辛开苦降法代表方半夏学与心汤防治大鼠应激性胃黏膜损伤及抗凋亡机制的实验研究
|
摘要
目的:结合中医“治未病”思想和脾胃气机升降失常的病理,预先给予辛开苦降法中调理脾胃气机的代表方剂半夏泻心汤,观察其对水浸束缚应激导致的大鼠胃黏膜损伤、血清和胃黏膜相关细胞因子EGF、PGE2、IL-1β、IL-8、IL-10、TNF-α含量,凋亡相关物质p38MAPK、 Bcl-2、Bax、caspase-3的表达,探讨辛开苦降法防治应激性胃黏膜损伤过程中对胃黏膜上皮细胞凋亡的影响,以及发生作用的机制。
方法:SD大鼠随机分为四组:空白组、模型组、中药组、西药组。采用WRS法制备大鼠应激性胃黏膜损伤模型,以半夏泻心汤为被试因素,参照Guth标准观察记录大鼠胃黏膜损伤指数(UI),观察胃黏膜组织形态学变化;采用酶免法(ELISA)检测IL-1β、IL-8、IL-10、 TNF-α、EGF、PGE2的含量;免疫组化法检测p-p38MAPK蛋白表达;RT-PCR检测Bel-2、BaxmRNA表达;Western-blot检测caspase-3蛋白表达。
结果:
(1)造模后,模型组大鼠胃黏膜损伤明显,损伤指数(UI)最高,与空白组有显著性差异(p<0.01),说明WRS法造模成功;中药组大鼠胃黏膜损伤指数明显降低,与模型组比较有显著性差异(p<0.01)。
(2)中药组可升高WRS大鼠胃黏膜EGF、PGE2的含量,降低WRS大鼠血清IL-1β、IL-8、TNF-α的含量,升高IL-10的含量,与模型组比较有显著性差异(p<0.01)。
(3)中药组可下调p-p38MAPK蛋白、上调Bcl-2mRNA表达,与模型组比较有显著性差异(p<0.01)。造模后,活化的caspase-3表达明显增加,与空白组比较有显著性差异。中药组可显著抑制caspase-3的活化,抑制胃黏膜上皮细胞发生凋亡,与模型组有显著性差异(p<0.01)。
结论:
(1)辛开苦降法能显著对抗应激性胃黏膜损伤,降低应激性胃黏膜损伤程度。
(2)辛开苦降法能升高胃黏膜保护因子EGF、PGE2、IL-10的含量,降低胃黏膜攻击因子IL-1β、IL-8、TNF-α的含量,发挥对胃黏膜的抗炎性损伤、抗凋亡保护作用。
(3)辛开苦降法可下调能引发胃黏膜上皮细胞凋亡信号转导的p-p38MAPK的表达,上调抑凋亡蛋白Bc1-2mRNA的表达,抑制细胞凋亡执行因子caspase-3的活化,从而抑制胃黏膜上皮细胞的凋亡。
Objective:Combination of traditional Chinese medicine "treatment of pathological disease not" thought and the spleen and stomach qi,pre administration of pungent dispersing and bitter descending method regulating qi activity of spleen and stomach in the representative prescription of Banxia Xiexin decoction. Observe the content of stress-induced gastric mucosal injury, rat serum and gastric mucosa associated cytokines EGF、PGE2、IL-1β、IL-8、IL-10、TNF-α,and. the expression of apoptosis related substances p38MAPK、Bcl-2、 Bax、caspase-3; Investigate pungent-opening and bitter-descending method of prevention in the process of stress-induced gastric mucosal injury effect on gastric epithelial cell apoptosis, and it's mechanism and effect.
Methods:SD rats were randomly divided into four groups:blank group, model group, Chinese medicine group, western medicine group, Model of stress-induced gastric mucosal injury in rats by WRS method, Taking Banxia Xiexin decoction as subjects factors, according to the standard of Guth to Observe and record the ulcer index (UI) of gastric mucosa in rats,observe the morphological changes of gastric mucosa; Using enzyme immunoassay (ELISA) to detect the content of IL-1β、IL-8、 IL-10、TNF-α、EGF、PGE2,immunohistochemistry was used to detect the expression of p-p38MAPK protein, RT-PCR was used to To detect the expression of Bcl-2, Bax protein, Western-blot was used to To detect the expression of caspase-3.
Results:
(1) After modeling, injury of gastric mucosa of the rats in the model group is obvious, The Ulcer index(UI) is the highest, there were significant compared with the normal group (p<0.01), indicating a successful model by WRS method; The injury index of gastric mucosa in rats decreased significantly, there were significant compared with the model group (p<0.01),
(2)After modeling, activation of Caspase-3expression increased significantly, there were significant compared with the blank group; Traditional Chinese medicine group could significantly inhibit the activation of Caspase-3, Inhibit the apoptosis of gastric epithelial cell, there were significant compared with the model group (p<0,01).
(3)In Traditional Chinese medicine group, Significant up-regulation of the content of EGF, PGE2was observed in gastric mucosa of WRS rats, down-regulation of the content of IL-1β、IL-8、TNF-α and up-regulation of the content of IL-10was observed in serum of WRS rats, there were significant compared with the model group(p<0.01).
(4)Traditional Chinese medicine group could down regulate p-p38MAPK expression, up-regulate the expression of Bcl-2 protein, there were significant compared with the model group (p<0.01).
Conclusions:
(1) Pungent dispersing and bitter descending method can significantly damage the gastric mucosa against stress, reduce the incidence of stress ulcer.
(2) Pungent dispersing and bitter descending method can perform significantly inhibit apoptosis factor caspase-3activation, thereby inhibiting apoptosis of gastric epithelial cells.
(3) Pungent dispersing and bitter descending method can up regulate the content of gastric mucosal protective factor EGF, PGE2, IL-10, down regulate the content of gastric mucosal attacking factor IL-1β、IL-8、TNF-α, play the anti inflammation injury, anti apoptotic protective effect on gastric mucosa.
(4) Pungent dispersing and bitter descending method can down regulate the expression of p-p38MAPK which can cause gastric mucosal epithelial cell apoptosis signal transduction, up regulate the anti apoptosis protein Bcl-2; so then inhibit the epithelial cell apoptosis of gastric mucosa.
