Neutrophil elastase-cleaved corticosteroid-binding globulin is absent in human plasma

Lesley A. Hill, Dimitra A. Vassiliadi, Ioanna Dimopoulou, Anna J. Anderson, Luke D. Boyle, Alixe H.M. Kilgour, Roland H. Stimson, Yoan Machado, Christopher M. Overall, Brian R. Walker, John G. Lewis, Geoffrey L. Hammond*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

Abstract / Description of output

Corticosteroid-binding globulin (CBG) transports glucocorticoids in blood and is a serine protease inhibitor family member. Human CBG has a reactive center loop (RCL) which, when cleaved by neutrophil elastase (NE), disrupts its steroid-binding activity. Measurements of CBG levels are typically based on steroid-binding capacity or immunoassays. Discrepancies in ELISAs using monoclonal antibodies that discriminate between intact vs RCL-cleaved CBG have been interpreted as evidence that CBG with a cleaved RCL and low affinity for cortisol exists in the circulation. We examined the biochemical properties of plasma CBG in samples with discordant ELISA measurements and sought to identify RCL-cleaved CBG in human blood samples. Plasma CBG-binding capacity and ELISA values were consistent in arterial and venous blood draining skeletal muscle, liver and brain, as well as from a tissue (adipose) expected to contain activated neutrophils in obese individuals. Moreover, RCL-cleaved CBG was undetectable in plasma from critically ill patients, irrespective of whether their ELISA measurements were concordant or discordant. We found no evidence of RCL-cleaved CBG in plasma using a heat-dependent polymerization assay, and CBG that resists immunoprecipitation with a monoclonal antibody designed to specifically recognize an intact RCL, bound steroids with a high affinity. In addition, mass spectrometry confirmed the absence of NE-cleaved CBG in plasma in which ELISA values were highly discordant. Human CBG with a NE-cleaved RCL and low affinity for steroids is absent in blood samples, and CBG ELISA discrepancies likely reflect structural differences that alter epitopes recognized by specific monoclonal antibodies.

Original languageEnglish
Pages (from-to)27-39
Number of pages13
JournalJournal of Endocrinology
Volume240
Issue number1
DOIs
Publication statusPublished - 1 Jan 2019

Keywords / Materials (for Non-textual outputs)

  • Cortisol
  • ELISA
  • Monoclonal antibody
  • Steroid binding

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