High potency STING agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilege

High potency STING agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilege

Background Intratumoral injection of cyclic dinucleotide (CDN) agonists of the stimulator of interferon genes (STING) pathway engages innate immune activation and priming of adaptive immune effectors to foster local and distal tumor clearance. Despite proven therapeutic efficacy in preclinical model...

Full description

Bibliographic Details
Main Authors: Michael A Curran, Casey R Ager, Philip Jones, Akash Boda, Kimal Rajapakshe, Spencer Thomas Lea, Maria Emilia Di Francesco, Priyamvada Jayaprakash, Ravaen B Slay, Brittany Morrow, Rishika Prasad, Meghan A Dean, Colm R Duffy, Cristian Coarfa
Format: Article
Language:English
Published: BMJ Publishing Group 2021-08-01
Series:Journal for ImmunoTherapy of Cancer
Online Access:https://jitc.bmj.com/content/9/8/e003246.full
id doaj-d0f57e0df0f34deebce56caf111fe5d1
record_format Article
spelling doaj-d0f57e0df0f34deebce56caf111fe5d12021-08-10T10:00:13ZengBMJ Publishing GroupJournal for ImmunoTherapy of Cancer2051-14262021-08-019810.1136/jitc-2021-003246High potency STING agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilegeMichael A Curran0Casey R Ager1Philip Jones2Akash Boda3Kimal Rajapakshe4Spencer Thomas Lea5Maria Emilia Di Francesco6Priyamvada Jayaprakash7Ravaen B Slay8Brittany Morrow9Rishika Prasad10Meghan A Dean11Colm R Duffy12Cristian Coarfa131 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA 1 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA 5 Institute for Applied Cancer Science, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA1 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA 4 Ahmed Center for Pancreatic Cancer Research, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA1 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA 5 Institute for Applied Cancer Science, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA1 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA1 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA1 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA 1 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA 1 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA1 Department of Immunology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA 6 Department of Molecular and Cellular Biology, Baylor College of Medicine, Houston, Texas, USABackground Intratumoral injection of cyclic dinucleotide (CDN) agonists of the stimulator of interferon genes (STING) pathway engages innate immune activation and priming of adaptive immune effectors to foster local and distal tumor clearance. Despite proven therapeutic efficacy in preclinical models, a thorough understanding of how CDNs reprogram suppressive myeloid stroma in mouse and man is lacking.Methods Here, we perform deep transcript-level and protein-level profiling of myeloid-derived suppressor cells and M2 macrophages following stimulation with CDNs of ascending potency. Additionally, we leverage orthotopic Kras+/G12DTP53+/R172HPdx1-Cre (KPC) derived models of pancreatic adenocarcinoma (PDAC) to determine the capacity for locally administered CDNs to sensitize PDAC to immune checkpoint blockade. We use bioluminescent in vivo imaging and 30-parameter flow cytometry to profile growth kinetics and remodeling of the tumor stroma post-therapy.Results Highly potent synthetic STING agonists repolarize suppressive myeloid populations of human and murine origin in part through inhibition of Myc signaling, metabolic modulation, and antagonism of cell cycle. Surprisingly, high-potency synthetic agonists engage qualitatively unique pathways as compared with natural CDNs. Consistent with our mechanistic observations, we find that intratumoral injection of the highest activity STING agonist, IACS-8803, into orthotopic pancreatic adenocarcinoma lesions unmasks sensitivity to checkpoint blockade immunotherapy. Dimensionality reduction analyses of high parameter flow cytometry data reveals substantial contributions of both myeloid repolarization and T cell activation underlying the in vivo therapeutic benefit of this approach.Conclusions This study defines the molecular basis of STING-mediated myeloid reprogramming, revealing previously unappreciated and qualitatively unique pathways engaged by CDNs of ascending potency during functional repolarization. Furthermore, we demonstrate the potential for high potency CDNs to overcome immunotherapy resistance in an orthotopic, multifocal model of PDAC.https://jitc.bmj.com/content/9/8/e003246.full
collection DOAJ
language English
format Article
sources DOAJ
author Michael A Curran
Casey R Ager
Philip Jones
Akash Boda
Kimal Rajapakshe
Spencer Thomas Lea
