Abstract

? PROJECT 2 Glioblastoma (GBM) has a dismal prognosis. Based on recent favorable results with other forms of cancer, immunotherapies are increasingly being tested in clinical trials of GBM. One type of immunotherapy consists of oncolytic viruses (OVs0 that exert their effects by direct tumor cytotoxicity with rounds of intratumoral infectious spread that elicit an antitumor immune response. In 2015 the first OV, based on oncolytic Herpes Simplex Virus (oHSV), was approved by the FDA. Over the last several years, we have preclinically developed a novel oHSV with GBM selectivity, designated as rQNestin34.5. The main difference between rQNestin34.5 and previous oHSVs that have been tested in human GBM clinical trials is that the HSV1 ?2 34.5 gene that encodes for the ICP34.5 protein is retained under transcriptional control of a nestin promoter/enhancer element highly expressed in GBM and in the GBM ?stem-like? cell population, but not expressed in the adult human brain. Extensive preclinical efficacy, toxicology and biodistribution studies have been carried out with rQNestin34.5 in mice, culminating in an IND (#16380) in 2016. We are now poised to initiate a ?first-in-man' Phase I clinical trial of rQNestin34.5 for recurrent GBM, which we plan to finish by the end of this proposed project. Our overarching hypothesis is that rQNestin34.5 in humans leads to evidence of an immune response and that a combination of oHSV-intratumoral oncolysis/ immunostimulation with inhibition of immune checkpoint signaling will provide increased effectiveness in animal models of glioma. We propose to test this hypothesis with the following 3 aims:
Aim 1 : Test if there is a maximum tolerated dose (MTD) and pilot correlative efficacy for a ?first-in-man? clinical trial of rQNestin34.5;
Aim 2 : Test if immune checkpoint (IC) blockade augments oHSV antiGBM effects in mice where T cells express high levels of PD-1;
and Aim 3 : Test if expression of IC antibodies by newly engineered oHSVs improves efficacy/toxicity profiles when compared to systemic IC antibody administration. As part of this PPG, we also plan to collaborate with Project 4 for the correlative science required for immune cell function in human specimens and with Project 3 for the science related to Notch signaling. Our trial will inform Project 1 in its design of the next generation of oHSV clinical trials. We will employ the services of Core 3 for biostatistical analyses. We will employ the services of Core 1 to generate oHSV and Core 2 for the use of glioma models. Finally, Core A provides the overall administrative functions required to integrate and manage this project with others.

Public Health Relevance

? PROJECT 2 Glioblastoma (GBM) is amongst the most lethal forms of cancer. We propose to utilize a novel tumor- killing virus, based on herpes simplex virus, designated as rQNestin34.5 in a ?first-in-man? clinical trial in humans with GBMs that have failed standard of care therapy. Based on recent advances in understanding how cancers keep the immune system in check, we also plan to test if rQNestin34.5 is even more powerful against GBM when combined with the new FDA-approved agents that block these ?cancer-mediated? immune checkpoints.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA163205-08
Application #
10019364
Study Section
Special Emphasis Panel (ZCA1)
Project Start
2013-02-07
Project End
2023-08-31
Budget Start
2020-09-01
Budget End
2021-08-31
Support Year
8
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
030811269
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Scoville, Steven D; Nalin, Ansel P; Chen, Luxi et al. (2018) Human AML activates the aryl hydrocarbon receptor pathway to impair NK cell development and function. Blood 132:1792-1804
Chan, Wing Keung; Kang, Siwen; Youssef, Youssef et al. (2018) A CS1-NKG2D Bispecific Antibody Collectively Activates Cytolytic Immune Cells against Multiple Myeloma. Cancer Immunol Res 6:776-787
Nakashima, Hiroshi; Alayo, Quazim A; Penaloza-MacMaster, Pablo et al. (2018) Modeling tumor immunity of mouse glioblastoma by exhausted CD8+ T cells. Sci Rep 8:208
Marzulli, M; Mazzacurati, L; Zhang, M et al. (2018) A Novel Oncolytic Herpes Simplex Virus Design based on the Common Overexpression of microRNA-21 in Tumors. J Gene Ther 3:
Russell, Luke; Swanner, Jessica; Jaime-Ramirez, Alena Cristina et al. (2018) PTEN expression by an oncolytic herpesvirus directs T-cell mediated tumor clearance. Nat Commun 9:5006
Dai, Hong-Sheng; Caligiuri, Michael A (2018) Molecular Basis for the Recognition of Herpes Simplex Virus Type 1 Infection by Human Natural Killer Cells. Front Immunol 9:183
Chen, Luxi; Youssef, Youssef; Robinson, Cameron et al. (2018) CD56 Expression Marks Human Group 2 Innate Lymphoid Cell Divergence from a Shared NK Cell and Group 3 Innate Lymphoid Cell Developmental Pathway. Immunity 49:464-476.e4
Victor, Aaron R; Weigel, Christoph; Scoville, Steven D et al. (2018) Epigenetic and Posttranscriptional Regulation of CD16 Expression during Human NK Cell Development. J Immunol 200:565-572
Kim, Yangjin; Yoo, Ji Young; Lee, Tae Jin et al. (2018) Complex role of NK cells in regulation of oncolytic virus-bortezomib therapy. Proc Natl Acad Sci U S A 115:4927-4932
Sadahiro, Hirokazu; Kang, Kyung-Don; Gibson, Justin T et al. (2018) Activation of the Receptor Tyrosine Kinase AXL Regulates the Immune Microenvironment in Glioblastoma. Cancer Res 78:3002-3013

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