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Transcript 
MEDICINAL PROPERTIES OF TRANSITION METAL COMPLEXES
Reported by Yen-Jun Ho
Oct. 4 2010
INTRODUCTION
Transition metals and medicinal applications were once thought to be mutually exclusive. The
metals were expected to be highly toxic and unstable in aqueous media. However, with the serendipitous
discovery of the antiproliferative effects of cis-diamine-dichloro-platinum(II) (cisplatin) in 1965 by
Rosenberg and coworkers, a new field of research emerged.1,2 Since then, transition metal complexes
have been used as radiation therapeutic, diagnostic and imaging agent, and as small molecule drugs.
This seminar will focus on the application of transition metals as small molecule drugs describing the
benefits and limitations of their use.
INTERACTIONS WITH DNA
Platinum-based and ruthenium-based metal complexes bind DNA and allow the design of cancer
therapeutics. Cisplatin (Figure 1a) forms intra-strand crosslinks with DNA, which leads to cell death
and is used as a anticancer compound.3 Although it is being used by 50-70% of all cancer patients,
cisplatin and its derivatives do have drawbacks, such as toxicity, rapid development of drug resistance,
and ineffectiveness against breast, prostate and colorectal cancer.4 Developments to improve upon the
drawbacks of cisplatin led to the discovery of several ruthenium complexes, such as KP1019 (Figure 1b)
and variations of ruthenium(II) arene complexes (Figure 1c-e).5 These compounds retain cisplatin’s
antiproliferative effects while reducing general toxicity as a result of preferential delivery to cancer
cells.6,7 Using the ability of the metal center to coordinate with DNA, cisplatin and the ruthenium
complexes are designed to be effective anticancer compounds.
Figure 1 Structure of transition metal complex (a) cisplatin (b) KP1019 (c) [( 6-C6H5Ph)Ru(N,N-en)Cl]+ [PF6]- by
Sadler (d) (
6
-p-MeC6H4Pri)Ru(P-pta)Cl2by Dyson (e) [(
6
-p-cymene)Ru(hydroxyphenyl-azopyridine)I]+ by Sadler
Copyright © 2010 by Yen-Jun Ho
GENERATION OF REACTIVE OXYGEN SPECIES
Besides binding to DNA, transition metal complexes can alter cellular equilibrium involving
reactive oxygen species (ROS). Jaouen and coworkers broadened the therapeutic scope of tamoxifen
through synthesis of a tamoxifen-ferrocene conjugate (ferrocifen). It is hypothesized that the generation
of ROS through one electron oxidation of iron allows ferrocifen to be effective for both hormoneindependent (ER-) and hormone-dependent (ER+) breast cancer as compared to tamoxifen which is only
effective for ER+ breast cancer.8 Another example involves Sadler and coworkers who discovered a
ruthenium complex (Fig. 1e) that catalyzes the oxidation of glutathione (GSH) to glutathione dimers
(GSSG), sensitizing cancer cells to ROS leading to an inhibition of growth.9 In both cases alteration of
ROS concentration in the cell leads to an observed therapeutic effect.
INHIBITON OF PROTEIN FUNCTION
Coordination around a metal center can lead to a more selective and potent protein kinase
inhibitor.
Meggers and coworkers designed a metal scaffold to replace a portion of the organic
framework in staurosporine, a known protein kinase inhibitor. The metal complex allowed for rapid
optimization due to the ease of screening coordinating ligands. The resulting metal complex
demonstrated increased and selective inhibition of GSK-3, which is involved in the insulin signaling
pathway.10 The coordination of ligands around the metal center allowed for efficient optimization of a
protein kinase inhibitor.
CONCLUSION AND OUTLOOK
Metal complexes can interact in the body by (1) binding to DNA (2) affecting cellular
equilibrium and (3) inhibit protein function. However, their use is still limited by observed toxicities
related to off-target effects and indiscriminate activity with biological nucleophiles. Thus, more work
must be done to discover compounds which can be more selective in interacting with therapeutic targets.
REFERENCES
(1)
(2)
(3)
(4)
(5)
(6)
(7)
(8)
(9)
(10)
Chavain, N.; Biot, C. Curr. Med. Chem. 2010, 17, 2729–2745.
Krigas, T.; Camp, L. V.; Rosenberg, B. Nature 1965, 205, 698–699.
Fricker, S. P. Dalton Trans. 2007, 43, 4903–4917.
Hannon, M. J. Pure Appl. Chem. 2007, 79, 2243–2261.
Suss-Fink, G. Dalton Trans. 2009, 39, 1673–1688.
Keppler, B.; Hartinger, C. et al. J. Inorg. Biochem. 2006, 100, 891–904.
Sadler, P. J. et al. Inorg. Biochem. 2010, 104, 79–86.
Jaouen, G. et al. Dalton Trans. 2005, 4, 529–541.
Sadler, P. J. et al. Proc. Nat. Acad. Sci. U.S.A. 2008, 105, 11628–11633.
Meggers, E. et al. ChemBioChem 2006, 7, 1443–1450.
Copyright © 2010 by Yen-Jun Ho
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