多巴胺参与P物质对胃肌电活动和胃运动的毒蕈碱抑制效应

我们以前的工作表明尾核注射Ｐ物质能抑制胃肌电快波和胃运动,该效应是通过胆碱能Ｍ受体介导的。本文观察到Ｐ物质的抑胃效应可分别被尾核注射Ｐ物质抗血清、Ｐ物质受体拮抗剂［Ａｒｇ＾６,Ｄ－Ｔｒｉｐ＾７,ＭｅＰｈｅ＾８］－ＳＰ６－１１以及多巴胺Ｄ２受体了民剂氟哌啶醇所消除;尾核注射多巴胺对胃肌电快波和胃运动也有抑制作用,且能被尾核注射氟哌啶醇以及阿托品所阻断。据此,我们高想尾核Ｐ物质可能是通过多巴胺Ｄ２受体     

尾核P物质对胃运动的抑制效应系通过黑质,迷走背核经迷走神经所介导

本工作观察损毁下丘脑外侧区,黑质,迷走背核及其传出神经对尾核微量注射Ｐ物质引起的胃肌电快波和胃运动抑制效应的影响。实验结果：该抑制效应不依赖于下丘脑外侧区的完整但可被损毁黑质,迷走背核或迷走上所消除。用利血平耗竭交感神经递质则不影响该效应。这些结果表明：尾核ＳＰ的抑胃效应系通过黑质、迷走背核经迷走神经所传出。     

P物质尾核微量注射抑制小鼠胃肌电活动和胃运动

本文观察了小鼠尾核微量注射Ｐ物质或乙酰胆碱对胃肌电和胃运动的ｍ影响;并初步探讨了两者作用的关系。用双极康铜导线引导胃窦部肌电;用水囊连接压力换能器记录胃窦部运动。上述信息经生物电放大器和载波放大器放大后,由四道记录仪描记曲线,同时输入微机进行采集、贮存和处理。计算出注药前后每分钟胃肌电快波、慢波和胃运动波的频率和总幅度的变化百分数。结果如下：尾核注射ＳＰ或ＡＣｈ胃电快波和胃运动呈明显的抑制效应。用     

光谱技术研究固氮酶铁硫簇的理化特性

Ｎ－甲基甲酰胺碱度是提取高质量固氮酶铁钼辅基的关键因素之一。过量的亚甲蓝能氧化并分解铁钼铺基为含双钼铁硫簇［Ｍｏ２Ｆｅ＾２＋Ｆｅ５＾３＋Ｓ６］＾－和铁硫簇（［Ｆｅ＾２＋Ｆｅ５＾３＋Ｓ６］＾－。固氮酶铁钼铺基和［Ｍｏ２Ｆｅ＾２＋Ｆｅ５＾３＋Ｓ６］＾－在紫外可见光谱区中均无特征吸收峰,而［Ｆｅ＾２＋Ｆｅ５＾３＋Ｓ６］＾－在３２０ｎｍ处却呈弱吸收峰。棕色固氮菌固氮酶和该菌的突变菌株ＵＷ４５固氮酶（缺铁钼     

下丘脑室旁核胃动素对胃运动影响的探讨

目的 :研究下丘脑室旁核 (paraventricularnucleus,PVN)胃动素对胃运动调节的参与作用及机制。 方法 :应用免疫组织化学的方法检测室旁核内胃动素神经元的表达情况及室旁核与延髓迷走复合体 (dorsalvagalcomplex ,DVC)间的神经联系 ,应用室旁核内微量注入胃动素的方法观察清醒大鼠胃运动的变化。结果 :①下丘脑室旁核有胃动素免疫阳性细胞 ,在饥饿组和十二指肠灌酸组 ,阳性细胞数有明显增加 (P <0 .0 1)。②迷走背核注入辣根过氧化物酶 (horseradishperoxidase ,HRP) ,在室旁核发现HRP标记细胞 ,证实室旁核与DVC间的纤维联系。③清醒大鼠室旁核内微量注射胃动素可使胃运动的幅度和频率明显增加 (P <0 .0 5 ) ,切断双侧膈下迷走神经后 ,胃动素对胃运动的作用消失。结论 :下丘脑室旁核内胃动素可增强胃运动 ,其作用可能是通过下丘脑 延髓迷走复合体 迷走神经实现的     

