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PRECIOUS METALS,
DIAMONDS & GEMSTONES
INVESTMENT SUMMIT
                2.40 – 3.05
                Metals in Medicine - PGMs in anti-cancer treatments
                Prof Peter Sadler – Professor of Chemistry, University
                of Warwick




THE LONDON CHAMBER OF COMMERCE AND INDUSTRY   ● THURSDAY, 20 MAY 2010
www.ObjectiveCapitalConferences.com
Metals in Medicine -
PGMs in anticancer treatments


       Peter J. Sadler FRS
     Professor of Chemistry
      University of Warwick
A Periodic Table
                of Medicines                               He
                                          B
LiLiBe                                    B    C         Ne
                                                  NO        F
         Mg                               Al              Ar
            Ti     Cr   Fe                            S Cl
         Sc Ti    Cr            Cu       Ga Ge As2O Br Kr
                                        Al
                                                 N
 Na         V    Mn                 Zn       Si P
Rb Sr Y Zr Nb       Ru       Rh Pd Ag Cd In     Sb Te     Xe
  K                          Co        67Ga
      Ca
Cs Ba La Hf Ta W Re Os       Ir Pt Au Hg Tl Pb Bi     Se
         90Y Mo 99m
                                             Sn           Br
                                                      Sedoneural
      Sr           Tc              Ag             As      I
                   188Re

 Cs La Ce153 Nd Gd Sm Eu Gd Tb Dy Ho Er Sb Yb Lu
           Pr                            Tm
            Sm                 201Tl
     Ba
                     Pt    Au               Bi 133Xe
         La
Metals in Medicine-
PGMs in anticancer treatments


   • Excited-state Platinum

   • Organo-PGMs
   - Ruthenium
   - Iridium
   - Osmium
Prof Peter Sadler’s Group > 30 years experience
Track record of patents/commercial development

• Pt radiosensitization agents (M&B/Rhône Poulenc)

• Gold anticancer compounds
  (SmithKlineFrench - preclinical development)

• Photactivated Pt anticancer agents (Scottish Enterprise/
  Univ Dundee/MRC/EPSRC/ERC)

• Organometallic Ru anticancer (Ru: Edinburgh Technology
  Fund/MMI/Oncosense - preclinical development)

• Organometallic Os and Ir anticancer (HEIF/EPSRC)
Major Unmet Medical Need
• Cytotoxics (drugs that kill cells) market
  segment that includes platinum-based
  therapeutics excluding monoclonal antibodies
• US $6b (12.5%) of the cancer market in 2006
  – Breast, lung, colorectal and ovarian cancers
• 5-year survival rates
  – 40-60% for colorectal cancer
  – 35-38% ovarian cancer
• No one effective treatment for many cancers
Barnett Rosenberg
             1961 Professor of Biophysics
             Michigan State University




    +         -




Electric field lines      Mitotic spindle
for equal and opposite    formation
point charges             during division of
(electric dipole)         a eukaryotic cell
Effect of electric fields on cell growth

“Inert” Pt
electrodes



   Growth medium      E. coli   + cis- [PtCl2(NH3)2]
      (NH4Cl)                           cisplatin

Cisplatin
approved
by FDA
1978
 1844 Peyrone's chloride
Platinum treatment

Bob Champion MBE          Lance Armstrong




                         1996 diagnosed with
1979 diagnosed with      testicular cancer
testicular cancer        Won Tour de France
1981 won the             each year from
Grand National           1999 to 2005
Carboplatin           Picoplatin
                         Phase III
   FDA Approval          Colorectal Metastatic
   1989                  Cancer




Structure:               Structure:
S.Neidle, I.M. Ismail,   Y. Chen, Z. Guo,
P.J. Sadler              S. Parsons, P.J. Sadler
J. Inorg. Biochem.       Chem. Eur. J.
1980 13 , 205-212.       1998, 4, 672-676.
Clinically Approved Platinum
        Anticancer Compounds
            H3N
                                    Carboplatin
                       Cl
                  Pt                $673m 2004
            H3N        Cl

