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Sydney Cancer Institute

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Title: Sydney Cancer Institute


1
Sydney Cancer Institute
  • University of Sydney 19th Jan 2004

2
Organisation and Research Direction
  • The Sydney Cancer Institute is an independent
    research institute established in February 2003
    by
  • Sydney Cancer Centre
  • The Central Sydney Area Heath Service (CSAHS)
  • The University of Sydney
  • The Sydney National Cancer Foundation
  • The primary function of the institute is
  • Conducting research to substantially improve
    cancer outcomes

3
Objectives and Research Directions
  • The Sydney Cancer Institutes research programs
    are based around a clinically driven set of
    research priorities
  • The Sydney Cancer Institute comprises the
    following divisions
  • Molecular Oncology
  • Cancer Biology
  • Experimental Therapeutics
  • Cancer Care and Control

4
Research Goals
  • The Sydney Cancer Institute aims to pursue
    research excellence, depth and relevance by
  • Integration with clinical cancer medicine by the
    development of translational research programs
  • Providing core research facilities such as
  • A clinical cancer register
  • Statistician and information technology
  • Shared instruments and operators
  • A tumour bank available to all SCI researchers
  • Providing more structured national and
    international connections

5
Scientific Advisory Board
  • The SCI scientific advisory board includes
    researchers with a diverse array of skills and
    interests
  • Prof. W McCarthy (Director Melanoma Foundation)
  • Prof. J Bishop (Director Sydney Cancer Centre)
  • Prof. B Armstrong (Head School of Public Health,
    USyd)
  • Prof. G Halliday (Department of Dermatology,
    USyd)
  • Prof. P Lay (Centre for Heavy Metals Research,
    USyd)
  • Prof. B Roufogalis (Pro-Dean Pharmaceutical
    Chemistry, USyd)
  • Prof. J Simes (Director NHMRC Clinical Trials
    Centre, USyd)
  • Prof. J Thompson (Director Sydney Melanoma Unit)
  • A/Prof. P Buttow (Executive Director, Medical
    Psychology Unit, USyd)
  • A/Prof. M Millward (Head Clinical Research, SCI)
  • Dr S Clarke (Senior Research Fellow, SCI)

6
Affiliations
  • The SCI has affiliation agreements with
  • The University of Sydney
  • Central Sydney Area Health Service
  • The Sydney National Cancer Foundation
  • The John Wayne Cancer Institute Los Angeles
  • The National Institutes of Health (USA)
  • National Cancer Institute (CTEP, USA)
  • Cancer Therapeutics Research Group (Singapore)
  • National Cancer Centre (Singapore)
  • John Hopkins (Singapore)

7
Research programs
  • The SCI has a diverse research program including
  • DNA Methylation (Dr Susan Clarke)
  • Cancer Genetics and Drug Resistance (Dr Quihan
    Dong, Dr John Young)
  • Viral Oncology (Professor Y Cossart and Dr Carol
    Thompson)
  • Tumour Pathology and Molecular Biology (A/Prof.
    Soon Lee)
  • Skin Cancer Biology (Prof. Gary Halliday)
  • Skin Cancer and Photobiology (Dr Vivienne Reeve)
  • Cancer Invasion and Metastasis (Dr Guy Lyons)
  • Heavy Metals Research Program (Prof. Peter Lay)
  • Clinical Pharmacology (A/Prof. Stephen Clarke)
  • Pharmaco Oncology (Prof. Basil Roufogalis)
  • Gene Therapy (A/Prof John Rasko)
  • Molecular Imaging (A/Prof Michael Fulham)
  • Clinical Trials (A/Prof. Michael Millwood)
  • Early Detection and Diagnosis (Dr Scott Menzies)

8
Biometals Section
  • Centre for Heavy Metals Research
  • School of Chemistry
  • University of Sydney

9
Biometals Section, CHMR
  • Associate Professor Robert Armstrong
  • Dr. Rachel Codd
  • Dr Carolyn Dillon
  • Dr. Ron Fenton
  • Professor Hans Freeman
  • Professor Trevor Hambley
  • Associate Professor Margaret Harding
  • Dr. Hugh Harris
  • Associate Professor Brendan Kennedy
  • Professor Peter Lay
  • Professor Len Lindoy
  • Associate Professor Tony Masters
  • Dr. Lou Rendina

