Chimeric Antigen Receptor T Cell Therapy · Central vs effector vs stem memory T cells ! Activated...

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Chimeric Antigen Receptor T Cell Therapy Yi Lin, MD, PhD Mayo Clinic, Rochester, MN Alliance Spring Group Meeting - May 13, 2016

Transcript of Chimeric Antigen Receptor T Cell Therapy · Central vs effector vs stem memory T cells ! Activated...

Page 1: Chimeric Antigen Receptor T Cell Therapy · Central vs effector vs stem memory T cells ! Activated vs exhausted state ! ... Hanren Dai et al. JNCI J Natl Cancer Inst 2016;108:djv439

Chimeric Antigen Receptor T Cell Therapy

Yi Lin, MD, PhD Mayo Clinic, Rochester, MN

Alliance Spring Group Meeting - May 13, 2016

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Presentation Objectives l  Scientific overview of chimeric antigen receptor

(CAR) T cell therapy l  CART Mechanism of action l  Overview of CART clinical trials l  CART patient eligibility considerations

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scFv: recognize tumor

surface proteins

Costimulatory Signal 2: CD28 or 4-1BB or OX40

Essential Signal 1:

CD3ζ

APC

CD28  

CD28L pMHC

TCR

CD3ζ

T Cell Receptor Chimeric Antigen Receptor CAR T cells are genetically altered to express CAR on the cell surface.

CAR Design: Critical Elements of T Cell Activation and Function in a Single Molecule

T Cell

Activation Independent of MHC Limited to cell surface proteins

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Kochenderfer, J. N. & Rosenberg, S. A. (2013) Treating B‑cell cancer with T cells expressing anti-CD19 chimeric antigen receptors. Nat. Rev. Clin. Oncol. doi:10.1038/nrclinonc.2013.46

Schema of CAR T manufacturing and administration

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Milone MC, et al. Mol Ther. 2009 Porter DL et al. NEJM 2011

Kalos M, et al. Sci Transl Med. 2011 Maude et al. NEJM 2014.!

Lentiviral vector

T cell

CD19

Native TCR

Tumor cell

CTL019 cell

Dead tumor cell

Anti-CD19 CAR construct

Chimeric Antigen Receptor T cells (CARTs)

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Kenderian et al. Cancer Research 2014

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First Successful Report of CART19 in CLL (UPenn Trial)

Kalos et al, Sci Transl Med 2011 Porter et al, NEJM 2011

Results from this report ü  3 patients R/R CLL

ü  2 à sustained CR, 1 àPR ü  Eradicated bulky disease

ü  T cells persisted ü  Memory phenotype

ü  Potent (1 cell killed 1000 tumor cells)

ü  Cytokine release syndrome ü  Tumor lysis syndrome

UPenn Construct (CTL019)

41BB

LV Vector

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Grupp et al, ASH Abstract #380 Maude et al, NEJM 2014

High Response Rates in ALL

Page 9: Chimeric Antigen Receptor T Cell Therapy · Central vs effector vs stem memory T cells ! Activated vs exhausted state ! ... Hanren Dai et al. JNCI J Natl Cancer Inst 2016;108:djv439

High Response Rates in ALL

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Cancer Immunotherapy Breakthrough of the Year 2013

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l  CAR construct

l  CAR delivery system

l  CART phenotype and function

l  CART persistence

Critical Components of CART as a Drug

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CAR Construct: What generation is your CAR?

Pioneered by Eshhar et al 1989

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CAR Construct: CD28 vs 41BB

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CAR Construct: Antigen Selection

•  CD19 expression is generally restricted to B cells and B cell precursors1

•  CD19 is not expressed on hematopoietic stem cells or other tissue

•  CD19 is expressed by most B-cell malignancies

•  CLL, B-ALL, DLBCL, FL, MCL

Image adapted from Janeway CA, Travers P, Walport M, et al. Immunobiology. 5th ed. New York, NY: Garland Science; 2001:221-293; Scheuermann RH, et al. Leuk Lymphoma. 1995;18:385-397; and Feldman M, Marini JC. Cell cooperation in the antibody response. In: Roitt I, Brostoff J, Male D, eds. Immunology. 6th ed. Maryland Heights, Missouri: Mosby;2001:131-146.

Pro-B Pre-B Activated B cell

Hematopoietic stem cell

Memory B cell

(IgG, IgA)

Plasma cell

(IgG)

Immature (IgM)

Mature (IgM, IgD)

CD19 expression

B cell lymphomas and leukemias preB-ALL

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l  On target, off-tumor toxicity l  High binding affinity results in recognition of low

antigen expression in normal tissue l  Ex. Liver injury with anti-carbonic anhydrase IX

CART l  Ex. Pulmonary toxicity with anti-Her2 CART l  Can be fatal

CAR Construct: Antigen Selection

Morgan RA et al. Mol Ther 2010; 18(4):843-851. Lamers CH. JCO 2006;24(13):e20-e22.

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CAR Construct: Delivery System

Viral System l  Lentivirus, retrovirus l  Most commonly used in

trials to date l  Permanent genetic

modification l  Costly

Non-Viral System l  Transposon/Transposase

l  Permanent genetic modification

l  Less expensive for manufacturing

l  RNA transfection l  Temporary genetic

expression l  Strategy for limiting toxicity

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l  Optimize T cell population l  CD4 to CD8 proportion l  Central vs effector vs stem memory T cells

l  Activated vs exhausted state l  Duration of culture l  Cytokines

CAR T Phenotype & Function

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CAR T Persistence in vivo: Clinical Relevance

Grupp et al, ASH Abstract #380 Maude et al, NEJM 2014

CD19 positive relapses (4/30 patients, 13.3%) Poor expansion - CTL019 cells are lost

CD19 negative relapses (3/30 patients, 10%) Good expansion and persistence of CTL019

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CAR T Persistence in vivo: Conditioning Chemotherapy

Cameron J Turtle et al. Blood 2015;126:184

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Challice L Bonifant, published online 20 April 2016. doi:10.1038/mto.2016.11

CAR T Toxicities

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Challice L Bonifant, published online 20 April 2016. doi:10.1038/mto.2016.11

Strategies to Manage CAR Toxicities

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ONGOING CLINICAL TRIALS

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CART Programs at Academic Centers

Kenderian et al. BBMT in press.

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Hanren Dai et al. JNCI J Natl Cancer Inst 2016;108:djv439

CART Research Directions

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The CAR T Cell Race. The Scientist April 2015.

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CART Clinical Trials

Clinicaltrials.gov

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Hematologic Malignancies l  Lymphomas, ALL (n=34) l  Myeloma (n=3) l  AML (n=2)

Solid tumors (n=10) l  Types

l  GBM l  Neuroblastoma l  Pancreas cancer l  Sarcoma l  NSCLC l  Triple negative breast

cancer

l  Antigens l  EGFRvIII, PSCA, GD2,

Her2, ROR1, CD171

CART Clinical Trials

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l  Adequate blood cell count for leukapheresis l  Relative disease stability

l  CART manufacturing generally 2 – 4 weeks l  Disease not progressing rapidly through

manufacturing period l  Patient ability to tolerate CAR T toxicities

l  Good major organ functions l  heart, lung, kidney, liver

l  Neurologic considerations l  Seizure risk, CVA, CNS disease

Patient Eligibility Considerations

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Conclusion l  Questions from Audience l  Answers from Presenter