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“RUTHENIUM ROLES IN BIOLOGY, CHEMISTRY
AND MEDICINE AS ANTICANCER COMPOUNDS”




               FATEMEH BABAEI
         CITY UNIVERSITY OF HONG KONG
                 NOVEMBER 2011
What does the
          ?
 word cancer
mean to you?
While cancer can affect people of all ages, and a few types of cancer are more
common in children, the risk of developing cancer generally increases with
age. In 2007, cancer caused about 13% of all human deaths worldwide
(7.9 million). Rates are rising as more people live to an old age and as mass
lifestyle changes occur in the developing world.
Ruthenium has found its way into the clinic :

 Radiophysical properties of Ru can be applied to radiodiagnostic
 imaging
 Immunosuppressants
 Antimicrobials (against malaria and Chaga s disease)
 Antibiotics (against Salmonella typhi and Enterobacteria faecalis
 Nitrosyl delivery/scavenger tools
 Vasodilator/vasoconstrictor agents


                             Ruthenium compounds are known to be less toxic and
                            no cross resistant than platinum counterpart.
 Cancer chemotherapy
                            Ruthenium has a range of oxidation state (II,III and IV)
                            accessible under physiological Condition, which is unique
                            among the platinum-group metals.
Cancer cells




Cancer cells need considerably more energy than healthy cells. Their metabolism runs at full
           speed and requires large amounts of micronutrients, particularly iron.


                                       Ruthenium


   Ruthenium have the ability to bind albumin and transferrin And because cancer cells
   need more Iron, transferrin receptors are over expressed, Thereby allowing ruthenium-
   based drugs to be more efficiently delivered to cancer cells.
The oxidation state changes of ruthenium (II/III) in cancer and healthy cells




                     “activation by reduction” mechanism
Classification of ruthenium complexes with anticancer properties



 Ammine-chlorido derivatives
 The cytotoxicity tests had disappointing results
 Poor water solubility

 Dimethylsulfoxide complexes
  Water soluble
  Anti metastatic activity
  No cross resistant

 Ruthenium polyaminocarboxylate complexes
   Similar to biological molecules,
   Low systematic toxicity,
   Binding to DNA and alter the normal conformation
   and inducing the DNA cleavage

 Organoruthenium complexes
Typical structure of ruthenium complexes

Typically, the Organomtallic anticancer complexes
have a half-sandwich “piano-stool” [(g6-arene)
Ru(X)(Y)(Z)] structure.
As shown in the figure, the complexes consist of
three main building blocks, the arene forms the seat
of piano stool and the ligands resemble the legs.
Linking the ligands Y and Z to form a bidentate
chelating ligand (L) seems to be advantageous for
anticancer activity.                                 IC50 values of Ru(II) arene complexes, carboplatin
                                                       and cisplatin in A2780 human ovarian cancer cells
                                                       after 24 h drug exposure.

 Cytotoxic activity

Activity appears to increase with the size of the
coordinated arene: benzene < p-cymene < bi-
phenyle        <       dihydroantracene           <
tetrahydroantracene, in this cell line, the arene =
biphenyle complex has similar cytotoxicity to
the anticancer drug carboplatin.
How these drugs work: mechanisms of action

                                         Cancer therapy



 Classical way: ruthenium coordinatively
 bind to DNA double helix via nitrogen atoms           New method : “targeted therapy”




The reactivity of the various binding sites of         Targeting cellular signaling pathway
nucleobases towards Ru (II) at neutral pH              Highly effective and specific
decreases in the order G (N7) > T (N3) >               Side effects are less sever &controllable
C(N3) > A(N7), A(N1).                                 cytotoxicity




                                                 The factors that up-regulated in cancer cells are:
The preferable binding is with guanine           epidermal growth factor receptor
over adenine, same as cisplatin.                 (EGFR), vascular endothelial growth factor
                                                 (VEGF), cyclin-dependent kinases (CDK).
Interactions within guanine (G) and adenine (A) adducts of arene Ru-en
                         anticancer complexes




 when the size of Arene increased, it seems that the hydrophobic arene- purine base
 π-π stacking interactions will be increased.
Ruthenium complexes with anticancer properties


 NAMI-A binds strongly to serum proteins, including the iron transporter transferrin
and it induces cell arrest in the premitotic G (2)-M phase.

 KP1019 drug induce cell death and have a significant cytotoxicity in vitro against
colorectal cell lines SW480 and HT29. This drug was also found to be highly
effective in in vivo tests and it induces apoptosis in colorectal cell lines mainly via the
intrinsic mitochondria apoptosis pathway.




              Clinically evaluated ruthenium-based anticancer drugs
Strategy to tether Organometallic ruthenium arene anticancer compounds to recombinant
                                 Human Serum Albumin




  The main role of Human serum
 albumin (HSA) is to maintain the osmotic
 pressure in the blood and to scavenge free
 radicals as an antioxidant.

  HSA is known to accumulate in tumors.

