血管活性肠肽诱导豚鼠肠道平滑肌细胞舒张：环磷酸腺苷和一氧化氮的相继参与

VIP-induced relaxation of guinea-pig intestinal smooth muscle cells: sequential involvement of cyclic AMP and nitric oxide.

作者信息

Rekik M, Delvaux M, Tack I, Frexinos J, Bueno L

机构信息

Department of Pharmacology, INRA, BP3, F-31931 Toulouse, France.

出版信息

Br J Pharmacol. 1996 Jun;118(3):477-84. doi: 10.1111/j.1476-5381.1996.tb15428.x.

DOI:10.1111/j.1476-5381.1996.tb15428.x

PMID:8762068

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1909695/

Abstract

A possible interaction between cyclic AMP and nitric oxide (NO) in mediating the relaxant effect of vasoactive intestinal polypeptide (VIP) on intestinal smooth muscle cells has been investigated. The effects of the inhibitor of NO synthesis, NG-nitro-L-arginine methyl ester (L-NAME), have been studied on VIP-, forskolin-, and 8 bromo-cyclic AMP- induced relaxation of cells, dispersed by enzymatic digestion of muscle strips from the circular layer of guinea-pig ileum. 2. VIP alone did not modify the length of isolated muscle cells. By contrast, when the cells were contracted by cholecystokinin octapeptide, CCK8 (10 nM), VIP inhibited this contraction, inducing a concentration-dependent relaxation of the cells. Maximal relaxation was induced by 1 microM VIP (EC50 = 408.2 +/- 16.7 pM). 3. N-ethylmaleimide, inhibitors of adenylate cyclase or somatostatin, abolished the relaxing effect of VIP. (R)-p-cAMPs, an antagonist of cyclic AMP on protein kinase A also inhibited the VIP-induced relaxation by 92.1 +/- 6.3%. Inhibitors of nitric oxide synthase (NOS), L-NAME and L-NMMA, partially inhibited VIP-induced relaxation. The effect of L-NAME was reversed by L-arginine but not by D-arginine. 4. (R)-p-cAMPS and L-NAME also inhibited the cell relaxation induced either by forskolin which directly stimulates adenylate cyclase activity or 8-bromo-cyclic AMP, an analogue of cyclic AMP. 5. When cells were incubated for 30 min with dexamethasone 10 microM, a glucocorticoid known to decrease the synthesis of iNOS, the relaxing effect of a maximal concentration of VIP was decreased by 52 +/- 4% and L-NMMA had no further effect on this residual VIP-induced relaxation. Milrinone, a phosphodiesterase type III inhibitor, potentiated the relaxant effect of VIP. 6. These data demonstrate that the intracellular pathway mediating the relaxant effect of VIP in intestinal smooth muscle cells includes the sequential activation of adenylate cyclase, protein kinase A, activation of NOS and finally production of NO and cyclic GMP. NO could in turn regulate the cyclic AMP-dependent pathway of cell relaxation.

摘要

研究了环磷酸腺苷（cAMP）与一氧化氮（NO）在介导血管活性肠肽（VIP）对肠道平滑肌细胞舒张作用中可能存在的相互作用。通过酶消化豚鼠回肠环形肌条分散细胞，研究了NO合成抑制剂N-硝基-L-精氨酸甲酯（L-NAME）对VIP、福斯可林和8-溴环磷酸腺苷诱导的细胞舒张的影响。2. 单独使用VIP不会改变分离的肌肉细胞长度。相比之下，当细胞被八肽胆囊收缩素（CCK8，10 nM）收缩时，VIP可抑制这种收缩，诱导细胞浓度依赖性舒张。1 μM VIP诱导最大舒张（EC50 = 408.2±16.7 pM）。3. N-乙基马来酰胺、腺苷酸环化酶抑制剂或生长抑素可消除VIP的舒张作用。（R）-p-cAMPs是cAMP对蛋白激酶A的拮抗剂，也可使VIP诱导的舒张作用降低92.1±6.3%。一氧化氮合酶（NOS）抑制剂L-NAME和L-NMMA可部分抑制VIP诱导的舒张。L-精氨酸可逆转L-NAME的作用，而D-精氨酸则不能。4. （R）-p-cAMPS和L-NAME也可抑制由直接刺激腺苷酸环化酶活性的福斯可林或cAMP类似物8-溴环磷酸腺苷诱导的细胞舒张。5. 当细胞与已知可降低诱导型NOS合成的糖皮质激素10 μM地塞米松孵育30分钟时，最大浓度VIP的舒张作用降低52±4%，L-NMMA对这种残余VIP诱导的舒张作用不再有进一步影响。米力农是一种III型磷酸二酯酶抑制剂，可增强VIP的舒张作用。6. 这些数据表明，介导VIP对肠道平滑肌细胞舒张作用的细胞内途径包括腺苷酸环化酶的顺序激活、蛋白激酶A、NOS的激活，最终产生NO和环鸟苷酸（cGMP）。NO进而可调节细胞舒张的cAMP依赖性途径

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血管活性肠肽诱导豚鼠肠道平滑肌细胞舒张：环磷酸腺苷和一氧化氮的相继参与

VIP-induced relaxation of guinea-pig intestinal smooth muscle cells: sequential involvement of cyclic AMP and nitric oxide.

