Abstract

During the progression of prostatic cancer, malignant cells undergo molecular changes in which ARinteracts with partner proteins to generate genomic as well as non-genomic signaling which allows theircontinuing growth in the presence of low circulating serum T produced by androgen ablation. Thus, these cellsare not eliminated by standard androgen ablation (i.e.,LHRH+/-casodex) and their continuous growth eventuallykills the patient. Such lethality is highest among our African-American males within the United States. Toaddress this health disparity, developing effective therapy for such androgen ablation resistant patients is thefocus of the present application. Our working hypothesis is that why present androoen ablation therapy is oflimited efficacy because the conformation of the AR protein when either unoccupied or bound bv low molecularweight partial agonist or antagonist, like Casodex. can be 'forced' by the binding of co-activators to displaceco-repressors and undergo a change to a full agonist conformation inducing growth stimulation signaling.Therefore, a novel strategy to block such AR growth signaling in androgen ablation failing patients is todevelop 'bulky bifunctional anti-androgens which bind to the ligand binding domain of AR and structurally lockthe AF-2 domain of the AR surface in an antagonist conformation not allowing its AF-2 domain to be 'forced'into the agonist state. Therefore Specific Aim 1 is to design and synthesize a series of benzyl or alkyl 11beta and7alpha side chain-delta9-19-nortestosterone analogs and determine their affinity for binding to the ligand bindingdomain (LED) of human AR and their in vitro anti-androgen ability against a series of human prostate cancercell lines.
In Specific Aim 2. the best of each of the four classes of analogs will be coupled via their side chainto a synthetic ligand for FK-506 binding protein (i.e., denoted SLF) to produce bifunctional binding analogswhich while tethered to the LBD of AR also binds FK-506 producing an adduct sterically bulky enough toprevent any AR co-activator binding.
In Specific Aim 3. the SLF bifunctional analogs will be tested for theirefficacy vs. casodex in vitro and in vivo against a series of human prostate cancers in an androgen ablatedenvironment. To achieve these goals in a timely fashion, a team approach is reguired involving thecollaboration of Dr. Oladapo Bakare of Howard University and Dr. John Isaacs of Johns Hopkins University.Dr. Bakare's expertise is in organic chemical synthesis and his laboratory will synthesize all of the proposedanalogs. Dr. Isaacs' expertise is in tumor biology and chemical therapeutics focused particularly on prostatecancer, and his laboratory will perform all of the biochemical, and in vitro/in vivo evaluations of the newlysynthesized compounds.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
2U54CA091409-06A1
Application #
7250612
Study Section
Special Emphasis Panel (ZCA1-SRRB-Y (O1))
Project Start
2006-12-01
Project End
2011-08-31
Budget Start
2006-12-01
Budget End
2007-08-31
Support Year
6
Fiscal Year
2006
Total Cost
$81,062
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
DUNS #
001910777
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Weber, Kari A; Heaphy, Christopher M; Joshu, Corinne E et al. (2018) Racial differences in maternal and umbilical cord blood leukocyte telomere length and their correlations. Cancer Causes Control 29:759-767
Weber, Kari A; Heaphy, Christopher M; Rohrmann, Sabine et al. (2016) Influence of In Utero Maternal and Neonate Factors on Cord Blood Leukocyte Telomere Length: Clues to the Racial Disparity in Prostate Cancer? Prostate Cancer 2016:3691650
Antony, Lizamma; van der Schoor, Freek; Dalrymple, Susan L et al. (2014) Androgen receptor (AR) suppresses normal human prostate epithelial cell proliferation via AR/?-catenin/TCF-4 complex inhibition of c-MYC transcription. Prostate 74:1118-31
Wilson-Frederick, Shondelle M; Thorpe Jr, Roland J; Bell, Caryn N et al. (2014) Examination of race disparities in physical inactivity among adults of similar social context. Ethn Dis 24:363-9
Dejea, Christine M; Wick, Elizabeth C; Hechenbleikner, Elizabeth M et al. (2014) Microbiota organization is a distinct feature of proximal colorectal cancers. Proc Natl Acad Sci U S A 111:18321-6
Rohrmann, Sabine; Platz, Elizabeth A (2014) To adjust or not in studies on racial differences in hormone concentrations? Depends on the question! J Clin Endocrinol Metab 99:407-8
Milam, Adam J; Bone, Lee R; Byron, M Justin et al. (2013) Cigarillo use among high-risk urban young adults. J Health Care Poor Underserved 24:1657-65
Martinez, Kathryn A; Pollack, Craig E; Phelan, Darcy F et al. (2013) Gender differences in correlates of colorectal cancer screening among Black Medicare beneficiaries in Baltimore. Cancer Epidemiol Biomarkers Prev 22:1037-42
Eichholzer, Monika; Platz, Elizabeth A; Bienstock, Jessica L et al. (2013) Racial variation in vitamin D cord blood concentration in white and black male neonates. Cancer Causes Control 24:91-8
Shinohara, Debika Biswal; Vaghasia, Ajay M; Yu, Shu-Han et al. (2013) A mouse model of chronic prostatic inflammation using a human prostate cancer-derived isolate of Propionibacterium acnes. Prostate 73:1007-15

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