November 21, 2024
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Authors: Gaëlle H. Martin1, Alexis Gonon1, Perrine Martin-Jeantet1, Florence Renart-Depontieu1, Zuzana Biesova2, Anokhi Cifuentes2, Arnab Mukherjee2, Thomas Thisted2, Astrid Doerner3, Dean O. Campbell3, Ludovic Bourre´3, Edward H. van der Horst2, Ame´ lie Rezza1 and Kader Thiam1
1genOway, Lyon, France, 2Sensei Biotherapeutics Inc., Boston, MA, United States, 3Crown Bioscience Inc., San Diego, CA, United States
Some immunotherapies have been shown to induce immune-related adverse events, including the potentially life-threatening cytokine release syndrome (CRS).
As a result, there is a need for reliable and translational preclinical models to predict potential safety issues and investigate their rescue.
The study presented in this article tested the reliability of humanized BRGSF mice for the assessment of therapeutics-induced CRS features in preclinical settings. The study included the investigation of human myeloid and dendritic cells’ contribution in hFlt3L-boosted BRGSF-CBC mice.
Read the full article, published in Frontiers in Immunology, for an in-depth review of the study aim, methods, and results.
