Preferential inhibition of adaptive immune system dynamics by glucocorticoids in patients after acute surgical trauma

Author:

Ganio Edward A.,Stanley Natalie,Lindberg-Larsen ViktoriaORCID,Einhaus JakobORCID,Tsai Amy S.ORCID,Verdonk FranckORCID,Culos AnthonyORCID,Ghaemi Sajjad,Rumer Kristen K.,Stelzer Ina A.ORCID,Gaudilliere Dyani,Tsai Eileen,Fallahzadeh Ramin,Choisy Benjamin,Kehlet HenrikORCID,Aghaeepour NimaORCID,Angst Martin S.ORCID,Gaudilliere BriceORCID

Abstract

AbstractGlucocorticoids (GC) are a controversial yet commonly used intervention in the clinical management of acute inflammatory conditions, including sepsis or traumatic injury. In the context of major trauma such as surgery, concerns have been raised regarding adverse effects from GC, thereby necessitating a better understanding of how GCs modulate the immune response. Here we report the results of a randomized controlled trial (NCT02542592) in which we employ a high-dimensional mass cytometry approach to characterize innate and adaptive cell signaling dynamics after a major surgery (primary outcome) in patients treated with placebo or methylprednisolone (MP). A robust, unsupervised bootstrap clustering of immune cell subsets coupled with random forest analysis shows profound (AUC = 0.92, p-value = 3.16E-8) MP-induced alterations of immune cell signaling trajectories, particularly in the adaptive compartments. By contrast, key innate signaling responses previously associated with pain and functional recovery after surgery, including STAT3 and CREB phosphorylation, are not affected by MP. These results imply cell-specific and pathway-specific effects of GCs, and also prompt future studies to examine GCs’ effects on clinical outcomes likely dependent on functional adaptive immune responses.

Funder

SU | School of Medicine, Stanford University

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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