作者信息

Rekik M, Delvaux M, Tack I, Frexinos J, Bueno L

机构信息

Department of Pharmacology, INRA, BP3, F-31931 Toulouse, France.

出版信息

Br J Pharmacol. 1996 Jun;118(3):477-84. doi: 10.1111/j.1476-5381.1996.tb15428.x.

DOI:10.1111/j.1476-5381.1996.tb15428.x

PMID:8762068

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1909695/

Abstract

A possible interaction between cyclic AMP and nitric oxide (NO) in mediating the relaxant effect of vasoactive intestinal polypeptide (VIP) on intestinal smooth muscle cells has been investigated. The effects of the inhibitor of NO synthesis, NG-nitro-L-arginine methyl ester (L-NAME), have been studied on VIP-, forskolin-, and 8 bromo-cyclic AMP- induced relaxation of cells, dispersed by enzymatic digestion of muscle strips from the circular layer of guinea-pig ileum. 2. VIP alone did not modify the length of isolated muscle cells. By contrast, when the cells were contracted by cholecystokinin octapeptide, CCK8 (10 nM), VIP inhibited this contraction, inducing a concentration-dependent relaxation of the cells. Maximal relaxation was induced by 1 microM VIP (EC50 = 408.2 +/- 16.7 pM). 3. N-ethylmaleimide, inhibitors of adenylate cyclase or somatostatin, abolished the relaxing effect of VIP. (R)-p-cAMPs, an antagonist of cyclic AMP on protein kinase A also inhibited the VIP-induced relaxation by 92.1 +/- 6.3%. Inhibitors of nitric oxide synthase (NOS), L-NAME and L-NMMA, partially inhibited VIP-induced relaxation. The effect of L-NAME was reversed by L-arginine but not by D-arginine. 4. (R)-p-cAMPS and L-NAME also inhibited the cell relaxation induced either by forskolin which directly stimulates adenylate cyclase activity or 8-bromo-cyclic AMP, an analogue of cyclic AMP. 5. When cells were incubated for 30 min with dexamethasone 10 microM, a glucocorticoid known to decrease the synthesis of iNOS, the relaxing effect of a maximal concentration of VIP was decreased by 52 +/- 4% and L-NMMA had no further effect on this residual VIP-induced relaxation. Milrinone, a phosphodiesterase type III inhibitor, potentiated the relaxant effect of VIP. 6. These data demonstrate that the intracellular pathway mediating the relaxant effect of VIP in intestinal smooth muscle cells includes the sequential activation of adenylate cyclase, protein kinase A, activation of NOS and finally production of NO and cyclic GMP. NO could in turn regulate the cyclic AMP-dependent pathway of cell relaxation.

摘要

研究了环磷酸腺苷（cAMP）与一氧化氮（NO）在介导血管活性肠肽（VIP）对肠道平滑肌细胞舒张作用中可能存在的相互作用。通过酶消化豚鼠回肠环形肌条分散细胞，研究了NO合成抑制剂N-硝基-L-精氨酸甲酯（L-NAME）对VIP、福斯可林和8-溴环磷酸腺苷诱导的细胞舒张的影响。2. 单独使用VIP不会改变分离的肌肉细胞长度。相比之下，当细胞被八肽胆囊收缩素（CCK8，10 nM）收缩时，VIP可抑制这种收缩，诱导细胞浓度依赖性舒张。1 μM VIP诱导最大舒张（EC50 = 408.2±16.7 pM）。3. N-乙基马来酰胺、腺苷酸环化酶抑制剂或生长抑素可消除VIP的舒张作用。（R）-p-cAMPs是cAMP对蛋白激酶A的拮抗剂，也可使VIP诱导的舒张作用降低92.1±6.3%。一氧化氮合酶（NOS）抑制剂L-NAME和L-NMMA可部分抑制VIP诱导的舒张。L-精氨酸可逆转L-NAME的作用，而D-精氨酸则不能。4. （R）-p-cAMPS和L-NAME也可抑制由直接刺激腺苷酸环化酶活性的福斯可林或cAMP类似物8-溴环磷酸腺苷诱导的细胞舒张。5. 当细胞与已知可降低诱导型NOS合成的糖皮质激素10 μM地塞米松孵育30分钟时，最大浓度VIP的舒张作用降低52±4%，L-NMMA对这种残余VIP诱导的舒张作用不再有进一步影响。米力农是一种III型磷酸二酯酶抑制剂，可增强VIP的舒张作用。6. 这些数据表明，介导VIP对肠道平滑肌细胞舒张作用的细胞内途径包括腺苷酸环化酶的顺序激活、蛋白激酶A、NOS的激活，最终产生NO和环鸟苷酸（cGMP）。NO进而可调节细胞舒张的cAMP依赖性途径

血管活性肠肽诱导豚鼠肠道平滑肌细胞舒张：环磷酸腺苷和一氧化氮的相继参与

VIP-induced relaxation of guinea-pig intestinal smooth muscle cells: sequential involvement of cyclic AMP and nitric oxide.

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血管活性肠肽诱导豚鼠肠道平滑肌细胞舒张：环磷酸腺苷和一氧化氮的相继参与

VIP-induced relaxation of guinea-pig intestinal smooth muscle cells: sequential involvement of cyclic AMP and nitric oxide.

作者信息

机构信息

出版信息