Gylfe E
Acta Diabetol Lat. 1976 Jan-Apr;13(1-2):20-4. doi: 10.1007/BF02591577.
Glutamate dehydrogenase (GLDH) from bovine liver was employed in model system for testing a possible role of GLDH in insulin release. The ability of different insulin secretagogues to stimulate the activity of the diethylstilbestrol-inhibited enzyme was tested. The two insulin-releasing amino acids, L-leucine and its non-metabolizable analogue 2-aminobicyclo(2, 2, 1)heptane-2-carboxylic acid [b(--)-BCH], were the best stimulators of GLDH activity. The non-secreting stereoisomers, D-leucine and b(+)-BCH, were less effective. Glucose, L-arginine and the leucine metabolite alpha-ketoisocaproic acid lacked significant effects on GLDH activity. Small and diverging effects were obtained with sulfonvlurea compounds: whereas carbutamide caused slight stimulation, tolbutamide and glipizide had no effect, and glibenclamide was an inhibitor. The specificity of the insulin-releasing amino acids L-leucine and b(--)-BCH in stimulating GLDH activity makes it tempting to speculate about a connection between allosteric regulation of pyridine nucleotide-dependent enzymes and insulin release.
牛肝谷氨酸脱氢酶(GLDH)被用于模型系统,以测试GLDH在胰岛素释放中可能发挥的作用。测试了不同胰岛素促分泌剂刺激己烯雌酚抑制的该酶活性的能力。两种胰岛素释放氨基酸,L-亮氨酸及其不可代谢类似物2-氨基双环(2,2,1)庚烷-2-羧酸[b(-)-BCH],是GLDH活性的最佳刺激剂。无分泌作用的立体异构体D-亮氨酸和b(+)-BCH效果较差。葡萄糖、L-精氨酸和亮氨酸代谢物α-酮异己酸对GLDH活性缺乏显著影响。磺脲类化合物产生的作用较小且存在差异:卡比马脲引起轻微刺激,甲苯磺丁脲和格列吡嗪无作用,而格列本脲是一种抑制剂。胰岛素释放氨基酸L-亮氨酸和b(-)-BCH在刺激GLDH活性方面的特异性使得人们不禁推测吡啶核苷酸依赖性酶的变构调节与胰岛素释放之间存在联系。