中央杏仁核,外侧下丘脑／穹窿周围区,室旁核均参与岛皮层升压反应

实验用乌拉坦麻醉、箭毒制动、人工呼吸的大鼠。将谷氨酸注入岛皮层（ＩＮＳ）以及将Ｐ物质（ＳＰ）注入外侧下丘脑／穹窿周围区（ＬＨ／ＰＦ）或室旁核均引起升压反应。ＩＮＳ－升压反应可被杏仁核（ＡＣ）内预先注射普鲁卡因或谷氨酸二乙酯（ＧＤＥＥ,谷氨酸拮抗剂）以及ＬＨ／ＰＦ内注射［Ｄ－Ｐｒｏ＾２,Ｄ－Ｐｈｅ＾７,Ｄ－Ｔｒｐ＾９］－ＳＰ（ＤＰＤＰＤＴ,ＳＰ拮抗剂）明显衰减,但ＬＨ／ＰＦ内ＧＤＥＥ预处理对该反应无     

杏仁核内注射CCK—8抑制胃运动的机制

应用脑核团内微量注射和核团电刺激方法,观察杏仁基底内侧（ＢＭＡ）对胃运动的影响,分析ＢＭＡ与下丘脑腹内侧核（ＶＭＨ）的机能联系。结果如下：（１）双侧ＢＭＡ内注射八肽胆囊收缩素（ＣＣＫ－８）（５０ｎｇ／ｌμｌ）,出现胃内压（ＩＧＰ）和胃运动频率（ＧＭＦ）显著下降（Ｐ〈０．０１）。（２）ＢＭＡ内注射ＣＣＫ－Ａ受体阻断剂［Ｌ３６４,７１８］（１００ｎｇ／ｌμｌ）或ＣＣＫ－Ｂ受体阻断剂［Ｌ３６５,２６０］     

迷走背核复合体微量注射血管活性肠肽刺激大鼠胃酸分泌

本工作采用Ｇｈｏｓｈ－Ｓｃｈｉｌｄ法收集大鼠胃酸,观察了小脑延髓池、迷走背核复合体和脊髓蛛网膜下腔微量注射血管活性肠肽对胃酸分泌的影响,并初步分析其机制。结果表明：（１）小脑延髓池注射ＶＩＰ（１０μｇ）ｓ可强烈地刺激胃酸分泌,高峰期在注射后６０至８０ｍｉｎ,持续时间超过２．５ｈ。（２）双侧膈下迷走神经切断可完全阻断小脑延髓池微量注射ＶＩＰ刺激胃酸分泌的效应,（３）迷走背核复合体微量注射ＶＩＰ（１μ     

迷走背核复合区微量注射五肽胃泌素对大鼠胃运动的加强作用

在清醒大鼠研究延髓迷走背核复合区(DVC)微量注射五肽胃泌素(G5)对胃窦运动的作用。用慢性植入胃腔外应力传感器记录胃窦运动。单侧DVC内注入G5 0.0025,0.005,0.01μg可明显刺激胃窦的运动,并有一定的剂量相关性,反应发生迅速,时间持续长。外周静脉注入中枢量G5无兴奋胃运动效应。DVC内注G5前20min预先注入抗胃泌素血清(1:100)可取消G5兴奋胃窦运动效应。静脉灌流阿托品(100μg·kg~(-1)·h~(-1))和切断膈下迷走神经可阻断DVC注G5兴奋胃窦运动的作用。DVC注G5对肝门静脉血浆胃动素含量没有影响。研究结果表明,DVC是G5兴奋胃窦运动的脑内作用部位。G5兴奋胃运动的中枢效应是经由迷走胆碱能神经传出的。     

人胃腺苷脱氨酶的分离纯化及性质研究

用硫酸铵分级沉淀、ＤＥＡＥ－纤维素离子交换层析、免疫亲和层析、ＳｅｐｈａｄｅｘＧ－１００凝胶柱层析从人胃组织中提取出腺苷脱氨酶。酶纯化１９３２４倍,比活力为５７９７Ｕ／ｍｇ蛋白。提取酶液经ＰＡＧＥ、ＳＤＳ－ＰＡＧＥ和等电聚焦只呈现一条区带。测得该酶的分子量为４１．２ｋＤ,等电点为ｐＨ４．８,氨基酸组成分析表明该酶由３８８个氨基酸残基组成,Ｎ端氨基酸为精氨酸。酶的最适ｐＨ为６．５,ｐＨ小于５．０或大     

