高氧预适应对大鼠心肌缺血损伤时抗氧化酶的影响

抗氧化酶具有减轻心肌缺血再灌注损伤的作用,在抗氧化酶中,比较重要的是超氧化物歧化酶（ＳＯＤ）,谷胱甘肽过氧化物酶（ＧｌｕｔａｔｈｉｏｎｅＰｅｒｏｘｉｄａｓｅ,ＧＳＨｐｘ）和过氧化氢酶（ＣＡＴ）。为了解高氧预适应（ＨｙｐｅｒｏｘｉｃＰｒｅｃｏｎｄｉｔｉｏｎｉｎｇ,ＨＯＰ）对大鼠心肌缺血损伤时抗氧化酶的影响,本实验将实验组大鼠放入高压氧舱内,每日吸８０－８５％氧气（１ａｔｍ,１５－２０％为氮气）６ｈ,连续７ｄ。利用Ｌａｎｇｅｎｄｏｒｆ装置做成心肌缺血再灌注模型。实验动物随机分为二个部分。第一部分可逆性心肌缺血（ＨＯＰＡ组与对照Ａ组）：缺血１０ｍｉｎ,再灌注６０ｍｉｎ。观察冠脉回流液中ＳＯＤ活力,检测心肌内抗氧化酶活力（ＳＯＤ,ＧＳＨｐｘ,ＣＡＴ）。第二部分不可逆性心肌缺血（ＨＯＰＢ组与对照Ｂ组）：缺血６０ｍｉｎ,再灌注６０ｍｉｎ。测定冠脉回流液中肌酸磷酸激酶（ＣＰＫ）含量,ＳＯＤ及心肌内抗氧化酶活力。结果表明：对于可逆性心肌缺血：ＳＯＤ,ＧＳＨｐｘ活力升高;对于不可逆性心肌缺血损伤：ＨＯＰ能减少ＣＰＫ释放,ＳＯＤ活力升高。     

DDPH对猪肺动脉平滑肌细胞PDGF·BB和bFGF表达的影响：免疫细胞化学研究

ＤＤＰＨ［１－（２．６－二甲基苯乙氧基）－２－（３．４二甲氧基苯乙胺基）丙烷盐酸盐］是南京药科大学合成的降压新化合物,也具有降低肺动脉高压和抑制肺动脉平滑肌细胞增殖作用。本实验用细胞培养、免疫细胞化学、图像分析、３Ｈ－ＴｄＲ、细胞周期测定等方法,进一步探讨ＤＤＰＨ对缺氧性肺动脉平滑肌细胞（ＰＡＳＭＣＳ）增殖的抑制机制。结果：缺氧促进肺动脉内皮细胞（ＰＡＥＣｓ）的ＰＤＧＦ·ＢＢ和ｂＦＧＦ两种生长因子的表达（积分光密度ＯＤ值）增高。缺氧内皮细胞条件培养液（ＨＥＣＣＭ）能促进ＰＡＳＭＣＳ的ＰＤＧＦ·ＢＢ的ＯＤ值增高,ｂＦＧＦ的ＯＤ值无明显改变。加药组（ＨＥＣ－ＣＭ＋ＤＤＰＨ）的ＰＤＧＦ·ＢＢ和ｂＦＧＦ的ＯＤ值均显著降低,尤以ＰＤＧＦ·ＢＢ的ＯＤ值减少最多．提示：ＤＤＰＨ能抑制ＨＥＣＣＭ引起ＰＡＳＭＣＳ的ＰＤＧＦ·ＢＢ和ｂＦＧＦ表达增多和细胞增殖。结果与大鼠实验观察相符。     

