Abstract

CORE C: CORRELATIVE SCIENCES Immuno-gene therapies have demonstrated an unparalleled anti-cancer efficacy in very poor prognosis patients. Limitations in the in vivo efficacy of the patient?s own T cells in CLL, antigen escape-related relapse in ALL, a CAR-engineered T cell pool outpaced by tumor cells in myeloma, and lack of appropriate, tumor- selective CAR in AML has given rise to the current proposal wherein innovative approaches are expected to solve the aforementioned challenges in cellular immunotherapy. Our trials will be the first to use CRISPR/Cas9-enhanced immune-gene therapy to treat some of the most challenging cases in each clinical indication; the first to use CART cells targeting two different antigens; the first to target AML with normal donor CART cells targeting CD33 while repopulating the host with CD33-edited hematopoietic stem cells. Critical to the success of cell therapies is a central correlative sciences laboratory to study the in vivo kinetics and homing of the infusion product(s) and the response of the tumor and the bioactivity of the infused cells; Core C provides this GCLP-based yet nimble infrastructure to support the clinical trials proposed herein, where SOP-specified molecular, cellular, and biochemical assays will be performed, reviewed by qualified personnel, and entered into a database for aggregate analysis to evaluate the efficacy of our proposed trials and compare with previously run CART cell trials at UPenn.

Public Health Relevance

CORE C: CORRELATIVE SCIENCES Vice President Biden, in his announcement of his Moonshot to Cure Cancer, recognizing that cancer is the leading cause of death worldwide, but also recognizing that we have made significant progress in the past four years, declared that we have a chance of curing cancer if we promote cutting-edge therapies. Each of the projects proposed herein represents a chance of achieving that goal, and, combined with cutting-edge correlative sciences, may not only drive the cure rate up, but also enhance our understanding of the difference between success and failure, which will inform and direct our strategies for manufacture of our gene therapy products. Our aim is a cure for all; we have come close to this lofty goal with our recently described pediatric ALL clinical trials, and the studies proposed here aspire to use technologically innovative strategies to also achieve this mark in other cancers.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
1P01CA214278-01
Application #
9280425
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2017-05-01
Budget End
2018-04-30
Support Year
1
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Type
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Fraietta, Joseph A; Nobles, Christopher L; Sammons, Morgan A et al. (2018) Disruption of TET2 promotes the therapeutic efficacy of CD19-targeted T cells. Nature 558:307-312
June, Carl H; O'Connor, Roddy S; Kawalekar, Omkar U et al. (2018) CAR T cell immunotherapy for human cancer. Science 359:1361-1365
Watanabe, Keisuke; Kuramitsu, Shunichiro; Posey Jr, Avery D et al. (2018) Expanding the Therapeutic Window for CAR T Cell Therapy in Solid Tumors: The Knowns and Unknowns of CAR T Cell Biology. Front Immunol 9:2486
Fraietta, Joseph A; Lacey, Simon F; Orlando, Elena J et al. (2018) Determinants of response and resistance to CD19 chimeric antigen receptor (CAR) T cell therapy of chronic lymphocytic leukemia. Nat Med 24:563-571
Williams, Austin D; Payne, Kyle K; Posey Jr, Avery D et al. (2017) Immunotherapy for Breast Cancer: Current and Future Strategies. Curr Surg Rep 5:
Cameron, Brian J; Gerry, Andrew B; Dukes, Joseph et al. (2013) Identification of a Titin-derived HLA-A1-presented peptide as a cross-reactive target for engineered MAGE A3-directed T cells. Sci Transl Med 5:197ra103