Pharmacology of Exenatide in Pediatric Sepsis

Phase 1

Withdrawn

• Conditions: Organ Dysfunction; Inflammation; Septic Shock; Glucose Homeostasis; Health-related Quality of Life
• Interventions: Drug: Exenatide; Drug: Exenatide vehicle

• Registration Number: NCT01573806
• Lead Sponsor: Seattle Children's Hospital

Brief Summary

Pharmacology of Exenatide in Pediatric Sepsis, PEPS is a phase 1-2 research study that will examine drug safety, drug metabolism, drug action and preliminary drug clinical effects of four does of exenatide injected every 12 hours to children with shock from infection (septic shock). The investigators hypothesize that exenatide can be safely dosed to children with sepsis to achieve blood levels of drug similar to that achieved in teenagers with type 2 diabetes. The investigators further hypothesize that injection of exenatide to children with septic shock will normalize blood glucose levels and decrease levels of inflammation proteins in the blood during the early course of sepsis.

Detailed Description

Pharmacology of Exenatide in Pediatric Sepsis, PEPS is a phase 1-2 investigation that will examine safety, pharmacokinetics, pharmacodynamics, and preliminary clinical efficacy of 4 subcutaneous doses of exenatide administered every 12 hours to children with newly diagnosed septic shock. The investigators' long term goal is to explore the potential benefit of exenatide on: early immunomodulation and glucose homeostasis, organ dysfunction, and clinically meaningful outcomes associated with pediatric sepsis. The current study objectives are to conduct a "3+3" dose escalation study, and then examine a "best exenatide allometric dose" to generate safety, pharmacokinetic, pharmacodynamic, and initial efficacy data in a larger cohort. In Phase 1 (three allometric doses; three age strata)the investigators will identify an exenatide dosing regimen that mimics area under the exenatide concentration curve for exenatide dosing among adolescents with type 2 diabetes with minimal or no adverse events. A total of 18 subjects are expected to be enrolled in Phase 1. In Phase 2 the investigators will utilize this "best exenatide allometric dose" to further clarify exenatide safety (adverse event occurence: e.g. nausea, abdominal pain, delayed gastric emptying, hypoglycemia, pancreatitis, renal dysfunction), pharmacokinetics, pharmacodynamics (glucose homeostasis; inflammatory cytokine serum concentrations), and effect on clinical outcomes (AUC of Saturation Index, AUC Vasoactive-Inotropic Score, AUC RIFLE Criteria, Pediatric Logistic Organ Dysfunction Score; changes in health-related quality of life and functional status). In Phase 2, 30 subjects in each age strata in the ratio of 4:1, exenatide: vehicle, are expected to be enrolled.

Study Timeline

• Study First Submitted: 2012-03-28
• Study First Submitted QC: 2012-04-05
• Study First Posted: 2012-04-10
• Study Start: 2012-10
• Primary Completion: 2014-10
• Study Completion: 2014-10
• Status Verified: 2017-10
• Last Update Submitted: 2017-10-03
• Last Update Posted: 2017-10-05

Recruitment & Eligibility

• Status: WITHDRAWN
• Sex: All
• Target Recruitment: Not specified

Inclusion Criteria

• Age 44 weeks estimated gestational age to 18 years AND
• Admitted to the PICU for the sepsis event AND
• Vascular catheter capable of providing serial blood samples in place AND
• Diagnosis of septic shock = sepsis with cardiovascular organ dysfunction AND
• Parents speak English or Spanish

Exclusion Criteria

• Greater than 12 hours from admission to PICU to enrollment OR
• Chronic or acute dialytic therapy, history of renal impairment or renal transplantation OR
• History of pancreatitis OR
• History of hypersensitivity to Byetta OR
• History of severe gastrointestinal disease or gastroparesis OR
• History of diabetes mellitus, type I or type II OR
• History of insulin, sulfonyl urea drugs, or coumarin use OR
• History of hypoglycemia OR
• History of active pregnancy (effect of exenatide on the fetus is unknown) OR
• Inability to collect serial blood samples OR
• Previously enrolled in the PEPS study OR
• Lack of commitment to aggressive sepsis therapy OR
• Expectation to succumb from the sepsis event OR
• Patient is a foster child and/or ward of the state OR
• Sepsis event associated with a PICU-acquired nosocomial infection OR
• Patient is enrolled in another interventional investigation that might obscure the potential effects of exenatide dosing.

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Exenatide	Exenatide	Subjects dosed with exenatide in Phase 2
Exenatide vehicle	Exenatide vehicle	Subjects dosed with exenatide vehicle in Phase 2

Primary Outcome Measures

Name	Time	Method
Exenatide associated adverse event occurence	From PICU admission to PICU discharge, an average interval of 7.5 days	Potential adverse events associated with exenatide: nausea, abdominal pain, hypoglycemia, delayed gastric emptying, pancreatitis, renal dysfunction, reactions at injection site. Adverse event occurence will be tabulated while the subject remains in the PICU.
Exenatide pharmacokinetics: Area under the exenatide concentration curve for 4 subcutaneous exenatide injections administered every 12 hours.	48 hours following the first exenatide dose	Delineation of the pharmacokinetics of subcutaneously dosed exenatide among children with de novo septic shock.

Secondary Outcome Measures

Name	Time	Method
Exenatide clinical efficacy: Effect of exenatide on intensity and duration of pulmonary failure.	From onset to discontinuation of mechanical ventilator support, an average interval of 4.5 days	AUC of daily Saturation Indices (\[FiO2\*MAP\]/SpO2)
Exenatide pharmacodynamics: Effect of exenatide on glucose homeostasis	60 hours following first exenatide dose	Delineation of exenatide pharmacodynamics among children with de novo septic shock: AUC of all serum glucose values or results of continuous glucose monitoring obtained during the 60 hours following the first dose of exenatide (or drug vehicle).
Exenatide pharmacodynamics: Effect of exenatide on serum inflammatory cytokine concentrations.	60 hours following first exenatide dose	Delineation of exenatide pharmacodynamics among children with de novo septic shock: AUC of serial serum inflammatory cytokine concentrations.
Exenatide clinical efficacy: Effect of exenatide on intensity and duration of organ dysfunctions.	From PICU admission to PICU discharge, an average interval of 7.5 days	AUC of daily Pediatric Logistic Organ Dysfunction (PELOD) scores while the subject remains in the PICU
Exenatide clinical efficacy: Effect of exenatide on intensity and duration of renal failure	From PICU admission to PICU discharge, an average interval of 7.5 days	AUC of daily RIFLE criteria
Exenatide clinical efficacy: Effect of exenatide on intensity and duration of hemodynamic instability.	From onset to discontinuation of vasoactive-inotropic support, an average interval of 4 days	AUC of daily Vasoactive-Inotropic Scores while the subject remains on vasoactive-inotropic support.
Exenatide clinical efficacy: Effect of exenatide on magnitude of sepsis-associated change in functional status.	2 measurements: baseline and PICU discharge, the latter occuring on average at 7.5 days	Determination per parent report of declination from baseline to PICU discharge of, Pediatric Overall Performance Category Score and Functional Status Score
Exenatide clinical efficacy: Effect of exenatide on magnitude of sepsis-associated change in health-related quality of life	2 measurements: baseline and PICU discharge, the latter occuring on average at 7.5 days	Determination per parent report of declination from baseline to PICU discharge of, Pediatric Quality of Life Inventory, Generic Core Scales, 4.0 (PedsQL)

Trial Locations

Locations (1)

Seattle Children's Hospital; 🇺🇸 Seattle, Washington, United States