钙对水稻幼苗抗冷性的影响

ＣａＣｌ２浸种提高水稻幼苗叶片中结合态钙、内源抗氧化剂（ＧＳＨ、ＡｓＡ）含量和膜保护酶（ＣＡＴ、ＳＯＤ和ＰＯＤ）活性,也增加可溶性蛋白质中煮沸稳定蛋白质（ｂｏｉｌｉｎｇ－ｓｔａｂｌｅｐｒｏｔｅｉｎ）的含量。冷胁迫期间,ＣａＣｌ２并能减少因冷胁迫引起的ＧＳＨ、ＡｓＡ含量,ＣＡＴ、ＳＯＤ和ＰＯＤ活性以及煮沸稳定蛋白质下降的程度。在恢复期间,经ＣａＣｌ２处理的幼苗其ＧＳＨ、ＡＳＡ、ＣＡＴ、ＳＯＤ和ＰＯＤ以及煮沸稳定蛋白质水平均有回升。     

三唑酮对绿豆幼苗叶片衰老的延缓作用

三唑酮处理可提高离体绿豆（ＰｈａｓｅｏｌｕｓｒａｄｉａｔｕｓＬ．）幼苗叶片叶绿素和蛋白质含量。叶片衰老过程中超氧物歧化酶（ＳＯＤ）、过氧化物酶（ＰＯＤ）、过氧化氢酶（ＣＡＴ）和抗坏血酸过氧化物酶（ＡｓＡＰＯＤ）活性及抗坏血酸（ＡｓＡ）和还原型谷胱甘肽（ＧＳＨ）含量降低。２０ｍｇ／Ｌ三唑酮可提高ＰＯＤ、ＡｓＡＰＯＤ活性和ＡｓＡ、ＧＳＨ含量,对ＳＯＤ、ＣＡＴ活性无影响。丙二醛（ＭＤＡ）含量在叶片衰老过程中提高,并与ＰＯＤ、ＡｓＡＰＯＤ活性和ＡｓＡ、ＧＳＨ含量呈显著负相关,三唑酮可降低ＭＤＡ含量。表明三唑酮有提高植物对膜脂过氧化作用的保护能力,延缓叶片的衰老作用。     

6－Dimethylaminopurine（6－DMAP） Spontaneously Induces Interphase Transition Of Metaphase Mouse Oocytes

６－Ｄｉｍｅｔｈｙｌａｍｉｎｏｐｕｒｉｎｅ（６－ＤＭＡＰ）ＳｐｏｎｔａｎｅｏｕｓｌｙＩｎｄｕｃｅｓＩｎｔｅｒｐｈａｓｅＴｒａｎｓｉｔｉｏｎＯｆＭｅｔａｐｈａｓｅＭｏｕｓｅＯｏｃｙｔｅｓ￥ＳＵＮＱｉｎｇ－ｙｕａｎ（孙青原）;ＧＡＯＳｈａｏ－ｒｏｎｇ（高...     

大鼠中缝隐核增强dPAG诱导的vPAG的c－Fos表达及对vPAG神经元放电的影响

本实验通过Ｐｏｓ免疫细胞化学、电生理及微量注射法对中缝隐核（ＮＲＯ）的交感抑制作用的相关途径进行探讨。实验在成巴比妥钠或α－氯醛糖和氨基甲酸乙脂麻醉的Ｓｐｒａｇｕｅ－Ｄａｗｌｅｙ（ＳＤ）大鼠上进行。同时予以ＮＲＯ,中脑导水管周围灰质背侧部（ｄＰＡＧ）方波脉冲串刺激,诱导中脑和延髓的ｃ－Ｆｏｓ表达。刺激ＮＲＯ过程中,基础血压升高（Ｐ＜０．０５）,刺激ｄＰＡＧ引起的防御性升压反应则减少（Ｐ＜０．０１）;中脑导水管周围灰质腹侧部（ｖＰＡＧ）、巨细胞旁外侧核（ＰＧＬ）的Ｆｏｓ样免疫阳性反应（ＦＬＩ）细胞计数分别为６６．５±８．３和１０．８±１．５（刺激ＮＲＯ＋ｄＰＡＧ组）,较单独刺激ｄＰＡＧ组明显增加,Ｐ值分别小于０．０１和０．００１;单或双脉冲刺激中缝隐核在ｖＰＡＧ可以记录到相关单位,其中８４％为兴奋单位,抑制单位占１６％。双侧ｖＰＡＧ内微量注射利多卡因（每侧２μｇ／０．１μｌ）,基础血压无明显变化,而刺激ＮＲＯ引起的降压反应幅度减小（Ｐ＜０．０１）,提示,延髓腹外侧区（ＶＬＭ）、ＮＲＯ存在不同功能分化的神经元;ＮＲＯ可能有向ｖＰＡＧ的兴奋性投射,此投射可加强ＮＲＯ的交感抑制效应。     

