The Influence of Indisulam on Human Immune Effector Cells: Is a Combination with Immunotherapy Feasible?
Lisa Arnet, Lisabeth Emilius, Annett Hamann, Maria Carmo-Fonseca, Carola Berking, Jan Dörrie, Niels Schaft

TL;DR
This study examines how the drug indisulam affects human immune cells and whether combining it with immunotherapy is feasible.
Contribution
The study reveals how different immune cell functions respond to varying concentrations of indisulam, informing potential combination therapies.
Findings
Indisulam inhibits T cell activation in a dose-dependent manner.
T cell cytotoxicity is impaired at higher concentrations of indisulam.
T cell priming by dendritic cells is significantly reduced at 10 µM indisulam.
Abstract
Background: As a modulator of pre-mRNA splicing, the anti-cancer agent indisulam can induce aberrantly spliced neoantigens, enabling immunologic anti-tumor activity. Consequently, combining indisulam with immunotherapy is expected to be a promising novel approach in cancer therapy. However, a prerequisite for such a combination is that immune effector cells remain functional and unharmed by the chemical. Methods: To ensure the immunocompetence of human immune effector cells is maintained, we investigated the influence of indisulam on ex vivo-isolated T cells and monocyte-derived dendritic cells (moDCs) from healthy donors. We used indisulam concentrations from 0.625 µM to 160 µM and examined the impact on the following: (i) the activation of CD4+ and CD8+ T cells by CD3-crosslinking and via a high-affinity TCR, (ii) the cytotoxicity of CD8+ T cells, (iii) the maturation process of…
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Taxonomy
TopicsCAR-T cell therapy research · Immune Cell Function and Interaction · Immunotherapy and Immune Responses
