首页> 美国卫生研究院文献>British Journal of Pharmacology and Chemotherapy >Cholinoceptor-mediated effects on glycerol output from human adipose tissue using in situ microdialysis.
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Cholinoceptor-mediated effects on glycerol output from human adipose tissue using in situ microdialysis.

机译:使用原位微透析胆醇受体介导的对人脂肪组织甘油输出的影响。

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摘要

1. Possible cholinoceptor-mediated effects on lipolysis were investigated in vivo in human subcutaneous adipose tissue of non-obese, non-smoking, healthy subjects, by use of microdialysis. Cholinomimetic and sympathomimetic agents were added to the ingoing dialysate solvent. 2. Addition of nicotine to the perfusion solvent caused a concentration-dependent reversible increase in the levels of glycerol in the dialysate (lipolysis index). The opposite effect (also concentration-dependent and reversible) was caused by the addition of carbachol. The maximum effects were 100% stimulation and 50% inhibition, respectively, by nicotine and carbachol. Neither nicotine nor carbachol stimulated nutritive blood flow in adipose tissue (as measured with an ethanol escape technique). 3. The nicotine effect in situ was concentration-dependently counteracted by the nicotinic cholinoceptor antagonist, mecamylamine. Likewise, the carbachol effect was concentration-dependently counteracted by the muscarinic cholinoceptor antagonist, atropine. 4. When adipose tissue was pretreated with phentolamine plus propranolol in order to obtain a complete alpha and beta-adrenoceptor blockade, the subsequent addition of nicotine or carbachol still induced an increase and decrease in dialysate glycerol levels (lipolytic or antilipolytic effects), respectively. When adipose tissue was pretreated with mecamylamine or atropine, the subsequent addition of acetylcholine caused a reversible decrease and increase, respectively, of the dialysate glycerol levels. 5. Nicotine and carbachol had no effects on glycerol release from human isolated subcutaneous fat cells that were incubated in vivo.(ABSTRACT TRUNCATED AT 250 WORDS)
机译:1.通过微透析,在非肥胖,非吸烟,健康受试者的人皮下脂肪组织中,体内研究了胆甾醇介导的对脂肪分解的作用。将拟胆碱剂和拟交感神经剂添加到传入的透析液溶剂中。 2.在灌注溶剂中添加尼古丁会导致透析液中甘油水平的浓度依赖性可逆增加(脂解指数)。相反的作用(也是浓度依赖性的和可逆的)是由于加入了卡巴胆碱引起的。尼古丁和卡巴胆碱的最大作用分别为100%刺激和50%抑制。尼古丁或卡巴胆碱都不能刺激脂肪组织中的营养性血流(用乙醇逃逸技术测量)。 3.烟碱类胆碱受体拮抗剂美卡明胺可浓度依赖性地抵消烟碱原位作用。同样,毒蕈碱型胆碱受体拮抗剂阿托品可浓度依赖性地抵消卡巴胆碱的作用。 4.当用酚妥拉明加心得安对脂肪组织进行预处理以获得完全的α和β肾上腺素受体阻滞剂时,随后加入尼古丁或卡巴胆碱仍分别引起透析液甘油水平的升高和降低(脂解或抗脂解作用)。当用美甲胺或阿托品对脂肪组织进行预处理时,随后添加的乙酰胆碱分别引起透析液甘油水平的可逆降低和升高。 5.尼古丁和卡巴胆碱对体内培养的人分离的皮下脂肪细胞中的甘油释放没有影响。(摘要截短为250字)

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