Killing effect of TNF-related apoptosis inducing ligand regulated by tetracycline on gastric cancer cell line NCI-N87

AIM: To clone the cDNA fragment of human TRAIL (TNF-related apoptosis inducing ligand) into a tetracycline-regulated gene expression system, the RevTet-On system, transduce expression vectors into a gastric carcinoma cell line-NCI-N87 and examine the effects of controlled expression of TRAIL in vitro on the gastric carcinoma cells. METHODS: The full-length cDNA of TRAIL was inserted into a vector under the control of the tetracycline-responsive element (TRE) to obtain the plasmid pRevTRE-TRAIL, which was transfected into a packaging cell line PT67. In addition, vector pRev-Tet On and pRevTRE were also transfected into PT67 separately. After hygromycin and G418 selection, the viral titer was determined. The medium containing retroviral vectors was collected and used to transduce a gastric carcinoma cell line NCI-N87. The resulting cell line NCI-N87-Tet On TRE-TRAIL and a control cell line, NCI-N87 Tet On-TRE, were established. TRAIL expression in the cell line was induced by incubating cells with doxycycline (Dox), which is a tetracycline analogue. The killing effect on gastric carcinoma cells was analyzed after induction. RESULTS: The recombinant plasmid pRev-TRE-TRAIL was constructed. After hygromycin or G418 selection, the producer cell lines PT67-TRE, PT67-TRE-TRAIL and PT67-Tet On were obtained,with titers of about 10(8)CFU.L(-1). By transducing NCI-N87 cells with retroviral vectors from these cell lines, stable cell lines NCI-N87-Tet-On TRE-TRAIL (NN3T) and control cell line NCI-N87-Tet-On-TRE (NN2T) were established. The growth curves of the selected cell lines were the same with the wild type NCI-N87. When Dox was added, cell death was obvious in the test groups (29%-77%), whereas no difference was observed in control and wild type cell lines. With the addition of a medium from the test group, human leukemia cell line Jurkat was activated till death (83%), indicating the secretion of active TRAIL proteins from the test cells to the medium. CONCLUSION: With the use of the RevTet-On system, a regulated expression system for TRAIL was constructed. Using this system, the selected killing effect of TRAIL on gastric carcinoma cell line NCI-N87 could be observed.

胃粘膜相关淋巴组织型淋巴瘤形态学研究

目的：研究胃粘膜相关淋巴组织（ＭＡＬＴ）型淋巴瘤及其与胃粘膜套细胞淋巴瘤和滤泡性淋巴瘤的鉴别诊断。方法：应用ＨＥ染色和免疫组化ＡＢＣ法检测胃ＭＡＬＴ型淋巴瘤，内镜作幽门螺杆菌（ＨＰ）培养或尿素试验检测ＨＰ感染。结果：３１例胃ＭＡＬＴ型淋巴瘤中低度恶性２７例，高度恶性４例。细胞类型以ＣＣＬ型最常见。免疫表型以ＩｇＭ为主，缺乏ＩｇＤ。３１例中２８例有ＨＰ感染（占９０．５２％）。结论：①低恶ＭＡＬＴ型淋巴瘤常见到淋巴上皮病变，滤泡性克隆化和反应性滤泡，具有诊断和鉴别诊断价值。②高恶ＭＡＬＴ型淋巴瘤伴有低恶成分。

胃癌及癌前病变中抑癌基因p16表达的意义

目的探讨p16基因在胃癌发生、发展中的重要作用以及在胃癌早期诊断中的意义。方法取胃粘膜由正常经癌前病变到癌不同阶段的手术切除标本,运用原位分子杂交技术检测其中p16基因mRNA的表达。结果 p16基因mRNA在各型胃粘膜中阳性率分别为:正常胃粘膜94.1％,轻、中、重度异型增生分别为93.9％,80.0％,31.3％;小肠型肠化为69.5％,结肠型肠化为21.4％;胃癌为25.0％;其中正常胃粘膜,轻、中度异型增生,小肠型肠化间差异无显著性(P>0.05);结肠型肠化,重度异型增生、胃癌间差异无显著性(P>0.05),而两组间的差异则有显著性(P<0.01)。结论 P16基因的变异在胃癌的发生、发展中起重要作用;重度异型增生、结肠型肠化是一种重要的癌前病变;对异型增生和肠化胃粘膜进行p16基因mRNA检测有助于胃癌的早期诊断和治疗。

慢性浅表性胃炎脾胃湿热证胃粘膜病理、幽门螺杆菌感染及胃粘膜分泌特点

[目的]探讨慢性浅表性胃炎脾胃湿热证与胃粘膜的病理改变、胃粘膜分泌白细胞介素-8(IL-8)、肿瘤坏死因子α(TNF-α)和分泌型免疫球蛋白A(sIgA)、及幽门螺杆菌(HP)感染的关系。[方法]选择55例慢性浅表性胃炎患者为观察对象,其中脾胃湿热证35例,脾虚证20例,并设无临床症状者15例为正常对照组,检测胃粘膜病理组织学改变,观察胃粘膜组织中IL-8、TNF-α和sIgA水平以及HP感染情况。[结果]脾胃湿热证患者的HP感染率、胃粘膜炎症程度要高于脾虚证组和正常组(P<0.05或P<0.01);脾胃湿热证胃粘膜组织中的IL-8、TNF-α要高于脾虚证组(P<0.05或P<0.01),而sIgA却低于脾虚证组(P<0.01);在脾胃湿热证中,HP阳性者的胃粘膜炎症程度明显重于阴性者(P<0.01),且HP阳性者胃粘膜组织中的IL-8、TNF-α要高于阴性者(P<0.05),而sIgA在两组间无显著性差异(P>0.05)。[结论]脾胃湿热证的胃粘膜呈现一种活动性炎症改变,这可能与局部炎症因子(IL-8、TNF-α)分泌增加、防御因子(sIgA)分泌减少有关;而HP感染可能是引起和加重脾胃湿热证内在病理变化的因素之一。