方法:SD大鼠随机分为四组:空白组、模型组、中药组、西药组。采用WRS法制备大鼠应激性胃黏膜损伤模型,以半夏泻心汤为被试因素,参照Guth标准观察记录大鼠胃黏膜损伤指数(UI),观察胃黏膜组织形态学变化;采用酶免法(ELISA)检测IL-1β、IL-8、IL-10、 TNF-α、EGF、PGE2的含量;免疫组化法检测p-p38MAPK蛋白表达;RT-PCR检测Bel-2、BaxmRNA表达;Western-blot检测caspase-3蛋白表达。
结果:
(1)造模后,模型组大鼠胃黏膜损伤明显,损伤指数(UI)最高,与空白组有显著性差异(p<0.01),说明WRS法造模成功;中药组大鼠胃黏膜损伤指数明显降低,与模型组比较有显著性差异(p<0.01)。
(2)中药组可升高WRS大鼠胃黏膜EGF、PGE2的含量,降低WRS大鼠血清IL-1β、IL-8、TNF-α的含量,升高IL-10的含量,与模型组比较有显著性差异(p<0.01)。
(3)中药组可下调p-p38MAPK蛋白、上调Bcl-2mRNA表达,与模型组比较有显著性差异(p<0.01)。造模后,活化的caspase-3表达明显增加,与空白组比较有显著性差异。中药组可显著抑制caspase-3的活化,抑制胃黏膜上皮细胞发生凋亡,与模型组有显著性差异(p<0.01)。
结论:
(1)辛开苦降法能显著对抗应激性胃黏膜损伤,降低应激性胃黏膜损伤程度。
(2)辛开苦降法能升高胃黏膜保护因子EGF、PGE2、IL-10的含量,降低胃黏膜攻击因子IL-1β、IL-8、TNF-α的含量,发挥对胃黏膜的抗炎性损伤、抗凋亡保护作用。
(3)辛开苦降法可下调能引发胃黏膜上皮细胞凋亡信号转导的p-p38MAPK的表达,上调抑凋亡蛋白Bc1-2mRNA的表达,抑制细胞凋亡执行因子caspase-3的活化,从而抑制胃黏膜上皮细胞的凋亡。
Objective:Combination of traditional Chinese medicine "treatment of pathological disease not" thought and the spleen and stomach qi,pre administration of pungent dispersing and bitter descending method regulating qi activity of spleen and stomach in the representative prescription of Banxia Xiexin decoction. Observe the content of stress-induced gastric mucosal injury, rat serum and gastric mucosa associated cytokines EGF、PGE2、IL-1β、IL-8、IL-10、TNF-α,and. the expression of apoptosis related substances p38MAPK、Bcl-2、 Bax、caspase-3; Investigate pungent-opening and bitter-descending method of prevention in the process of stress-induced gastric mucosal injury effect on gastric epithelial cell apoptosis, and it's mechanism and effect.
Methods:SD rats were randomly divided into four groups:blank group, model group, Chinese medicine group, western medicine group, Model of stress-induced gastric mucosal injury in rats by WRS method, Taking Banxia Xiexin decoction as subjects factors, according to the standard of Guth to Observe and record the ulcer index (UI) of gastric mucosa in rats,observe the morphological changes of gastric mucosa; Using enzyme immunoassay (ELISA) to detect the content of IL-1β、IL-8、 IL-10、TNF-α、EGF、PGE2,immunohistochemistry was used to detect the expression of p-p38MAPK protein, RT-PCR was used to To detect the expression of Bcl-2, Bax protein, Western-blot was used to To detect the expression of caspase-3.
Results:
(1) After modeling, injury of gastric mucosa of the rats in the model group is obvious, The Ulcer index(UI) is the highest, there were significant compared with the normal group (p<0.01), indicating a successful model by WRS method; The injury index of gastric mucosa in rats decreased significantly, there were significant compared with the model group (p<0.01),
(2)After modeling, activation of Caspase-3expression increased significantly, there were significant compared with the blank group; Traditional Chinese medicine group could significantly inhibit the activation of Caspase-3, Inhibit the apoptosis of gastric epithelial cell, there were significant compared with the model group (p<0,01).
(3)In Traditional Chinese medicine group, Significant up-regulation of the content of EGF, PGE2was observed in gastric mucosa of WRS rats, down-regulation of the content of IL-1β、IL-8、TNF-α and up-regulation of the content of IL-10was observed in serum of WRS rats, there were significant compared with the model group(p<0.01).
(4)Traditional Chinese medicine group could down regulate p-p38MAPK expression, up-regulate the expression of Bcl-2 protein, there were significant compared with the model group (p<0.01).
Conclusions:
(1) Pungent dispersing and bitter descending method can significantly damage the gastric mucosa against stress, reduce the incidence of stress ulcer.
(2) Pungent dispersing and bitter descending method can perform significantly inhibit apoptosis factor caspase-3activation, thereby inhibiting apoptosis of gastric epithelial cells.
(3) Pungent dispersing and bitter descending method can up regulate the content of gastric mucosal protective factor EGF, PGE2, IL-10, down regulate the content of gastric mucosal attacking factor IL-1β、IL-8、TNF-α, play the anti inflammation injury, anti apoptotic protective effect on gastric mucosa.
(4) Pungent dispersing and bitter descending method can down regulate the expression of p-p38MAPK which can cause gastric mucosal epithelial cell apoptosis signal transduction, up regulate the anti apoptosis protein Bcl-2; so then inhibit the epithelial cell apoptosis of gastric mucosa.
引文
[1]刘婧,李兆申.大鼠应激性胃黏膜损伤时细胞发生凋亡[J].基础医学与临床,2007,27(9):1038-1042
[2]李杰,刘长江.心理应激对大鼠下丘脑、胃黏膜CRF基因表达的影响及中药干预的实验研究[J].中医杂志,2002.43(9):699-700
[3]Lou L X, Gen g B, Yu F, et al. Endoplasmic reticulum stress response is involved in the pathogenesis of stress induced gastric in rats [J]. Life Sci,2006,79 (19):1856-1864
[4]柯雪帆,赵章忠,张玉萍,等.《伤寒论》和《金匮要略》中的药物剂量问题[J].中国中医药杂,1983.(12):36-38
