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Association of a Network of Immunologic Response and Clinical Features With the Functional Recovery From Crotalinae Snakebite Envenoming.
Abstract
<h4>Background</h4>The immunologic pathways activated during snakebite envenoming
(SBE) are poorly described, and their association with recovery is unclear. The immunologic
response in SBE could inform a prognostic model to predict recovery. The purpose of
this study was to develop pre- and post-antivenom prognostic models comprised of clinical
features and immunologic cytokine data that are associated with recovery from SBE.<h4>Materials
and methods</h4>We performed a prospective cohort study in an academic medical center
emergency department. We enrolled consecutive patients with Crotalinae SBE and obtained
serum samples based on previously described criteria for the Surgical Critical Care
Initiative (SC2i)(ClinicalTrials.gov Identifier: NCT02182180). We assessed a standard
set of clinical variables and measured 35 unique cytokines using Luminex Cytokine
35-Plex Human Panel pre- and post-antivenom administration. The Patient-Specific Functional
Scale (PSFS), a well-validated patient-reported outcome of functional recovery, was
assessed at 0, 7, 14, 21 and 28 days and the area under the patient curve (PSFS AUPC)
determined. We performed Bayesian Belief Network (BBN) modeling to represent relationships
with a diagram composed of nodes and arcs. Each node represents a cytokine or clinical
feature and each arc represents a joint-probability distribution (JPD).<h4>Results</h4>Twenty-eight
SBE patients were enrolled. Preliminary results from 24 patients with clinical data,
9 patients with pre-antivenom and 11 patients with post-antivenom cytokine data are
presented. The group was mostly female (82%) with a mean age of 38.1 (SD ± 9.8) years.
In the pre-antivenom model, the variables most closely associated with the PSFS AUPC
are predominantly clinical features. In the post-antivenom model, cytokines are more
fully incorporated into the model. The variables most closely associated with the
PSFS AUPC are age, antihistamines, white blood cell count (WBC), HGF, CCL5 and VEGF.
The most influential variables are age, antihistamines and EGF. Both the pre- and
post-antivenom models perform well with AUCs of 0.87 and 0.90 respectively.<h4>Discussion</h4>Pre-
and post-antivenom networks of cytokines and clinical features were associated with
functional recovery measured by the PSFS AUPC over 28 days. With additional data,
we can identify prognostic models using immunologic and clinical variables to predict
recovery from SBE.
Type
Journal articleSubject
AnimalsHumans
Snake Bites
Crotalid Venoms
Antivenins
Cytokines
Treatment Outcome
Prospective Studies
Predictive Value of Tests
Recovery of Function
Models, Immunological
Time Factors
Adult
Aged
Middle Aged
Female
Male
Biomarkers
Crotalinae
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https://hdl.handle.net/10161/23881Published Version (Please cite this version)
10.3389/fimmu.2021.628113Publication Info
Gerardo, Charles J; Silvius, Elizabeth; Schobel, Seth; Eppensteiner, John C; McGowan,
Lauren M; Elster, Eric A; ... Limkakeng, Alexander T (2021). Association of a Network of Immunologic Response and Clinical Features With the Functional
Recovery From Crotalinae Snakebite Envenoming. Frontiers in immunology, 12. pp. 628113. 10.3389/fimmu.2021.628113. Retrieved from https://hdl.handle.net/10161/23881.This is constructed from limited available data and may be imprecise. To cite this
article, please review & use the official citation provided by the journal.
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John C Eppensteiner
Assistant Professor of Emergency Medicine
John Eppensteiner, MD is an Assistant Professor in the Department of Emergency Medicine.
He completed his emergency medicine training here at Duke University during which
time he served as chief resident. He also completed the first-of-its-kind integrated
research fellowship year which is now an established pathway in the Duke Emergency
Medicine Residency Program. His research interests are primarily focused on the immune
response to trauma and early inflammatory biomarkers used in predictive mo
Charles John Gerardo
Professor of Emergency Medicine
Dr. Gerardo is Professor and interim Chair for the Department of Emergency Medicine.
He graduated with honors from Stanford University with a Bachelor’s of Science in
Biology, and received his MD degree from University of California, Davis. He went
on to complete his residency training in Emergency Medicine at Loma Linda University
Medical Center. He completed his Masters of Health Sciences from the Duke University
Clinical Research and Training Program. In 2000,
Allan Douglas Kirk
David C. Sabiston, Jr. Distinguished Professor of Surgery
I am a surgeon with interest in immune management of transplant recipients. I am particularly
interested in therapies that influence T cell costimulation pathways and adjuvant
therapies that facilitate costimulation blockade to prevent the rejection of transplanted
organs without undue suppression of protective immunity. I am also interested in understanding
how injury, such as that occurring during trauma or in elective surgery, influences
immune responses and subsequent healing following injur
Alexander Tan Limkakeng Jr.
Professor of Emergency Medicine
Dr. Alexander T. Limkakeng, Jr., MD, MHSc, FACEP is a Professor of Emergency Medicine,
Vice Chair of Clinical Research, Director of the Acute Care Research Team, and Director
of the Resident Research Fellowship for the Department of Emergency Medicine in the
Duke University School of Medicine in Durham, North Carolina.
Dr. Limkakeng has served as chair of the American College of Emergency Physicians
(ACEP) Research Committee, and been the Course Directo
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