感染性休克患者中性粒细胞弹性酶裂解皮质类固醇结合球蛋白的质谱检测及其与Asn347位点糖基化的关系。

IF 3.2 3区 医学 Q2 MEDICAL LABORATORY TECHNOLOGY
Clinica Chimica Acta Pub Date : 2025-02-01 Epub Date: 2024-12-20 DOI:10.1016/j.cca.2024.120108
Jessica H Lee, Zeynep Sumer-Bayraktar, Parul Mittal, Leigh Donnellan, Clifford Young, R Louise Rushworth, John G Lewis, Marni Nenke, Wayne Rankin, Manuela Klingler-Hoffman, Peter Hoffmann, Morten Thaysen-Andersen, David J Torpy, Emily J Meyer
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引用次数: 0

摘要

背景:皮质类固醇结合球蛋白(CBG)通过调节皮质醇:CBG结合亲和力来响应多种因素,包括中性粒细胞弹性酶(NE)裂解反应性中心环(RCL),将高亲和力CBG (haCBG)转化为低亲和力CBG (laCBG)。体外,Asn347位点RCL的糖基化影响NE的裂解敏感性。迄今为止,还没有直接测量laCBG来证实NE解理的报道。目的:采用质谱法测定感染性休克患者血清laCBG,确认NE在体内的裂解情况,并采用Asn347位点糖基化分析,确定其对NE裂解的影响,并确定%laCBG对感染性休克临床结局的影响。方法:采用质谱法分析某三级医院重症监护病房脓毒性休克患者血清中CBG亲和形式和CBG免疫沉淀后Asn347糖基化谱。数据与脓毒性休克临床结果相关。结果:NE切割RCL n端肽(AVLQLNEEGVDTAGSTGV)在患者血清中持续检测到,尽管浓度较低。感染性休克的平均laCBG/总CBG %为0.23 %(范围 = 0.07-0.74 %,SD = 0.12 %);健康对照组的平均laCBG %为0.04 %(范围0.02-0.08 %,SD = 0.03 %)。三脉Asn347聚糖与%laCBG、血清CBG浓度呈负相关;TS3 (r = -0.190,p = 0.040)和TS3F (r = -0.252,p = 0.006)。结论:感染性休克患者血清中存在NE cleaved CBG (laCBG),且laCBG百分比与Asn347糖基化占用和组成相关。然而,血清laCBG百分比与感染性休克的临床结果无关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Mass spectrometric detection of neutrophil elastase cleaved corticosteroid binding globulin and its association with Asn347 site glycosylation, in septic shock patients.

Background: Corticosteroid-binding globulin (CBG) modulates tissue cortisol availability via modification of cortisol:CBG binding affinity in response to multiple factors, including neutrophil elastase (NE) cleavage of the reactive centre loop (RCL), converting high affinity CBG (haCBG) to low affinity CBG (laCBG). In vitro, glycosylation of the RCL at Asn347 affects NE cleavage susceptibility. To date, no direct measurement of laCBG, which would verify NE cleavage, has been reported.

Objective: To measure serum laCBG in septic shock patients by mass spectrometry to confirm NE cleavage in vivo, with Asn347 site glycosylation profiling to determine its impact on NE cleavage, and determine effect of %laCBG on septic shock clinical outcome.

Methods: Serum from septic shock patients from a tertiary hospital intensive care unit was analysed by mass spectrometry for CBG affinity forms and Asn347 glycosylation profile, following CBG immunoprecipitation. Data was correlated with septic shock clinical outcome.

Results: N-terminal peptide of NE cleaved RCL (AVLQLNEEGVDTAGSTGV) was consistently detected in patient serum, although at low concentrations. Mean %laCBG/total CBG was 0.23 % in septic shock (range = 0.07-0.74 %, SD = 0.12 %); in comparison healthy controls mean %laCBG was 0.04 % (range 0.02-0.08 %, SD = 0.03 %). There was a negative correlation between %laCBG and serum concentrations of CBG with triantennary Asn347 glycans; TS3 (r = -0.190, p = 0.040) and TS3F (r = -0.252, p = 0.006).

Conclusions: NE cleaved CBG (laCBG) is present in septic shock patient serum, and %laCBG correlates with Asn347 glycosylation occupancy and composition. However, serum %laCBG did not correlate with septic shock clinical outcome.

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来源期刊
Clinica Chimica Acta
Clinica Chimica Acta 医学-医学实验技术
CiteScore
10.10
自引率
2.00%
发文量
1268
审稿时长
23 days
期刊介绍: The Official Journal of the International Federation of Clinical Chemistry and Laboratory Medicine (IFCC) Clinica Chimica Acta is a high-quality journal which publishes original Research Communications in the field of clinical chemistry and laboratory medicine, defined as the diagnostic application of chemistry, biochemistry, immunochemistry, biochemical aspects of hematology, toxicology, and molecular biology to the study of human disease in body fluids and cells. The objective of the journal is to publish novel information leading to a better understanding of biological mechanisms of human diseases, their prevention, diagnosis, and patient management. Reports of an applied clinical character are also welcome. Papers concerned with normal metabolic processes or with constituents of normal cells or body fluids, such as reports of experimental or clinical studies in animals, are only considered when they are clearly and directly relevant to human disease. Evaluation of commercial products have a low priority for publication, unless they are novel or represent a technological breakthrough. Studies dealing with effects of drugs and natural products and studies dealing with the redox status in various diseases are not within the journal''s scope. Development and evaluation of novel analytical methodologies where applicable to diagnostic clinical chemistry and laboratory medicine, including point-of-care testing, and topics on laboratory management and informatics will also be considered. Studies focused on emerging diagnostic technologies and (big) data analysis procedures including digitalization, mobile Health, and artificial Intelligence applied to Laboratory Medicine are also of interest.
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