A functional subset of CD8+ T cells during chronic exhaustion is defined by SIRPα expression

Myers, Lara; Tal, Michal Caspi; Dulgeroff, Laughing Bear Torrez; Carmody, Aaron B.; Messer, Ronald J.; Gulati, Gunsagar S.; Yiu, Ying Ying; Staron, Matthew; Angel, Cesar J. Lopez; Sinha, Rahul; Markovic, Maxim; Pham, Edward A.; Fram, Benjamin; Ahmed, Aijaz; Newman, Aaron M.; Glenn, Jeffrey S.; Davis, Mark M.; Kaech, Susan M.; Weissman, Irving L.; Hasenkrug, Kim J.

doi:10.1038/s41467-019-08637-9

Cited by 50 publications

(51 citation statements)

References 81 publications

(92 reference statements)

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“…Our findings show that low DCLK1 expression correlated with high or low CD8 + T cells predicts better survival in colon and stomach cancer patients, suggesting DCLK1 has the potential to be an adjuvant target to promote sensitivity in immunotherapy-resistant patients. Additionally, it is widely reported that exhausted CD8+ T cells also express CD8A but lose the ability to eradicate the tumor cell [86,87]. This is hypothesized to be one significant reason why immune blockade increases the function of exhausted CD8+ T cells [88,89].…”

Section: Discussionmentioning

confidence: 99%

Cancer Stem Cell Marker DCLK1 Correlates with Tumorigenic Immune Infiltrates in the Colon and Gastric Adenocarcinoma Microenvironments

Weygant

et al. 2020

Cancers

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Immunotherapy that has proven efficacy in several solid cancers plays a partial role in improving clinical outcomes of advanced gastrointestinal (GI) cancers. There is an unmet need to find new immune-related therapeutic targets. Doublecortin-like kinase 1 (DCLK1) marks tuft cells which are recognized as cancer-initiating cells and regulators of the type II immune response, and has been studied for its role in many cancers including colon and gastric cancers, but its role in tumor immunity remains unexplored. In the current study, we analyzed colon and gastric cancer RNA sequencing data from 283 and 415 patients, respectively, from The Cancer Genome Atlas (TCGA). High DCLK1 expression predicted the worse clinical outcomes in colon and gastric cancer patients and correlated with increased immune and stromal components. Further analysis indicated that DCLK1 was strongly linked to infiltration of multiple immune cell types, especially TAMs and Treg, and strongly correlated with increased CD8+ T cell inhibitors TGFB1 and CXCL12 and their receptors, suggesting it may contribute to TAM-mediated inhibition of CD8+ T cells. Interestingly, we found that DCLK1 was a prognostic biomarker in left-sided colon cancer, which has worse outcomes and demonstrates a reduced response to existing immunotherapies. In conclusion, our results demonstrate that DCLK1 is linked with functional regulation of the tumor microenvironment and may have potential as a prognostic biomarker and adjuvant target to promote immunotherapy sensitivity in colon and gastric cancer patients.

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Section: Discussionmentioning

confidence: 99%

Cancer Stem Cell Marker DCLK1 Correlates with Tumorigenic Immune Infiltrates in the Colon and Gastric Adenocarcinoma Microenvironments

Weygant

et al. 2020

Cancers

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“…Recently, SIRP was also reported to be selectively expressed on a small subset of T lymphocytes, i.e. exhausted CD8+ memory T cells emerging after chronic viral infection (Myers et al, 2019). For a long time the general assumption has been that SIRP is, at least among hematopoietic cells, restricted to the myeloid lineage (Adams et al, 1998;Brooke et al, 1998).…”

Section: Discussionmentioning

confidence: 99%

SIRPα on mouse B1 cells restricts lymphoid tissue migration and natural antibody production

Berg

Franke

Pillai

et al. 2020

Preprint

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The inhibitory immunoreceptor SIRP is expressed on myeloid and neuronal cells and interacts with the broadly expressed CD47. CD47-SIRP interactions form an innate immune checkpoint and its targeting has shown promising results in cancer patients. Here, we report expression of SIRP on B1 lymphocytes, a non-conventional subpopulation of murine B cells responsible for the production of natural antibodies. Mice defective in SIRP signaling (SIRP CYT mice) displayed an enhanced CD11b/CD18 integrin-dependent B1 cell migration from the peritoneal cavity to the spleen, local B1 cell accumulation, and enhanced circulating natural antibody levels, which was further amplified upon immunization with T-independent type 2 antigen. As natural antibodies are atheroprotective we investigated the involvement of SIRP signaling in atherosclerosis development. Bone marrow (SIRP CYT >LDLR -/-) chimaeric mice developed reduced atherosclerosis accompanied by increased natural antibody production. Collectively, our data identify SIRP as a unique B1 cell inhibitory receptor acting to control B1 cell migration, and imply SIRPas a potential therapeutic target in atherosclerosis.