  The carrier conjugate of various
 organic anticancer drugs such as
 chlorambucil, doxorubicin, and paclitaxel.



 RAPTA: 1,3,5-triaza-7-phosphatricyclo[3.3.1.1]-
 decane ligand
Strategy to tether Organometallic ruthenium arene anticancer compounds to
                    recombinant Human Serum Albumin




       RAPTA-C, theprototype compound with a p-cymene ring



According to these results Organometallic ruthenium (II)-arene anticancer
compound to rHSA could collected in tumor cells, and rHAS could be taken
 as a carrier biomolecules for drug delivery of RAPTA complexes in vivo, but
 in these area of targeted drug delivery more researches are needed.
Reactions with other amino acids and proteins
 Researchers showed (η6-benzene) Ru (DMSO) Cl2 strongly inhibit topoisomerase II activity
by cleavage complex formation. They suggest that the ruthenium complex interacts with DNA
and forms cross links with topoisomerase II. The complex exhibited antiproliferative activity in
vitro.

 Prof. Sadler and his colleagues found that the reaction of [(η6 -Bip) Ru(en)Cl][PF6] complex
with thiol containing amino acids L-cysteine is slow in aqueous solution, and they showed that
thiols couldn’t directly inactive Ru (II)-en arene complexes in blood plasma or in the cells. The
similar results also were found for L-methionine amino acid.

 Sulfur containing ligands in ruthenium compounds also could rapidly react with guanine and
displaced by this nucleobase. Although glutathione intermediates could help for the ruthenation
of DNA or RNA in redox mediated pathway.

 Other studies on cytochrom C and this compound, [(η 6-Bip)Ru(en)Cl][PF6] , have been done
and 2D [1H, 15N] HSQC NMR results showed that the ruthenium complexes are bound to
carboxylate groups (ca. 30%) and the amino terminus (ca. 70%), instead of the histidine
residues, of cytochrome c.

 In summary, in comparison with DNA, amino acids and proteins have lower reactivity to
ruthenium compounds. The result of this point could be less toxicity and side effects of these
compounds. In addition, relatively weak binding of amino acids and proteins to these compounds
could make them great candidate for transport and delivery of these drugs to cancer cells.
conclusion

Based on many researches groups’ results, ruthenium arene
complexes showed promising anticancer activity in vitro and in
vivo. These complexes are non-cross-resistant towards cancer
cells and they became good candidates as anticancer agents but
more researches and clinical trials are needed to prove its safety
and low systemic toxicity and its efficacy.
Acknowledgements

Prof. Richard H. Fish

My dear classmates

Professors :Sadler, Dyson, Hartinger, Juillerat-Jeanneret, Clarke, and other
research groups


                         Questions
                             &
                         Answers

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Ruthenium role in cancer therapy

