Fcγ-Receptor-Independent Controlled Activation of CD40 Canonical Signaling by Novel Therapeutic Antibodies for Cancer Therapy

Overview

Journal Antibodies (Basel)

Date 2024 Apr 23

PMID 38651411

Authors

Karsten Beckmann

Carmen Reitinger

Xianglei Yan

Anna Carle

Eva Blumle

Nicole Jurkschat

Claudia Paulmann

Sandra Prassl

Linda V Kazandjian

Karin Lore

Falk Nimmerjahn

Stephan Fischer

Affiliations

Soon will be listed here.

Abstract

The activation of CD40-mediated signaling in antigen-presenting cells is a promising therapeutic strategy to promote immune responses against tumors. Most agonistic anti-CD40 antibodies currently in development require the Fcγ-receptor (FcγR)-mediated crosslinking of CD40 molecules for a meaningful activation of CD40 signaling but have limitations due to dose-limiting toxicities. Here we describe the identification of CD40 antibodies which strongly stimulate antigen-presenting cells in an entirely FcγR-independent manner. These Fc-silenced anti-CD40 antibodies induce an efficient upregulation of costimulatory receptors and cytokine release by dendritic cells. Finally, the most active identified anti-CD40 antibody shows activity in humanized mice. More importantly, there are no signs of obvious toxicities. These studies thus demonstrate the potent activation of antigen-presenting cells with anti-CD40 antibodies lacking FcγR-binding activity and open the possibility for an efficacious and safe combination therapy for cancer patients.

Citing Articles

Cell targeting and immunostimulatory properties of a novel Fcγ-receptor-independent agonistic anti-CD40 antibody in rhesus macaques.

Yan X, Ols S, Cerveira R, Lenart K, Hellgren F, Ye K Cell Mol Life Sci. 2023; 80(7):189.

PMID: 37353664 PMC: 10289945. DOI: 10.1007/s00018-023-04828-2.

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