测仪测定51例残胃患者空腹胃内pH值,根据24h胃内平均pH值分为低泌酸组(pH≥3)和正常泌酸组(pH<3)。胃镜观察残胃黏膜以及Hp检测。结果低泌酸组患者35例,其中29例黏膜呈重度萎缩;正常泌酸组16例,其中4例呈重度黏膜炎症(P=0.006)。胆汁反流率在低泌酸组和正常泌酸组分别为37.4%和18.7%(P=0.014)。两组间Hp感染率差异无显著性。62.7%的患者胃酸分泌减少,已接受抑酸药物治疗。结论24h动态胃pH监测可有效评价残胃患者胃黏膜泌酸功能。胆汁反流和残胃炎症程度与黏膜泌酸功能有相关性。约1/3残胃患者保持正常胃酸分泌功能,临床上有大量患者接受了不必要的抑酸治疗。

胃大部切除术式与幽门螺杆菌感染相关性的研究

目的观察BillrothI式和BillrothII式术后、胆汁反流与残胃幽门螺杆菌(HP)感染之间的关系。方法残胃组患者101例,其中BillrothⅠ式58例,BillrothII式43例,同期未手术患者4501例作为对照组。残胃组内又分别根据HP、胆汁反流与否、反流程度分层比较。以快速尿素酶试验法及改良Giemsa染色检测HP。结果残胃组HP感染率(21.79%)显著低于对照组(41.16%),两组之间比较具有统计学意义(p<0.05);BillrothI式组HP感染率为21.43%、BillrothII式组HP感染率为22.22%,两组比较无统计学意义;BillrothI式组胆汁反流阳性率57.14%与BillrothII式组的88.89%相比较具有统计学意义(p<0.001);残胃胆汁反流阳性患者HP感染率为35.44%、胆汁反流阴性患者HP感染率为45.45%,两组比较具有统计学意义(p<0.01);残胃组患者不同程度胆汁反流的HP感染率之间无统计学意义;不同程度胆汁反流的HP现患比均<1.0。结论残胃HP感染率低于未手术者,胆汁反流是HP感染的保护因素,但与HP感染严重程度无线性关系。

携带幽门螺杆菌ureB和IL-2质粒DNA的减毒鼠伤寒沙门菌疫苗构建

目的 构建编码幽门螺杆菌 (Helicobacterpylori,H .pylori)尿素酶B亚单位 (ureB)基因和小鼠IL 2基因以减毒鼠伤寒沙门菌为载体的核酸疫苗 ,体外转染Cos 7细胞 ,鉴定其表达蛋白的免疫性。方法 应用聚合酶链式反应 (PCR)技术从H .pylori标准菌株CCUG1 7874基因组DNA扩增ureB基因 ,从重组质粒 pCIneo IL 2扩增小鼠IL 2基因 ,通过T A克隆分别插入 pUCmT载体 ,检测ureB及IL 2的核苷酸序列 ,通过酶切、连接反应分别克隆入真核表达载体 pIRES ,PCR和酶切反应进行鉴定 ;重组载体 pIRES ureB和 pIRES ureB IL 2转入减毒鼠伤寒沙门菌LB50 0 0 ,抽提质粒 ,再次转入SL72 0 7,反复传代 ,鉴定核酸疫苗载体菌的稳定性。通过脂质体法将重组载体 pIRES ureB和pIRES ureB IL 2转染Cos 7细胞 ,SDS PAGE及Westernblot法检测表达蛋白的免疫性。结果 扩增出长约 1 70 0bp的ureB基因和 51 0bpIL 2 ,测序结果表明 ,扩增出的ureB基因与基因库H .pyloriureB序列一致 ,IL 2序列和小鼠的IL 2序列一致 ,PCR和酶切鉴定结果证实ureB和IL 2基因克隆入真核表达载体 pIRES ,并成功构建了稳定的幽门螺杆菌ureB和IL 2基因以减毒鼠伤寒沙门菌为载体的核酸疫苗 ,并且以Westernblot检测到特异性的相对分子质量 (Mr)为 6 6× 1 0 3的UreB蛋白?