NMR法研究天花粉蛋白TDK肽片段的溶液构象

用ＨＮＭＲ法测定ＴＤＫ肽在Ｈ２Ｏ（ＨＯＤＫ）,５０％六氟丙醇（ＦＰＤＫ）和２ｍｏｌ／ＬＧｕ．ＨＣｌ（ＧＵＤＫ）溶液构象。在ＨＯＤＫ和ＦＰＤＫ中,ＴＤＫ肽的两段序列Ａｓｐ０－Ｉｌｅ４,Ｓｅｒ９－Ｉｌｉ１７分别具有较稳定的α－螺旋含量;而ＧＵＤＫ的ＳＡＬＳ序列仍能检测到有序残存结构。并假设ＳＡＬＳ序列是肽链形成二级结构的原始核心。     

大鼠实验性脾虚证胰腺组织化学研究

用成年雄性Ｗｉｓｔａｒ大鼠３０只,分为（１）正常对照组,喂饲自来水。（２）脾虚组,用苦降破气中药和饮食失节法致成脾虚模型。（３）自然恢复组,动物致虚后,喂饲自来水。（４）中药治疗组。取四组动物胰腺进行ＲＮＡ,琥珀酸脱氢酶（ＳＤＨ）,乳酸脱氢酶（ＬＤＨ）,三磷酸腺苷酶（ＡＴＰａｓｅ）,葡萄糖－６－磷酸酶（Ｇ－６－Ｐａｓｅ）和硫胺素焦磷酸酶（ＴＰＰａｓｅ）组织化学反应和观察,并对ＳＤＨ,ＬＤＨ,ＲＮＡ进行了显微分光光度计定量测定。本研究结果表明,脾虚组胰腺泡细胞的ＲＮＡ,ＳＤＨ,ＡＴＰａｓｅ,Ｇ－６－Ｐａｓｅ,ＴＰＰａｓｅ含量和活性都低于对照组,而ＬＤＨ活性高于对照组。治疗组与自然恢复组相比,治疗组胰腺泡细胞以上指标接近对照组。定量测定与定性的结果一致。本研究表明,脾虚证时胰腺泡细胞上述几种酶活性和ＲＮＡ明显下降,可能在脾虚证发病中起主要作用,中药治疗有显著改善     

刺五加在大鼠实验性肝癌诱发过程中作用的探讨

目的探讨大鼠实验性肝癌发病中刺五加对肌体免疫功能和抗氧化酶活性的影响。方法４６只ＳＤ雄性大鼠被随机分成对照组（喂普通饲料）、３－甲基４－双甲氨基偶氮苯（３－Ｍｅ－ＤＡＢ）组（喂含０．０６％３Ｍｅ－ＤＡＢ饲料 １０周）和刺五加组（饲喂同 ３－Ｍｅ－ＤＡＢ外、另加入刺五加 ４．５ｇ／ｋｇ饲料,用常规方法检测全血谷光甘肽过氧化物酶（ＧＳＨ－ＰＸ）、血清超氧化物歧化酶（ＳＯＤ）活性和丙二醛（ＭＤＡ）含量,用微量化学发光造检测吞噬细胞活性（ＰＭＮ－ＣＬ）。结果１．ＰＭＮ－ＣＬ检测峰值、积分值和吞噬细胞指数,３－ＭｅＤＡＢ组较正常组和刺五加组均有显著升高（Ｐ＜０．０５和Ｐ＜０．０１）２．全血ＧＳＨ－ＰＸ活性、ＳＯＤ活性,刺五加组较３－ＭｅＤＡＢ组均有显著升高（Ｐ＜０．０５）。ＭＤＡ含量刺五加组和３－ＭｅＤＡＢ组均较正常组升高（均Ｐ＜０．０５）。结论刺五加在大鼠实验性肝癌诱发过程中有提高抗氧化酶活性和对抗致癌剂引起的机体中性粒细胞吞噬功能代偿性增高的作用。     

