Altered interactions between circulating and tissue-resident CD8 T cells with the colonic mucosa define colitis associated with immune checkpoint inhibitors

Thomas, Molly; Slowikowski, Kamil; Manakongtreecheep, Kasidet; Sen, Pritha; Tantivit, Jessica; Nasrallah, Mazen; Smith, Neal; Ramesh, Swetha; Zubiri, Leyre; Tirard, Alice; Arnold, Benjamin Y.; Nieman, Linda T.; Chen, Jonathan; Eisenhaure, Thomas; Pelka, Karin; Xu, Katherine; Jorgji, Vjola; Pinto, Christopher J.; Sharova, Tatyana; Glasser, Rachel; Chan, Elaina PuiYee; Sullivan, Ryan J.; Khalili, Hamed; Juric, Dejan; Boland, Genevieve M.; Dougan, Michael; Hacohen, Nir; Reynolds, Kerry L.; Li, Bo; Villani, Alexandra‐Chloé

doi:10.1101/2021.09.17.460868

Cited by 12 publications

(22 citation statements)

References 118 publications

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“…In melanoma patients, it has been shown that untreated patients with untreated metastatic disease have decreased CD14 + monocytes in the peripheral blood compared to healthy controls, a finding recapitulated in our analysis, and that the phenotypes of these monocytes may be a predictor of disease response to CBI [ 22 ]. Although limited data exists thus far on monocyte dynamics in tissue during irAEs, early analyses of colitis patients point to an influx of monocytes with a phenotype resembling that of the CD14 + population reported here [ 23 ]. While additional studies are needed, the existing data clearly suggests an important role for these monocyte populations in irAE development.…”

Section: Discussionmentioning

confidence: 99%

A Novel Potential Role for Monocytes Revealed by Single Cell Analysis of Immunotherapy Induced Immune Related Adverse Events

Garrison

Chang

Hornick

et al. 2022

Cancers

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Immune related adverse events (irAEs) are one of the leading causes of discontinuation of cancer immunotherapy treatment. Despite extensive research into the frequency and types of irAEs, little is known about the cell types and pathways through which these drugs cause the observed side effects. To identify cell types and pathways of interest, we have analyzed single cell sequencing data of PBMCs from patients who developed skin irAEs as a result of their immunotherapy treatment. Using Azimuth’s cell type identification software for PBMCs and GSEA pathway analysis, we found macrophage cell populations and reactive oxygen species related pathways to be upregulated. These results provide important groundwork to build a complete picture of the mechanisms which cause irAEs and finding ways to more effectively treat them.

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Section: Discussionmentioning

confidence: 99%

A Novel Potential Role for Monocytes Revealed by Single Cell Analysis of Immunotherapy Induced Immune Related Adverse Events

Garrison

Chang

Hornick

et al. 2022

Cancers

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“…As our understanding of irAE mechanisms in patients evolve, it will help to identify which, if any, animal models most accurately recapitulate organ-specific irAEs in patients and inform the next generation of irAE models that can be used to test the relationship between irAE therapeutics and antitumor efficacy. 53 As T cells are thought to be central to the antitumor responses driven by ICIs 4,9 and are found to predominate the immune cell infiltrate in irAE tissue biopsies across organ systems, 8,10,11,13,16,23,38,[54][55][56][57] many studies have looked at the relationship of T cells in irAEs and paired tumors. While central and peripheral tolerance mechanisms cause many autoreactive T cells to become anergic or die during Tcell development, autoreactive T cells are still commonly found in humans 14,44 and are anticipated to play a role in the development of irAEs.…”

Section: The Molecul Ar Rel Ati On S Hip B E T Ween Irae S and Antitu...mentioning

confidence: 99%

“…Depending on the drugs and doses used, 66%–96% of patients will have side effects from ICIs, and 7%–59% of patients will experience severe irAEs, which are also commonly referred to as “high‐grade” irAEs 6,7 . While the prevailing hypothesis in the field suggests that irAEs are due to a loss of self‐tolerance, 8,9 the mechanistic drivers of irAEs are only beginning to emerge 10–16 . As murine tumor models typically utilized to study ICI efficacy do not develop severe irAEs, 17 insights into the relationship between irAEs and antitumor immunity have been guided by clinical observations and translational research.…”

