Issue 53, 2021, Issue in Progress
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RSC Advances

Selective targeting of CD38 hydrolase and cyclase activity as an approach to immunostimulation

Thomas Z. Benton,a   Catherine M. Mills,a   Jonathan M. Turner,a   Megan J. Francis,a   Dalan J. Solomon,a   Pieter B. Burger,a   Yuri K. Peterson,a   Nathan G. Dolloff,b   André S. Bachmannc  and  Patrick M. Woster ORCID logo *a  

* Corresponding authors

a Dept. of Drug Discovery and Biomedical Sciences, Medical University of South Carolina, 70 President St, Charleston, SC 29425, USA
E-mail: woster@musc.edu

b Dept of Cell and Molecular Pharmacology and Experimental Therapeutics, Medical University of South Carolina, 173 Ashley Ave., Charleston, SC 29425, USA

c Dept of Pediatrics and Human Development, College of Human Medicine, Michigan State University, 400 Monroe Ave. NW, Grand Rapids, MI 49503, USA

Abstract

The ectoenzyme CD38 is highly expressed on the surface of mature immune cells, where they are a marker for cell activation, and also on the surface of multiple tumor cells such as multiple myeloma (MM). CD38-targeted monoclonal antibodies (MABs) such as daratumumab and isatuximab bind to CD38 and promote cancer cell death by stimulating the antitumor immune response. Although MABs are achieving unprecedented success in a percentage of cases, high rates of resistance limit their efficacy. Formation of the immunosuppressive intermediate adenosine is a major route by which this resistance is mediated. Thus there is an urgent need for small molecule agents that boost the immune response in T-cells. Importantly, CD38 is a dual-function enzyme, serving as a hydrolase and a nicotinamide adenine dinucleotide (NAD+) cyclase, and both of these activities promote immunosuppression. We have employed virtual and physical screening to identify novel compounds that are selective for either the hydrolase or the cyclase activity of CD38, and have demonstrated that these compounds activate T cells in vitro. We are currently optimizing these inhibitors for use in immunotherapy. These small molecule inhibitors of the CD38-hydrolase or cyclase activity can serve as chemical probes to determine the mechanism by which CD38 promotes resistance to MAB therapy, and could become novel and effective therapeutic agents that produce immunostimulatory effects. Our studies have identified the first small molecule inhibitors of CD38 specifically for use as immunostimulants.

Graphical abstract: Selective targeting of CD38 hydrolase and cyclase activity as an approach to immunostimulation

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Article information

DOI
https://doi.org/10.1039/D1RA06266B
Article type
Paper
Submitted
18 Aug 2021
Accepted
03 Oct 2021
First published
11 Oct 2021
This article is Open Access
Creative Commons BY-NC license

RSC Adv., 2021,11, 33260-33270

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Selective targeting of CD38 hydrolase and cyclase activity as an approach to immunostimulation

T. Z. Benton, C. M. Mills, J. M. Turner, M. J. Francis, D. J. Solomon, P. B. Burger, Y. K. Peterson, N. G. Dolloff, A. S. Bachmann and P. M. Woster, RSC Adv., 2021, 11, 33260 DOI: 10.1039/D1RA06266B

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