Maria Emilia Di Francesco
Priyamvada Jayaprakash
Ravaen B Slay
Brittany Morrow
Rishika Prasad
Meghan A Dean
Colm R Duffy
Cristian Coarfa
spellingShingle Michael A Curran
Casey R Ager
Philip Jones
Akash Boda
Kimal Rajapakshe
Spencer Thomas Lea
Maria Emilia Di Francesco
Priyamvada Jayaprakash
Ravaen B Slay
Brittany Morrow
Rishika Prasad
Meghan A Dean
Colm R Duffy
Cristian Coarfa
High potency STING agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilege
Journal for ImmunoTherapy of Cancer
author_facet Michael A Curran
Casey R Ager
Philip Jones
Akash Boda
Kimal Rajapakshe
Spencer Thomas Lea
Maria Emilia Di Francesco
Priyamvada Jayaprakash
Ravaen B Slay
Brittany Morrow
Rishika Prasad
Meghan A Dean
Colm R Duffy
Cristian Coarfa
author_sort Michael A Curran
title High potency STING agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilege
title_short High potency STING agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilege
title_full High potency STING agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilege
title_fullStr High potency STING agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilege
title_full_unstemmed High potency STING agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilege
title_sort high potency sting agonists engage unique myeloid pathways to reverse pancreatic cancer immune privilege
publisher BMJ Publishing Group
series Journal for ImmunoTherapy of Cancer
issn 2051-1426
publishDate 2021-08-01
description Background Intratumoral injection of cyclic dinucleotide (CDN) agonists of the stimulator of interferon genes (STING) pathway engages innate immune activation and priming of adaptive immune effectors to foster local and distal tumor clearance. Despite proven therapeutic efficacy in preclinical models, a thorough understanding of how CDNs reprogram suppressive myeloid stroma in mouse and man is lacking.Methods Here, we perform deep transcript-level and protein-level profiling of myeloid-derived suppressor cells and M2 macrophages following stimulation with CDNs of ascending potency. Additionally, we leverage orthotopic Kras+/G12DTP53+/R172HPdx1-Cre (KPC) derived models of pancreatic adenocarcinoma (PDAC) to determine the capacity for locally administered CDNs to sensitize PDAC to immune checkpoint blockade. We use bioluminescent in vivo imaging and 30-parameter flow cytometry to profile growth kinetics and remodeling of the tumor stroma post-therapy.Results Highly potent synthetic STING agonists repolarize suppressive myeloid populations of human and murine origin in part through inhibition of Myc signaling, metabolic modulation, and antagonism of cell cycle. Surprisingly, high-potency synthetic agonists engage qualitatively unique pathways as compared with natural CDNs. Consistent with our mechanistic observations, we find that intratumoral injection of the highest activity STING agonist, IACS-8803, into orthotopic pancreatic adenocarcinoma lesions unmasks sensitivity to checkpoint blockade immunotherapy. Dimensionality reduction analyses of high parameter flow cytometry data reveals substantial contributions of both myeloid repolarization and T cell activation underlying the in vivo therapeutic benefit of this approach.Conclusions This study defines the molecular basis of STING-mediated myeloid reprogramming, revealing previously unappreciated and qualitatively unique pathways engaged by CDNs of ascending potency during functional repolarization. Furthermore, we demonstrate the potential for high potency CDNs to overcome immunotherapy resistance in an orthotopic, multifocal model of PDAC.
url https://jitc.bmj.com/content/9/8/e003246.full
work_keys_str_mv AT michaelacurran highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT caseyrager highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT philipjones highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT akashboda highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT kimalrajapakshe highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT spencerthomaslea highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT mariaemiliadifrancesco highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT priyamvadajayaprakash highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT ravaenbslay highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT brittanymorrow highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT rishikaprasad highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT meghanadean highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT colmrduffy highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
AT cristiancoarfa highpotencystingagonistsengageuniquemyeloidpathwaystoreversepancreaticcancerimmuneprivilege
_version_ 1721212389776424960

Similar Items