[5]Guth PH, Aures D,Paulsen G. Topical aspf in plus HCI gastric lesions in the rat. Cytoprotective effect of prostaglandin, cimetidine, and probanthine [J]. Gastroenterology,1979,76 (1):88-93
[6]付艾妮,全国芳.中医升降理论及其在脾胃病证中的运用[J].河南中医,2010,30(2):130-131
[7]孙广仁,郑洪新.中医基础理论[M].第3版.北京:中国中医药出版社,2012,7:217
[8]陈正,王庆其.510例脾胃病与情志关系调研[J].中国中医基础医学杂志,2Q08,14(6):439-440,444
[9]白晓莉,宋清江,刘红燕.辛开苦降法与消化系统疾病[J].光明中医,2010,25(12):2184-2185
[10]王泽凤,王敏,史新萍.半夏泻心汤在胃肠疾病方面的应用[J].中国实用医药,2009,4(9):167-168
[11]唐虹.辛开苦降法治疗脾胃病浅析[J].中医研究,2010,23(5):59-60
[12]刘晋平,薄敏敏,李慧吉.中药干预应激性溃疡大鼠模型的实验研究[J].天津中医药,2005,22(4):324-325
[13]叶任高.内科学[M].第5版.北京:人民卫生出版社,2002:398
[14]李兆申.胃黏膜保护剂与急性胃黏膜病变[J].中华消化杂志,2007,27(11):761-762
[15]王玮,孙梅.胃肠黏膜抗损伤和修复新进展[J].世界华人消化杂 志,2005,13(19):2355-2359
[16]Morini G,GrandiD,Schunack W. Ligands for histamine H(3) receptors modulate cell proliferation and migration in rat oxyntic mucosa[J].Br J Pharmacol,2002,137(5):237-244
[17]易受乡,杜燕,林亚平,等.艾灸预处理对急性胃黏膜损伤大鼠血清中eHSP70及胃黏膜细胞NF-κB的影响[J].中华中医药杂志(原中国医药学报),2010,25(9):1462-1467
[18]郁洁,易受乡,林亚平,等.线粒体信号通路Cyt-c和Apaf-1表达及艾灸足阳明经穴保护胃黏膜损伤机制的研究[J].中华中国医药学刊,2012,30(11):2409-2411
[19]唐冬良,戴禄寿,肖雁等.应急作战部队应激性溃疡出血50例分析[J].人民军医,2005,48(2):82
[20]宋清.精神因素致急性胃黏膜病变67例报告[J].山东医药,2004,44(7):10
[21]孙云红.心理性应激对大鼠胃酸分泌和胃黏膜损伤的影响[J].第四军医大学学报,2005.25(10):1
[22]李兆申,湛先保,许国铭.胃黏膜损伤与保护:基础与临床[M].第1版.上海:上海科学技术出版社,2004,04:540
[23]刘婧,李兆申,宛新建,等.凋亡相关基因Bcl-2/Bax和Fas/Fas L在应激性溃疡发生发展过程中的表达及作用[J].中华医学杂志,2003,83(6):504-509
[24]牛廷献,史智勇,姜进军.凋亡相关基因bcl-2和Bax在大鼠应激性溃疡中的表达及作用[J].中国实验动物学报,2005,13(3):170-172
[25]黄莛庭.腹部外科手术并发症[M].第一版.北京:人民卫生出版社,2000:188-195
[26]杨君,解建.应激性溃疡的发病机制研究进展[J].中国急救医学.2007,27(11):1035-1038
[27]房亚洲.半夏泻心汤治疗消化性溃疡临床分析[J].光明中医,2011.26(1):97-98
[28]李兴华,姜玉,郝小鹰.连朴饮合半夏泻心汤加减治疗脾胃湿热证慢性浅表性胃炎55例[J].中国实验方剂学杂志,2013,19(15):293-297
[29]杨勤,李军祥,李晓红.半夏泻心汤加减对非糜烂性反流病症状和生活质量的影响[J].北京中医药大学学报,2013,36(4):280-285
[30]刘剑.半夏泻心汤配合铋剂治疗Hp相关性消化性溃疡25例[J].陕西中医,2009,30(7):830-831
[31]孙小卉.半夏泻心汤对三联未根除HP感染者的治疗作用观察[J].世界中医药,2013,8(1):50-53
[32]许景峰,王金萍,许茜.半夏泻心汤对大鼠胃溃疡及小肠功能的影响[J].中国药业,2002,11(2):48-49
[33]吴丽芹,姜惟,姚欣,等.半夏泻心汤对合并幽门螺杆菌感染大鼠慢性胃炎模型胃粘液层磷脂、氨基己糖的影响[J].中国中医药信息杂志,2001,8(5):29-30
[34]王历,刘春红,田明健.半夏泻心汤不同服药方法对乙酸性胃溃疡大鼠疗效影响的实验研究[J].中医药信息,2005,22(6):54-55
[35]张忠,司银楚,白丽敏,吴海霞.许红半夏泻心汤及其拆方对应激性胃溃疡大鼠胃泌素的影响[J].世界华人消化杂志,2005,13(10):1223-1225
[36]赵琰,李宇航,王庆国,等.半夏泻心汤不同性味拆房对胃溃疡大鼠血清胃泌素的影响[J].上海中医药杂志,2004,38(10):45
[37]王庆国,李宇航,牛欣,等.半夏泻心汤及其拆方对慢性胃溃疡大鼠表皮生长因子的影响[J].中国中西医结合急救杂志,2001,6(3):137-139
[38]邱冰峰,王志勇.半夏泻心汤加减方对胃溃疡大鼠胃组织热休克蛋白27表达的影响[J].中国中西医结合消化杂志,2009,17(5):292-295
[39]姜惟,顾武军,周春祥.半夏泻心汤对慢性胃炎合并幽门螺杆菌感染大鼠一氧化氮的影响[J].中国医药学报,2003,18(11):666-669
[40]王晓梅,皮明钧.半夏泻心汤及其拆方对幽门螺杆菌相关性胃炎小鼠血清炎性相关因子的影响[J].中国中医药科技,2007,14(2):72-73
[41]罗桂香,尹抗抗,谭达全.半夏泻心汤及其有效组分黄芩苷对幽门螺杆菌相关性胃炎胃黏膜保护作用和对TNF-α影响的研究[J].中国中医药现代远程教育,2009,7(1):19-20
[42]莫莉,皮明钧,伍参荣,等.半夏泻心汤及其拆方对幽门螺杆菌感染小鼠 胃黏膜CD4、CD8表达的影响[J].湖南中医学院学报,2006,26(1):8-10,15
[43]吴忠祥,贺龙刚,谭达全,等.半夏泻心汤及其拆方对Hp感染小鼠黏膜保护作用的研究[J].湖南中医药大学学报,2010,30(5):23-25
[44]徐颖,张祖志,方正清,等.半夏泻心汤对应激性胃黏膜损伤大鼠血管活性肠肽含量的影响[J].中医药临床杂志,2004,16(2):97-98
[45]张忠,司银楚,吴海霞,等.半夏泻心汤及其拆方对应激性胃溃疡大鼠胆碱能神经元的影响[J].中国中医基础医学杂志,2005,11(4):283-284
[46]张忠,司银楚,白丽敏.半夏泻心汤及其拆方对应激性胃溃疡大鼠P物质的影响[J].中国医药学报,2003,18(11):669-671
[47]渡边泰雄.半夏泻心汤对水浸拘束诱发大鼠胃溃疡的抑制作用以及脑和胃的单胺调节[J].国外医学(中医中药分册),1998,20(6):23-24
[48]李志强,常红娟.半夏泻心汤抗抑郁作用实验研究[J].中国实验方剂学杂志,2013,19(4):280-282
[49]Yanaka A, Suzuki H, Shibahara, et al.EGF promotes gastric mucosal restitution by activating Na+/H+ exchange of epithelial cells[J].Am J Physiol Gastrointest Liver Physiol,2002,282 (5):866-876
[50]Milani S,Calabro A. Role of growth factors and their receptors in gastric ulcer healing [J]. Microsc Res Tech,2001,53 (5):360-371
[51]Hoffmann P, Eysselein VE,Zeeh JM, et al. Epidermal growth factor increases basal mucosal blood flow in the rat colon, a prostaglandin dependent effect[J]. Eur J Gastroenterol Hepatol,1999,11 (11):1305-1310
[52]徐俊,宋于刚,武金宝,等.应激性溃疡大鼠血浆EGF水平和胃上皮细胞凋亡的变化[J].苏州大学学报(医学版),2004,24(2):160-163,175
[53]Celebi N, Turkyilmaz, Gonul B, et al. Effects of epidermal growth factor microemulsion formulation on the healing of stress-induced gastric ulcers in rats[J].J Control Release.2002,83(2):197-210
[54]Akbulut KG, Gonul B, Turkyilmaz A, et al. The role of epidermal growth factor formulation on stress ulcer healing of the gastric mucosa[J]. Surg Today,2002,32 (10):880-883
[55]Kontuiek PC, Brzozowski T, Duda A, et al. Epidermal growth factor and prostaglandin E(2) accelerate mucosal recovery from stress-induced gastric lesions via inhibition of apoptosis[J].J Physiol Paris,2001:95(1-6):361-367
[56]Kwiecien, Brzozow ski S, Konturek SJ. Effects of reactive oxygen species action on gastric mucosa in various models of mucosal injury[J].J Physiol Pharmacol,2002,53(1):39
[57]施征,吴焕淦,谭卫林,等.隔药灸对大鼠溃疡性结肠炎IL-1β、TNF-α影响[J].上海针灸杂志,2000,19(S1):50-52
[58]王觅柱,邬彩虹,陈吉.溃疡性结肠炎患者血清IL-1β、TNF-α和IL-10的表达及其意义[J].国际消化病杂志,2009.29(5):362-364
