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Learn about the use of algorithms and the Gleason Score in optimizing androgen deprivation therapy (ADT) for prostate cancer. Explore the role of biomarkers and different medications in treatment decisions. Discover strategies to block androgen access to the cancer cells and minimize bone-derived growth factors. Understand the importance of monitoring testosterone levels and using ultra-sensitive PSA testing. Learn how to address androgen receptor-related dysfunction and prevent bone resorption during ADT.
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Themen der Veranstaltung in DARMSTADT Algorithmen Gleason Score Optimierte ADT Androgenentzugs -syndrom Zeichen des AUPK Wann Chemotherapie High vs Low doseTaxotere Andere Medikamente Falldiskussionen
KEY CONCEPTS
GLEASON SCORE (GS) & ALGORITHMS • GS Integral Part of All Risk Assessment Tools • Patient Status is Endpoint for these Tools • Nomograms, ANN (Artificial Neural Nets) are involved at all stages of PC (prevention to end of life) • GS relates to Nature of PC • PSA less reliable as GS gets higher (8 to 10) • Need to check other Biomarkers with GS 8-10 such as CEA, CGA, NSE, PAP. See page 64 in Primer.
Moving Concepts into Strategy This is the thought flow that is critical in any assessment of a living entity. It is the key to obtaining successful outcomes.
6 Ways to Optimize ADT Block androgen access to the PC cell Ensure significant lowering of Testosterone Measure testosterone using accurate lab assay Use US-PSA as biologic endpoint for ADT Use measures that down-regulate (dR) sensitivity of the androgen receptor (AR) Block bone-derived growth factors that are released due to excessive osteoclast activity (induced by androgen deprivation)
Are We Using the Optima Dose of Dutasteride ? Dr. Mostaghel's group looked for gene changes in 75 men with localized PC. Twenty-five had RP alone, 26 were given neoadjuvant dutasteride at 0.5 mg, and the remaining 24 received dutasteride, 3.5 mg orally per day for 4 months prior to RP.
ADT is about Androgen Availability • PC growth is mediated by androgens. • We call it Androgen Dependent PC (ADPC) or Androgen Independent PC (AIPC) or Castration Resistant PC (CRPC) but PC growth is androgen related. • PC mets even synthesize their own androgens. • Testosterone level (T) is a key Biological End Point. • T not measured in 95% of men with PC. • “Castration” threshold should be < 20 ng/dl. • Further lowering of T may enhance response. Huggins won Nobel Prize 43 years ago showing PC dependence on Androgens. Testosterone assays inaccurate at low T levels: need to use LC/MS/MS based assays.
Lowest T level with impact on survival was 32 ng/dl. • Mean survival, free of developing AIPC, in men with breakthrough increases in T > 32 ng/dl was 88 months (CI 55-121 mos). • Mean survival in men with T < 20 ng/dl and no breakthrough increases > 32 ng/dl was 137 mos (CI 104-170). • In men with breakthrough increases > 50 ng/dl, those men with maximal ADT had a significantly longer survival free of AIPC. <20 20-50 > 50
Importance of US-PSA (ultra-sensitive) to Monitor ADT • PSA nadir > 0.05 highly correlated with shorter time to progressive PC & prostate cancer-specific survival.
The achievement of a PSA nadir of 0.05 or less was the most significant endpoint insofar as time to progressive PC and PC mortality.
Androgen Receptor (AR) Related Dysfunction • (1) Reduce AR sensitivity • Prolactin Inhibitors • 5AR inhibitors • EGCG • HSP inhibitors • PPAR-G ligands • DIM & POMx • Silymarin • Melatonin • (2) Avoid Drugs Stimulating “Promiscuous” AR • Avoid or use cautiously standard glucocorticoids such as prednisone & dexamethasone • Use triamcinolone instead e.g. HDK with triamcinolone instead of Hydrocortisone (HC)
Androgen Receptor (AR) Related Dysfunction • (3) Evaluate for ARM (androgen receptor mutation)– see http://www.prostate-cancer.org/education/andeprv/Strum_IADT.html • Withdraw anti-androgen, progestin, estrogen to see if PSA or other marker is reduced. • If possible ARM due to Casodex need 6 weeks to eliminate Casodex (bicalutamide) from body. • (4) Avoid agents that stimulate ARM • Steroidal anti-androgens such as CPA (cyproterone acetate) • Progestins, in certain contexts.