           Cisplatin
           $100m 1999
                               Oxaliplatin
                               $1.9b 2006
Drawbacks                      $3.4b 2012
• Acquired or inherent resistance
• Toxic side effects
Rh          Prices of
                                       2600         platinum
Platinum group metals
                                                  group metals
                                                             Pt
Global                 Oxaliplatin                          1610
$48,000M               $1,900M
(2006)                 (2006)
                    Carboplatin
                    $673M
                    (2004)                     Pd      Ir
                 Cisplatin                     483 Os 510
                 $100M
      Platinum   (1999)              Ru            380
      ca. 6%
                                     190

Cancer market Platinum sales               US Dollars per troy
                                           oz (31.1 g) [04/10]
Photochemotherapy


 Activation by light


  Directed therapy
  Destroys the cancer cells
  Less side-effects
Photochemotherapy



       Laser

                    Cancer
                      cell



 Drug Activation
Human Ovarian Cancer Cells
                                                   Dark
IC50         >288            >288
μM
                        N3
                             OH
                                  NH3         >244
200                          Pt                                 152
                   H3N            N3
                             OH
                                              OH
                                        H3N         N3

                                              Pt          H3N        Cl
100           OH                         N3                     Pt
       H3N         N3
                                                    N
                                              OH
                                                          H3N        Cl
             Pt

       H3N         N3
              OH
Human Ovarian Cancer Cells

IC50                                    Light Dark
             >288            >288
μM
                        N3
                             OH
                                  NH3          >244
200                          Pt                             152
      133
                   H3N
                             OH
                                  N3                     151
                                               OH
                                         H3N        N3
                         99
                                               Pt        H3N        Cl
100           OH                          N3                   Pt
       H3N         N3
                                                    N
                                               OH
                                                         H3N        Cl
             Pt

       H3N
              OH
                   N3
                                           2
Potent photoactivated
                                           platinum anticancer
                                                 compound



                                             100             Light                          Dark
                                Viable
                                Cells 50
                                (%)
                                                                            Cisplatin
                                               0
                                                     1            10            100 µM
Mackay, Woods, Heringová, Kaspárková, Pizarro, Moggach, Parsons, Brabec, Sadler PNAS 2007, 104, 20743-20748.
Human bladder cancer cells

       +100 µM Pt (dark)                            +100 µM Pt (light)

     50 µm                                          50 µm




            Rapid rounding, “ballooning” of cells in light
[Bednarski, Grünert, Zielzki, Wellner, Mackay, Sadler, Chemistry & Biology, 2006, 13, 61-67]
Human bladder cancer cells




  25 µM        50 µM       100 µM




DAPI Fluorescence: stains duplex DNA
  Cell shrinkage, loss of contact,
 nuclear packing and loss of nucleus
Organo-PGMs
       • Seat coated
         with carbon




• Reactive                 Cisplatin
  leg(s)               Different shape
Ru(II) Arene Anticancer Complexes

                   R
                                              η6-arene



                             Ru          Z
                    X
    Leaving                        Y
    Group(s)
Yan, Melchart, Habtemariam, Sadler Chem. Commun. 2005, 4764 – 4776
Dougan, Sadler Chimia , 2007, 61, 704-715
Ru(II) Arene Anticancer Complexes

                   R
                                              η6-arene

  Tether
                             Ru          Z
                    X                              Chelated
    Leaving                        Y               Ligand
    Group(s)
Yan, Melchart, Habtemariam, Sadler Chem. Commun. 2005, 4764 – 4776
Dougan, Sadler Chimia , 2007, 61, 704-715
Tuning the activity
of osmium compounds     IC50(µM)
                                50

                                40

                                 30
                         Inactive
                                 20

                                10



                      Human ovarian
                       cancer cells
Tuning the activity
of osmium compounds     IC50(µM)
                                  50

                                  40

                                  30
                         active
                                  20
                                       As active as
                                         Cisplatin
                                  10



                      Human ovarian
                       cancer cells
Tuning the activity
of osmium compounds     IC50(µM)
                                 50

                                 40


 I                               30
                        highly active
                                 20

                                     10x more
                                 10
                                    Active than
                                     Cisplatin
                      Human ovarian
                       cancer cells
Tuning the reactivity of osmium complexes
                                       Reaction   DNA                       Dose
                                        (hours) binding%                    (µM)
                                                   5                 100           50

                                                   4                 80            40

                                                   3                 60      30
                                                           Weak
                                          Slow                       Non-toxic
                                                          binding
                                                   2              40         20

