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体内胰岛素降解:高效液相色谱分析

Insulin degradation in vivo: a high-performance liquid chromatographic analysis.

作者信息

Benzi L, Cecchetti P, Ciccarone A M, Di Cianni G, Iozzi L C, Caricato F, Navalesi R

机构信息

Cattedra di Malattie del Metabolismo, Università e Istituto di Fisiologia Clinica del CNR, Pisa, Italy.

出版信息

J Chromatogr. 1990 Dec 14;534:37-46. doi: 10.1016/s0378-4347(00)82146-5.

Abstract

The metabolism of insulin in vivo was investigated using an isocratic reversed-phase high-performance liquid chromatographic (RP-HPLC) method. After intravenous injection of A14-[125I]insulin into normals, eight labelled insulin derivatives were found in plasma (peaks 1-8). Two of them (peaks 1 and 7) showed an elution pattern identical with those of reference [125I]monoiodotyrosine and intact A14-[125I]insulin, respectively. Of the other six peaks, five (2-6) eluted before and one (peak 8) after insulin. This pattern was highly reproducible in terms of capacity factors and peak heights. Radioactivity separated by RP-HPLC was further characterized for its trichloroacetic acid precipitability and immunoprecipitability. Fractions corresponding to peaks 4-6 and 8, which showed an immunoprecipitability higher than 50%, were pooled in order to obtain sufficient radioactivity and were found to be insulin separated by Sephadex G-50 chromatography, containing in its structure, after sulphitolysis, intact A-chain and to be partially rebindable to monocyte insulin receptors. These data demonstrate that in blood, products of insulin metabolism circulate which retain a part of the immunological and biological properties of the hormone. These products are clearly separated from one another and from intact insulin by RP-HPLC, suggesting that the appropriate use of this technique may allow a further and more accurate qualitative and quantitative characterization of in vivo insulin metabolism in physiological and pathological conditions.

摘要

采用等度反相高效液相色谱(RP-HPLC)法研究了胰岛素在体内的代谢情况。向正常受试者静脉注射A14-[125I]胰岛素后,在血浆中发现了8种标记的胰岛素衍生物(峰1 - 8)。其中两种(峰1和峰7)的洗脱模式分别与参考[125I]单碘酪氨酸和完整的A14-[125I]胰岛素相同。在其他六个峰中,五个(峰2 - 6)在胰岛素之前洗脱,一个(峰8)在胰岛素之后洗脱。就容量因子和峰高而言,这种模式具有高度的可重复性。通过RP-HPLC分离的放射性物质进一步根据其对三氯乙酸的沉淀性和免疫沉淀性进行了表征。将对应于峰4 - 6和峰8的馏分合并,这些馏分的免疫沉淀性高于50%,以便获得足够的放射性,结果发现它们是通过Sephadex G-50色谱法分离的胰岛素,在亚硫酸解后其结构中含有完整的A链,并且能够部分重新结合到单核细胞胰岛素受体上。这些数据表明,在血液中,胰岛素代谢产物会循环,它们保留了该激素的部分免疫和生物学特性。这些产物通过RP-HPLC彼此之间以及与完整胰岛素明显分离,这表明适当使用该技术可能有助于在生理和病理条件下对体内胰岛素代谢进行更深入、更准确的定性和定量表征。

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