[59]张爽,刘海峰,张成岗.应激性胃黏膜损伤发病机制的研究进展[J].世界华人消化杂志,2009,17(17):1697-1701
[60]Raddatz D, Bockemuhl M, Ramadori G. Quantitative measurement of cytokinemRNA in inflammatory bowel disease:relation to clinical and endoscopic activity and outcome[J]. Eur J Gastroenterol Hepatol,2005,17(3):547-557
[61]T Watanabe, K Higuchi, K Tominaga, et al. Acid regulates inflammatory response in a rat model of induction of gastric ulcer recurrence by interleukin 1β [J]. Gut,2001,48(9):774-781
[62]Indaram AV, Visvalingam V.Locke M. et al.Mucosal cytokine production in radiation-induced proctosig moiditis eompared with inflammatory bowel disease [J]. Am J Gastroenterol,2000,95(11):1221-1225
[63]Toshio Watanabe, Kazuhide Higuchi, Masaki Hamaguchi,et al.Monocyte chemotactic protein-1 regulates leukocyte recruitment during gastric ulcer recurrence induced by tumor necrosis factor-α [J].Am J Physiol Gastrointest Liver Physiol,2004,287(1):919-928
[64]Isobe H, Okajima K, Harada N, et al. Activated protein C reduces stress-induced gastric mucosal injury in rats by inhibiting the endothelial cell injury[J].J Thromb Haemost,2004Feb,2 (2):313-320
[65]张宏亮,徐杨,范晓.不同病因导致的应激性胃黏膜损伤及其血液ET、TNF-α的改变[J].医学研究杂志,2010,39(1):67-70
[66]Castro-Santos P,Suarez A,Mozo L,et al. Association of IL-10 and TNF-α genotypes with ANCA appearance in ulcerative colitis [J]. Clin Immunol,2007,122 (6):108-114
[67]Y Yamaoka, K Yamauchi,H Ota,et al. Natural History of Gastric Mucosal Cytokine Expression in Helicobacter pylori Gastritis in Mongolian Gerbils[J]. Infection and Immunity,2005,73 (4):2205-2212
[68]口锁堂,吴涣淦,施达仁.白介素与溃疡性结肠炎[J].世界华人消化杂志,2006,14(4):405-411
[69]Indaram AV, Visvalingam V, Locke M, et al. Mucosal cytokineProduction in radiation-induced Proetosigmoiditis comparedwithinflammatory bowel disease [J]. Am J Gastroenterol,2000,95 (5):1221-1225
[70]Scatena R, Bottoni P, Botta G, et al. The role of mitochondria in pharmacotoxicology:a reevaluation of an old,newly emerging topic[J]. Am J Physiol Cell Physiol,2007,293(1):C12-21
[71]Hacker G, Paschen SA. Therapeutic targets in the mitochondrial apoptotic pathway[J]. Expert Opin Ther Targets,2007,11 (4):515-526
[72]Cryns V, Yuan J. Protease to die for [J]. Genes Dev,1998,12(11):1551-1570
[73]Irving EA,Bamford M.Role of mitogen and stress activated kinases in ischemic injury [J].J Cereb Blood Flow Metab,2002,22 (6):631-647
[74]罗云,朱文静,徐运.MK801对氧糖剥夺神经元P38MAPK和BCL2/BAX蛋白表达的影响[J].中国组织化学与细胞化学杂志,2008,17(5):433-436
[75]Martin-Blanco E. p38MAPK signalling cascades ancient roles and new functions [J].Bioessays,2000,22(7):637-645.
[76]Ono K, Han J. The p38 signal transduction pathway: activation and function [J]. Cell Signal,2000,12 (1):1-13
[77]贾一韬,韦多,夏照帆等.p38丝裂原活化蛋白激酶在应激性溃疡发病中的作用[J].中华外科杂志,2005,43(19):1284-1286
[78]刘文军,贾一韬,夏照帆,等.Tempol对浸水束缚应激大鼠胃黏膜p38MAPK活化的影响[J].解放军医学杂志,2008,33(2):163-165
[79]付永锋,樊廷俊.Bcl-2家族蛋白与细胞凋亡[J].生物化学与生物物理学报,2002,34(4):289-294
[1]唐冬良,戴禄寿,肖雁等.应急作战部队应激性溃疡出血50例分析[J].人民军医,2005,48(2):82
[2]宋清.精神因素致急性胃黏膜病变67例报告[J].山东医药,2004,44(7):10
[3]刘良,王建华,邵庭荫,等.大鼠束缚水浸应激性胃溃疡模型的实验控制[J].中国药理学通报,1988,4(4):246-248
[4]刘婧,李兆申,宛新建,等.凋亡相关基因Bcl-2/Bax和Fas/Fas L在应激性溃疡发生发展过程中的表达及作用[J].中华医学杂志,2003,83(6):504-509
[5]牛廷献,史智勇,姜进军.凋亡相关基因bcl-2和Bax在大鼠应激性 溃疡中的表达及作用[J].中国实验动物学报,2005,13(3):170-172
[6]颜兵,秦志丰,施俊,等.消痰通腑法防治应激性溃疡的理论探讨[J].中国中医急症,2012,21(1):36-37
[7]张茂,张超,杨宗诚.丹参对大鼠腹腔感染状态下胃粘膜Na,K-ATPase和pH值的影响[J].西安交通大学学报(医学版),2003,24(5):461-490
[8]赵洁,张文.丹参对幼年大鼠应激性溃疡预防作用机制的实验研究[J].儿科药学杂志,2009,15(6):7-10,16
[9]周海英,谭慧敏,于海萍,等.生大黄治疗应激性溃疡出血40例[J].四川中医,2002,20(12):36
[10]曹晓林,刘莉,王志鹏,等.唐古特大黄多糖对大鼠应激性胃溃疡的保护作用[J].中国临床药理学与治疗学,2004,9(10):1115-1118
[11]谭明义,陈根成,卢梅生.大黄胶囊预防大鼠脑出血并发应激性胃溃疡的研究简报[J].中药新药与临床药理,2000,11(6):356-357
[12]汶希,陈楚杰,陈建新.大黄提取液干预运动应激性胃溃疡大鼠模型的实验研究[J].中医学报.2012,27(5):585-587
[13]董淑云,郑素琴,门秀丽,等.应激性溃疡的发生及川芎嗪的防治效应[J].中国中西医结合脾胃杂志,1996,4(4):218
[14]万军利,王昌留,崔胜忠.川芎嗪对大鼠浸水应激性胃溃疡的影响[J].中草药,2000,31(2):115-117
[15]李峰,张浩,华桦,等.黄连碱对应激所致小鼠胃黏膜损伤的保护作用[J].华西药学杂志,2007,22(6):713-714
[16]赵敬国.山楂叶总黄酮对大鼠运动应激性溃疡防治作用的实验研究[J].山东体育科技,2001,23(4):29-35
[17]辛益妹,王忠,谷顺才.芦荟对缺氧与疲劳应激小鼠血清白细胞介素-1、6、8含量的影响[J].航空军医,2003,31(1):18-20
[18]严亨秀,殷红梅,王爱华,等.芦荟对应激性溃疡的保护作用[J].中国实用神经疾病杂志,2006,9(6):136-137
[19]付丽新,唐冬梅,严亨秀.芦荟抗应激性胃溃疡的迷走神经机制 [J].西南民族大学学报:自然科学版,2013,39(2):171-175
[20]吴清和,操电群,黄萍,等.高良姜超临界萃取物对应激性溃疡大鼠溃疡形成及表皮生长因子和白介素-2水平的影响[J].中药药理与临床,2004,20(6):17-18
[21]彭钧,操电群,李小月.高良姜超临界萃取物对应激性溃疡模型大鼠溃疡形成和胃液分泌及生长抑素水平的影响[J].安徽医药,2008,12(10):895-897
[22]王琼,赵维中,马传庚.银杏叶提取物的胃粘膜保护作用[J].中国药理学报,2000,21(12):1153-1156
[23]张根葆,孙俊,钱大青,等.银杏叶提取物预防应激性胃溃疡作用机制分析[J].中国危重病急救医学,2000,12(2):80-82
[24]李佳,张常娥.银杏内酯A预防大鼠应激性溃疡的实验研究[J].咸宁学院学报(医学版),2004,18(2):95-97
[25]王福文,李杰,徐学明.复方丹参注射液对大鼠应激性胃溃疡和胃运动的影响[J].山东医药工业,2001,20(5):43-44
[26]曹霞,余良主,赵小玉.复方丹参注射液对大鼠运动应激性溃疡的影响[J].咸宁学院学报(医学版),2003,17(5):318-321
[27]黄铁军,余良主.复方丹参注射液对大鼠应激性胃黏膜损伤的保护作用[J].国际中医中药杂志,2013,35(7):604-606
[28]董亚琳,邢建峰,封卫毅.舒肝丸抗实验性胃溃疡的作用[J].西安交通大学学报(医学版),2004,25(1):79-82.
