4.7 Article

Agent-based computational modeling of glioblastoma predicts that stromal density is central to oncolytic virus efficacy

期刊

ISCIENCE
卷 25, 期 6, 页码 -

出版社

CELL PRESS
DOI: 10.1016/j.isci.2022.104395

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资金

  1. Fonds de recherche du Quebec-Sante Programme de bourse de formation postdoctorale pour les citoyens d'autres pays
  2. Centre for Applied Mathematics in Bioscience and Medicine (CAMBAM) Postdoctoral fellowship
  3. Breast Cancer Alliance Young Investigator Award
  4. Ben and Catherine Ivy Foundation
  5. Jayne Koskinas Ted Giovannis Foundation for Health and Policy
  6. National Cancer Institute [U01-CA232137]
  7. National Science Foundation [1720625]
  8. NSERC [RGPIN-2018-04546]
  9. Fonds de Recherche du Quebec - Sante

向作者/读者索取更多资源

This study investigated the therapeutic efficacy of herpes simplex virus in glioblastoma using an ex vivo tumor model and a computational model. The findings suggest that stromal density plays a crucial role in determining the success of oncolytic virus therapy, and this was validated in patient samples.
Oncolytic viruses (OVs) are emerging cancer immunotherapy. Despite notable successes in the treatment of some tumors, OV therapy for central nervous system cancers has failed to show efficacy. We used an ex vivo tumor model developed from human glioblastoma tissue to evaluate the infiltration of herpes simplex OV rQNestin (oHSV-1) into glioblastoma tumors. We next leveraged our data to develop a computational, model of glioblastoma dynamics that accounts for cellular interactions within the tumor. Using our computational model, we found that low stromal density was highly predictive of oHSV-1 therapeutic success, suggesting that the efficacy of oHSV-1 in glioblastoma may be determined by stromal-to-tumor cell regional density. We validated these findings in heterogenous patient samples from brain metastatic adenocarcinoma. Our integrated modeling strategy can be applied to suggest mechanisms of therapeutic responses for central nervous system cancers and to facilitate the successful translation of OVs into the clinic.

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