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生物测定和物理化学测定方法相结合的研究表明,血清通过皮质类固醇结合球蛋白依赖性和非依赖性机制调节皮质醇的生物活性。

Serum regulates cortisol bioactivity by corticosteroid-binding globulin-dependent and independent mechanisms, as revealed by combined bioassay and physicochemical assay approaches.

作者信息

Perogamvros I, Kayahara M, Trainer P J, Ray D W

机构信息

Department of Endocrinology, Christie HospitalEndocrine Sciences Research Group, University of Manchester, Manchester, UK.

出版信息

Clin Endocrinol (Oxf). 2011 Jul;75(1):31-8. doi: 10.1111/j.1365-2265.2011.04003.x.

Abstract

CONTEXT

Corticosteroid-binding globulin (CBG) is the principal carrier of natural glucocorticoids in the circulation, and we hypothesized that it modulates glucocorticoid bioactivity (GBA). Alterations in CBG, the presence of noncortisol, naturally occurring glucocorticoids and the use of potent, synthetic glucocorticoids, all make it difficult to assess adrenal activity in-vivo; these problems can be addressed by a glucocorticoid bioassay.

DESIGN AND SUBJECTS

A bioassay was developed for serum GBA and a physicochemical ultrafiltration-liquid chromatography-tandem mass spectrometry assay for free serum cortisol (FreeF). We studied individuals homozygous and heterozygous for a nonfunctioning CBG variant (CBG G237V) and healthy controls.

RESULTS

FreeF concentrations were similar in healthy controls, and those with absent functional CBG, but surprisingly we found low GBA in CBG null individuals. This may suggest that CBG delivers cortisol to target cells. However, further experiments revealed that dilution of serum in the bioassay caused release of cortisol from CBG, resulting in elevated GBA measurements in all but the CBG G237V homozygotes. Furthermore, we identified a specific and potent inhibitory effect of high concentration serum on glucocorticoid sensitivity of the recipient cells used in the bioassay. Analysis of inflammatory synovial fluid, a filtrate of serum with lower CBG concentration, revealed elevated free cortisol compared to noninflammatory synovial fluid, a change not attributable to interconversion between cortisol and cortisone.

CONCLUSIONS

Our findings reveal that dilution of CBG enhances cortisol release, and so bioactivity, and also that serum potently induces glucocorticoid resistance in target cells.

摘要

背景

皮质类固醇结合球蛋白(CBG)是循环中天然糖皮质激素的主要载体,我们推测它可调节糖皮质激素生物活性(GBA)。CBG的改变、非皮质醇天然存在的糖皮质激素的存在以及强效合成糖皮质激素的使用,均使得体内肾上腺活动的评估变得困难;这些问题可通过糖皮质激素生物测定法来解决。

设计与研究对象

我们开发了一种用于血清GBA的生物测定法以及一种用于游离血清皮质醇(FreeF)的物理化学超滤-液相色谱-串联质谱测定法。我们研究了无功能CBG变异体(CBG G237V)的纯合子和杂合子个体以及健康对照者。

结果

健康对照者与缺乏功能性CBG的个体的FreeF浓度相似,但令人惊讶的是,我们发现CBG缺失个体的GBA较低。这可能表明CBG将皮质醇输送到靶细胞。然而,进一步的实验表明,生物测定中血清的稀释导致皮质醇从CBG中释放出来,导致除CBG G237V纯合子外的所有个体的GBA测量值升高。此外,我们确定了高浓度血清对生物测定中所用受体细胞的糖皮质激素敏感性具有特异性和强效抑制作用。与非炎性滑液相比,对CBG浓度较低的血清滤液炎性滑液的分析显示游离皮质醇升高,这种变化并非归因于皮质醇和可的松之间的相互转化。

结论

我们的研究结果表明,CBG的稀释会增强皮质醇的释放,进而增强生物活性,并且血清会有效诱导靶细胞中的糖皮质激素抵抗。

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