[29]梁媛,谭达全,张文将,等.左金丸对大鼠应激性胃溃疡保护作用的实验研究[J].湖南中医杂志,2013,29(9):120-122
[30]刘晓伟,张红梅,曲宏达,等.左金丸对应激性胃溃疡粘膜损伤保护作用机理的研究[J].江西中医药,2004,35(260):18-19
[31]张红梅,刘晓伟,曲宏达,等.左金丸对应激性溃疡大鼠下丘脑室旁核c-fos及HPA轴的调节作用[J].中国中西医结合急救杂志,2004,11(5):276-279
[32]林科名,丁世兰,王强松,等.左金丸总生物碱对束缚水浸应激性胃溃疡模型大鼠神经体液调节的影响[J].中国药理通 报,2013,29(3):401-405
[33]李杰,刘长江,李庆和,等.心理应激对大鼠下丘脑、胃粘膜CRF基因表达的影响及中药干预的实验研究[J].中医杂志,2002,43(9):699-700
[34]吕树泉,贾锡莲,杨玉龙,等.心身1号片对大鼠应激性溃疡胃黏膜Bcl-2和Bax表达的影响[J].天津中医药,2008,25(2):147-149
[35]周艳艳,周安方,蔡丽芬,等.大柴胡汤对大鼠应激性胃溃疡的防治作用研究[J].中医药学刊,2006,24(6):1056-1058
[36]徐安莉,蔡丽芬,周艳艳.大柴胡汤防治应激性溃疡的实验研究[J].中国中医药科技,2004,11(5):289
[37]罗丹,熊家平.大柴胡汤对应激性溃疡大鼠血清内皮素(ET)和血清前列腺I2(PGI2)的影响[J].中华实用中西医杂志,2003,3(16):1741-1742
[38]徐颖,张祖志,方正清,等.半夏泻心汤对应激性胃黏膜损伤大鼠血管活性肠肽含量的影响[J].中医药临床杂志,2004,16(2):97-98
[39]张忠,司银楚,吴海霞,等.半夏泻心汤及其拆方对应激性胃溃疡大鼠胆碱能神经元的影响[J].中国中医基础医学杂志,2005,11(4):283-284
[40]张忠,司银楚,白丽敏,等.半夏泻心汤及共拆方对应激性胃溃疡大鼠胃泌素的影响[J].世界华人消化杂志,2005,13(10):1223-1224
[41]彭磊.针刺对应激性溃疡模型大鼠脑源性神经营养因子等影响的实验研究[D],北京中医药大学,2010
[42]孙锦平,田淑君,田庆华,等.针刺足三里穴对大鼠冷应激性溃疡下丘脑NOS表达的影响[J],世界华人消化杂志,2004,12(9):2095-2098
[43]孙锦平,王路宁,柳国芳,等.针刺足三里穴对冷应激性胃溃疡大鼠下丘脑与肾上腺SP和POMC表达的影响[J].世界华人消化杂志,2008,16(15):1602-1606
[44]易受乡,彭艳,常小荣,等.艾灸预处理对应激性溃疡大鼠胃黏膜增殖修复的影响[J].世界中西医结合杂志,2007,2(1):21-24
[45]刘密,常小荣,严洁,等.艾灸预处理对应激性溃疡大鼠胃黏膜GSH-Px, SOD, MDA的影响[J].Journal of Acupuncture and Tuina Science,2011,9(1):17-20
[46]刘密,常小荣,严洁,等.艾灸预处理对应激性胃黏膜损伤大鼠血清IL-1α,TNF-α和IL-10的影响[J].中国中医急症,2011,20(6):906-908
[47]于浩.不同针灸配穴防治应激性胃溃疡大鼠的差异蛋白表达分析[J].中国中医药咨讯,2010,2(11):241-242
[48]严洁,黎喜平,黄艾,等.电针足阳明经穴对大鼠胃黏膜损伤修复机制的研究[J].中国中医药信息杂志,2006,13(05):20-23
[49]杨宗保,严洁,常小荣,等.电针胃经穴对应激大鼠血清胃黏膜细胞表皮生长因子受体表达的作用[J].中国行为医学科学,2006,15(12):1066-1068
[50]杨宗保,严洁,邹小平,等.电针大鼠胃经后血清对其胃黏膜细胞表皮生长因子受体表达的影响及浓度效应[J].中国临床康复,2006,10(35):87-89
[51]严洁,杨宗保,常小荣,等.电针大鼠胃经穴的血清对胃黏膜细胞表皮生长因子受体后信息物质表达的影响[J].中西医结合学报,2007,5(03):338-342
[52]杨宗保,严洁,易受乡,等.电针胃经穴的大鼠血清对胃黏膜细胞EGFR阻断后c-myc的影响[J].江西中医学院学报,2009,21(04):27-29
[53]杨宗保,严洁,易受乡,等.电针胃经穴的大鼠血清上调胃黏膜细胞ERK磷酸化[J].基础医学与临床,2009,29(02):135-138
[54]严洁,杨宗保,邹晓平,等.电针胃经穴后胃溃疡大鼠胃黏膜细胞蛋白激酶C活性的变化[J].中国临床康复,2006,10(19):122-24
[2]李杰,刘长江.心理应激对大鼠下丘脑、胃黏膜CRF基因表达的影响及中药干预的实验研究[J].中医杂志,2002.43(9):699-700
[3]Lou L X, Gen g B, Yu F, et al. Endoplasmic reticulum stress response is involved in the pathogenesis of stress induced gastric in rats [J]. Life Sci,2006,79 (19):1856-1864
[4]柯雪帆,赵章忠,张玉萍,等.《伤寒论》和《金匮要略》中的药物剂量问题[J].中国中医药杂,1983.(12):36-38
[5]Guth PH, Aures D,Paulsen G. Topical aspf in plus HCI gastric lesions in the rat. Cytoprotective effect of prostaglandin, cimetidine, and probanthine [J]. Gastroenterology,1979,76 (1):88-93
[6]付艾妮,全国芳.中医升降理论及其在脾胃病证中的运用[J].河南中医,2010,30(2):130-131
[7]孙广仁,郑洪新.中医基础理论[M].第3版.北京:中国中医药出版社,2012,7:217
[8]陈正,王庆其.510例脾胃病与情志关系调研[J].中国中医基础医学杂志,2Q08,14(6):439-440,444
[9]白晓莉,宋清江,刘红燕.辛开苦降法与消化系统疾病[J].光明中医,2010,25(12):2184-2185
[10]王泽凤,王敏,史新萍.半夏泻心汤在胃肠疾病方面的应用[J].中国实用医药,2009,4(9):167-168
[11]唐虹.辛开苦降法治疗脾胃病浅析[J].中医研究,2010,23(5):59-60
[12]刘晋平,薄敏敏,李慧吉.中药干预应激性溃疡大鼠模型的实验研究[J].天津中医药,2005,22(4):324-325
[13]叶任高.内科学[M].第5版.北京:人民卫生出版社,2002:398
[14]李兆申.胃黏膜保护剂与急性胃黏膜病变[J].中华消化杂志,2007,27(11):761-762
[15]王玮,孙梅.胃肠黏膜抗损伤和修复新进展[J].世界华人消化杂 志,2005,13(19):2355-2359
[16]Morini G,GrandiD,Schunack W. Ligands for histamine H(3) receptors modulate cell proliferation and migration in rat oxyntic mucosa[J].Br J Pharmacol,2002,137(5):237-244
[17]易受乡,杜燕,林亚平,等.艾灸预处理对急性胃黏膜损伤大鼠血清中eHSP70及胃黏膜细胞NF-κB的影响[J].中华中医药杂志(原中国医药学报),2010,25(9):1462-1467
[18]郁洁,易受乡,林亚平,等.线粒体信号通路Cyt-c和Apaf-1表达及艾灸足阳明经穴保护胃黏膜损伤机制的研究[J].中华中国医药学刊,2012,30(11):2409-2411
[19]唐冬良,戴禄寿,肖雁等.应急作战部队应激性溃疡出血50例分析[J].人民军医,2005,48(2):82
