Tumor Regression upon Intratumoral and Subcutaneous Dosing of the STING Agonist ALG-031048 in Mouse Efficacy Models

Stimulator of interferon genes (STING) agonists have shown potent anti-tumor efficacy in various mouse tumor models and have the potential to overcome resistance to immune checkpoint inhibitors (ICI) by linking the innate and acquired immune systems. First-generation STING agonists are administered...

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Autores principales: Jekle, Andreas, Thatikonda, Santosh Kumar, Jaisinghani, Ruchika, Ren, Suping, Kinkade, April, Stevens, Sarah K., Stoycheva, Antitsa, Rajwanshi, Vivek K., Williams, Caroline, Deval, Jerome, Mukherjee, Sucheta, Zhang, Qingling, Chanda, Sushmita, Smith, David B., Blatt, Lawrence M., Symons, Julian A., Gonzalvez, Francois, Beigelman, Leonid
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10671074/
https://www.ncbi.nlm.nih.gov/pubmed/38003463
http://dx.doi.org/10.3390/ijms242216274
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author Jekle, Andreas
Thatikonda, Santosh Kumar
Jaisinghani, Ruchika
Ren, Suping
Kinkade, April
Stevens, Sarah K.
Stoycheva, Antitsa
Rajwanshi, Vivek K.
Williams, Caroline
Deval, Jerome
Mukherjee, Sucheta
Zhang, Qingling
Chanda, Sushmita
Smith, David B.
Blatt, Lawrence M.
Symons, Julian A.
Gonzalvez, Francois
Beigelman, Leonid
author_facet Jekle, Andreas
Thatikonda, Santosh Kumar
Jaisinghani, Ruchika
Ren, Suping
Kinkade, April
Stevens, Sarah K.
Stoycheva, Antitsa
Rajwanshi, Vivek K.
Williams, Caroline
Deval, Jerome
Mukherjee, Sucheta
Zhang, Qingling
Chanda, Sushmita
Smith, David B.
Blatt, Lawrence M.
Symons, Julian A.
Gonzalvez, Francois
Beigelman, Leonid
author_sort Jekle, Andreas
collection PubMed
description Stimulator of interferon genes (STING) agonists have shown potent anti-tumor efficacy in various mouse tumor models and have the potential to overcome resistance to immune checkpoint inhibitors (ICI) by linking the innate and acquired immune systems. First-generation STING agonists are administered intratumorally; however, a systemic delivery route would greatly expand the clinical use of STING agonists. Biochemical and cell-based experiments, as well as syngeneic mouse efficacy models, were used to demonstrate the anti-tumoral activity of ALG-031048, a novel STING agonist. In vitro, ALG-031048 is highly stable in plasma and liver microsomes and is resistant to degradation via phosphodiesterases. The high stability in biological matrices translated to good cellular potency in a HEK 293 STING R232 reporter assay, efficient activation and maturation of primary human dendritic cells and monocytes, as well as long-lasting, antigen-specific anti-tumor activity in up to 90% of animals in the CT26 mouse colon carcinoma model. Significant reductions in tumor growth were observed in two syngeneic mouse tumor models following subcutaneous administration. Combinations of ALG-031048 and ICIs further enhanced the in vivo anti-tumor activity. This initial demonstration of anti-tumor activity after systemic administration of ALG-031048 warrants further investigation, while the combination of systemically administered ALG-031048 with ICIs offers an attractive approach to overcome key limitations of ICIs in the clinic.
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spelling pubmed-106710742023-11-13 Tumor Regression upon Intratumoral and Subcutaneous Dosing of the STING Agonist ALG-031048 in Mouse Efficacy Models Jekle, Andreas Thatikonda, Santosh Kumar Jaisinghani, Ruchika Ren, Suping Kinkade, April Stevens, Sarah K. Stoycheva, Antitsa Rajwanshi, Vivek K. Williams, Caroline Deval, Jerome Mukherjee, Sucheta Zhang, Qingling Chanda, Sushmita Smith, David B. Blatt, Lawrence M. Symons, Julian A. Gonzalvez, Francois Beigelman, Leonid Int J Mol Sci Article Stimulator of interferon genes (STING) agonists have shown potent anti-tumor efficacy in various mouse tumor models and have the potential to overcome resistance to immune checkpoint inhibitors (ICI) by linking the innate and acquired immune systems. First-generation STING agonists are administered intratumorally; however, a systemic delivery route would greatly expand the clinical use of STING agonists. Biochemical and cell-based experiments, as well as syngeneic mouse efficacy models, were used to demonstrate the anti-tumoral activity of ALG-031048, a novel STING agonist. In vitro, ALG-031048 is highly stable in plasma and liver microsomes and is resistant to degradation via phosphodiesterases. The high stability in biological matrices translated to good cellular potency in a HEK 293 STING R232 reporter assay, efficient activation and maturation of primary human dendritic cells and monocytes, as well as long-lasting, antigen-specific anti-tumor activity in up to 90% of animals in the CT26 mouse colon carcinoma model. Significant reductions in tumor growth were observed in two syngeneic mouse tumor models following subcutaneous administration. Combinations of ALG-031048 and ICIs further enhanced the in vivo anti-tumor activity. This initial demonstration of anti-tumor activity after systemic administration of ALG-031048 warrants further investigation, while the combination of systemically administered ALG-031048 with ICIs offers an attractive approach to overcome key limitations of ICIs in the clinic. MDPI 2023-11-13 /pmc/articles/PMC10671074/ /pubmed/38003463 http://dx.doi.org/10.3390/ijms242216274 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Jekle, Andreas
Thatikonda, Santosh Kumar
Jaisinghani, Ruchika
Ren, Suping
Kinkade, April
Stevens, Sarah K.
Stoycheva, Antitsa
Rajwanshi, Vivek K.
Williams, Caroline
Deval, Jerome
Mukherjee, Sucheta
Zhang, Qingling
Chanda, Sushmita
Smith, David B.
Blatt, Lawrence M.
Symons, Julian A.
Gonzalvez, Francois
Beigelman, Leonid
Tumor Regression upon Intratumoral and Subcutaneous Dosing of the STING Agonist ALG-031048 in Mouse Efficacy Models
title Tumor Regression upon Intratumoral and Subcutaneous Dosing of the STING Agonist ALG-031048 in Mouse Efficacy Models
title_full Tumor Regression upon Intratumoral and Subcutaneous Dosing of the STING Agonist ALG-031048 in Mouse Efficacy Models
title_fullStr Tumor Regression upon Intratumoral and Subcutaneous Dosing of the STING Agonist ALG-031048 in Mouse Efficacy Models
title_full_unstemmed Tumor Regression upon Intratumoral and Subcutaneous Dosing of the STING Agonist ALG-031048 in Mouse Efficacy Models
title_short Tumor Regression upon Intratumoral and Subcutaneous Dosing of the STING Agonist ALG-031048 in Mouse Efficacy Models
title_sort tumor regression upon intratumoral and subcutaneous dosing of the sting agonist alg-031048 in mouse efficacy models
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10671074/
https://www.ncbi.nlm.nih.gov/pubmed/38003463
http://dx.doi.org/10.3390/ijms242216274
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