胃窦粘膜TNF-α与胃癌及幽门螺杆菌感染的相关性研究

目的探讨胃窦粘膜肿瘤坏死因子(TNF-α)含量与胃癌及幽门螺杆菌(Hp)感染的相互关系。方法应用放射免疫法(RIA)检查117例接受胃镜检查的患者胃窦粘膜TNF-α含量,并对所有病例进行幽门螺杆菌感染检查。结果117例受检者中,Hp感染者64例(54.7%),GCa患者胃窦粘膜TNF-α明显高于CG组、DU组及组织正常胃粘膜组(P<0.05),GCa和CG组中Hp感染者胃粘膜TNF-α高于非Hp感染者(P<0.05)。结论TNF-α在Hp感染过程中与胃癌的发生发展有关。

胃癌患者胃窦粘膜TNF-α含量的检测及临床意义

目的:探讨胃癌患者胃窦粘膜TNF-α含量与胃癌间关系。方法:应用放射免疫法(RIA)检查92例接受胃镜检查的患者胃窦粘膜TNF-α含量,比较胃癌与非癌性胃十二指肠患者之间的差异。其中胃粘膜正常者5例,单纯性慢性胃炎(CG)30例。十二指肠球部溃疡(DU)35例,胃癌(GCa)22例。结果:GCa患者胃窦粘膜TNF-α明显高于CG组及组织正常胃粘膜(p<0.05),但与DU组比较无明显差别(p>0.05)。结论:TNF-α含量在胃癌患者胃窦部增高,但与DU组比较无明显差别。提示TNF-α与胃癌发生、发展有关,但胃粘膜TNF-α并非胃癌的特异性标志物。

健脾益胃汤治疗慢性萎缩性胃炎的随机对照研究

目的:观察自拟健脾益胃汤治疗慢性萎缩性胃炎的临床效果。方法:选取2017年6月至2018年6月在本院治疗的慢性萎缩性胃炎患者90例,随机分为观察组和对照组,每组45例。对照组给予养胃舒胶囊治疗,观察组给予自拟健脾益胃汤治疗。观察两组患者治疗后临床疗效、幽门螺杆菌(helicobacter pylori,Hp)根除效果以及治疗前后中医证候积分、胃黏膜病理评分、血清炎性因子[肿瘤坏死因子-α(tumor necrosis factor-α,TNF-α)、白细胞介素-1β(interleukin-1β,IL-1β)、白细胞介素-8 (interleukin-8,IL-8)]水平变化情况。结果:观察组有效率97. 78%,Hp转阴率为90. 32%,对照组有效率82. 22%,Hp转阴率为70. 00%,观察组有效率、Hp转阴率高于对照组,差异有统计学意义(P <0. 05);观察组治疗后中医证候积分低于对照组,差异有统计学意义(P <0. 05);观察组治疗后胃黏膜萎缩、肠化生、异型增生评分均低于对照组,差异有统计学意义(P <0. 05);观察组治疗后TNF-α、IL-1β、IL-8水平均低于对照组,差异有统计学意义(P <0. 05)。结论:自拟健脾益胃汤治疗慢性萎缩性胃炎疗效显著,可明显改善患者炎症和胃黏膜状态。

胃粘膜p53抑癌基因异常与癌变的研究

目的系统研究各种胃粘膜病变中ｐ５３抑癌基因的变异和意义．方法内镜活检组织１５４例，其中浅表性胃炎３０例，萎缩性胃炎３３例，萎缩性胃炎伴肠上皮化生３１例，萎缩性胃炎伴异型增生３０例，胃腺癌３０例．用免疫组化法检测Ｐ５３蛋白表达；用单链构象多态性分析及ＤＮＡ测序检测ｐ５３第５～８外显子点突变．结果胃良性病变粘膜未见Ｐ５３蛋白表达．胃癌中Ｐ５３蛋白阳性表达率为３３３％（１０／３０例）．单链构象多态性分析ｐ５３点突变的检出率，在胃癌为５４５％（６／１１例），异型增生为２０％（３／１５例），肠化生为６７％（１／１５例），测序证实１例胃癌在第５外显子存在点错义突变和碱基缺失，２例异型增生在第６外显子存在点错义突变．结论ｐ５３抑癌基因变异与胃粘膜癌变有关．

胃粘膜癌前病变的分子生物学研究

胃粘膜癌前病变的分子生物学研究石雪迎赵凤志Ｓｕｂｊｅｃｔｈｅａｄｉｎｇｓｓｔｏｍａｃｈｎｅｏｐｌａｓｍｓ／ｇｅｎｅｔｉｃｓ；ｇａｓｔｒｉｃｍｕｃｏｓａ／ｐａｔｈｏｌｏｇｙ；ｐｒｅｃａｎｃｅｒｏｕｓｃｏｎｄｉｔｉｏｎｓ／ｇｅｎｅｔｉｃｓ；ｐｒｏｔｏ?..