[20]宋清.精神因素致急性胃黏膜病变67例报告[J].山东医药,2004,44(7):10
[21]孙云红.心理性应激对大鼠胃酸分泌和胃黏膜损伤的影响[J].第四军医大学学报,2005.25(10):1
[22]李兆申,湛先保,许国铭.胃黏膜损伤与保护:基础与临床[M].第1版.上海:上海科学技术出版社,2004,04:540
[23]刘婧,李兆申,宛新建,等.凋亡相关基因Bcl-2/Bax和Fas/Fas L在应激性溃疡发生发展过程中的表达及作用[J].中华医学杂志,2003,83(6):504-509
[24]牛廷献,史智勇,姜进军.凋亡相关基因bcl-2和Bax在大鼠应激性溃疡中的表达及作用[J].中国实验动物学报,2005,13(3):170-172
[25]黄莛庭.腹部外科手术并发症[M].第一版.北京:人民卫生出版社,2000:188-195
[26]杨君,解建.应激性溃疡的发病机制研究进展[J].中国急救医学.2007,27(11):1035-1038
[27]房亚洲.半夏泻心汤治疗消化性溃疡临床分析[J].光明中医,2011.26(1):97-98
[28]李兴华,姜玉,郝小鹰.连朴饮合半夏泻心汤加减治疗脾胃湿热证慢性浅表性胃炎55例[J].中国实验方剂学杂志,2013,19(15):293-297
[29]杨勤,李军祥,李晓红.半夏泻心汤加减对非糜烂性反流病症状和生活质量的影响[J].北京中医药大学学报,2013,36(4):280-285
[30]刘剑.半夏泻心汤配合铋剂治疗Hp相关性消化性溃疡25例[J].陕西中医,2009,30(7):830-831
[31]孙小卉.半夏泻心汤对三联未根除HP感染者的治疗作用观察[J].世界中医药,2013,8(1):50-53
[32]许景峰,王金萍,许茜.半夏泻心汤对大鼠胃溃疡及小肠功能的影响[J].中国药业,2002,11(2):48-49
[33]吴丽芹,姜惟,姚欣,等.半夏泻心汤对合并幽门螺杆菌感染大鼠慢性胃炎模型胃粘液层磷脂、氨基己糖的影响[J].中国中医药信息杂志,2001,8(5):29-30
[34]王历,刘春红,田明健.半夏泻心汤不同服药方法对乙酸性胃溃疡大鼠疗效影响的实验研究[J].中医药信息,2005,22(6):54-55
[35]张忠,司银楚,白丽敏,吴海霞.许红半夏泻心汤及其拆方对应激性胃溃疡大鼠胃泌素的影响[J].世界华人消化杂志,2005,13(10):1223-1225
[36]赵琰,李宇航,王庆国,等.半夏泻心汤不同性味拆房对胃溃疡大鼠血清胃泌素的影响[J].上海中医药杂志,2004,38(10):45
[37]王庆国,李宇航,牛欣,等.半夏泻心汤及其拆方对慢性胃溃疡大鼠表皮生长因子的影响[J].中国中西医结合急救杂志,2001,6(3):137-139
[38]邱冰峰,王志勇.半夏泻心汤加减方对胃溃疡大鼠胃组织热休克蛋白27表达的影响[J].中国中西医结合消化杂志,2009,17(5):292-295
[39]姜惟,顾武军,周春祥.半夏泻心汤对慢性胃炎合并幽门螺杆菌感染大鼠一氧化氮的影响[J].中国医药学报,2003,18(11):666-669
[40]王晓梅,皮明钧.半夏泻心汤及其拆方对幽门螺杆菌相关性胃炎小鼠血清炎性相关因子的影响[J].中国中医药科技,2007,14(2):72-73
[41]罗桂香,尹抗抗,谭达全.半夏泻心汤及其有效组分黄芩苷对幽门螺杆菌相关性胃炎胃黏膜保护作用和对TNF-α影响的研究[J].中国中医药现代远程教育,2009,7(1):19-20
[42]莫莉,皮明钧,伍参荣,等.半夏泻心汤及其拆方对幽门螺杆菌感染小鼠 胃黏膜CD4、CD8表达的影响[J].湖南中医学院学报,2006,26(1):8-10,15
[43]吴忠祥,贺龙刚,谭达全,等.半夏泻心汤及其拆方对Hp感染小鼠黏膜保护作用的研究[J].湖南中医药大学学报,2010,30(5):23-25
[44]徐颖,张祖志,方正清,等.半夏泻心汤对应激性胃黏膜损伤大鼠血管活性肠肽含量的影响[J].中医药临床杂志,2004,16(2):97-98
[45]张忠,司银楚,吴海霞,等.半夏泻心汤及其拆方对应激性胃溃疡大鼠胆碱能神经元的影响[J].中国中医基础医学杂志,2005,11(4):283-284
[46]张忠,司银楚,白丽敏.半夏泻心汤及其拆方对应激性胃溃疡大鼠P物质的影响[J].中国医药学报,2003,18(11):669-671
[47]渡边泰雄.半夏泻心汤对水浸拘束诱发大鼠胃溃疡的抑制作用以及脑和胃的单胺调节[J].国外医学(中医中药分册),1998,20(6):23-24
[48]李志强,常红娟.半夏泻心汤抗抑郁作用实验研究[J].中国实验方剂学杂志,2013,19(4):280-282
[49]Yanaka A, Suzuki H, Shibahara, et al.EGF promotes gastric mucosal restitution by activating Na+/H+ exchange of epithelial cells[J].Am J Physiol Gastrointest Liver Physiol,2002,282 (5):866-876
[50]Milani S,Calabro A. Role of growth factors and their receptors in gastric ulcer healing [J]. Microsc Res Tech,2001,53 (5):360-371
[51]Hoffmann P, Eysselein VE,Zeeh JM, et al. Epidermal growth factor increases basal mucosal blood flow in the rat colon, a prostaglandin dependent effect[J]. Eur J Gastroenterol Hepatol,1999,11 (11):1305-1310
[52]徐俊,宋于刚,武金宝,等.应激性溃疡大鼠血浆EGF水平和胃上皮细胞凋亡的变化[J].苏州大学学报(医学版),2004,24(2):160-163,175
[53]Celebi N, Turkyilmaz, Gonul B, et al. Effects of epidermal growth factor microemulsion formulation on the healing of stress-induced gastric ulcers in rats[J].J Control Release.2002,83(2):197-210
[54]Akbulut KG, Gonul B, Turkyilmaz A, et al. The role of epidermal growth factor formulation on stress ulcer healing of the gastric mucosa[J]. Surg Today,2002,32 (10):880-883
[55]Kontuiek PC, Brzozowski T, Duda A, et al. Epidermal growth factor and prostaglandin E(2) accelerate mucosal recovery from stress-induced gastric lesions via inhibition of apoptosis[J].J Physiol Paris,2001:95(1-6):361-367
[56]Kwiecien, Brzozow ski S, Konturek SJ. Effects of reactive oxygen species action on gastric mucosa in various models of mucosal injury[J].J Physiol Pharmacol,2002,53(1):39
