Myeloid and dendritic cells enhance therapeutics-induced cytokine release syndrome features in humanized BRGSF-HIS preclinical model

Gaëlle H. Martin; Alexis Gonon; Perrine Martin-Jeantet; Florence Renart-Depontieu; Zuzana Biesova; Anokhi Cifuentes; Arnab Mukherjee; Thomas Thisted; Astrid Doerner; Dean O. Campbell; Ludovic Bourré; Edward H. van der Horst; Amélie Rezza; Kader Thiam

doi:10.3389/fimmu.2024.1357716

Myeloid and dendritic cells enhance therapeutics-induced cytokine release syndrome features in humanized BRGSF-HIS preclinical model

Gaëlle H. Martin
, Alexis Gonon
, Perrine Martin-Jeantet
, Florence Renart-Depontieu
, Zuzana Biesova
, Anokhi Cifuentes
, Arnab Mukherjee
, Thomas Thisted
, Astrid Doerner
, Dean O. Campbell
, Ludovic Bourré
, Edward H. van der Horst
, Amélie Rezza
, Kader Thiam

Research output: Contribution to journal › Article › peer-review

5 Scopus citations

Abstract

Objectives: Despite their efficacy, some immunotherapies have been shown to induce immune-related adverse events, including the potentially life-threatening cytokine release syndrome (CRS), calling for reliable and translational preclinical models to predict potential safety issues and investigate their rescue. Here, we tested the reliability of humanized BRGSF mice for the assessment of therapeutics-induced CRS features in preclinical settings. Methods: BRGSF mice reconstituted with human umbilical cord blood CD34⁺ cells (BRGSF-CBC) were injected with anti-CD3 antibody (OKT3), anti-CD3/CD19 bispecific T-cell engager Blinatumomab, or VISTA-targeting antibody. Human myeloid and dendritic cells’ contribution was investigated in hFlt3L-boosted BRGSF-CBC mice. OKT3 treatment was also tested in human PBMC-reconstituted BRGSF mice (BRGSF-PBMC). Cytokine release, immune cell distribution, and clinical signs were followed. Results: OKT3 injection in BRGSF-CBC mice induced hallmark features of CRS, specifically inflammatory cytokines release, modifications of immune cell distribution and activation, body weight loss, and temperature drop. hFlt3L-boosted BRGSF-CBC mice displayed enhanced CRS features, revealing a significant role of myeloid and dendritic cells in this process. Clinical CRS-managing treatment Infliximab efficiently attenuated OKT3-induced toxicity. Comparison of OKT3 treatment’s effect on BRGSF-CBC and BRGSF-PBMC mice showed broadened CRS features in BRGSF-CBC mice. CRS-associated features were also observed in hFlt3L-boosted BRGSF-CBC mice upon treatment with other T-cell or myeloid-targeting compounds. Conclusions: These data show that BRGSF-CBC mice represent a relevant model for the preclinical assessment of CRS and CRS-managing therapies. They also confirm a significant role of myeloid and dendritic cells in CRS development and exhibit the versatility of this model for therapeutics-induced safety assessment.

Original language	English
Article number	1357716
Journal	Frontiers in Immunology
Volume	15
DOIs	https://doi.org/10.3389/fimmu.2024.1357716
State	Published - 2024
Externally published	Yes

Keywords

BRGSF mice
cytokine release syndrome
humanized preclinical models
immunotherapy
myeloid cells
safety assessment

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10.3389/fimmu.2024.1357716

Cite this

Martin, G. H., Gonon, A., Martin-Jeantet, P., Renart-Depontieu, F., Biesova, Z., Cifuentes, A., Mukherjee, A., Thisted, T., Doerner, A., Campbell, D. O., Bourré, L., van der Horst, E. H., Rezza, A., & Thiam, K. (2024). Myeloid and dendritic cells enhance therapeutics-induced cytokine release syndrome features in humanized BRGSF-HIS preclinical model. Frontiers in Immunology, 15, Article 1357716. https://doi.org/10.3389/fimmu.2024.1357716

