Immune characterization of pre-clinical murine models of neuroblastoma

Webb, Emily R.; Lanati, Silvia; Wareham, Carol; Easton, Alistair; Dunn, Stuart N.; Inzhelevskaya, Tatyana; Sadler, Freja M; James, Sonya; Ashton‐Key, Margaret; Cragg, Mark S.; Beers, Stephen A.; Gray, Juliet

doi:10.1038/s41598-020-73695-9

Cited by 25 publications

(33 citation statements)

References 59 publications

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“…Mouse neuroblastoma 9464D cells were cultured as previously described. 20 Antibodies Parental anti-mouse PD-1 (EW1-9) rIgG1 was raised using conventional hybridoma technology. 28 Mouse and human anti-PD-1 EW1-9 mIgG1, mIgG2a, mIgG1-N297A, hIgG4 and hIgG4-FALA 26 were constructed as previously described.…”

Section: Animals and Cellsmentioning

confidence: 99%

“…To this end, we compared the immunogenic MC38 model, which bears a high tumor mutational burden (TMB), 19 with the 9464D pediatric neuroblastoma model. 20 21 Pediatric cancers represent a paradigm of immunologically cold tumors with a low mutational load, limited T-cell infiltration, and generally poor responsiveness to anti-PD-1/PD-L1. 22 However, like many adult cancers, there is evidence of PD-1/PD-L1 expression in pediatric tumors, 23 24 supporting the use of preclinical models to better understand how to target PD-1.…”

Section: Introductionmentioning

confidence: 99%

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Fc-null anti-PD-1 monoclonal antibodies deliver optimal checkpoint blockade in diverse immune environments

Moreno-Vicente

Willoughby

Taylor

et al. 2022

J Immunother Cancer

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BackgroundDespite extensive clinical use, the mechanisms that lead to therapeutic resistance to anti-programmed cell-death (PD)-1 monoclonal antibodies (mAbs) remain elusive. Here, we sought to determine how interactions between the Fc region of anti-PD-1 mAbs and Fcγ receptors (FcγRs) affect therapeutic activity and how these are impacted by the immune environment.MethodsMouse and human anti-PD-1 mAbs with different Fc binding profiles were generated and characterized in vitro. The ability of these mAbs to elicit T-cell responses in vivo was first assessed in a vaccination setting using the model antigen ovalbumin. The antitumor activity of anti-PD-1 mAbs was investigated in the context of immune ‘hot’ MC38 versus ‘cold’ neuroblastoma tumor models, and flow cytometry performed to assess immune infiltration.ResultsEngagement of activating FcγRs by anti-PD-1 mAbs led to depletion of activated CD8 T cells in vitro and in vivo, abrogating therapeutic activity. Importantly, the extent of this Fc-mediated modulation was determined by the surrounding immune environment. Low FcγR-engaging mouse anti-PD-1 isotypes, which are frequently used as surrogates for human mAbs, were unable to expand ovalbumin-reactive CD8 T cells, in contrast to Fc-null mAbs. These results were recapitulated in mice expressing human FcγRs, in which clinically relevant hIgG4 anti-PD-1 led to reduced endogenous expansion of CD8 T cells compared with its engineered Fc-null counterpart. In the context of an immunologically ‘hot’ tumor however, both low-engaging and Fc-null mAbs induced long-term antitumor immunity in MC38-bearing mice. Finally, a similar anti-PD-1 isotype hierarchy was demonstrated in the less responsive ‘cold’ 9464D neuroblastoma model, where the most effective mAbs were able to delay tumor growth but could not induce long-term protection.ConclusionsOur data collectively support a critical role for Fc:FcγR interactions in inhibiting immune responses to both mouse and human anti-PD-1 mAbs, and highlight the context-dependent effect that anti-PD-1 mAb isotypes can have on T-cell responses. We propose that engineering of Fc-null anti-PD-1 mAbs would prevent FcγR-mediated resistance in vivo and allow maximal T-cell stimulation independent of the immunological environment.

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Section: Animals and Cellsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Fc-null anti-PD-1 monoclonal antibodies deliver optimal checkpoint blockade in diverse immune environments

Moreno-Vicente

Willoughby

Taylor

et al. 2022

J Immunother Cancer

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“…Similar results using TH-MYCN +/mice were recently shown, along with a synergistic effect of adding chemotherapy to GD2-directed antibody, analogous to the findings in children with relapsed neuroblastoma in the COG ANBL1221 chemoimmunotherapy trial. [8,17] Moreover, we found a reduced proportion of neuroblasts from 14G2a-treated mice expressed GD2 with decreased MFI when compared with PBS-treated tumors at both the midpoint and terminal time points, suggesting a selective pressure was exerted by 14G2a treatment. Recent work has suggested that GD2 serves as a macrophage checkpoint or "don't eat me" signal between neuroblasts and TAM.…”

