Umoja Biopharma Presents New Preclinical Data at ASGCT 2022 Annual Meeting on its VivoVec Platform Describing Preclinical Safety Data for UB-VV100 Product Candidate, VivoVec Engineering for Improved in vivo CAR T cell Generation and Development of a Scalable Manufacturing Platform
UB-VV100 preclinical safety data demonstrates overall low risk for off target transduction and has a favorable safety and biodistribution profile
Next generation VivoVec surface engineering promotes “immune synapse”-formation for improved in vivo CAR T cell generation
Manufacturing process development demonstrates steps for scalable manufacturing of cGMP-grade lentiviral vector drug product
SEATTLE, May 19, 2022 – Umoja Biopharma, Inc., an immuno-oncology company pioneering off-the-shelf, integrated therapeutics that reprogram immune cells in vivo for patients with solid and hematologic malignancies, announced data from three presentations at the American Society of Gene and Cell Therapy (ASGCT) Annual Meeting on its scalable, off-the-shelf in vivo lentiviral vector-based platform, termed VivoVec, that has the potential to achieve efficient T cell transduction upon direct administration to patients.
“At this year’s ASGCT conference we’re excited to share for the very first time preclinical data showing our efforts to engineer lentiviral surface particles to structurally mimic the immune synapse. The immune synapse is the space formed between antigen presenting cells and T cells during T cell activation and we show that optimization of this synapse can enhance the efficiency of our in vivo CAR T cell platform, VivoVec, to create therapeutic T cells,” said Andy Scharenberg, M.D., co-founder and Chief Executive Officer of Umoja. “Our research team is also sharing updates on improvements made to our proprietary manufacturing process for VivoVec particles that supports scalable cGMP production for clinical trials. Altogether these studies continue to provide additional evidence that our multi-component in vivo CAR T cell therapeutics platform, which also includes universal TumorTag small molecules and the RACR/CAR for natural expansion and proliferation of therapeutic CAR T cells, has great potential to overcome critical obstacles facing the cell therapy industry.”
Umoja’s one oral and two poster presentations demonstrate progress in UB-VV100 IND-enabling studies, manufacturing platform development, and next generation VivoVec surface engineering. Preclinical data provides early evidence of the anti-tumor activity and preliminary preclinical safety of UB-VV100, Umoja’s preclinical candidate for the treatment of B cell malignancies. Preclinical safety studies completed to-date demonstrate the overall low risk for off target transduction after in vivo administration of UB-VV100 in two animal models, including a model of intranodal delivery. Additional development of next generation VivoVec particle surface engineering with costimulatory ligands to promote T cell binding, activation, and transduction by replicating immune synapse formation will enable efficient in vivo CAR T cell generation and subsequent anti-tumor immune activity. Umoja further describes a scalable, suspension cell culture-based manufacturing process capable of producing cGMP-grade lentiviral vector product for in vivo CAR T cell therapy.
Abstract #: 1242
Title: Preclinical Activity and Safety of UB-VV100, A Novel Lentiviral Vector Product Designed for Selective and Effective In Vivo Engineering of Therapeutic Anti-CD19 CAR T Cells for B cell Malignancies
Presenter: Alissa Brandes, Ph.D., Principal Scientist, Umoja Biopharma
- Presentation describes the preclinical activity and safety of UB-VV100, a VivoVec particle containing a payload encoding an anti-CD19 4-1BBz CAR and a novel synthetic receptor, rapamycin-activated cytokine receptor (RACR).
- Administration of UB-VV100 in a humanized mouse model of B cell malignancies results in the activation and transduction of T cells resulting in CAR expression, RACR enhanced CAR T cell expansion, and anti-tumor activity
- UB-VV100 preliminary toxicology studies demonstrate a favorable safety and biodistribution profile in two preclinical animal models: intranodal administration to canines and systemic administration to humanized mice
- Intranodal administration in canines, the proposed clinical route of administration, resulted in transduction that was largely restricted to the injected lymph nodes and no quantifiable transduction of non-immune tissues
Abstract #: 879
Title: A Lentiviral-Based In Vivo CAR T Cell Generation Platform with Viral Particle Surface Engineering Incorporating Anti-CD3 Single Chain Variable Fragment and T Cell Costimulatory Molecules
Presenter: Christopher Nicolai, Ph.D., Senior Scientist, Umoja Biopharma
- Investigation of multiple novel surface particle engineering approaches for VivoVec lentiviral vectors to replicate immune synapse formation, resulting in enhanced particle-T cell binding, T cell activation, transduction, and transduced T cell quality.
- VivoVec particles pseudotyped with the Cocal fusion glycoprotein and engineered to express T cell costimulatory ligands exhibited enhanced activation and transduction efficiency
- CAR T cells generated with next generation VivoVec particles demonstrate enhanced anti-tumor activity and persistence in preclinical models of hematologic malignancy
Abstract #: 1166
Title: Development of a Scalable, Suspension Cell Culture-Based Manufacturing Process for VivoVec, a Lentiviral Vector Platform for In Vivo CAR-T Cell Generation
Presenter: Jeff Plomer, Ph.D., Senior Director Process Development, Umoja Biopharma
- Poster describes the development of a scalable, suspension cell culture-based manufacturing process capable of producing lentiviral vector product with quality characteristics suitable for direct injection
- The VivoVec platform is built on 3rd generation lentiviral vector gene delivery technology
- Establishes a Quality Target Product Profile (QTPP) providing lentiviral vector product design that forms the basis for development
- Utilizes well established biopharmaceutical manufacturing methods to control lentiviral vector production and reduce process-related impurities
- Results will be used to identify critical process parameters and establish the operating ranges for the clinical and commercial manufacturing control strategy
Presentations can be accessed from the ASGCT website at https://annualmeeting.asgct.org/.
About Umoja Biopharma, Inc. Umoja Biopharma, Inc. is a preclinical stage company advancing an entirely new approach to immunotherapy. Umoja Biopharma, Inc. is a transformative multi-platform immuno-oncology company founded with the goal of creating curative treatments for solid and hematological malignancies by reprogramming a patient’s immune system in vivo. Founded based on pioneering work performed at Seattle Children’s Research Institute and Purdue University, Umoja’s novel approach is powered by integrated cellular immunotherapy technologies including the VivoVec in vivo delivery platform, the RACR/CAR in vivo cell expansion/control platform, and the TumorTag targeting platform. Designed from the ground up to work together, these platforms are being developed to create and harness a powerful immune response in the body to directly, safely, and controllably attack cancer. Umoja believes that its approach can provide broader access to the most advanced immunotherapies and enable more patients to live better, fuller lives. To learn more, visit http://umoja-biopharma.com/.
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Darren Opland, Ph.D.