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GenVivo to Present at the 2023 American Society of Gene and Cell Therapy (ASGCT) Annual Meeting
Non-Replicating, Non-Integrating Vectors, Vector Production using Continuous Perfusion Bioprocessing and Optimization of a Suicide Gene
PASADENA, CA, UNITED STATES, May 19, 2023/EINPresswire.com/ — GenVivo, Inc., a clinical stage biopharmaceutical company utilizing gene therapy to develop novel vector-based immunotherapies, today announced that three posters are being presented at the ongoing American Society of Gene and Cell Therapy (ASGCT), which is being held in-person from May 16-20, in Los Angeles, CA. The posters will cover the optimization of the suicide gene, Herpes Simplex Virus Thymidine Kinase (HSV-TK), for cancer immunotherapy; the engineering of a non-replicating, non-integrating vector based on a highly modified Moloney Murine Leukemia Viral (MoMLV) vector; and the development of a method for production of an enveloped vector using continuous perfusion bioprocessing.
Presentation details
• Abstract Link: https://annualmeeting.asgct.org/abstracts
• Session Title: Poster Session III in Exhibit Hall/West Hall A
• Session Date and Time: Friday, May 19, 2023 from 12:00 PM to 1:30 PM PST
Poster 1
• Abstract Title: Non-Replicating, Non-Integrating Vector for Immunotherapy and Vaccine Applications
• Presenter: Jackie Fischer-Lougheed, PhD., Principal Scientist at GenVivo, Inc.
• Abstract Number: 1423
Non-replicating, non-integrating vectors represent an attractive alternative for transgene therapy as the duration of payload expression outperforms current approaches, such as with formulated mRNA. This study demonstrates the ability to engineer a non-replicating Moloney Murine Leukemia Viral (MoMLV) vector to become non-integrating. Multiple mutants were constructed at the Mg2+ binding motif of the catalytic core domain of the integrase in the vector gagpol gene. All mutants of defective integrase successfully generated vector particles at high titers similar to the wild-type gagpol sequence and resulted in similar levels of expression of the payload protein HSV-TK in transduced target cells. These constructs provide a new platform with improved safety for testing various future therapeutic and prophylactic applications, ranging from cancer therapy to vaccine delivery.
Poster 2
• Abstract Title: Intensified Enveloped Vector Production Using Continuous Perfusion Bioprocessing
• Presenter: Lynn Svay, Process Development and Engineering, Director at GenVivo, Inc.
• Abstract Number: 1575
This study addresses the need to overcome vector production limitations using established technologies by applying tangential flow depth filtration (TFDF) technology in a perfusion process. The process provides high efficiency cell retention, producing a high-quality vector while minimizing filter fouling risks. Various permeate flow rates were tested in Mobius and Distek bioreactors while reaching a maximum viable cell density of 60 x 10^6 vc/mL. The infectious titer in the permeate was significantly higher than that in the retentate suggesting the vectors could maintain their infectivity after filtration from the bioreactor. Remarkably, no fouling of the TFDF filters was observed during five runs that lasted up to 10 days. This study demonstrates the expected feasibility of utilizing a TFDF system for enveloped vector production.
Poster 3
• Abstract Title: Optimization of a Suicide Gene Vector for the GEN2 Cancer Immunotherapy Clinical Trial
• Presenter: Cecilia Roh, PhD., Gene Therapy Research and Development, Director at GenVivo, Inc.
• Abstract Number: 1634
This study demonstrates the successful optimization of a suicide gene, Herpes Simplex Virus Thymidine Kinase (HSV-TK), to create a more potent cancer cell killing therapeutic. HSV-TK gene was modified and demonstrated localization of the protein to the cytoplasm and increased level of cell killing activity & bystander effect activity. Tumor bearing animal experiments were undertaken to investigate the effect of the suicide plus Granulocyte Macrophage Colony Stimulating Factor (GM-CSF) genes on tumor eradication and against tumor re-challenge. The in vivo and in vitro data indicate that an optimized suicide gene along with a gene encoding GM-CSF can stimulate immune responses directed against the tumor, leading to tumor eradication and a durable immunological response against the tumor.
About GenVivo
GenVivo is a clinical stage biopharmaceutical company utilizing gene therapy to develop novel vector-based in-vivo immunotherapies focused on helping patients fight cancer. Our lead candidate, GEN2, is currently in a Phase 1 clinical trial (NCT04313868).
For more information about GenVivo, visit https://genvivoinc.com/
Forward-Looking Statements
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Victor Constantinescu
GenVivo, Inc.
+1 626-768-5162
[email protected]