大鼠20α羟类固醇脱氢酶在大肠杆菌中的表达

利用谷胱甘肽Ｓ－转移酶（Ｇｌｕｔａｔｈｉｏｎｅ　Ｓ－ｔｒａｎｓｆｅｒａｓｅ,ＧＳＴ）融合基因表达系统,大鼠２０α羟类固醇脱氢酶（２０αＨｙｄｒｏｘｙｓｔｅｒｏｉｄＤｅｈｙｄｒｏｇｅｎａｓｅ,２０αＨＳＤ）在大肠杆菌中得以成功地表达。亲和层析和Ｔｈｒｏｍｂｉｎ消化,可从融合蛋白中回收和纯化重组２０αＨＳＤＳＤＳ－ＰＡＧＥ、Ｗｅｓｔｅｒｎ印迹法和酶活性测定显示,重组２０αＨＳＤ具有天然蛋白质相同分子量、相似的抗原性和酶催化活性,其对ＮＡＤＰ的Ｋ＿ｍ值和Ｖ＿（ｍａｘ）分别为９．５μｍｏｌ／Ｌ、３３４ｎｍｏ１／（ｍｉｎ·ｍｇ）,对底物２０α羟孕酮（２０αＨｙｄｒｏｘｙｐｒｏｇｅｓｔｅｒｏｎｅ,２０αＯＨＰ）的Ｋ＿ｍ值和Ｖ＿（ｍａｘ）分别为５．９μｍｏｌ／Ｌ和３４７ｎｍｏｌ／（ｍｉｎ·ｍｇ）,利用该表达系统大量制备大鼠重组２０αＨＳＤ,为深入研究２０αＨＳＤ的生理活性和功能创造条件。     

糖尿病痛过敏大鼠尾神经中传入单位对交感传出的反应

实验观察了刺激交感神经（sympathetic stimulation,SS）、静脉注射去甲肾上素（noradrenaline,NA）和酚妥拉明对糖尿病痛过敏大鼠尾神经中各种传入单位的影响。结果发现,糖尿病痛过敏大鼠的具有自发放电的C单位和Aδ单位在SS后放电频率增加,α－受体阻断剂能消除这些自发放电活动;在无自发放电的C单位和Aδ单位中,SS能使部分C单位和Aδ单位由静息状态转入活动状态;它虽不能诱发C－机械感受单位（C mechanical receptive unit,C-M）产生传入放电,但可诱发部分C－机械热单位（C mechano-heat unit,C-MH）和C－多型单位（C polymodal unit,C-Pol）的活动;SS还能使部分Aδ－机械单位（Aδ mechanical receptive unit,Aδ-M）和Aδ－机械热单位（Aδ mechano-heat unit,Aδ-MH）产生传入放电;它所诱发的C单位和Aδ单位反应的潜伏期不等,但不短于5s;SS不能引起糖尿病痛过敏大鼠Aβ机械感受性单位和对照组大鼠各类感受性单位产生新的传入活动。静脉注射NA可诱发糖尿病痛过敏大鼠的部分C单位和Aδ单位产生新的传入活动。结果提示,交感神经末梢释放的NA对糖尿病痛过敏大鼠C单位和Aδ单位的兴奋作用是糖尿病大鼠产生痛过敏和感觉异常的外周因素。     