                                                   1                 20            10



                                                                   Human ovarian
                                                                    cancer cells
 van Rijt, Peacock, Johnstone, Parsons, Sadler, Inorg. Chem., 2009, 48 , 1753-62
Tuning the reactivity of osmium complexes
                                       Reaction   DNA                       Dose
                                        (hours) binding%                    (µM)
                                                    5                100             50

                                                    4                80              40

                                                    3                60              30
                                                          Strong
                                          Fast                              Active
                                                          binding
                                                    2                40              20

                                                    1                20              10


                                                                   Human ovarian
                                                                    cancer cells
 van Rijt, Peacock, Johnstone, Parsons, Sadler, Inorg. Chem., 2009, 48 , 1753-62
Anticancer Organo-PGMs




Novel DNA interactions
Organo-osmium in
        ovarian cancer cell




New target sites: new mechanism of action
Opportunities
• Activity in human cancer cell lines
  comparable to or better than cisplatin
• Different mechanism of action :
  activity against cisplatin-resistant cells
• Potentially less severe side-effects
• Easy synthesis, high yields and lower cost
• Potential for combination therapy
Next Steps
                • Structure-activity relationships
   University

                • Mechanism of cancer cell cytotoxicity including cell
                  uptake
                • Activity of lead compounds in well-established in vivo
                  cancer models
Collaboration
 Grants for




                • Establish a panel of 6 lead compounds for
                  preclinical development
                • Use hepatocyte assays as indicators of low toxicity
                  to refine panel of compounds
                • Initial clinical trials.
   License




                • Out license lead with initial preclinical & clinical data
                • License is a further Collaboration
Historic License Deals
• University deal values are often not disclosed
• May 2009 - Sanofi-Aventis will pay Exelixis up front
  fees of $141m for license rights to several cancer
  drugs
  – XL147 and XL765, both of which are in phase I trials
  – discovery of inhibitors of phosphoinositide-3 kinase for
    the treatment of cancer
• May 2009 - Celgene will pay GlobeImmune $40m
  up front for an exclusive option
  – GlobeImmune's oncology programs, including GI-4000,
    currently in Phase II trials for pancreatic cancer
Advances in PGM Anticancer Agents


     • Excited-state
       Platinum
                                                     • Organo-PGMs
                                                       Ruthenium
                                                       Osmium
                                                       Iridium



                      Opportunities for
                     • Licensing patents
         • Collaboration in pre-clinical development
Contacts:
• Professor Peter Sadler, University of Warwick
• Dr Shum Prakash, Business Development Manager
  Warwick Ventures, University House, Kirby Corner Road, Coventry CV4 8UW
  Tel: 024 7657 4145 E-mail: s.prakash@warwick.ac.uk
Acknowledgements




• University of Warwick   • ICT Biosciences, Bradford
• University of Dundee/   • Czech Academy of Science
  Ninewells Hospital      • Greifswald University
• Warwick Ventures

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Objective Capital Precious Metals, Diamonds and Gemstones Investment Summit: Metals in Medicine - PGMs in anti-cancer treatments - Peter Sadler

