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肠道碱性磷酸酶对L-高精氨酸的敏感性及其通过亚基-亚基相互作用的调节。

Sensitivity of intestinal alkaline phosphatase to L-homoarginine and its regulation by subunit-subunit interaction.

作者信息

Suzuki K, Yoshimura Y, Hisada Y, Matsumoto A

机构信息

Department of Dental Pharmacology, School of Dentistry, Hokkaido University, Sapporo, Japan.

出版信息

Jpn J Pharmacol. 1994 Feb;64(2):97-102. doi: 10.1254/jjp.64.97.

Abstract

The inhibitory effect of levamisole and L-homoarginine on alkaline phosphatases (ALP, orthophosphoric monoester phosphohydrolase, EC. 3.1.3.1) in various tissues was studied to characterize differences in the mechanism of inhibition of ALP isoenzymes. The ALP activity from the placenta, kidneys, and a clonal osteogenic cell line, MC3T3-E1, was hyperbolically inhibited with a dependency on the concentration of levamisole (Ki0.5 = 10-12 microM) or L-homoarginine (Ki0.5 = 1 mM), but the activity of intestinal ALP was little inhibited by 240 microM levamisole and sigmoidally inhibited by L-homoarginine (Ki0.5 = 13 mM). Hill plot analysis of the L-homoarginine inhibition data showed that the Hill coefficient values of the placenta, kidney, and osteogenic cells were around 0.9-1.0 and that of the intestine was 1.8. The effect of sodium dodecyl sulfate (SDS), which may decrease the subunit-subunit interaction, on the L-homoarginine inhibition of the intestinal ALP was tested. The L-homoarginine concentration-dependent inhibition curve changed from sigmoidal to hyperbolic, and the Hill coefficients decreased with increasing concentrations of SDS. These results suggest that the differences in inhibition by L-homoarginine and affinity changes of intestinal ALP for L-homoarginine are caused by the subunit-subunit interaction of oligomers.

摘要

研究了左旋咪唑和L-高精氨酸对各种组织中碱性磷酸酶(ALP,正磷酸单酯磷酸水解酶,EC. 3.1.3.1)的抑制作用,以表征碱性磷酸酶同工酶抑制机制的差异。胎盘、肾脏和克隆性成骨细胞系MC3T3-E1中的碱性磷酸酶活性呈双曲线抑制,其依赖于左旋咪唑(Ki0.5 = 10-12 microM)或L-高精氨酸(Ki0.5 = 1 mM)的浓度,但240 microM左旋咪唑对肠碱性磷酸酶活性的抑制作用很小,而L-高精氨酸对其呈S形抑制(Ki0.5 = 13 mM)。对L-高精氨酸抑制数据的希尔图分析表明,胎盘、肾脏和成骨细胞的希尔系数值约为0.9 - 1.0,而肠道的希尔系数值为1.8。测试了可能会降低亚基-亚基相互作用的十二烷基硫酸钠(SDS)对L-高精氨酸抑制肠碱性磷酸酶的影响。L-高精氨酸浓度依赖性抑制曲线从S形变为双曲线,并且希尔系数随着SDS浓度的增加而降低。这些结果表明,L-高精氨酸抑制作用的差异以及肠碱性磷酸酶对L-高精氨酸亲和力的变化是由寡聚体的亚基-亚基相互作用引起的。

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