@article{e8f69e3621e04eefbab846d8a0081940,

title = "Myeloid and dendritic cells enhance therapeutics-induced cytokine release syndrome features in humanized BRGSF-HIS preclinical model",

abstract = "Objectives: Despite their efficacy, some immunotherapies have been shown to induce immune-related adverse events, including the potentially life-threatening cytokine release syndrome (CRS), calling for reliable and translational preclinical models to predict potential safety issues and investigate their rescue. Here, we tested the reliability of humanized BRGSF mice for the assessment of therapeutics-induced CRS features in preclinical settings. Methods: BRGSF mice reconstituted with human umbilical cord blood CD34+ cells (BRGSF-CBC) were injected with anti-CD3 antibody (OKT3), anti-CD3/CD19 bispecific T-cell engager Blinatumomab, or VISTA-targeting antibody. Human myeloid and dendritic cells{\textquoteright} contribution was investigated in hFlt3L-boosted BRGSF-CBC mice. OKT3 treatment was also tested in human PBMC-reconstituted BRGSF mice (BRGSF-PBMC). Cytokine release, immune cell distribution, and clinical signs were followed. Results: OKT3 injection in BRGSF-CBC mice induced hallmark features of CRS, specifically inflammatory cytokines release, modifications of immune cell distribution and activation, body weight loss, and temperature drop. hFlt3L-boosted BRGSF-CBC mice displayed enhanced CRS features, revealing a significant role of myeloid and dendritic cells in this process. Clinical CRS-managing treatment Infliximab efficiently attenuated OKT3-induced toxicity. Comparison of OKT3 treatment{\textquoteright}s effect on BRGSF-CBC and BRGSF-PBMC mice showed broadened CRS features in BRGSF-CBC mice. CRS-associated features were also observed in hFlt3L-boosted BRGSF-CBC mice upon treatment with other T-cell or myeloid-targeting compounds. Conclusions: These data show that BRGSF-CBC mice represent a relevant model for the preclinical assessment of CRS and CRS-managing therapies. They also confirm a significant role of myeloid and dendritic cells in CRS development and exhibit the versatility of this model for therapeutics-induced safety assessment.",

keywords = "BRGSF mice, cytokine release syndrome, humanized preclinical models, immunotherapy, myeloid cells, safety assessment",

author = "Martin, \{Ga{\"e}lle H.\} and Alexis Gonon and Perrine Martin-Jeantet and Florence Renart-Depontieu and Zuzana Biesova and Anokhi Cifuentes and Arnab Mukherjee and Thomas Thisted and Astrid Doerner and Campbell, \{Dean O.\} and Ludovic Bourr{\'e} and \{van der Horst\}, \{Edward H.\} and Am{\'e}lie Rezza and Kader Thiam",

note = "Publisher Copyright: Copyright {\textcopyright} 2024 Martin, Gonon, Martin-Jeantet, Renart-Depontieu, Biesova, Cifuentes, Mukherjee, Thisted, Doerner, Campbell, Bourr{\'e}, van der Horst, Rezza and Thiam.",

year = "2024",

doi = "10.3389/fimmu.2024.1357716",

language = "English",

volume = "15",

journal = "Frontiers in Immunology",

issn = "1664-3224",

publisher = "Frontiers Media SA",

}

Martin, GH, Gonon, A, Martin-Jeantet, P, Renart-Depontieu, F, Biesova, Z, Cifuentes, A, Mukherjee, A, Thisted, T, Doerner, A, Campbell, DO, Bourré, L, van der Horst, EH, Rezza, A & Thiam, K 2024, 'Myeloid and dendritic cells enhance therapeutics-induced cytokine release syndrome features in humanized BRGSF-HIS preclinical model', Frontiers in Immunology, vol. 15, 1357716. https://doi.org/10.3389/fimmu.2024.1357716

TY - JOUR

T1 - Myeloid and dendritic cells enhance therapeutics-induced cytokine release syndrome features in humanized BRGSF-HIS preclinical model

AU - Martin, Gaëlle H.

AU - Gonon, Alexis

AU - Martin-Jeantet, Perrine

AU - Renart-Depontieu, Florence

AU - Biesova, Zuzana

AU - Cifuentes, Anokhi

AU - Mukherjee, Arnab

AU - Thisted, Thomas

AU - Doerner, Astrid

AU - Campbell, Dean O.

AU - Bourré, Ludovic

AU - van der Horst, Edward H.

