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肝脏内质网激素敏感性钙离子摄取活性的表征

Characterization of the hormone-sensitive Ca2+ uptake activity of the hepatic endoplasmic reticulum.

作者信息

Andia-Waltenbaugh A M, Lam A, Hummel L, Friedmann N

出版信息

Biochim Biophys Acta. 1980 Jun 19;630(2):165-75. doi: 10.1016/0304-4165(80)90418-3.

Abstract

The characteristics and kinetics of calcium uptake activity were studied in isolated hepatic microsomes. The sustained accumulation of calcium was ATP- and oxalate-dependent. Glucagon increased microsomal Ca2+ uptake upon either in vivo injection, or in vitro perfusion of the hormone in the liver. In contrast, the effect of insulin depended on the route of administration. Calcium accumulation by subsequently isolated hepatic microsomes increased when insulin was injected intraperitoneally whereas it decreased when the hormone was perfused directly into the liver. These effects of glucagon and insulin were dose dependent. When insulin was added to the perfusate prior to the addition of glucagon, insulin blocked the glucagon-stimulated increase in microsomal Ca2+ uptake. Cyclic AMP mimicked the effect of glucagon on microsomal Ca2+ accumulation when the cyclic nucleotide was perfused into the liver. The effects of glucagon and insulin on the kinetics of hepatic microsomal Ca2+ uptake were investigated. In microsomes isolated from perfused rat livers treated with glucagon the V of the uptake was significantly increased over the control values (12.2 vs. 8.6 nmol Ca2+ per min per mg protein, P less than 0.02). In contrast, the addition of insulin to the perfusate significantly decreased the V of Ca2+ uptake by subsequently isolated microsomes (6.8 vs. 8.3 nmol Ca2+ per min per mg protein, P less than 0.05). However, neither hormone had an effect on the apparent Km for Ca2+ (4.1 +/- 0.5 microM) of the reaction. The effect of these hormones on the activity of Ca2+-stimulated ATPase was also studied. No significant changes in either V or Km for Ca2+ of the enzymatic reaction were detected.

摘要

在分离的肝微粒体中研究了钙摄取活性的特征和动力学。钙的持续积累依赖于ATP和草酸盐。胰高血糖素在体内注射或在肝脏中体外灌注该激素后,会增加微粒体对Ca2+的摄取。相比之下,胰岛素的作用取决于给药途径。当腹腔注射胰岛素时,随后分离的肝微粒体的钙积累增加,而当该激素直接灌注到肝脏中时,钙积累减少。胰高血糖素和胰岛素的这些作用是剂量依赖性的。当在添加胰高血糖素之前将胰岛素添加到灌注液中时,胰岛素会阻断胰高血糖素刺激的微粒体Ca2+摄取增加。当将环磷酸腺苷灌注到肝脏中时,它模拟了胰高血糖素对微粒体Ca2+积累的作用。研究了胰高血糖素和胰岛素对肝微粒体Ca2+摄取动力学的影响。在用胰高血糖素处理的灌注大鼠肝脏中分离的微粒体中,摄取的V值比对照值显著增加(12.2对8.6 nmol Ca2+每分钟每毫克蛋白质,P小于0.02)。相比之下,向灌注液中添加胰岛素会显著降低随后分离的微粒体对Ca2+摄取的V值(6.8对8.3 nmol Ca2+每分钟每毫克蛋白质,P小于0.05)。然而,两种激素对该反应中Ca2+的表观Km(4.1±0.5 microM)均无影响。还研究了这些激素对Ca2+刺激的ATP酶活性的影响。未检测到酶促反应中Ca2+的V或Km有显著变化。

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