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胰高血糖素对体内肝微粒体葡萄糖-6-磷酸酶的影响。

Effects of glucagon on hepatic microsomal glucose-6-phosphatase in vivo.

作者信息

Striffler J S, Garfield S A, Cardell E L, Cardell R R

出版信息

Diabete Metab. 1984 May;10(2):91-7.

PMID:6086418
Abstract

The smooth endoplasmic reticulum (SER) has been implicated in glycogen deposition and depletion. It has been suggested that SER proliferation plays a role in elevated glucose release during rapid glycogenolysis (Striffler et al., Am. J. Anat. 160: 363, 1981). In these studies, the role of SER in glucagon-stimulated hepatic glucose release was examined by assessing changes in microsomal glucose-6-phosphatase (G-6-Pase) and membrane cholesterol to phospholipid ratios. In control fed rats given 6 i.p. injections of glucagon 350 micrograms/injection) at hourly intervals, percentage hepatic glycogen decreased nearly 30 fold, with liver homogenate G-6-Pase (U/mg protein) increasing 50% (p less than .02 relative to vehicle-injected controls) from .055 +/- .003 at 0h (n = 12) to .081 +/- .004 at 6h (n = 11). The increase in homogenate G-6-Pase was reflected in the isolated SER fraction by a 48% rise (p less than .01 relative to controls) in activity from a 0h value of .210 +/- .010 (n = 10) to a peak activity of .310 +/- .027 U/mg microsomal protein at 5 h (n = 12). G-6-Pase also increased in the rough endoplasmic reticulum (RER) reaching .242 +/- .023 U/mg protein at 4h (n = 14), but then declining to .209 +/- .019 U/mg protein at 6 h (n = 11). The changes in G-6-Pase were accompanied by alterations in the ratio of microsomal cholesterol to phospholipid, which decreased by 50% (p less than .002) in both RER and SER fractions signifying changes in membrane lipid environment. Ultrastructural analysis revealed a marked reduction in hepatic glycogen and conspicuous presence of elements of the SER in regions of the cytoplasm where glycogen was or presumably had been located.

摘要

滑面内质网(SER)与糖原的沉积和消耗有关。有人提出,在快速糖原分解过程中,滑面内质网的增殖在葡萄糖释放增加中起作用(斯特里弗勒等人,《美国解剖学杂志》160:363,1981)。在这些研究中,通过评估微粒体葡萄糖-6-磷酸酶(G-6-Pase)和膜胆固醇与磷脂比率的变化,研究了滑面内质网在胰高血糖素刺激的肝葡萄糖释放中的作用。在每小时腹腔注射6次胰高血糖素(每次350微克)的对照喂食大鼠中,肝糖原百分比下降了近30倍,肝匀浆G-6-Pase(单位/毫克蛋白质)从0小时时的0.055±0.003(n = 12)增加了50%(相对于注射赋形剂的对照,p<0.02),至6小时时的0.081±0.004(n = 11)。匀浆G-6-Pase的增加在分离的滑面内质网部分中表现为活性增加48%(相对于对照,p<0.01),从0小时时的0.210±0.010(n = 10)增加到5小时时的峰值活性0.310±0.027单位/毫克微粒体蛋白质(n = 12)。粗面内质网(RER)中的G-6-Pase也增加,在4小时时达到0.242±0.023单位/毫克蛋白质(n = 14),但在6小时时降至0.209±0.019单位/毫克蛋白质(n = 11)。G-6-Pase的变化伴随着微粒体胆固醇与磷脂比率的改变,粗面内质网和滑面内质网部分的该比率均下降了50%(p<0.002),这表明膜脂质环境发生了变化。超微结构分析显示,肝糖原明显减少,在糖原所在或可能曾经所在的细胞质区域中,滑面内质网的成分明显存在。

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