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“…As a consequence most FVspecific CD8+ T cells appear functionally exhausted and are very inefficient in killing peptide-labeled targets in vivo (Zelinskyy et al 2009a). However, a small subset of functional CD8+ T cells are preserved even in chronic infection and uniquely express the cell surface protein SIRPα (Myers et al 2019). CD8+ T cell exhaustion contributes to the subsequent development of FV chronicity , similar to what has been described for chronic LCMV infection (Barber et al 2006).…”

Section: Cd8+ T Cell Responsesmentioning

confidence: 99%

“…During chronic infection PD-1 expression can be used as a surrogate marker for exhausted CD8+ T cells and blocking the signaling of this receptor with antibodies can reactivate exhausted T cells (Barber et al 2006;Dietze et al 2013). Blocking the PD-1/PDL-1 axis results in the expansion of functional CD8+ T cells that express SIRPα (Myers et al 2019). Increased expression of co-inhibitory molecules such as PD-1 is likely to prevent immunopathogenic effects from overstimulated CD8+ T cells responses.…”

Section: Cd8+ T Cell Responsesmentioning

confidence: 99%

“…The combination of chronic antigen stimulation and suppression by Tregs and MDSCs establishes an immunosuppressive milieu that presents a complicated therapeutic situation. During the chronic phase of infection, the cytotoxic and cytokine-mediated antiviral activities of effector CD8+ T cells are largely incapacitated (Zelinskyy et al 2005;Zelinskyy et al 2009a), although recent results indicate that a small subset of CD8+ T cells expressing SIRPα remains functional (Myers et al 2019). Thus, immunotherapy in chronic viral infection mainly aims to restore the functionality of virusspecific T cells or expand the functional subsets.…”

Section: Immunotherapies In Fv Infectionmentioning

confidence: 99%

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Friend retrovirus studies reveal complex interactions between intrinsic, innate and adaptive immunity

Dittmer

Sutter

Kassiotis

et al. 2019

FEMS Microbiology Reviews

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Approximately 4.4% of the human genome is comprised of endogenous retroviral sequences, a record of an evolutionary battle between man and retroviruses. Much of what we know about viral immunity comes from studies using mouse models. Experiments using the Friend virus (FV) model have been particularly informative in defining highly complex anti-retroviral mechanisms of the intrinsic, innate and adaptive arms of immunity. FV studies have unraveled fundamental principles about how the immune system controls both acute and chronic viral infections. They led to a more complete understanding of retroviral immunity that begins with cellular sensing, production of type I interferons, and the induction of intrinsic restriction factors. Novel mechanisms have been revealed, which demonstrate that these earliest responses affect not only virus replication, but also subsequent innate and adaptive immunity. This review on FV immunity not only surveys the complex host responses to a retroviral infection from acute infection to chronicity, but also highlights the many feedback mechanisms that regulate and counter-regulate the various arms of the immune system. In addition, the discovery of molecular mechanisms of immunity in this model have led to therapeutic interventions with implications for HIV cure and vaccine development.

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A functional subset of CD8+ T cells during chronic exhaustion is defined by SIRPα expression

Cited by 50 publications

References 81 publications

Cancer Stem Cell Marker DCLK1 Correlates with Tumorigenic Immune Infiltrates in the Colon and Gastric Adenocarcinoma Microenvironments

Cancer Stem Cell Marker DCLK1 Correlates with Tumorigenic Immune Infiltrates in the Colon and Gastric Adenocarcinoma Microenvironments

SIRPα on mouse B1 cells restricts lymphoid tissue migration and natural antibody production

Friend retrovirus studies reveal complex interactions between intrinsic, innate and adaptive immunity

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