神经节苷脂对6-OHDA损毁交感神经末梢的对抗作用

单次6-OHDA (15mg/kg.i.p.)注射后24h,可使雌性成年小鼠颌下腺内儿茶酚胺荧光神经末梢几乎完全消失;同时用 HPLC 测得腺体内去甲肾上腺素(NA)和多巴胺(DA)的含量下降至正常值的3—4%以下。随着受损交感神经末梢再生过程,NA 和 DA 水平有缓慢的恢复。在损毁2周时 NA 和 DA 含量分别达到正常水平的50%和28%,且在4周时完全恢复。在注射6-OHDA 的同时,和在损伤后12h 内给动物注射4次神经节苷脂(每次50mg/kg.i.p.)并在其后的一周內每天注射一次,可使颌下腺内 NA 含量维持在正常水平;在损毁后4h 及损毁前4d 开始施用神经节苷脂,也可不同程度地对抗交感神经末梢损伤,但作用强度不如前者。实验结果提示:(1)神经节苷脂通过减弱6-OHDA 及其代谢产物的损伤效应能够保护交感神经末梢膜,它可能还有促损伤末梢再生性长芽的作用;(2)损伤后神经节苷脂处理得越早,其效果越好。     

Effects of 6-hydroxydopamine on brain and blood catecholamines, ammonia, and amino acids in rats

The effect of 6-hydroxydopamine (6-OHDA) upon brain and blood catecholamines, ammonia, and amino acids has been studied in rats subjected to increasing doses of the drug. Time dependent effects after injection have also been studied. Systemically injected 6-OHDA significantly, acutely reduced brain adrenaline (A), noradrenaline (NA), total catecholamines (TC), gamma-aminobutyric acid (GABA), and glutamic acid (Glu); concomitantly brain ammonia (NH3) increased. In blood, NA and TC were reduced and A and NH3 increased. The changes in brain monoamines are surprising since it has been reported that 6-OHDA does not cross the blood-brain barrier. We have proposed that these changes result from a general stress response or a reflex peripheral sympathetic response to falling blood pressure which in some manner communicates to the central nervous system. As the dose of 6-OHDA increased, brain NH3 increased and Glu decreased. A similar effect was seen from a single dose as the time after injection for sampling brain and blood constituents increased. Blood ammonia increases without change in Glu, glutamine, or asparagine. The source of NH3 may be from deamination of adenine nucleotide or catechols released from nerve terminals under the abnormal stimulus of 6-OHDA.     

Prostaglandin inhibitor indomethacin inhibits afferent activities of Adelta and C units in the saphenous nerve of diabetic hyperalgesic rats

The effects of a non-selective inhibitor of cyclo-oxygenase (COX) indomethacin, and exogenous prostaglandin E(2) (PGE(2)) on A(delta) units and C units in the saphenous nerve of diabetic hyperagesic rats were studied. The results showed that the conduction velocity of A(delta) units and C units and their mechanical threshold in diabetic hyperagesic rats were obviously decreased, and a small number of A(delta) units (4/24) and C units (2/18) produced increased spontaneous activities. Intraperitoneal injection of indomethacin in diabetic hyperagesic rats significantly relieved mechanical hyperalgesia, and resulted in a decrease in spontaneous afferent activities of the A(delta) units and C units. Subcutaneous injection of exogenous PGE(2) into the diabetic hyperagesic and control rats produced a significant decrease in mechanical threshold of the A(delta) units and C units, and elicited discharge from 3 A(delta) units (3/24) and 1 C unit (1/18) in diabetic hyperagesic rats and from 2 A(delta) units (2/13) in control rats. The present data suggest that the synthesis and release of PGs are increased in diabetic neuropathy, PGs can sensitize and /or activate A(delta) units and C units and elicit hyperagesia and allodynia in diabetic rats.     

