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Developmental Therapeutics Research Program

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Regulation of gene expression and mechanisms of cellular drug resistance ... Expand collaborations with Signal Transduction Program and other YCC Research Programs ... – PowerPoint PPT presentation

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Title: Developmental Therapeutics Research Program


1
Developmental Therapeutics Research
Program Co-Program Leaders Yung-chi Cheng,
Ph.D. Edward Chu, M.D.
2
Mission/Scientific Goals
  • Identify and characterize novel biological and/or
    molecular targets
  • Develop novel agents and/or treatment regimens
    for clinical application


3
Leadership
  • Leaders since 1996
  • Expertise in cancer therapeutics with
    complementary interests in basic, translational,
    and clinical research
  • Yung-chi Cheng, Ph.D. (Professor of Pharmacology)
  • Antiviral and anticancer chemotherapy
  • Pre-clinical design and development of novel
    agents and treatment regimens
  • Chinese herbal medicine
  • Edward Chu, M.D. (Professor of Medicine and
    Pharmacology)
  • Fluoropyrimidine biochemistry
  • Regulation of gene expression and mechanisms
    of cellular drug resistance
  • Clinical development of novel drugs and drug
    regimens (colorectal cancer and solid tumors)


4
Membership
  • 36 faculty
  • 13 departments and 2 schools
  • Recruitment new basic scientists (4)
  • Hamilton (Chemistry)
  • Saltzman (Biomedical Engineering)
  • Ha (Pharmacology)
  • Hodson (Laboratory Medicine)
  • Recruitment new clinical investigators (12)
  • Sznol, Foss, Kelly, Harris, Saif, Rose,
    Deshpande, Lee, Gettinger, Abu-Khalaf, Cha,
    Baehring
  • Nucleus of Phase I, clinical investigations
    team


5
Cancer-Related Funding
1
2
.
0
10.3
1
0
.
0
Dollars in Millions
8
.
0
Total Funding
6
.
0
NCI Funding
.
3.8
3.3
4
.
0
1.7
2
.
0
0
.
0
1997
2006
6
Contribution of Program Members to Non-RO1 Grants
  • P50 SPORE in Skin Cancer (M. Sznol, Co-P.I.)
  • NCI RAID grant for the GGT inhibitor GGTI-2418
  • (A. Hamilton, P.I.)
  • NCI RAID grant for GFB-204 (A. Hamilton, P.I.)
  • NCI Training Program in Cancer Pharmacology (Y.
    Cheng, P.I.)
  • NCI/OCCAM grant for the development of Chinese
    herbal medicine in cancer therapy
  • (Y. Cheng, E. Chu, W. Saif, J. Lee, M. Sznol,
    P.I.)
  • NCCN grant for novel clinical study of Chinese
    herbal medicine plus chemotherapy in pancreatic
    cancer
  • (W. Saif, P.I.)


7
Scientific Accomplishments Molecules
Discovered/Developed
  • 25 molecules discovered/developed by DT members
  • 18 licensed to pharma
  • 9 undergoing pre-clinical testing
  • 6 anticancer agents in clinical testing - phase
    I, II, and III
  • 3 antiviral agents in clinical testing - phase
    II, III , and market

8
Molecules Discovered/Developed
  • Clevudine (L-FMAU) - L-nucleoside
  • Troxacitabine - L-nucleoside
  • IPdR - thymidine analog
  • 4-ED4T HIV RT inhibitor
  • Small Organic Molecules
  • Benzylacyclouridine nucleoside analog
  • DB3505 tyloindocine analog
  • Cloretazine - alkylating agent
  • KS119 - alkylating agent
  • Triapine - ribonucleotide reductase inhibitor
  • Phenoxodiol isoflavenoid
  • Natural Products
  • Epoxomicin - proteasome inhibitor
  • NF-?B inhibitor more potent than bortezomib
  • Eriocalyxin B diterpenoid
  • Nucleic Acids
  • TS siRNA
  • HIF-1? siRNA
  • VEGF siRNA
  • Peptides/Peptidomimetics
  • Cavtratin - inhibits eNOS and VEGF signaling
  • ISS610 - inhibits Stat3 dimerization
  • GGTI-2418 - GGT inhibitor
  • GFB-204 - calixarene derivative that blocks VEGF
    and PDGF signaling
  • Chinese herbal medicine
  • PHY-906
  • Biologic Agents
  • FVII/Fc icon - targets tissue factor
  • TAPET

9
Scientific Accomplishments Molecules
Discovered/Developed
  • Phenoxodiol (G. Mor) - isoflavonoid
  • Inhibits XIAP activity
  • Restores chemosensitivity to taxanes and
    cisplatin
  • Novel analogs NV-143 and NV-196 being developed
  • GFB-204 (A. Hamilton) - calixarene derivative
  • Binds to protein surfaces
  • Binds with high affinity to VEGF and PDGF and
    inhibits their downstream signaling
  • Epoxomicin (C. Crews) - epoxyketone peptide
  • Inhibits 20S proteasome
  • Prevents IkB degradation resulting in NF-kB
    inhibition
  • More potent than bortezomib

10
Phase I Clinical Trials
1998-2004 18 phase I studies 2005-2006 15
phase I studies Focus on YCC-based
discoveries/science

11
DT - Phase I AccrualsImpact of 2005 Recruitments
120
100
80
Subject Enrollment
60
40
20
0
2005
2006 (Annualized)
Calendar Year
12
Value Added of YCC to ProgramIntra- and
Inter-Programmatic Initiatives
  • Targeted Areas of Research Excellence (TARE)
    projects
  • DT members involved in 6 of 8 TARE
  • Development of novel multitargeted molecules for
    cancer therapy
  • Y. Cheng, E. Chu, A. Hamilton, J. Schlessinger,
  • M. Saltzman
  • Nanoparticles for cancer diagnosis and therapy
  • M. Saltzman, J. Piepmeier, J. Costa, I. Mellman
  • HPV Vaccination - Molecular Virology
  • Breast Cancer - Signal Transduction
  • Lymphoma - Immunobiology Immunotherapy
  • DNA Repair - Radiation Biology Radiotherapy


13
Value Added Program to Members
  • Facilitate collaborations/interactions
  • Intra-programmatic
  • Inter-programmatic
  • Basic scientists and clinical investigators
  • Facilitate collaborations/interactions with
    academic centers and industry
  • Facilitate collaborations/interactions with NCI
  • Cancer Treatment Evaluation Program (CTEP)
  • Office of Complementary and Alternative
    Medicine (OCCAM)
  • Developmental Therapeutics Program (DTP)


14
Interaction with YCC Research Programs
Radiobiology Radiotherapy
Developmental Therapeutics
15
Value Added Shared Resources
Genetic Counseling
Clinical Research Services
Developmental Therapeutics
Biostatistics
16
Future Plans
  • Develop new strategies for drug design,
    discovery, and formulation
  • Expand collaborations with Signal Transduction
    Program and other YCC Research Programs
  • Translate DT / YCC discoveries/science into
    clinical trials (e.g. Epoxomicin, GFB204,
    GGTI-2418)
  • Design novel pilot clinical trials with
    biomarkers of response
  • Enhance collaborative efforts with
    Clinical/Translational Research Programs
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