10
Research Areas/Interests
  • Anti-Cancer Drugs
  • - Boron complexes boron neutron capture
    therapy (Rendina)
  • - Co(III) Hypoxic Agents (Hambley)
  • - Copper Complexes (Dillon, Hambley, Harris,
    Kennedy, Lay)
  • - Metallocenes (Dillon, Harding)
  • - Metal Complexes of Organic Anti-Cancer Drugs
    (Hambley,
  • Harding)
  • - Metalloporphyrin/Fullerenes (Armstrong, Lay)
  • - Pt(IV) and Pt(II) (Fenton, Hambley)
  • - Ruthenium (Armstrong, Dillon, Lay)
  • Radiopharmaceuticals
  • - Use of copper-64 in macrocyclic systems for
    the imaging
  • and therapy of cancer (Lindoy)
  • - Improved 99Tc Generators (Masters)

11
Research Areas/Interests
  • Metal-Induced Cancers and Toxicity
  • - Cr- and Ni-induced cancers (Codd, Dillon,
    Harris, Lay)
  • - As carcinogenesis and toxicity (Dillon,
    Harris)
  • Anti-Inflammatory Drugs
  • - Cu, Zn, Ni, Zn complexes as
    anti-inflammatories (Dillon,
  • Hambley, Kennedy, Lay)
  • Anti-Diabetics
  • - Cr(III) (Dillon, Harris, Lay)
  • - Vanadium (Codd, Lay)

12
Research Areas/Interests
  • Metalloproteins
  • - structure of heme proteins and their roles in
    the immune system, and heart disease (Armstrong,
    Lay)
  • Chelation Therapy and Metabolic Processes
  • - role of transition metal-sialic acid species
    in metal
  • homeostasis/disease (Codd)
  • - cold-adapted 'super-siderophores' for metal
    chelation
  • therapies (Codd).
  • Diagnostics
  • - use of vibrational spectroscopy in the
    diagnosis of cancer
  • (Armstrong, Lay)

13
Facilities/Expertise
  • Structural Biology and Structural Chemistry
  • X-ray, Neutron Electron Scattering and
    Diffraction Synchrotron Techniques NMR
    Spectroscopy See separate presentation on CSBSC
  • Mass Spectrometry
  • Electrospray (including HPLC front end) GC-MS
    Maldi
  • Vibrational Spectroscopy
  • IR, Raman and Resonance Raman including tissue
    mapping
  • EPR Spectroscopy
  • L, Q and X band, ENDOR, He cryogenics, Whole cell
  • Cell Biology
  • Cytotoxicity Genotoxicity Permeability
    Imaging, Spectroscopy
  • Animal Studies
  • Pharmacology Pharmacokinetics Efficacy
    Toxicity

14
Anti-Cancer Drugs
15
Boron Neutron Capture - Rendina
2
0

energy
(2.28 MeV)
5
5
3
16
Clinical BNCT Agents
Malignant brain tumours Malignant melanoma
  • Two new classes
  • Platinum(II)-amine complexes
  • Metallo-intercalator complexes

17
Dinuclear Platinum Complexes
Woodhouse, S. L. Rendina, L. M. Chem. Commun.,
2001, 2464. International Patent PCT/AU02/00943
18
Metallo-intercalator Complexes
Todd, J. A. Rendina, L. M. Inorg. Chem., 2002,
41, 3331. International Patent PCT/AU02/00943.
19
Control A375 Melanoma Cells
J. Aitken, H. Harris, P. A. Lay, USyd, P. Farmer,
UC Irvine
20
CuDSF-treated A375 Melanoma Cells
J. Aitken, H. Harris, P. A. Lay, USyd, P. Farmer,
UC Irvine
21
Cu XANES of Melanoma Cells
J. Aitken, H. Harris, P. A. Lay, USyd, P. Farmer,
UC Irvine
22
Selective activation in solid tumours Hambley
necrotic
Pt(IV)
suboxic
normoxic
23
MicroXANES of Pt obtained from A2780 ovarian
cancer cells treated with Pt(IV)
24
Identification of Novel Intercalating Platinum
Compounds - Fenton, Aldrich-Wright
  • CISPLATIN analogs bind to DNANew Pt compounds
    intercalate into DNA - IP protection- PCT
    filing, Priority date February 22nd 2001

25
EFFICACY of lead compound - Comparison with
Cisplatin in Cisplatin-resistant cell lines

L1210 mouse leukemia 2008 human ovarian
tumor PC3 prostate tumor DDP
Cisplatin-resistant C13 acquired SKOV3
intrinsic Cisplatin resistance