Section: Introductionmentioning

confidence: 99%

“…6,7 While the prevailing hypothesis in the field suggests that irAEs are due to a loss of self-tolerance, 8,9 the mechanistic drivers of irAEs are only beginning to emerge. [10][11][12][13][14][15][16] As murine tumor models typically utilized to study ICI efficacy do not develop severe irAEs, 17 insights into the relationship between irAEs and antitumor immunity have been guided by clinical observations and translational research. Currently, the management of severe irAEs involves discontinuing ICI therapy and administering glucocorticoids and other immunosuppressive medications, [18][19][20][21] which may adversely impact antitumor immunity.…”

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confidence: 99%

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Effects of immune‐related adverse events (irAEs) and their treatment on antitumor immune responses

Blum

Rouhani

Sullivan

2023

Immunological Reviews

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SummaryImmune checkpoint inhibitors (ICIs) are potentially life‐saving cancer therapies that can trigger immune‐related adverse events (irAEs). irAEs can impact any organ and range in their presentation from mild side effects to life‐threatening complications. The relationship between irAEs and antitumor immune responses is nuanced and may depend on the irAE organ, the tumor histology, and the patient. While some irAEs likely represent an immune response against antigens shared between tumor cells and healthy tissues, other irAEs may be entirely unrelated to antitumor immune responses. Clinical observations suggest that low‐grade irAEs have a positive association with responses to ICIs, but the correlation between severe irAEs and clinical benefit is less clear. Currently, severe irAEs are typically treated by interrupting or permanently discontinuing ICI treatment and administering empirically selected systemic immunosuppressive agents. However, these interventions could potentially diminish the antitumor effects of ICIs. Efforts to understand the mechanistic relationship between irAEs and the tumor microenvironment have yielded meaningful insights and nominated therapeutic targets for irAE management that may preserve or even boost ICI efficacy. We explore the clinical and molecular relationship between irAEs and antitumor immunity as well as the role that irAE treatments may play in shaping antitumor immune responses.

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“…These T cells are activated (expressing IFNG and HAVCR2 ), proliferative, and are more clonal 38,39 . Phenotypically similar activated PDCD1 hi CXCL13 + CD8A + T cells have been found to be enriched in irAE‐colitis, 40 again expressing high IFNG and HAVCR2 but, in contrast to those in irArthritis, also coexpressing Th17 cytokines IL17A and IL26 . The same population is enriched in checkpoint inhibitor pneumonitis, again overexpressing IL17A and IFNG but also here expressing CSF2 41 .…”

Section: Immune Phenotyping Of Rheumatic Iraesmentioning

confidence: 99%

Rheumatic complications of checkpoint inhibitors: Lessons from autoimmunity

Reynolds

2023

Immunological Reviews

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SummaryImmune checkpoint inhibitors are now an established treatment in the management of a range of cancers. Their success means that their use is likely to increase in future in terms of the numbers of patients treated, the indications and the range of immune checkpoints targeted. They function by counteracting immune evasion by the tumor but, as a consequence, can breach self‐tolerance at other sites leading to a range of immune‐related adverse events. Included among these complications are a range of rheumatologic complications, including inflammatory arthritis and keratoconjunctivitis sicca. These superficially resemble immune‐mediated rheumatic diseases (IMRDs) such as rheumatoid arthritis and Sjogren's disease but preliminary studies suggest they are clinically and immunologically distinct entities. However, there appear to be common processes that predispose to the development of both that may inform preventative interventions and predictive tools. Both groups of conditions highlight the centrality of immune checkpoints in controlling tolerance and how it can be restored. Here we will discuss some of these commonalities and differences between rheumatic irAEs and IMRDs.

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Altered interactions between circulating and tissue-resident CD8 T cells with the colonic mucosa define colitis associated with immune checkpoint inhibitors

Cited by 12 publications

References 118 publications

A Novel Potential Role for Monocytes Revealed by Single Cell Analysis of Immunotherapy Induced Immune Related Adverse Events

A Novel Potential Role for Monocytes Revealed by Single Cell Analysis of Immunotherapy Induced Immune Related Adverse Events

Effects of immune‐related adverse events (irAEs) and their treatment on antitumor immune responses

Rheumatic complications of checkpoint inhibitors: Lessons from autoimmunity

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