An Engineered IL15 Cytokine Mutein Fused to an Anti-PD1 Improves Intratumoral T-cell Function and Antitumor Immunity

Xu, Yuanming; Carrascosa, Lucia Campos; Yeung, Yik Andy; Chu, Matthew L. H.; Yang, Wenjing; Djuretic, Ivana; Pappas, Danielle; Zeytounian, John; Ge, Zhouhong; Ruiter, Valeska de; Starbeck-Miller, Gabriel R.; Patterson, James C.; Rigas, Diamanda; Chen, Shih-Hsun; Kraynov, Eugenia; Boor, Patrick P.C.; Noordam, Lisanne; Doukas, Michael; Tsao, Dave; IJzermans, Jan N.M.; Guo, Jie; Grünhagen, Dirk J.; Erdmann, Joris I.; Verheij, Joanne; Royen, Martin E. van; Doornebosch, Pascal G.; Feldman, R. M. Renny; Park, Terrence; Mahmoudi, Salah; Dorywalska, Magdalena; Ni, Irene; Chin, Sherman M.; Mistry, Tına; Mosyak, Lidia; Lin, Laura; Ching, Keith A.; Lindquist, Kevin C.; Ji, Changhua; Londono, Luz M.; Kuang, Bing; Rickert, Robert C.; Kwekkeboom, Jaap; Sprengers, Dave; Huang, Tzu-Hsuan; Chaparro‐Riggers, Javier

doi:10.1158/2326-6066.cir-21-0058

Cited by 46 publications

(42 citation statements)

References 58 publications

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“…Moreover, targeting TNF was proved to alleviate Zika virus complications in mouse models [ 61 ]. Besides, among 1,057 specific DEGs in U-251 MG cells, IL15 regulates T and natural killer cell activation and proliferation [ 62 ]. MYD88 encodes a cytosolic adapter protein that plays a central role in the innate and adaptive immune response, which functions as an essential signal transducer in the interleukin-1 and Toll-like receptor signaling pathways [ 63 ].…”

Section: Discussionmentioning

confidence: 99%

Revealing the characteristics of ZIKV infection through tissue-specific transcriptome sequencing analysis

et al. 2022

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Background Recently, Zika virus (ZIKV) re-emerged in India and was potentially associated with microcephaly. However, the molecular mechanisms underlying ZIKV pathogenesis remain to be explored. Results Herein, we performed a comprehensive RNA-sequencing analysis on ZIKV-infected JEG-3, U-251 MG, and HK-2 cells versus corresponding uninfected controls. Combined with a series of functional analyses, including gene annotation, pathway enrichment, and protein–protein interaction (PPI) network analysis, we defined the molecular characteristics induced by ZIKV infection in different tissues and invasion time points. Data showed that ZIKV infection and replication in each susceptible organ commonly stimulated interferon production and down-regulated metabolic-related processes. Also, tissue-specific immune responses or biological processes (BPs) were induced after ZIKV infection, including GnRH signaling pathway in JEG-3 cells, MAPK signaling pathway in U-251 MG cells, and PPAR signaling pathway in HK-2 cells. Of note, ZIKV infection induced delayed antiviral interferon responses in the placenta-derived cell lines, which potentially explains the molecular mechanism by which ZIKV replicates rapidly in the placenta and subsequential vertical transmission occurs. Conclusions Together, these data may provide a systemic insight into the pathogenesis of ZIKV infection in distinct human tissue-derived cell lines, which is likely to help develop prophylactic and therapeutic strategies against ZIKV infection.

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Section: Discussionmentioning

confidence: 99%

Revealing the characteristics of ZIKV infection through tissue-specific transcriptome sequencing analysis

et al. 2022

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“…The HepG2 killing assay was performed as described previously [ 29 ]. PBMCs were activated with anti-human CD3/CD28 dynabeads at a 1:100 bead:cell ratio for 3 days.…”

Section: Methodsmentioning

confidence: 99%

“…1e). We tested the cytotoxic properties of PBMCs in OM without the addition of nicotinamide in our previously established model of immune cell-mediated killing of tumour cell line HepG2 [29]. PBMCs were pre-activated with anti-CD3/CD28-coated beads, then co-cultured for 7 days with HepG2 cells that were genetically labelled with RFP.…”

