Abstract

More widespread reports of complete tumor responses to cell therapies are paralleled by increasing clinical, scientific and public interest in, therapies that can produce antitumor effects without the devastating consequences of standard chemo-radiotherapies. However, much remains to be achieved before these eariy phase therapies become a standard of clinical practice. During our prior SPORE funding , we demonstrated, that EBV antigen-specific T cells produced over 60% complete remission rate without toxicity, in 21 patients with relapsed EBV-positive lymphoma. Our complex T cell generation process was, however, identified as a critical regulatory barrier to the progress of this study to pivotal clinical studies and a biologies licensing application (BLA). The manufacturing process required live virus (EBV) and (adeno)viral vectors, as well as B cells for the generation of autologous antigen-presenting cells (APCs) - a severe limitation now that most patients receive the B cell depleting antibody rituxan upon diagnosis. We therefore developed a strategy for the production of EBV-specific T cells that does not require live virus or viral vectors and reduces both complexity and the manufacturing time (from >3 riionths to <4 weeks);increases the number of viral tumor antigens recognized from 2 to 4;and is effective for any patient regardless of HLA type or prior treatment with rituxan. In the current application, we plan a phase 1 trial to validate the biological and clinical equivalency of T cells made with the new manufacturing strategies, which will enable us to proceed to a pivotal trial (outside the scope of the SPORE) and then a BLA. In the second part of our proposal, we plan to further improve upon our 60% CR rate in relapsed disease, by combining ithe tumor-directed T cells with small molecule histone deacetylase inhibitors (HDAC-ls). These drugs have both direct anti-lymphoma activity and multiple proimmune effects that should increase the efficacy of tumor-specific T cells. Since HDAC-ls can also inhibit T cells, we will use mouse lymphoma models to evaluate how HDAC-ls and adoptive T cell transfer can best be used in combination, by identifying the mechanisms of tumor immuneresistance that can be effectively altered by HDAC-I to augment T cell persistence, proliferation and antitumor activity.

Public Health Relevance

There is increasing excitement over the use of cellular immunotherapies in the treatment of cancer, but many of the current approaches are overiy complex or pose excessive risks for the patient. The modifications proposed in the application are designed to bring virus-specific T cell therapy for lymphoma to the bedside, in a manner that is straightfonward, reproducible and cost effective.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
2P50CA126752-06
Application #
8339659
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2012-09-01
Budget End
2013-08-31
Support Year
6
Fiscal Year
2012
Total Cost
$228,471
Indirect Cost
$72,324

  Institution

Name
Baylor College of Medicine
Department
Type
DUNS #
051113330
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Morita, Daisuke; Nishio, Nobuhiro; Saito, Shoji et al. (2018) Enhanced Expression of Anti-CD19 Chimeric Antigen Receptor in piggyBac Transposon-Engineered T Cells. Mol Ther Methods Clin Dev 8:131-140
Bollard, Catherine M; Tripic, Tamara; Cruz, Conrad Russell et al. (2018) Tumor-Specific T-Cells Engineered to Overcome Tumor Immune Evasion Induce Clinical Responses in Patients With Relapsed Hodgkin Lymphoma. J Clin Oncol 36:1128-1139
Lyon, Deborah; Lapteva, Natasha; Gee, Adrian P (2018) Absence of Replication-Competent Retrovirus in Vectors, T Cell Products, and Patient Follow-Up Samples. Mol Ther 26:6-7
Su, Jianzhong; Huang, Yung-Hsin; Cui, Xiaodong et al. (2018) Homeobox oncogene activation by pan-cancer DNA hypermethylation. Genome Biol 19:108
Nabekura, Tsukasa; Chen, Zhiying; Schroeder, Casey et al. (2018) Crk Adaptor Proteins Regulate NK Cell Expansion and Differentiation during Mouse Cytomegalovirus Infection. J Immunol 200:3420-3428
Shum, Thomas; Kruse, Robert L; Rooney, Cliona M (2018) Strategies for enhancing adoptive T-cell immunotherapy against solid tumors using engineered cytokine signaling and other modalities. Expert Opin Biol Ther 18:653-664
Bajgain, Pradip; Tawinwung, Supannikar; D'Elia, Lindsey et al. (2018) CAR T cell therapy for breast cancer: harnessing the tumor milieu to drive T cell activation. J Immunother Cancer 6:34
McLaughlin, Lauren P; Rouce, Rayne; Gottschalk, Stephen et al. (2018) EBV/LMP-specific T cells maintain remissions of T- and B-cell EBV lymphomas after allogeneic bone marrow transplantation. Blood 132:2351-2361
McClain, Kenneth L; Picarsic, Jennifer; Chakraborty, Rikhia et al. (2018) CNS Langerhans cell histiocytosis: Common hematopoietic origin for LCH-associated neurodegeneration and mass lesions. Cancer 124:2607-2620
Gomes-Silva, Diogo; Ramos, Carlos A (2018) Cancer Immunotherapy Using CAR-T Cells: From the Research Bench to the Assembly Line. Biotechnol J 13:

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