  • 1. PRECIOUS METALS, DIAMONDS & GEMSTONES INVESTMENT SUMMIT 2.40 – 3.05 Metals in Medicine - PGMs in anti-cancer treatments Prof Peter Sadler – Professor of Chemistry, University of Warwick THE LONDON CHAMBER OF COMMERCE AND INDUSTRY ● THURSDAY, 20 MAY 2010 www.ObjectiveCapitalConferences.com
  • 2. Metals in Medicine - PGMs in anticancer treatments Peter J. Sadler FRS Professor of Chemistry University of Warwick
  • 3. A Periodic Table of Medicines He B LiLiBe B C Ne NO F Mg Al Ar Ti Cr Fe S Cl Sc Ti Cr Cu Ga Ge As2O Br Kr Al N Na V Mn Zn Si P Rb Sr Y Zr Nb Ru Rh Pd Ag Cd In Sb Te Xe K Co 67Ga Ca Cs Ba La Hf Ta W Re Os Ir Pt Au Hg Tl Pb Bi Se 90Y Mo 99m Sn Br Sedoneural Sr Tc Ag As I 188Re Cs La Ce153 Nd Gd Sm Eu Gd Tb Dy Ho Er Sb Yb Lu Pr Tm Sm 201Tl Ba Pt Au Bi 133Xe La
  • 4. Metals in Medicine- PGMs in anticancer treatments • Excited-state Platinum • Organo-PGMs - Ruthenium - Iridium - Osmium
  • 5. Prof Peter Sadler’s Group > 30 years experience Track record of patents/commercial development • Pt radiosensitization agents (M&B/Rhône Poulenc) • Gold anticancer compounds (SmithKlineFrench - preclinical development) • Photactivated Pt anticancer agents (Scottish Enterprise/ Univ Dundee/MRC/EPSRC/ERC) • Organometallic Ru anticancer (Ru: Edinburgh Technology Fund/MMI/Oncosense - preclinical development) • Organometallic Os and Ir anticancer (HEIF/EPSRC)
  • 6. Major Unmet Medical Need • Cytotoxics (drugs that kill cells) market segment that includes platinum-based therapeutics excluding monoclonal antibodies • US $6b (12.5%) of the cancer market in 2006 – Breast, lung, colorectal and ovarian cancers • 5-year survival rates – 40-60% for colorectal cancer – 35-38% ovarian cancer • No one effective treatment for many cancers
  • 7. Barnett Rosenberg 1961 Professor of Biophysics Michigan State University + - Electric field lines Mitotic spindle for equal and opposite formation point charges during division of (electric dipole) a eukaryotic cell
  • 8. Effect of electric fields on cell growth “Inert” Pt electrodes Growth medium E. coli + cis- [PtCl2(NH3)2] (NH4Cl) cisplatin Cisplatin approved by FDA 1978 1844 Peyrone's chloride
  • 9. Platinum treatment Bob Champion MBE Lance Armstrong 1996 diagnosed with 1979 diagnosed with testicular cancer testicular cancer Won Tour de France 1981 won the each year from Grand National 1999 to 2005
  • 10. Carboplatin Picoplatin Phase III FDA Approval Colorectal Metastatic 1989 Cancer Structure: Structure: S.Neidle, I.M. Ismail, Y. Chen, Z. Guo, P.J. Sadler S. Parsons, P.J. Sadler J. Inorg. Biochem. Chem. Eur. J. 1980 13 , 205-212. 1998, 4, 672-676.
  • 11. Clinically Approved Platinum Anticancer Compounds H3N Carboplatin Cl Pt $673m 2004 H3N Cl Cisplatin $100m 1999 Oxaliplatin $1.9b 2006 Drawbacks $3.4b 2012 • Acquired or inherent resistance • Toxic side effects
  • 12. Rh Prices of 2600 platinum Platinum group metals group metals Pt Global Oxaliplatin 1610 $48,000M $1,900M (2006) (2006) Carboplatin $673M (2004) Pd Ir Cisplatin 483 Os 510 $100M Platinum (1999) Ru 380 ca. 6% 190 Cancer market Platinum sales US Dollars per troy oz (31.1 g) [04/10]
  • 13. Photochemotherapy Activation by light Directed therapy Destroys the cancer cells Less side-effects
  • 14. Photochemotherapy Laser Cancer cell Drug Activation
  • 15. Human Ovarian Cancer Cells Dark IC50 >288 >288 μM N3 OH NH3 >244 200 Pt 152 H3N N3 OH OH H3N N3 Pt H3N Cl 100 OH N3 Pt H3N N3 N OH H3N Cl Pt H3N N3 OH
  • 16. Human Ovarian Cancer Cells IC50 Light Dark >288 >288 μM N3 OH NH3 >244 200 Pt 152 133 H3N OH N3 151 OH H3N N3 99 Pt H3N Cl 100 OH N3 Pt H3N N3 N OH H3N Cl Pt H3N OH N3 2
  • 17. Potent photoactivated platinum anticancer compound 100 Light Dark Viable Cells 50 (%) Cisplatin 0 1 10 100 µM Mackay, Woods, Heringová, Kaspárková, Pizarro, Moggach, Parsons, Brabec, Sadler PNAS 2007, 104, 20743-20748.