26
Titanocene Dichloride
Phase I clinical trials toxic effects
hypoglycaemia, metallic after taste bone
marrow largely unaffected liver toxicity
does-limiting side-effect
Phase II clinical trials breast cancer
renal cell carcinoma
  • poor hydrolytic stability in water pHgt 4.0
  • Ti accumulates in nucleic rich regions tumour
    cells
  • species formed in vivo and how interaction with
    DNA occurs not understood
  • mechanism is distinct from platinum based drugs

A/Prof Margaret Harding, School of Chemistry
27
Antitumour Metallocenes
Ti
V
Mn
Cr
Tc
Zr
Nb
Mo
Re
Hf
Ta
W
Y Cl, Br, I, NCS, N3
  • Each complex has independent mechanism of action
  • Current studies focus on cellular distribution,
    interaction with biomolecules of Mo, Nb
    complexes
  • M Mo targets thiols

Design water soluble, stable derivs
A/Prof Margaret Harding, School of Chemistry
28
Streptonigrin
  • Clinical use human cancers until 1977
  • broad spectrum antitumor activity
  • lymphoma, melanoma
  • cancers of the breast, cervix, head, neck
  • severe and unpredictable side-effects

Water, pH 6.5
A/Prof Margaret Harding, School of Chemistry
29
Streptonigrin Metal Complexes
affects DNA binding topo II recognition site
Redox related to DNA cleavage ACCELERATED
BY METAL IONS
bipyridyl
zwitterion
labile metal complexes
  • Ru(II) complex
  • Reductively activated to semiquinone
  • Strong DNA binding/cleavage predicted

A/Prof Margaret Harding, School of Chemistry
30
Radiopharmaceuticals
31
Improved Tc-99 Generators - Masters
  • Understanding the interactions between alumina
    and molybdates has led to improvements in the
    process for generating 99Tc for radio-diagnostics

Schematic outline of 99Mo production process at
ANSTO.
32
Metal-Induced Cancers and Toxicity
33
Cellular Metabolism of Chromium
34
Effect of Oxidation State on Cr Genotoxicity
Cr(VI)
Cr(V)
Cr(III)
Dillon, C. T. et al. Chem. Res. Toxicol. 1998,
11, 119-129 Dillon, C. T. et al. Chem. Res.
Toxicol. 2000, 13, 742-748.
35
Exposure of Whole Cells to Cr(VI) and Cr(III)
Cr(III)-Treated Cell
P
K
Cr
Zn
Cr(VI)-Treated Cell
P
K
Cr
Zn
Min
Max
Dillon, C. T. Lay, P. A. Kennedy, B. J.
Stampfl, A. P. J. Cai, Z. Ilinski, P.
Rodrigues, W. Legnini, D. G. Lai, B. Maser, J.
J. Biol. Inorg. Chem. 2002, 7, 640-645.
36
Anti-Inflammatory Drugs
37
Copper Indomethacin Lay, Hambley, Kennedy, Dillon
  • Copper indomethacin is a dimeric copper complex
    containing 4 indomethacin ligands bound to Cu
    through the carboxylic acid group.
  • Cu-algesic (CuIndo) is an effective
  • anti-inflammatory drug commonly used in dogs and
    horses.
  • Importantly, CuIndo is much less TOXIC in dogs
    than IndoH.

38
Assessment of Small Intestinal Ulceration
39
Effect of the Formulation on Gastro-Intestinal
Damage
  • Equivalent doses of indomethacin (10 mg/kg) were
    administered to each animal.
  • The number of animals tested per treatment ranged
    from 4-6.

40
Anti-Diabetics
  • Codd, Harris, Lay

41
Efficacy of Cr Dietary Supplements
  • Chromium supplements are the second biggest
    market for dietary supplements (over 1B
    industry).
  • Taken to convert fat into muscle in athletes
    (used instead of steroids for humans) and food
    animals.
  • Used to help prevent diabetes.
  • There is no compelling evidence (epidemiology,
    cell work, or biochemical assays) that Cr
    supplements convert fat into muscle or help
    prevent diabetes.
  • The FDA has prevented companies from advertising
    such health benefits.
  • There are anti-diabetic effects exhibited in
    animal studies for certain Cr complexes and they
    are believed to have anti-diabetic effects on
    humans.

