Targeting IGF2 to reprogram the tumor microenvironment for enhanced viro-immunotherapy

Author:

Noh Min Hye1,Kang Jin Muk12,Miller Alexandra A31,Nguyen Grace1,Huang Minxin1,Shim Ji Seon1,Bueso-Perez Alberto J1,Murphy Sara A34,Rivera-Caraballo Kimberly A34,Otani Yoshihiro51,Kim Eunju67,Yoo Seung-Hee7,Yan Yuanqing81,Banasavadi-Siddegowda Yeshavanth9,Nakashima Hiroshi10,Chiocca E Antonio10,Kaur Balveen4,Zhao Zhongming11ORCID,Lee Tae Jin31,Yoo Ji Young31ORCID

Affiliation:

1. Department of Neurosurgery, McGovern Medical School, The University of Texas Health Science Center at Houston , Houston, Texas , USA

2. Department of Pediatric Hematology & Oncology, University Hospitals Cleveland Medical Center , Cleveland, Ohio , USA

3. The University of Texas MD Anderson Cancer Center UTHealth Houston Graduate School of Biomedical Science , Houston, Texas , USA

4. Georgia Cancer Center and Department of Pathology, Medical College of Georgia, Augusta University , Augusta, Georgia , USA

5. Department of Neurological Surgery, Okayama University Graduate School of Medicine, Dentistry, and Pharmaceutical Sciences , Okayama , Japan

6. Department of Food and Nutriton, Kongju National University , Yesan, Chungnam , South Korea

7. Department of Biochemistry, McGovern Medical School, The University of Texas Health Science Center at Houston , Houston, Texas , USA

8. Department of Surgery, Northwestern University Feinberg School of Medicine , Chicago, Illinois , USA

9. Surgical Neurology Branch, National Institute of Neurological Disorders and Stroke, National Institutes of Health , Bethesda, Maryland , USA

10. Department of Neurosurgery, Brigham and Women’s Hospital and Harvard Medical School , Boston, Maryland , USA

11. Center for Precision Health, McWilliams School of Biomedical Informatics, The University of Texas Health Science Center at Houston , Houston, Texas , USA

Abstract

Abstract Background The FDA approval of oncolytic herpes simplex-1 virus (oHSV) therapy underscores its therapeutic promise and safety as a cancer immunotherapy. Despite this promise, the current efficacy of oHSV is significantly limited to a small subset of patients largely due to the resistance in tumor and tumor microenvironment (TME). Methods RNA sequencing (RNA-Seq) was used to identify molecular targets of oHSV resistance. Intracranial human and murine glioma or breast cancer brain metastasis (BCBM) tumor-bearing mouse models were employed to elucidate the mechanism underlying oHSV therapy-induced resistance. Results Transcriptome analysis identified IGF2 as one of the top-secreted proteins following oHSV treatment. Moreover, IGF2 expression was significantly upregulated in 10 out of 14 recurrent GBM patients after treatment with oHSV, rQNestin34.5v.2 (71.4%; P = .0020) (ClinicalTrials.gov, NCT03152318). Depletion of IGF2 substantially enhanced oHSV-mediated tumor cell killing in vitro and improved survival of mice bearing BCBM tumors in vivo. To mitigate the oHSV-induced IGF2 in the TME, we constructed a novel oHSV, oHSV-D11mt, secreting a modified IGF2R domain 11 (IGF2RD11mt) that acts as IGF2 decoy receptor. Selective blocking of IGF2 by IGF2RD11mt significantly increased cytotoxicity, reduced oHSV-induced neutrophils/PMN-MDSCs infiltration, and reduced secretion of immune suppressive/proangiogenic cytokines, while increased CD8 + cytotoxic T lymphocytes (CTLs) infiltration, leading to enhanced survival in GBM or BCBM tumor-bearing mice. Conclusions This is the first study reporting that oHSV-induced secreted IGF2 exerts a critical role in resistance to oHSV therapy, which can be overcome by oHSV-D11mt as a promising therapeutic advance for enhanced viro-immunotherapy.

Funder

American Cancer Society

National Institutes of Health

Publisher

Oxford University Press (OUP)

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