Section: Establishment and Optimisation Of 3d Co-culture Conditionsmentioning

confidence: 99%

Modelling immune cytotoxicity for cholangiocarcinoma with tumour-derived organoids and effector T cells

et al. 2022

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Background Immunotherapy with immune checkpoint inhibitors (ICIs) is being explored to improve cholangiocarcinoma (CCA) therapy. However, it remains difficult to predict which ICI will be effective for individual patients. Therefore, the aim of this study is to develop a co-culture method with patient-derived CCA organoids and immune cells, which could represent anti-cancer immunity in vitro. Methods CCA organoids were co-cultured with peripheral blood mononuclear cells or T cells. Flow cytometry, time-lapse confocal imaging for apoptosis, and quantification of cytokeratin 19 fragment (CYFRA) release were applied to analyse organoid and immune cell behaviour. CCA organoids were also cultured in immune cell-conditioned media to analyse the effect of soluble factors. Results The co-culture system demonstrated an effective anti-tumour organoid immune response by a decrease in live organoid cells and an increase in apoptosis and CYFRA release. Interpatient heterogeneity was observed. The cytotoxic effects could be mediated by direct cell–cell contact and by release of soluble factors, although soluble factors only decreased viability in one organoid line. Conclusions In this proof-of-concept study, a novel CCA organoid and immune cell co-culture method was established. This can be the first step towards personalised immunotherapy for CCA by predicting which ICIs are most effective for individual patients.

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“…24 ). This is a different approach as compared with targeting cytokines to specific immune cells by fusion to immune receptor-targeting antibodies such as in PD1-IL2v or other recently reported fusion proteins 25,26 . We therefore produced a FAP-IL2 superkine analogue with increased binding affinity for IL-2Rβ and compared it with PD1-IL2v for potency and cis targeting in the cis-trans STAT5-P assay in activated T cells.…”

Section: Comparison Of Pd1-il2v To Il-2rb-biased Il-2 Mutantmentioning

confidence: 99%

PD-1-cis IL-2R agonism yields better effectors from stem-like CD8+ T cells

Deak

Nicolini

Hashimoto

et al. 2022

Nature

130

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Expansion and differentiation of antigen-experienced PD-1+TCF-1+ stem-like CD8+ T cells into effector cells is critical for the success of immunotherapies based on PD-1 blockade1–4. Hashimoto et al. have shown that, in chronic infections, administration of the cytokine interleukin (IL)-2 triggers an alternative differentiation path of stem-like T cells towards a distinct population of ‘better effector’ CD8+ T cells similar to those generated in an acute infection5. IL-2 binding to the IL-2 receptor α-chain (CD25) was essential in triggering this alternative differentiation path and expanding better effectors with distinct transcriptional and epigenetic profiles. However, constitutive expression of CD25 on regulatory T cells and some endothelial cells also contributes to unwanted systemic effects from IL-2 therapy. Therefore, engineered IL-2 receptor β- and γ-chain (IL-2Rβγ)-biased agonists are currently being developed6–10. Here we show that IL-2Rβγ-biased agonists are unable to preferentially expand better effector T cells in cancer models and describe PD1-IL2v, a new immunocytokine that overcomes the need for CD25 binding by docking in cis to PD-1. Cis binding of PD1-IL2v to PD-1 and IL-2Rβγ on the same cell recovers the ability to differentiate stem-like CD8+ T cells into better effectors in the absence of CD25 binding in both chronic infection and cancer models and provides superior efficacy. By contrast, PD-1- or PD-L1-blocking antibodies alone, or their combination with clinically relevant doses of non-PD-1-targeted IL2v, cannot expand this unique subset of better effector T cells and instead lead to the accumulation of terminally differentiated, exhausted T cells. These findings provide the basis for the development of a new generation of PD-1 cis-targeted IL-2R agonists with enhanced therapeutic potential for the treatment of cancer and chronic infections.

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An Engineered IL15 Cytokine Mutein Fused to an Anti-PD1 Improves Intratumoral T-cell Function and Antitumor Immunity

Cited by 46 publications

References 58 publications

Revealing the characteristics of ZIKV infection through tissue-specific transcriptome sequencing analysis

Revealing the characteristics of ZIKV infection through tissue-specific transcriptome sequencing analysis

Modelling immune cytotoxicity for cholangiocarcinoma with tumour-derived organoids and effector T cells

PD-1-cis IL-2R agonism yields better effectors from stem-like CD8+ T cells

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