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在分离的肝内体中,胰岛素的降解与ATP依赖的内体酸化在功能上相关联。

Degradation of insulin in isolated liver endosomes is functionally linked to ATP-dependent endosomal acidification.

作者信息

Desbuquois B, Janicot M, Dupuis A

机构信息

Institut National de la Santé et de la Recherche Médicale, Unité 30, Hôpital Necker Enfants-Malades, Paris, France.

出版信息

Eur J Biochem. 1990 Oct 24;193(2):501-12. doi: 10.1111/j.1432-1033.1990.tb19365.x.

Abstract

The degradation of insulin in isolated liver endosomes and the relationships of this process with ATP-dependent endosomal acidification have been studied. Incubation of endosomal fractions containing 125I-insulin in isotonic KCl at 30 degrees C resulted in a rapid loss of insulin integrity as judged from trichloroacetic acid precipitability, Sephadex G-50 chromatography, immunoreactivity and receptor binding ability, with a maximum at pH 5-6 (t1/2: 10, 10, 6 and 6 min, respectively). On a log/log plot, the amount of acid-soluble products generated was linearly related to the amount of insulin associated with endosomes (slope, 0.80). Upon incubation, virtually all acid-soluble products diffused out of endosomes as judged from their solubility in aqueous poly(ethyleneglycol). In permeabilized endosomes, intact insulin was also released in part extraluminally, but only when degradation was inhibited did this release increase with lowering pH. ATP shifted the pH for maximal insulin degradation to about 7.5-8.5 and caused endosomal acidification as judged from the uptake of acridine orange and the fluorescence of internalized fluorescein-labeled dextran and galactosylated bovine serum albumin (delta pH about 0.8-0.9). GTP, ITP and UTP exerted comparable effects but with lower potencies. The ability of ATP to alter the pH dependence of insulin degradation was maximal in the presence of Cl-, other anions being less effective (Br- greater than gluconate = SO4(2-) greater than NO3- = sucrose = mannitol) and/or inhibitory (NO3-). Na+, K+ and Li+ supported more effectively ATP-dependent insulin degradation than did choline. Divalent cations were required for the ATP effect (Mg2+ = Mn2+ greater than Co2+ greater than Ni2+ = Zn2 greater than Ca2+). Little or no effects of ATP occurred in the presence of proton ionophores such as monensin and carbonyl cyanide chlorophenylhydrazone, and inhibitors of the proton ATPase such as N-ethylmaleimide. The abilities of nucleotides, ions and inhibitors to support or inhibit ATP-dependent insulin degradation were well correlated with their abilities to affect ATP-dependent acidification. The acidotropic agents chloroquine and quinacrine caused a leftward shift in the pH dependence of insulin degradation and a decrease in maximal degradation; in the presence of ATP, chloroquine almost completely inhibited degradation at pH 5-9. It is concluded that ATP-dependent acidification, in part by enhancing the dissociation of the insulin-receptor complex, is required for optimum degradation of insulin within liver endosomes.

摘要

研究了分离的肝内体中胰岛素的降解以及该过程与ATP依赖性内体酸化的关系。在30℃下,将含有125I胰岛素的内体组分在等渗KCl中孵育,从三氯乙酸沉淀性、Sephadex G - 50色谱、免疫反应性和受体结合能力判断,胰岛素完整性迅速丧失,在pH 5 - 6时达到最大值(半衰期分别为10、10、6和6分钟)。在对数/对数图上,产生的酸溶性产物量与内体相关的胰岛素量呈线性关系(斜率为0.80)。孵育后,几乎所有酸溶性产物都从内体中扩散出来,这可从它们在聚乙二醇水溶液中的溶解度判断。在通透的内体中,完整的胰岛素也有部分释放到腔外,但只有当降解受到抑制时,这种释放才会随着pH降低而增加。ATP将胰岛素最大降解的pH值移至约7.5 - 8.5,并导致内体酸化,这可从吖啶橙摄取以及内化的荧光素标记葡聚糖和半乳糖基化牛血清白蛋白的荧光判断(ΔpH约为0.8 - 0.9)。GTP、ITP和UTP产生类似作用,但效力较低。在Cl-存在下,ATP改变胰岛素降解pH依赖性的能力最大,其他阴离子效果较差(Br->葡萄糖酸盐 = SO4(2-)>NO3- = 蔗糖 = 甘露醇)和/或有抑制作用(NO3-)。Na+、K+和Li+比胆碱更有效地支持ATP依赖性胰岛素降解。二价阳离子是ATP发挥作用所必需的(Mg2+ = Mn2+>Co2+>Ni2+ = Zn2+>Ca2+)。在质子离子载体如莫能菌素和羰基氰化物间氯苯腙以及质子ATP酶抑制剂如N - 乙基马来酰胺存在下,ATP几乎没有作用。核苷酸、离子和抑制剂支持或抑制ATP依赖性胰岛素降解的能力与其影响ATP依赖性酸化的能力密切相关。亲酸剂氯喹和奎纳克林使胰岛素降解的pH依赖性向左移动并降低最大降解率;在ATP存在下,氯喹在pH 5 - 9时几乎完全抑制降解。结论是,ATP依赖性酸化部分通过增强胰岛素 - 受体复合物的解离,是肝内体中胰岛素最佳降解所必需的。

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