Androgen Deprivation Therapy (ADT) Immediately Induces Bone Resorption • Surgical Orchiectomy • LH-RH agonists like Zoladex, Lupron • GnRH antagonists like Degarelix • Anti-Androgens like bicalutamide, eulexin • Ketoconazole • Estrogens • Androgen Receptor Antagonists Goal Block bone-derived growth factors released due to ADT effect on bone resorption.
Clarke NW, McClure J, George NJR: The effects of orchidectomy on skeletal metabolism in metastatic prostate cancer. Scand J Urol Nephrol 27: 475-483, 1993. • This is NOT new information but we continue to neglect this downside of ADT. • We should be preventatively blocking bone resorption prior to starting ADT. • This may improve (likely) the natural history of men with PC, as well as other malignancies that metastasize to bone.
Testosterone (T) Inhibits Osteoclast Activation. • T normally inhibits PTH (parathormone). • PTH causes bone loss by activating osteoclasts. • ADT lowers T and osteoclast inhibition lost and bone loss occurs. Chen Q, Kaji H, Sugimoto T, et al: Testosterone inhibits osteoclast formation stimulated by parathyroid hormone through androgen receptor. FEBS Lett 491:91-3, 2001.
All of Biology is a Two Edged Sword • Part of optimizing ADT is recognition of the above statement. • We need to start therapies to minimize the down-sides of any treatment we use, including ADT. • A key focus should be to prevent osteoclast activation with release of bone-derived growth factors. • Agents like bisphoshonates & Denosumab should be used early in the treatment of men with PC.
Monoclonal antibody to Receptor Activator of Nuclear Kappa Ligand (RANKL) Stops Bone Resorption & Decreases Skeletal-Related Events Better then Aredia or Zometa.
When we decrease the side-effects of any treatment, we improve the therapeutic index (TI) Treatment Benefits Treatment Side Effects = TI http://www.prostate-cancer.org/resource/pdf/Is2-1.pdf
When to Start Chemo ? • Progressive PC on ADT • ADT3 or ADT4 used • HDK given • Estrogen Rx given • No chance for salvage RP, RT or Cryo • Other Rx options used • Vaccine • AR antagonist • Clinical trial • No serious patient co-morbidities present • Heart disease • Kidney disease • Bone marrow suppression More…
When to Start Chemo ? • Aggressive PC needing more intense Rx Neuroendocrine PC or other aggressive features, perhaps detected by gene expression signatures may require early chemo or chemo-hormonal therapy. See the very first issue of Insights at http://prostate-cancer.org/resource/pdf/Is1-1.pdf. • Expertise in administration of chemo exists and patient context indicates need
Taxotere: High or Low Dose ? • I prefer weekly Taxotere regimens at a lower dose (30 mg/m2) then every 3 week regimens at a higher dose (75 mg/m2). • Patient tolerance & quality of life is far better with weekly regimen. • Complaints of severe fatigue are less. • Pre-meds used with every 3 week do not need to be used with weekly (perhaps very low dose steroid in first few weeks). • Survival data in (TAX 327) randomized trial better for every 3 week Taxotere, but difference involved weeks: median survivals 18.9 mos versus 17.4 mos. • Patients, even older men in 70’s or greater, able to tolerate weekly chemo far better then every 3 wk Rx. • Lowering of WBC greater for every 3 wk regimen vs weekly regimen.
Alternative Medikamente • HDK + triamcinolone • Insights 2001 • Keto blood levels with goal of at least 3.0 • Monitor liver function • Estrogens • You have access to Estradurin which has good published results • End Point E2 level of at least 1,000 pg/ml • GM-CSF combos • Combine with retinoid acid • Combine with Thalidomide or Revlimid • Use alone as per Small et al • PPAR-gamma agonists • Low dose (7.5mg/d) Actos • Combine with HDAC inhibitor like Valproic acid or COX-2 inhibitor like Celebrex • Memantine: NMDA receptors on PC cells • Celebrex + Dostinex combination