42
Side-Effects of Cr Dietary Supplements
  • They react with enzyme systems such as glucose
    oxidase and xanthine oxidase to form highly
    genotoxic mixtures of high oxidation state Cr
    species, which are very damaging to DNA
  • The Cr(VI) generated in these enzymatic processes
    and strongly inhibits phosphatase enzymes, which
    is likely to be responsible for the anti-diabetic
    effects of Cr supplements
  • High-oxidation-state Cr and V species appear to
    act in the same way, through similar
    intermediates in their anti-diabetic effects

Inhibition of PTP (phosphatase enzyme by Cr(VI),
Cr(V) and V(V). Mulyani, Levina, Lay, JACS,
submitted
43
Metalloproteins
44
Heme Proteins - Armstrong, Harris, Lay
  • Characterized NO, CO and O2 adducts of heme
    proteins, many of which are too unstable to
    crystallise
  • Studied unfolding of cytochrome c
  • Collaborations with Paul Witting and Roland
    Stocker
  • - Studies on indolamine 2,3-dioxygenase (IDO) -
    important in the immune system
  • - Studies on the roles of heme proteins in heart
    disease

45
Heme Proteins
Rich, Cheng, Armstrong and Lay
46
Chelation Therapy and Metabolic Processes
47
Metal-Sialic Acid Speciation Codd
Insight into the nature and role of species
formed between sialic acid and transition metal
ions. This polyfunctional carbohydrate is
present as the terminal residue in many
glycopoteins involved in metal transport (e.g.,
transferrin ceruloplasmin)
Membrane glycoproteins and glyco- lipids
extracellular sugar residues on mammalian plasma
membranes
48
Metal-Sialic Speciation
Extension of studies of metal-sialic acid
speciation with other biologically relevant
transition metal ions (e.g., Cu, Fe, Zn, V).
Cu(II)-sialic acid profile
Cr(V)-sialic acid profile
Implications for metal transport, homeostasis,
and role(s) in sialylglycoprotein-dependent
disease
Development of transition metal EPR Spectroscopy
as a diagnostic technique for glycosylation
patterns
49
Diagnostics
50
Vibrational Spectroscopy in Breast Cancer
Diagnosis - Tam, Armstrong, Carter, Lay
51
Current Diagnostic TechniquesTriple Assessment
Side Effects
  • A combination of physical examination, mammogram
    and fine needle aspiration cytology.
  • Standard for breast diagnosis.
  • Side effects
  • Probable false positive and negative results from
    mammogram
  • Time consuming progress

52
New Diagnostic For Breast Cancer
  • 1H Magnetic Resonance Spectroscopy at IMRR
  • Simple and quick diagnosis of aspirated breast
    tissues
  • The choline-to-creatine peak ratio is being used
    to compare various breast disease states
  • Vibrational Spectroscopy
  • Infrared Spectroscopy
  • Quick diagnosis by comparing the spectral
    differences in proteins (amides), lipids and DNA
    levels of sectioned tissues
  • Raman Spectroscopy
  • By using various laser excitations to compare
    proteins, lipids and DNA levels of different
    breast diseases.
  • Imaging and mapping provide parallel results
    often difficult to determine in pathology.

53
1H Magnetic Resonance Spectroscopy
ppm
54
FT-IR Spectra
Malignant
Transmission
Benign
Wavenumbers (cm-1)
55
FT-IR Spectra
Transmission
Malignant
Wavenumbers (cm-1)
56
Malignant
Raman Intensity (a.u.)
Benign
FT-Raman Spectra
Wavenumber (cm-1)
57
  • Raman Imaging
  • New approach to compare results parallel to the
    native pathological examinations
  • Colour intensity of particular Raman marker
    bands have potential for identifying the progress
    of cancer
  • Proteins, lipids, DNA and other important
    components can be detected in tissues that
    require less preparation than for infrared and
    magnetic resonance spectroscopy

58
Summary
  • 1H Magnetic Resonance Spectroscopy
  • Fast and suitable for low-lipid content of breast
    lesions
  • Research is in collaboration with The Institute
    for Magnetic Resonance Research, University of
    Sydney
  • Vibrational Spectroscopy
  • Suitable for both high- and low-lipid content of
    breast lesions
  • Inexpensive and non-destructive.
  • can run in parallel with histopathology
  • Multivariate Statistical Analysis
  • Improve significance for the spectral data
  • Correlate and classify different breast diseases
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