Substance P immunoreactive nerve fibres are related to gastric cancer differentiation status and could promote proliferation and migration of gastric cancer cells

Tachykinins such as SP (substance P) may be involved in the progression of gastric adenocarcinoma through binding to NK-1 receptor. However, the existence and relationship between SP and gastric cancer progression and differentiation remained unknown. We have studied the NK-1 receptor in human gastric cancer tissue and MKN45 cell line and found SP-containing nerve fibres in human gastric cancer and found that the amounts of SP-positive nerves were related to gastric cancer differentiation. SP could promote proliferation, adhesion, migration and invasion of MKN45 cells in vitro. In addition, the intracellular calcium level of MKN45 cells was elevated after SP stimulation, and administration of CRACs (calcium release-activated calcium channels) inhibitor SKF-96365 could partially abolish these effects induced by SP. These results demonstrated that NK-1 receptor and SP-containing nerves existed in human gastric cancer; SP positive nerves may play an important role in human gastric cancer progression, and calcium is critically significant among SP-induced biological effects.     

十二指肠内胆盐对胃肌电和运动的影响及其神经...

Changes of gastric myoelectric fast wave, slow wave and gastric motility were studied after intraduodenal infusion of sodium taurocholate (ST) in an attempt to search the concerned neuromechanism. Frequency and total amplitude of the fast wave and slow wave of gastric myoelectric activity and of gastric contractile wave were recorded every five minutes before and after intraduodenal infusion of ST under the background action of various drugs. The frequency and amplitude were expressed in percentage change of the respective premedication value. After intraduodenal infusion of ST (n = 10) the frequency and the amplitude of fast wave and gastric contractile wave were suppressed. Blocking anesthesia of celiac plexus, reserpinization and intravenous infusion of carbachol could eliminate the inhibition induced by ST, which could be partly eliminated by intravenous infusion of propranolol but not affected by phentolamine at all. The results demonstrate that intraduodenal infusion of bile salt suppresses the fast wave of gastric myoelectric activity and gastric motility, most probably controlled by efferent sympathetic adrenergic fibres through beta-receptor.     

二氢杨梅素对人胃癌MKN45细胞迁移和侵袭的影响及其机制*

目的:探讨二氢杨梅素(DHM )对人胃癌MKN45细胞迁移和侵袭的作用及其分子机制。方法:培养人低分化胃癌MKN45细胞,用不同浓度的DHM(0,10,20,30,40,50 μmol/L)分别处理细胞24及48 h,每组实验重复3次,采用CCK8实验检测癌细胞增殖活力;划痕实验检测细胞迁移能力;Transwell小室检测细胞侵袭能力;免疫印迹分析细胞迁移和侵袭相关蛋白表达情况。结果:不同浓度DHM干预可降低MKN45细胞活力。20,30及40 μmol/L的DHM处理48 h可明显抑制细胞的迁移能力(P＜0.01)和侵袭能力(P＜0.05及0.01)。20及30 μmol/L的DHM处理48 h可增加E-cadherin蛋白表达(P＜0.01)、降低Vimentin表达(P＜0.01),从而逆转EMT过程;10,20及30 μmol/L的DHM处理48 h可明显降低pJNK的活性表达水平(P＜0.05及0.01),及MMP-2蛋白表达(P＜ 0.01);JNK通路特异性抑制剂SP600125预处理可明显促进DHM对癌细胞侵袭能力的抑制作用(P＜0.01)及降低MMP-2表达(P＜0.01)。结论:DHM具有抑制人胃癌MKN45细胞的迁移及侵袭的作用,其机制可能与通过JNK通路下调MMP-2蛋白表达水平、逆转上皮间质转化有关。     

Catabolism of gastrin releasing peptide and substance P by gastric membrane-bound peptidases

