“Cytokine storm” in the phase I trial of monoclonal antibody TGN1412: better understanding the causes to improve preclinical testing of immunotherapeutics

R Stebbings, L Findlay, C Edwards… - The Journal of …, 2007 - journals.aai.org
R Stebbings, L Findlay, C Edwards, D Eastwood, C Bird, D North, Y Mistry, P Dilger…
The Journal of Immunology, 2007journals.aai.org
Abstract The CD28-specific mAb TGN1412 rapidly caused a life-threatening “cytokine storm”
in all six healthy volunteers in the Phase I clinical trial of this superagonist, signaling a failure
of preclinical safety testing. We report novel in vitro procedures in which TGN1412,
immobilized in various ways, is presented to human white blood cells in a manner that
stimulates the striking release of cytokines and profound lymphocyte proliferation that
occurred in vivo in humans. The novel procedures would have predicted the toxicity of this …
Abstract
The CD28-specific mAb TGN1412 rapidly caused a life-threatening “cytokine storm” in all six healthy volunteers in the Phase I clinical trial of this superagonist, signaling a failure of preclinical safety testing. We report novel in vitro procedures in which TGN1412, immobilized in various ways, is presented to human white blood cells in a manner that stimulates the striking release of cytokines and profound lymphocyte proliferation that occurred in vivo in humans. The novel procedures would have predicted the toxicity of this superagonist and are now being applied to emerging immunotherapeutics and to other therapeutics that have the potential to act upon the immune system. Data from these novel procedures, along with data from in vitro and in vivo studies in nonhuman primates, suggest that the dose of TGN1412 given to human volunteers was close to the maximum immunostimulatory dose and that TGN1412 is not a superagonist in nonhuman primates.
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