Section: Discussionmentioning

confidence: 73%

“…[45] The TH-MYCN mouse model offers many advantages for the study of immune:tumor interactions, acknowledging there are certain limitations including the low frequency of macrometastases. [13,16,17,46,47] Anti-GD2 therapies against neuroblastoma have been studied…”

Section: Discussionmentioning

confidence: 99%

“…The tumor niche is important in influencing cancer progression as evidenced by syngeneic neuroblastoma transplant models in which subcutaneous implantation is 6 associated with reduced tumor growth and fewer infiltrating tumor-suppressive immune cells compared with the same tumor cells injected at orthotopic intra-adrenal sites. [17,18] Despite these advantages, an impediment to adoption of the highly penetrant 129x1/SvJ TH-MYCN model for studies into GD2-directed immunotherapies is the prevailing notion that these tumors lack sufficient surface GD2 to serve as an effective tumor antigen, primarily when investigated for syngeneic tumor transplantation studies. In the C57BL/6 background, preferred by many for immunologic studies, tumor penetrance for the TH-MYCN transgene is too low for efficient autochthonous modeling, and tumor-derived cell lines from this strain are found to express insufficient surface GD2 for therapeutic targeting unless they are manipulated pharmacologically or genetically.…”

Section: Introductionmentioning

confidence: 99%

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Anti-GD2 antibody therapy alters the neuroblastoma tumor microenvironment and extends survival in TH-MYCN mice

McNerney

Karageorgos

et al. 2021

Preprint

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Background: Neuroblastoma is a commonly lethal solid tumor of childhood and intensive chemoradiotherapy treatment cures ~50% of children with high-risk disease. The addition of immunotherapy using dinutuximab, a monoclonal antibody directed against the GD2 disialoganglioside expressed on neuroblasts, improves survival when incorporated into front-line therapy and shows robust activity in regressing relapsed disease when combined with chemotherapy. Still, many children succumb to neuroblastoma despite receiving dinutuximab-based immunotherapy, and efforts to counteract the immune suppressive signals responsible are warranted. Animal models of human cancers provide useful platforms to study immunotherapies. TH-MYCN transgenic mice are immunocompetent and develop neuroblastomas at autochthonous sites due to enforced MYCN expression in developing neural crest tissues. However, GD2-directed immunotherapy in this model has been underutilized due to the prevailing notion that TH-MYCN neuroblasts express insufficient GD2 to be targeted. Methods: TH-MYCN mice were treated with 14G2a (anti-GD2 antibody), isotype antibody, or phosphate buffered saline from day 14 of life until day 100 or signs of morbidity. Survival was recorded, and tumors were isolated in terminal surgeries for analysis of GD2 expression and immune cell frequencies. Tumors from untreated mice were explanted for generation into cell lines, and GD2 expression was recorded with serial passage in tissue culture. Immunocytology and immunoblotting were performed to evaluate for adrenergic and mesenchymal markers of neuroblasts. Survival curves compared using Kaplan-Meier method with a log-rank test for significance. Unpaired two-tailed Student's t-tests used for comparison of groups in flow cytometry analysis. Results: 14G2a markedly extends survival in such TH-MYCN mice. Additionally, neuroblasts in 14G2a-treated mice have reduced GD2 expression and fewer macrophage and myeloid-derived suppressor cells in their tumor microenvironments. Neuroblasts in TH-MYCN-driven tumors express GD2 at levels comparable to human neuroblastomas but rapidly lose GD2 expression when explanted ex vivo to establish tumor cell lines. The loss of GD2 expression ex vivo is associated with a transition from an adrenergic to mesenchymal state that is maintained when re-implanted in vivo. Conclusions: Our findings support the utility of the TH-MYCN model to inform GD2-directed immunotherapy approaches for neuroblastoma as well as opportunities to investigate drivers of adrenergic to mesenchymal fate decisions.

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SIRPα-specific monoclonal antibody enables antibody-dependent phagocytosis of neuroblastoma cells

Bahri

Kailayangiri

Vermeulen

et al. 2021

Cancer Immunol Immunother

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Immune characterization of pre-clinical murine models of neuroblastoma

Cited by 25 publications

References 59 publications

Fc-null anti-PD-1 monoclonal antibodies deliver optimal checkpoint blockade in diverse immune environments

Fc-null anti-PD-1 monoclonal antibodies deliver optimal checkpoint blockade in diverse immune environments

Anti-GD2 antibody therapy alters the neuroblastoma tumor microenvironment and extends survival in TH-MYCN mice

SIRPα-specific monoclonal antibody enables antibody-dependent phagocytosis of neuroblastoma cells

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