  • 1. “RUTHENIUM ROLES IN BIOLOGY, CHEMISTRY AND MEDICINE AS ANTICANCER COMPOUNDS” FATEMEH BABAEI CITY UNIVERSITY OF HONG KONG NOVEMBER 2011
  • 2. What does the ? word cancer mean to you?
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  • 4. While cancer can affect people of all ages, and a few types of cancer are more common in children, the risk of developing cancer generally increases with age. In 2007, cancer caused about 13% of all human deaths worldwide (7.9 million). Rates are rising as more people live to an old age and as mass lifestyle changes occur in the developing world.
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  • 6. Ruthenium has found its way into the clinic :  Radiophysical properties of Ru can be applied to radiodiagnostic imaging  Immunosuppressants  Antimicrobials (against malaria and Chaga s disease)  Antibiotics (against Salmonella typhi and Enterobacteria faecalis  Nitrosyl delivery/scavenger tools  Vasodilator/vasoconstrictor agents  Ruthenium compounds are known to be less toxic and no cross resistant than platinum counterpart.  Cancer chemotherapy Ruthenium has a range of oxidation state (II,III and IV) accessible under physiological Condition, which is unique among the platinum-group metals.
  • 7. Cancer cells Cancer cells need considerably more energy than healthy cells. Their metabolism runs at full speed and requires large amounts of micronutrients, particularly iron. Ruthenium Ruthenium have the ability to bind albumin and transferrin And because cancer cells need more Iron, transferrin receptors are over expressed, Thereby allowing ruthenium- based drugs to be more efficiently delivered to cancer cells.
  • 8. The oxidation state changes of ruthenium (II/III) in cancer and healthy cells “activation by reduction” mechanism
  • 9. Classification of ruthenium complexes with anticancer properties  Ammine-chlorido derivatives The cytotoxicity tests had disappointing results Poor water solubility  Dimethylsulfoxide complexes Water soluble Anti metastatic activity No cross resistant  Ruthenium polyaminocarboxylate complexes Similar to biological molecules, Low systematic toxicity, Binding to DNA and alter the normal conformation and inducing the DNA cleavage  Organoruthenium complexes
  • 10. Typical structure of ruthenium complexes Typically, the Organomtallic anticancer complexes have a half-sandwich “piano-stool” [(g6-arene) Ru(X)(Y)(Z)] structure. As shown in the figure, the complexes consist of three main building blocks, the arene forms the seat of piano stool and the ligands resemble the legs. Linking the ligands Y and Z to form a bidentate chelating ligand (L) seems to be advantageous for anticancer activity. IC50 values of Ru(II) arene complexes, carboplatin and cisplatin in A2780 human ovarian cancer cells after 24 h drug exposure. Cytotoxic activity Activity appears to increase with the size of the coordinated arene: benzene < p-cymene < bi- phenyle < dihydroantracene < tetrahydroantracene, in this cell line, the arene = biphenyle complex has similar cytotoxicity to the anticancer drug carboplatin.
  • 11. How these drugs work: mechanisms of action Cancer therapy Classical way: ruthenium coordinatively bind to DNA double helix via nitrogen atoms New method : “targeted therapy” The reactivity of the various binding sites of  Targeting cellular signaling pathway nucleobases towards Ru (II) at neutral pH  Highly effective and specific decreases in the order G (N7) > T (N3) >  Side effects are less sever &controllable C(N3) > A(N7), A(N1). cytotoxicity The factors that up-regulated in cancer cells are: The preferable binding is with guanine epidermal growth factor receptor over adenine, same as cisplatin. (EGFR), vascular endothelial growth factor (VEGF), cyclin-dependent kinases (CDK).
  • 12. Interactions within guanine (G) and adenine (A) adducts of arene Ru-en anticancer complexes when the size of Arene increased, it seems that the hydrophobic arene- purine base π-π stacking interactions will be increased.
  • 13. Ruthenium complexes with anticancer properties  NAMI-A binds strongly to serum proteins, including the iron transporter transferrin and it induces cell arrest in the premitotic G (2)-M phase.  KP1019 drug induce cell death and have a significant cytotoxicity in vitro against colorectal cell lines SW480 and HT29. This drug was also found to be highly effective in in vivo tests and it induces apoptosis in colorectal cell lines mainly via the intrinsic mitochondria apoptosis pathway. Clinically evaluated ruthenium-based anticancer drugs
  • 14. Strategy to tether Organometallic ruthenium arene anticancer compounds to recombinant Human Serum Albumin  The main role of Human serum albumin (HSA) is to maintain the osmotic pressure in the blood and to scavenge free radicals as an antioxidant.  HSA is known to accumulate in tumors.  The carrier conjugate of various organic anticancer drugs such as chlorambucil, doxorubicin, and paclitaxel. RAPTA: 1,3,5-triaza-7-phosphatricyclo[3.3.1.1]- decane ligand
  • 15. Strategy to tether Organometallic ruthenium arene anticancer compounds to recombinant Human Serum Albumin RAPTA-C, theprototype compound with a p-cymene ring According to these results Organometallic ruthenium (II)-arene anticancer compound to rHSA could collected in tumor cells, and rHAS could be taken as a carrier biomolecules for drug delivery of RAPTA complexes in vivo, but in these area of targeted drug delivery more researches are needed.
  • 16. Reactions with other amino acids and proteins  Researchers showed (η6-benzene) Ru (DMSO) Cl2 strongly inhibit topoisomerase II activity by cleavage complex formation. They suggest that the ruthenium complex interacts with DNA and forms cross links with topoisomerase II. The complex exhibited antiproliferative activity in vitro.  Prof. Sadler and his colleagues found that the reaction of [(η6 -Bip) Ru(en)Cl][PF6] complex with thiol containing amino acids L-cysteine is slow in aqueous solution, and they showed that thiols couldn’t directly inactive Ru (II)-en arene complexes in blood plasma or in the cells. The similar results also were found for L-methionine amino acid.  Sulfur containing ligands in ruthenium compounds also could rapidly react with guanine and displaced by this nucleobase. Although glutathione intermediates could help for the ruthenation of DNA or RNA in redox mediated pathway.  Other studies on cytochrom C and this compound, [(η 6-Bip)Ru(en)Cl][PF6] , have been done and 2D [1H, 15N] HSQC NMR results showed that the ruthenium complexes are bound to carboxylate groups (ca. 30%) and the amino terminus (ca. 70%), instead of the histidine residues, of cytochrome c.  In summary, in comparison with DNA, amino acids and proteins have lower reactivity to ruthenium compounds. The result of this point could be less toxicity and side effects of these compounds. In addition, relatively weak binding of amino acids and proteins to these compounds could make them great candidate for transport and delivery of these drugs to cancer cells.
  • 17. conclusion Based on many researches groups’ results, ruthenium arene complexes showed promising anticancer activity in vitro and in vivo. These complexes are non-cross-resistant towards cancer cells and they became good candidates as anticancer agents but more researches and clinical trials are needed to prove its safety and low systemic toxicity and its efficacy.
  • 18. Acknowledgements Prof. Richard H. Fish My dear classmates Professors :Sadler, Dyson, Hartinger, Juillerat-Jeanneret, Clarke, and other research groups Questions & Answers