Generation of immunocompetent syngeneic allograft mouse models for pediatric diffuse midline glioma

Chatinier, Aimée du; Meel, Michaël H.; Das, Arvid I; Metselaar, Dennis S.; Waranecki, Piotr; Bugiani, Marianna; Breur, Marjolein; Simonds, Erin F.; Lu, Edbert D; Weiss, William A.; Vallejo, Juan J. García; Hoving, Eelco W.; Phoenix, Timothy N.; Hulleman, Esther

doi:10.1093/noajnl/vdac079

Cited by 11 publications

(13 citation statements)

References 47 publications

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“…Interestingly, the highest TIM-3 expression intensity was observed in DC, macrophage, microglia, and Treg populations ( Figures S4 B and S4C). In addition, we confirmed TIM-3 expression in one additional in utero electroporation (IUE) DMG model (PPK 26 ) and in an isogenic orthotopic DMG model (24D-1: H3WT; 26C-7: H3.1K27M, and 26B-7 H3.3K27M) also develop by IUE model 27 ). The expression of TIM-3 in these additional models further supports the notion that, indeed, its expression in DMGs is observed across different models.…”

Section: Resultssupporting

confidence: 62%

TIM-3 blockade in diffuse intrinsic pontine glioma models promotes tumor regression and antitumor immune memory

Ausejo-Mauleon,

Labiano,

de la Nava

et al. 2023

Cancer Cell

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Section: Resultssupporting

confidence: 62%

TIM-3 blockade in diffuse intrinsic pontine glioma models promotes tumor regression and antitumor immune memory

Ausejo-Mauleon,

Labiano,

de la Nava

et al. 2023

Cancer Cell

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“… 40 , 132 , 133 , 134 , 135 , 136 , 137 Recently, the use of in utero electroporation has allowed for the generation of immunocompetent allograft models of brainstem tumors that closely mimic the immune microenvironment seen in patients, effectively addressing the limitation that has hindered replication of the complexity of the human immune response in traditional mouse models. 138 …”

Section: Discussionmentioning

confidence: 99%

Microglia in pediatric brain tumors: The missing link to successful immunotherapy

du Chatinier,

Velilla,

Meel

et al. 2023

Cell Reports Medicine

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“…Moreover, some immunocompetent models have been developed by introducing driver mutations that were identified in human tumours [28,98]. For example, an immunocompetent mouse model of DMG was successfully generated by Du Chatinier et al [99]. They established tumour cell lines from DMG mouse models that had been induced through intra-uterine electroporation of DMG-specific mutations into the embryonic brainstem [99].…”

Section: Overcoming Limitations and Obstacles Of Ov Therapy 61 Precli...mentioning

confidence: 99%

OV Modulators of the Paediatric Brain TIME: Current Status, Combination Strategies, Limitations and Future Directions

Vazaios,

van Berkum,

Calkoen

et al. 2024

IJMS

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Oncolytic viruses (OVs) are characterised by their preference for infecting and replicating in tumour cells either naturally or after genetic modification, resulting in oncolysis. Furthermore, OVs can elicit both local and systemic anticancer immune responses while specifically infecting and lysing tumour cells. These characteristics render them a promising therapeutic approach for paediatric brain tumours (PBTs). PBTs are frequently marked by a cold tumour immune microenvironment (TIME), which suppresses immunotherapies. Recent preclinical and clinical studies have demonstrated the capability of OVs to induce a proinflammatory immune response, thereby modifying the TIME. In-depth insights into the effect of OVs on different cell types in the TIME may therefore provide a compelling basis for using OVs in combination with other immunotherapy modalities. However, certain limitations persist in our understanding of oncolytic viruses’ ability to regulate the TIME to enhance anti-tumour activity. These limitations primarily stem from the translational limitations of model systems, the difficulties associated with tracking reliable markers of efficacy throughout the course of treatment and the role of pre-existing viral immunity. In this review, we describe the different alterations observed in the TIME in PBTs due to OV treatment, combination therapies of OVs with different immunotherapies and the hurdles limiting the development of effective OV therapies while suggesting future directions based on existing evidence.

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Generation of immunocompetent syngeneic allograft mouse models for pediatric diffuse midline glioma

Cited by 11 publications

References 47 publications

TIM-3 blockade in diffuse intrinsic pontine glioma models promotes tumor regression and antitumor immune memory

TIM-3 blockade in diffuse intrinsic pontine glioma models promotes tumor regression and antitumor immune memory

Microglia in pediatric brain tumors: The missing link to successful immunotherapy

OV Modulators of the Paediatric Brain TIME: Current Status, Combination Strategies, Limitations and Future Directions

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