Production of Hyperalgesic Prostaglandins by Sympathetic Postganglionic Neurons

Prostaglandin E2 and prostacyclin (prostaglandin I2) produce hyperalgesia in animals and humans. Because there is evidence that prostaglandins contribute to pain maintained by sympathetic nervous system activity, we evaluated whether sympathetic postganglionic neurons synthesize these hyperalgesic prostaglandins, and whether production of prostaglandins by these neurons can contribute to sensitization of primary afferent nociceptors. Intradermal injection of arachidonic acid but not linoleic acid, in the rat hindpaw, produces a decrease in mechanical nociceptive threshold. This hyperalgesic effect is prevented by indomethacin, an inhibitor of prostaglandin synthesis or by prior surgical removal of the lumbar sympathetic chain. To test the hypothesis that sympathetic postganglionic neurons are the source of prostaglandins, we measured production of prostaglandin E2 and 6-keto-prostaglandin F1 alpha (the stable metabolite of prostacyclin) by homogenates of adult rat sympathetic postganglionic neurons from superior cervical ganglia. These homogenates produced significant amounts of prostaglandin E2 and 6-keto-prostaglandin F1 alpha, and most of this production is eliminated by neonatal administration of 6-hydroxydopamine which selectively destroys sympathetic postganglionic neurons. These results demonstrate that sympathetic postganglionic neurons produce prostaglandins, and supports further the hypothesis that the release of prostaglandins from sympathetic postganglionic neurons contributes to the hyperalgesia associated with sympathetically maintained pain.     

动脉壁脑啡肽的含量,存在部位及作用途径

用放射免疫法测得兔动脉的亮氨酸脑啡肽(L-ENK)和甲硫氨酸脑啡肽(M-ENK)样免疫活性物的含量(pg/mg组织湿重)分别为耳动脉38.99±17.29,134.67±8.11;肾动脉31.10±7.76,93.60±18.22,肠系膜动脉25.70 13.60,88.43±18.16。动物经注射交感神经末梢化学切割剂6-OHDA后,这三种动脉中L-ENK样免疫活性物的含量均明显下降(P<0.001);切除颈上神经节使支配耳动脉的交感神经溃变后,或离体耳动脉条受电场刺激后,脑啡肽(ENK)样免疫活性物的含量也都显著下降(P<0.001);但注射利血平则无明显影响,用荧光法测定培育动脉条的浴槽液中NE的含量,观察到ENK可抑制电场刺激所引起的NE的释放。结果提示,动脉壁的L-ENK和M-ENK存在于交感神经末梢中,它可因受电场刺激而释放,可能通过激活突触前膜阿片受体,减少交感神经末梢释放NE,从而抑制动脉的收缩活动。     

EFFECTS OF 6-HYDROXYDOPAMINE ON CATECHOLAMINE CONTAINING NEURONES IN THE RAT BRAIN

After the intraventricular injection of 6-hydroxydopamine (6-OHDA), there was a long lasting reduction in the brain concentrations of noradrenaline (NA) and dopamine (DA). The brain concentration of NA was affected by lower doses of 6-OHDA than were required to deplete DA. A high dose of 6-OHDA which depleted the brain of NA and DA by 81 per cent and 66 per cent respectively, had no significant effect on brain concentrations of 5-hydroxytryptamine (5-HT) or γ-aminobutyric acid (GABA). The fall in catecholamines was accompanied by a long lasting reduction in the activities of tyrosine hydroxylase and DOPA decarboxylase in the hypothalamus and striatum, areas in the brain which are rich in catecholamine containing nerve endings. There was, however, no consistent effect on catechol-O-methyl transferase or monamine oxidase activity in these brain regions. The initial accumulation of [³H]NA into slices of the hypothalamus and striatum was markedly reduced 22–30 days after 6-OHDA treatment. These results are consistent with the evidence in the peripheral sympathetic nervous system that 6-OHDA causes a selective destruction of adrenergic nerve endings and suggest that this compound may have a similar destructive effect on catecholamine neurones in the CNS.     