[57]施征,吴焕淦,谭卫林,等.隔药灸对大鼠溃疡性结肠炎IL-1β、TNF-α影响[J].上海针灸杂志,2000,19(S1):50-52
[58]王觅柱,邬彩虹,陈吉.溃疡性结肠炎患者血清IL-1β、TNF-α和IL-10的表达及其意义[J].国际消化病杂志,2009.29(5):362-364
[59]张爽,刘海峰,张成岗.应激性胃黏膜损伤发病机制的研究进展[J].世界华人消化杂志,2009,17(17):1697-1701
[60]Raddatz D, Bockemuhl M, Ramadori G. Quantitative measurement of cytokinemRNA in inflammatory bowel disease:relation to clinical and endoscopic activity and outcome[J]. Eur J Gastroenterol Hepatol,2005,17(3):547-557
[61]T Watanabe, K Higuchi, K Tominaga, et al. Acid regulates inflammatory response in a rat model of induction of gastric ulcer recurrence by interleukin 1β [J]. Gut,2001,48(9):774-781
[62]Indaram AV, Visvalingam V.Locke M. et al.Mucosal cytokine production in radiation-induced proctosig moiditis eompared with inflammatory bowel disease [J]. Am J Gastroenterol,2000,95(11):1221-1225
[63]Toshio Watanabe, Kazuhide Higuchi, Masaki Hamaguchi,et al.Monocyte chemotactic protein-1 regulates leukocyte recruitment during gastric ulcer recurrence induced by tumor necrosis factor-α [J].Am J Physiol Gastrointest Liver Physiol,2004,287(1):919-928
[64]Isobe H, Okajima K, Harada N, et al. Activated protein C reduces stress-induced gastric mucosal injury in rats by inhibiting the endothelial cell injury[J].J Thromb Haemost,2004Feb,2 (2):313-320
[65]张宏亮,徐杨,范晓.不同病因导致的应激性胃黏膜损伤及其血液ET、TNF-α的改变[J].医学研究杂志,2010,39(1):67-70
[66]Castro-Santos P,Suarez A,Mozo L,et al. Association of IL-10 and TNF-α genotypes with ANCA appearance in ulcerative colitis [J]. Clin Immunol,2007,122 (6):108-114
[67]Y Yamaoka, K Yamauchi,H Ota,et al. Natural History of Gastric Mucosal Cytokine Expression in Helicobacter pylori Gastritis in Mongolian Gerbils[J]. Infection and Immunity,2005,73 (4):2205-2212
[68]口锁堂,吴涣淦,施达仁.白介素与溃疡性结肠炎[J].世界华人消化杂志,2006,14(4):405-411
[69]Indaram AV, Visvalingam V, Locke M, et al. Mucosal cytokineProduction in radiation-induced Proetosigmoiditis comparedwithinflammatory bowel disease [J]. Am J Gastroenterol,2000,95 (5):1221-1225
[70]Scatena R, Bottoni P, Botta G, et al. The role of mitochondria in pharmacotoxicology:a reevaluation of an old,newly emerging topic[J]. Am J Physiol Cell Physiol,2007,293(1):C12-21
[71]Hacker G, Paschen SA. Therapeutic targets in the mitochondrial apoptotic pathway[J]. Expert Opin Ther Targets,2007,11 (4):515-526
[72]Cryns V, Yuan J. Protease to die for [J]. Genes Dev,1998,12(11):1551-1570
[73]Irving EA,Bamford M.Role of mitogen and stress activated kinases in ischemic injury [J].J Cereb Blood Flow Metab,2002,22 (6):631-647
[74]罗云,朱文静,徐运.MK801对氧糖剥夺神经元P38MAPK和BCL2/BAX蛋白表达的影响[J].中国组织化学与细胞化学杂志,2008,17(5):433-436
[75]Martin-Blanco E. p38MAPK signalling cascades ancient roles and new functions [J].Bioessays,2000,22(7):637-645.
[76]Ono K, Han J. The p38 signal transduction pathway: activation and function [J]. Cell Signal,2000,12 (1):1-13
[77]贾一韬,韦多,夏照帆等.p38丝裂原活化蛋白激酶在应激性溃疡发病中的作用[J].中华外科杂志,2005,43(19):1284-1286
[78]刘文军,贾一韬,夏照帆,等.Tempol对浸水束缚应激大鼠胃黏膜p38MAPK活化的影响[J].解放军医学杂志,2008,33(2):163-165
[79]付永锋,樊廷俊.Bcl-2家族蛋白与细胞凋亡[J].生物化学与生物物理学报,2002,34(4):289-294
[1]唐冬良,戴禄寿,肖雁等.应急作战部队应激性溃疡出血50例分析[J].人民军医,2005,48(2):82
[2]宋清.精神因素致急性胃黏膜病变67例报告[J].山东医药,2004,44(7):10
[3]刘良,王建华,邵庭荫,等.大鼠束缚水浸应激性胃溃疡模型的实验控制[J].中国药理学通报,1988,4(4):246-248
[4]刘婧,李兆申,宛新建,等.凋亡相关基因Bcl-2/Bax和Fas/Fas L在应激性溃疡发生发展过程中的表达及作用[J].中华医学杂志,2003,83(6):504-509
[5]牛廷献,史智勇,姜进军.凋亡相关基因bcl-2和Bax在大鼠应激性 溃疡中的表达及作用[J].中国实验动物学报,2005,13(3):170-172
[6]颜兵,秦志丰,施俊,等.消痰通腑法防治应激性溃疡的理论探讨[J].中国中医急症,2012,21(1):36-37