The catabolism of two gastric neuropeptides, the C-terminal decapeptide of gastrin releasing peptide-27 (GRP10) and substance P (SP), by membrane-bound peptidases of the porcine gastric corpus and by porcine endopeptidase-24.11 ("enkephalinase") has been investigated. GRP10 was catabolized by gastric muscle peptidases (specific activity 1.8 nmol min-1 mg-1 protein) by hydrolysis of the His8-Leu9 bond and catabolism was inhibited by phosphoramidon (I50 approx. 10(-8) M), a specific inhibitor of endopeptidase-24.11. The same bond in GRP10 was cleaved by purified endopeptidase-24.11, and hydrolysis was equally sensitive to inhibition by phosphoramidon. SP was catabolized by gastric muscle peptidases (specific activity 1.7 nmol min-1 mg-1 protein) by hydrolysis of the Gln6-Phe7, Phe7-Phe8 and Gly9-Leu10 bonds, which is identical to the cleavage of SP by purified endopeptidase-24.11. The C-terminal cleavage of GRP10 and SP would inactivate the peptides. It is concluded that a membrane-bound peptidase in the stomach wall catabolizes and inactivates GRP10 and SP and that, in its specificity and sensitivity to phosphoramidon, this peptidase resembles endopeptidase-24.11.     

Effect of stress on the antioxidant enzymes and gastric ulceration

The effect of cold-restraint stress on the antioxidant enzymes of the rat gastric mucosa was studied with a view to finding out their role in stress induced gastric ulceration. Histological examination revealed stress induced extensive damage of the surface epithelial cell with lesions extending upto submucosa in some cases. Stress causes time-dependent increase in histamine and pepsin content but decrease in acid content of the gastric fluid with the progress of ulceration (ulcer index) for two hours. The tissue lipid peroxidation was significantly increased as evidenced by accumulation of malondialdehyde. Since lipid peroxidation results from the generation of reactive oxygen species, stress effect was studied on some antioxidant enzymes such as superoxide dismutase, peroxidases and prostaglandin synthetase as a function of time. The time dependent increase in stress ulcer correlates well with the concomitant increase in superoxide dismutase activity and decrease in peroxidase and prostaglandin synthetase activity. This creates a favourable condition for accumulation of endogenous H₂O₂ and more reactive hydroxyl radical (OH·). Administration of antioxidants such as reduced glutathione or sodium benzoate prior to stress causes significant decrease in ulcer index and lipid peroxidation and protection of gastric peroxidase activity suggesting the involvement of reactive oxygen species in stress induced gastric ulceration. This is supported by thein vitro observation that OH· can also inactivate peroxidase and induce lipid peroxidation. As prostaglandin is known to offer cytoprotection, stress-induced loss of prostaglandin synthetase activity appears to aggravate the oxidative damage caused by reactive oxygen species.Abbreviations ROS reactive oxygen species - GPO gastric peroxidase - SOD superoxide dismutase - MDA malondialdehyde - GSH reduced glutathione - TCA trichloroacetic acid     

Filamentous organisms in benign and malignant gastric cytology brushings

Review of 143 gastric brushing specimens from two centres in patients with a subsequent histological diagnosis on biopsy or gastrectomy specimens revealed filamentous organisms (FOs) in a large number of benign and malignant gastric brushings. The presence of FOs in significant numbers of brushings of benign gastric lesions contradicts the previously reported strong association of FOs with only gastric carcinoma, and questions the importance of finding these organisms in gastric brushing and biopsy material.     

喉癌中SP100 表达及其与临床病理关系

目的：通过对不同喉癌病人癌组织SP100蛋白进行测量,明确SP100 在喉癌的发生发展过程中的作用并探究其与临床病理 的关系。方法：通过对喉癌手术病人切除的癌组织和癌周组织进行固定、脱水、包埋、切片、免疫组织化学染色判断SP100 阳性细 胞个数以及探究其与临床病理学之间的关系。结果：在正常黏膜上皮细胞和分化良好的癌细胞中,以细胞核内染色为主,在低分 化癌细胞中,在细胞质内呈弥漫性分布。SP100 蛋白在癌旁正常黏膜上皮组织中表达的阳性率比喉癌原发灶中高。SP100 蛋白在 96 例喉癌组织中的表达水平与病理分化程度密切相关(P<0.05 ),而与患者性别、年龄、P-TNM 分期、淋巴结转移无相关性 (P>0.05)。结论：喉癌组织中SP100蛋白表达水平、细胞内分布状况在不同分化程度癌细提示在喉癌的不同阶段可能发挥不同的 作用。