AU - Rezza, Amélie

AU - Thiam, Kader

PY - 2024

Y1 - 2024

N2 - Objectives: Despite their efficacy, some immunotherapies have been shown to induce immune-related adverse events, including the potentially life-threatening cytokine release syndrome (CRS), calling for reliable and translational preclinical models to predict potential safety issues and investigate their rescue. Here, we tested the reliability of humanized BRGSF mice for the assessment of therapeutics-induced CRS features in preclinical settings. Methods: BRGSF mice reconstituted with human umbilical cord blood CD34+ cells (BRGSF-CBC) were injected with anti-CD3 antibody (OKT3), anti-CD3/CD19 bispecific T-cell engager Blinatumomab, or VISTA-targeting antibody. Human myeloid and dendritic cells’ contribution was investigated in hFlt3L-boosted BRGSF-CBC mice. OKT3 treatment was also tested in human PBMC-reconstituted BRGSF mice (BRGSF-PBMC). Cytokine release, immune cell distribution, and clinical signs were followed. Results: OKT3 injection in BRGSF-CBC mice induced hallmark features of CRS, specifically inflammatory cytokines release, modifications of immune cell distribution and activation, body weight loss, and temperature drop. hFlt3L-boosted BRGSF-CBC mice displayed enhanced CRS features, revealing a significant role of myeloid and dendritic cells in this process. Clinical CRS-managing treatment Infliximab efficiently attenuated OKT3-induced toxicity. Comparison of OKT3 treatment’s effect on BRGSF-CBC and BRGSF-PBMC mice showed broadened CRS features in BRGSF-CBC mice. CRS-associated features were also observed in hFlt3L-boosted BRGSF-CBC mice upon treatment with other T-cell or myeloid-targeting compounds. Conclusions: These data show that BRGSF-CBC mice represent a relevant model for the preclinical assessment of CRS and CRS-managing therapies. They also confirm a significant role of myeloid and dendritic cells in CRS development and exhibit the versatility of this model for therapeutics-induced safety assessment.

AB - Objectives: Despite their efficacy, some immunotherapies have been shown to induce immune-related adverse events, including the potentially life-threatening cytokine release syndrome (CRS), calling for reliable and translational preclinical models to predict potential safety issues and investigate their rescue. Here, we tested the reliability of humanized BRGSF mice for the assessment of therapeutics-induced CRS features in preclinical settings. Methods: BRGSF mice reconstituted with human umbilical cord blood CD34+ cells (BRGSF-CBC) were injected with anti-CD3 antibody (OKT3), anti-CD3/CD19 bispecific T-cell engager Blinatumomab, or VISTA-targeting antibody. Human myeloid and dendritic cells’ contribution was investigated in hFlt3L-boosted BRGSF-CBC mice. OKT3 treatment was also tested in human PBMC-reconstituted BRGSF mice (BRGSF-PBMC). Cytokine release, immune cell distribution, and clinical signs were followed. Results: OKT3 injection in BRGSF-CBC mice induced hallmark features of CRS, specifically inflammatory cytokines release, modifications of immune cell distribution and activation, body weight loss, and temperature drop. hFlt3L-boosted BRGSF-CBC mice displayed enhanced CRS features, revealing a significant role of myeloid and dendritic cells in this process. Clinical CRS-managing treatment Infliximab efficiently attenuated OKT3-induced toxicity. Comparison of OKT3 treatment’s effect on BRGSF-CBC and BRGSF-PBMC mice showed broadened CRS features in BRGSF-CBC mice. CRS-associated features were also observed in hFlt3L-boosted BRGSF-CBC mice upon treatment with other T-cell or myeloid-targeting compounds. Conclusions: These data show that BRGSF-CBC mice represent a relevant model for the preclinical assessment of CRS and CRS-managing therapies. They also confirm a significant role of myeloid and dendritic cells in CRS development and exhibit the versatility of this model for therapeutics-induced safety assessment.

KW - BRGSF mice

KW - cytokine release syndrome

KW - humanized preclinical models

KW - immunotherapy

KW - myeloid cells

KW - safety assessment

UR - https://www.scopus.com/pages/publications/85185838561

U2 - 10.3389/fimmu.2024.1357716

DO - 10.3389/fimmu.2024.1357716

M3 - Article

C2 - 38384461

AN - SCOPUS:85185838561

SN - 1664-3224

VL - 15

JO - Frontiers in Immunology

JF - Frontiers in Immunology

M1 - 1357716

ER -

Myeloid and dendritic cells enhance therapeutics-induced cytokine release syndrome features in humanized BRGSF-HIS preclinical model

Abstract

Keywords

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