[7]张茂,张超,杨宗诚.丹参对大鼠腹腔感染状态下胃粘膜Na,K-ATPase和pH值的影响[J].西安交通大学学报(医学版),2003,24(5):461-490
[8]赵洁,张文.丹参对幼年大鼠应激性溃疡预防作用机制的实验研究[J].儿科药学杂志,2009,15(6):7-10,16
[9]周海英,谭慧敏,于海萍,等.生大黄治疗应激性溃疡出血40例[J].四川中医,2002,20(12):36
[10]曹晓林,刘莉,王志鹏,等.唐古特大黄多糖对大鼠应激性胃溃疡的保护作用[J].中国临床药理学与治疗学,2004,9(10):1115-1118
[11]谭明义,陈根成,卢梅生.大黄胶囊预防大鼠脑出血并发应激性胃溃疡的研究简报[J].中药新药与临床药理,2000,11(6):356-357
[12]汶希,陈楚杰,陈建新.大黄提取液干预运动应激性胃溃疡大鼠模型的实验研究[J].中医学报.2012,27(5):585-587
[13]董淑云,郑素琴,门秀丽,等.应激性溃疡的发生及川芎嗪的防治效应[J].中国中西医结合脾胃杂志,1996,4(4):218
[14]万军利,王昌留,崔胜忠.川芎嗪对大鼠浸水应激性胃溃疡的影响[J].中草药,2000,31(2):115-117
[15]李峰,张浩,华桦,等.黄连碱对应激所致小鼠胃黏膜损伤的保护作用[J].华西药学杂志,2007,22(6):713-714
[16]赵敬国.山楂叶总黄酮对大鼠运动应激性溃疡防治作用的实验研究[J].山东体育科技,2001,23(4):29-35
[17]辛益妹,王忠,谷顺才.芦荟对缺氧与疲劳应激小鼠血清白细胞介素-1、6、8含量的影响[J].航空军医,2003,31(1):18-20
[18]严亨秀,殷红梅,王爱华,等.芦荟对应激性溃疡的保护作用[J].中国实用神经疾病杂志,2006,9(6):136-137
[19]付丽新,唐冬梅,严亨秀.芦荟抗应激性胃溃疡的迷走神经机制 [J].西南民族大学学报:自然科学版,2013,39(2):171-175
[20]吴清和,操电群,黄萍,等.高良姜超临界萃取物对应激性溃疡大鼠溃疡形成及表皮生长因子和白介素-2水平的影响[J].中药药理与临床,2004,20(6):17-18
[21]彭钧,操电群,李小月.高良姜超临界萃取物对应激性溃疡模型大鼠溃疡形成和胃液分泌及生长抑素水平的影响[J].安徽医药,2008,12(10):895-897
[22]王琼,赵维中,马传庚.银杏叶提取物的胃粘膜保护作用[J].中国药理学报,2000,21(12):1153-1156
[23]张根葆,孙俊,钱大青,等.银杏叶提取物预防应激性胃溃疡作用机制分析[J].中国危重病急救医学,2000,12(2):80-82
[24]李佳,张常娥.银杏内酯A预防大鼠应激性溃疡的实验研究[J].咸宁学院学报(医学版),2004,18(2):95-97
[25]王福文,李杰,徐学明.复方丹参注射液对大鼠应激性胃溃疡和胃运动的影响[J].山东医药工业,2001,20(5):43-44
[26]曹霞,余良主,赵小玉.复方丹参注射液对大鼠运动应激性溃疡的影响[J].咸宁学院学报(医学版),2003,17(5):318-321
[27]黄铁军,余良主.复方丹参注射液对大鼠应激性胃黏膜损伤的保护作用[J].国际中医中药杂志,2013,35(7):604-606
[28]董亚琳,邢建峰,封卫毅.舒肝丸抗实验性胃溃疡的作用[J].西安交通大学学报(医学版),2004,25(1):79-82.
[29]梁媛,谭达全,张文将,等.左金丸对大鼠应激性胃溃疡保护作用的实验研究[J].湖南中医杂志,2013,29(9):120-122
[30]刘晓伟,张红梅,曲宏达,等.左金丸对应激性胃溃疡粘膜损伤保护作用机理的研究[J].江西中医药,2004,35(260):18-19
[31]张红梅,刘晓伟,曲宏达,等.左金丸对应激性溃疡大鼠下丘脑室旁核c-fos及HPA轴的调节作用[J].中国中西医结合急救杂志,2004,11(5):276-279
[32]林科名,丁世兰,王强松,等.左金丸总生物碱对束缚水浸应激性胃溃疡模型大鼠神经体液调节的影响[J].中国药理通 报,2013,29(3):401-405
[33]李杰,刘长江,李庆和,等.心理应激对大鼠下丘脑、胃粘膜CRF基因表达的影响及中药干预的实验研究[J].中医杂志,2002,43(9):699-700
[34]吕树泉,贾锡莲,杨玉龙,等.心身1号片对大鼠应激性溃疡胃黏膜Bcl-2和Bax表达的影响[J].天津中医药,2008,25(2):147-149
[35]周艳艳,周安方,蔡丽芬,等.大柴胡汤对大鼠应激性胃溃疡的防治作用研究[J].中医药学刊,2006,24(6):1056-1058
[36]徐安莉,蔡丽芬,周艳艳.大柴胡汤防治应激性溃疡的实验研究[J].中国中医药科技,2004,11(5):289
[37]罗丹,熊家平.大柴胡汤对应激性溃疡大鼠血清内皮素(ET)和血清前列腺I2(PGI2)的影响[J].中华实用中西医杂志,2003,3(16):1741-1742
[38]徐颖,张祖志,方正清,等.半夏泻心汤对应激性胃黏膜损伤大鼠血管活性肠肽含量的影响[J].中医药临床杂志,2004,16(2):97-98
[39]张忠,司银楚,吴海霞,等.半夏泻心汤及其拆方对应激性胃溃疡大鼠胆碱能神经元的影响[J].中国中医基础医学杂志,2005,11(4):283-284
[40]张忠,司银楚,白丽敏,等.半夏泻心汤及共拆方对应激性胃溃疡大鼠胃泌素的影响[J].世界华人消化杂志,2005,13(10):1223-1224
[41]彭磊.针刺对应激性溃疡模型大鼠脑源性神经营养因子等影响的实验研究[D],北京中医药大学,2010
[42]孙锦平,田淑君,田庆华,等.针刺足三里穴对大鼠冷应激性溃疡下丘脑NOS表达的影响[J],世界华人消化杂志,2004,12(9):2095-2098
[43]孙锦平,王路宁,柳国芳,等.针刺足三里穴对冷应激性胃溃疡大鼠下丘脑与肾上腺SP和POMC表达的影响[J].世界华人消化杂志,2008,16(15):1602-1606
[44]易受乡,彭艳,常小荣,等.艾灸预处理对应激性溃疡大鼠胃黏膜增殖修复的影响[J].世界中西医结合杂志,2007,2(1):21-24
[45]刘密,常小荣,严洁,等.艾灸预处理对应激性溃疡大鼠胃黏膜GSH-Px, SOD, MDA的影响[J].Journal of Acupuncture and Tuina Science,2011,9(1):17-20
[46]刘密,常小荣,严洁,等.艾灸预处理对应激性胃黏膜损伤大鼠血清IL-1α,TNF-α和IL-10的影响[J].中国中医急症,2011,20(6):906-908
[47]于浩.不同针灸配穴防治应激性胃溃疡大鼠的差异蛋白表达分析[J].中国中医药咨讯,2010,2(11):241-242
[48]严洁,黎喜平,黄艾,等.电针足阳明经穴对大鼠胃黏膜损伤修复机制的研究[J].中国中医药信息杂志,2006,13(05):20-23
[49]杨宗保,严洁,常小荣,等.电针胃经穴对应激大鼠血清胃黏膜细胞表皮生长因子受体表达的作用[J].中国行为医学科学,2006,15(12):1066-1068
[50]杨宗保,严洁,邹小平,等.电针大鼠胃经后血清对其胃黏膜细胞表皮生长因子受体表达的影响及浓度效应[J].中国临床康复,2006,10(35):87-89
[51]严洁,杨宗保,常小荣,等.电针大鼠胃经穴的血清对胃黏膜细胞表皮生长因子受体后信息物质表达的影响[J].中西医结合学报,2007,5(03):338-342
[52]杨宗保,严洁,易受乡,等.电针胃经穴的大鼠血清对胃黏膜细胞EGFR阻断后c-myc的影响[J].江西中医学院学报,2009,21(04):27-29
[53]杨宗保,严洁,易受乡,等.电针胃经穴的大鼠血清上调胃黏膜细胞ERK磷酸化[J].基础医学与临床,2009,29(02):135-138
[54]严洁,杨宗保,邹晓平,等.电针胃经穴后胃溃疡大鼠胃黏膜细胞蛋白激酶C活性的变化[J].中国临床康复,2006,10(19):122-24