Resveratrol, a polyphenolic phytoalexin attenuates thermal hyperalgesia and cold allodynia in STZ-induced diabetic rats

The effects of resveratrol, a polyphenolic phytoalexin present in red wine have been investigated on hyperalgesia and cold allodynia in streptozotocin (STZ) induced diabetic rats. Diabetes was induced by a single intraperitoneal injection of streptozotocin (65mg/kg). After 4-weeks of STZ injection, diabetic rats exhibited a significant thermal hyperalgesia and cold allodynia along with increased plasma glucose and decreased body weights as compared with controls rats. Chronic treatment with resveratrol (10mg/kg orally) from week 4 to week 6 significantly attenuated the cold allodynia and thermal hyperalgesia. The results emphasize the role of oxidative stress in development of hyperalgesia and cold allodynia in diabetic animals and point towards the potential of resveratrol as an adjuvant therapy for the prevention and treatment of diabetic neuropathy.     

A possible role for spinal noradrenaline in the mechanisms of 6-hydroxydopamine against pentylenetetrazol induced convulsions in rats

The threshold of the generalized clonic convulsions induced by intravenous infusion of pentylenetetrazol (PTZ) was significantly increased by the intraperitoneal administration of noradrenaline (NA) neurotoxin, 6-hydroxydopamine, which produced no changes in the levels of catecholamines in discrete areas of rat brain, but the effect was accompanied by spinal depletion of NA. Moreover, the anticonvulsant effects of phenobarbitone (PB) and diphenylhydantoin (DPH) against PTZ convulsions were also significantly increased in the animals pretreated with 6-OHDA. These results suggest that the observed elevation of PTZ convulsive threshold and the potentiation of anticonvulsant activity of PB and DPH in 6-OHDA treated rats were possibly mediated through spinal cord depletion of NA.     

Opposite Effect of Mast Cell Stabilizers Ketotifen and Tranilast on the Vasoconstrictor Response to Electrical Field Stimulation in Rat Mesenteric Artery

Objectives

We analyzed whether mast cell stabilization by either ketotifen or tranilast could alter either sympathetic or nitrergic innervation function in rat mesenteric arteries.

Methods

Electrical field stimulation (EFS)-induced contraction was analyzed in mesenteric segments from 6-month-old Wistar rats in three experimental groups: control, 3-hour ketotifen incubated (0.1 αmol/L), and 3-hour tranilast incubated (0.1 mmol/L). To assess the possible participation of nitrergic or sympathetic innervation, EFS contraction was analyzed in the presence of non-selective nitric oxide synthase (NOS) inhibitor L-NAME (0.1 mmol/L), α-adrenergic receptor antagonist phentolamine (0.1 µmol/L), or the neurotoxin 6-hydroxydopamine (6-OHDA, 1.46 mmol/L). Nitric oxide (NO) and superoxide anion (O₂ ^.-) levels were measured, as were vasomotor responses to noradrenaline (NA) and to NO donor DEA-NO, in the presence and absence of 0.1 mmol/L tempol. Phosphorylated neuronal NOS (P-nNOS) expression was also analyzed.

Results

EFS-induced contraction was increased by ketotifen and decreased by tranilast. L-NAME increased the vasoconstrictor response to EFS only in control segments. The vasodilator response to DEA-NO was higher in ketotifen- and tranilast-incubated segments, while tempol increased vasodilator response to DEA-NO only in control segments. Both NO and O₂ ^- release, and P-nNOS expression were diminished by ketotifen and by tranilast treatment. The decrease in EFS-induced contraction produced by phentolamine was lower in tranilast-incubated segments. NA vasomotor response was decreased only by tranilast. The remnant vasoconstriction observed in control and ketotifen-incubated segments was abolished by 6-OHDA.

Conclusion

While both ketotifen and tranilast diminish nitrergic innervation function, only tranilast diminishes sympathetic innnervation function, thus they alter the vasoconstrictor response to EFS in opposing manners.