  • 18. Human bladder cancer cells +100 µM Pt (dark) +100 µM Pt (light) 50 µm 50 µm Rapid rounding, “ballooning” of cells in light [Bednarski, Grünert, Zielzki, Wellner, Mackay, Sadler, Chemistry & Biology, 2006, 13, 61-67]
  • 19. Human bladder cancer cells 25 µM 50 µM 100 µM DAPI Fluorescence: stains duplex DNA Cell shrinkage, loss of contact, nuclear packing and loss of nucleus
  • 20. Organo-PGMs • Seat coated with carbon • Reactive Cisplatin leg(s) Different shape
  • 21. Ru(II) Arene Anticancer Complexes R η6-arene Ru Z X Leaving Y Group(s) Yan, Melchart, Habtemariam, Sadler Chem. Commun. 2005, 4764 – 4776 Dougan, Sadler Chimia , 2007, 61, 704-715
  • 22. Ru(II) Arene Anticancer Complexes R η6-arene Tether Ru Z X Chelated Leaving Y Ligand Group(s) Yan, Melchart, Habtemariam, Sadler Chem. Commun. 2005, 4764 – 4776 Dougan, Sadler Chimia , 2007, 61, 704-715
  • 23. Tuning the activity of osmium compounds IC50(µM) 50 40 30 Inactive 20 10 Human ovarian cancer cells
  • 24. Tuning the activity of osmium compounds IC50(µM) 50 40 30 active 20 As active as Cisplatin 10 Human ovarian cancer cells
  • 25. Tuning the activity of osmium compounds IC50(µM) 50 40 I 30 highly active 20 10x more 10 Active than Cisplatin Human ovarian cancer cells
  • 26. Tuning the reactivity of osmium complexes Reaction DNA Dose (hours) binding% (µM) 5 100 50 4 80 40 3 60 30 Weak Slow Non-toxic binding 2 40 20 1 20 10 Human ovarian cancer cells van Rijt, Peacock, Johnstone, Parsons, Sadler, Inorg. Chem., 2009, 48 , 1753-62
  • 27. Tuning the reactivity of osmium complexes Reaction DNA Dose (hours) binding% (µM) 5 100 50 4 80 40 3 60 30 Strong Fast Active binding 2 40 20 1 20 10 Human ovarian cancer cells van Rijt, Peacock, Johnstone, Parsons, Sadler, Inorg. Chem., 2009, 48 , 1753-62
  • 29. Organo-osmium in ovarian cancer cell New target sites: new mechanism of action
  • 30. Opportunities • Activity in human cancer cell lines comparable to or better than cisplatin • Different mechanism of action : activity against cisplatin-resistant cells • Potentially less severe side-effects • Easy synthesis, high yields and lower cost • Potential for combination therapy
  • 31. Next Steps • Structure-activity relationships University • Mechanism of cancer cell cytotoxicity including cell uptake • Activity of lead compounds in well-established in vivo cancer models Collaboration Grants for • Establish a panel of 6 lead compounds for preclinical development • Use hepatocyte assays as indicators of low toxicity to refine panel of compounds • Initial clinical trials. License • Out license lead with initial preclinical & clinical data • License is a further Collaboration
  • 32. Historic License Deals • University deal values are often not disclosed • May 2009 - Sanofi-Aventis will pay Exelixis up front fees of $141m for license rights to several cancer drugs – XL147 and XL765, both of which are in phase I trials – discovery of inhibitors of phosphoinositide-3 kinase for the treatment of cancer • May 2009 - Celgene will pay GlobeImmune $40m up front for an exclusive option – GlobeImmune's oncology programs, including GI-4000, currently in Phase II trials for pancreatic cancer
  • 33. Advances in PGM Anticancer Agents • Excited-state Platinum • Organo-PGMs Ruthenium Osmium Iridium Opportunities for • Licensing patents • Collaboration in pre-clinical development Contacts: • Professor Peter Sadler, University of Warwick • Dr Shum Prakash, Business Development Manager Warwick Ventures, University House, Kirby Corner Road, Coventry CV4 8UW Tel: 024 7657 4145 E-mail: s.prakash@warwick.ac.uk
  • 34. Acknowledgements • University of Warwick • ICT Biosciences, Bradford • University of Dundee/ • Czech Academy of Science Ninewells Hospital • Greifswald University • Warwick Ventures