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Drug Control in Horse Racing in the U.S.

Drug Control in Horse Racing in the U.S. Scot Waterman, DVM Executive Director Racing Medication & Testing Consortium. Terminology. Testing Basics. Every winner of every race in the US goes to the test barn Depending on the state, one or two additional horses may be selected for testing

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Drug Control in Horse Racing in the U.S.

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  1. Drug Control in Horse Racing in the U.S. Scot Waterman, DVM Executive Director Racing Medication & Testing Consortium

  2. Terminology

  3. Testing Basics • Every winner of every race in the US goes to the test barn • Depending on the state, one or two additional horses may be selected for testing • Typically both urine and blood samples are drawn at the test barn • Samples are tagged with a unique identifier and sealed to begin a chain of custody

  4. Definitions • Screening test- rapid and sensitive, specificity not crucial. A sample with a positive screening test would be said to be “suspicious” • Confirmation test- sensitive and specific, if the result is positive the presence of a forbidden substance is said to be confirmed.

  5. Definitions • Limit of Detection—the lowest concentration of a drug that can be detected by a particular laboratory method. • Limit of Quantitation—the lowest concentration of a drug that can be reliably quantified by a particular laboratory method. Generally higher than the LOD.

  6. Definitions • Withdrawal Time – the time period that must elapse from the time of administration of the last dose of a drug formulation until the drug concentration decreases below some concentration in urine and/or blood. • That concentration may be the LOD, the LOQ, or some predetermined concentration. • Factors affecting withdrawal time include dose, route of administration, formulation, number of doses administered, accuracy and precision of the assay, and within-horse and between-horse variability among other factors

  7. Definitions • Regulatory Limit • When a drug and/or its metabolites are found in the urine or blood at a concentration that is at or below the regulatory limit, no administrative action is taken. • Also called a “threshold” or “decision level” • European terminology = “screening limit” • Can be a LOD, LOQ, arbitrary, based on data from administration studies

  8. Definitions • Zero Tolerance—somewhat of a myth since no testing methodology can detect down to a concentration of zero. • Usually suggests that the laboratory calls positive any concentration of drug that is detected • Entirely dependent on the method being used though

  9. Zero tolerance?

  10. Zero tolerance?

  11. Definitions • Hay, oats and water—there is really no definition since the phrase means different things to different people. • No drug administration on raceday? • No detectable concentrations of drugs on raceday? Since we can’t detect down to zero whose definition of “detectable” is used • No drugs ever?

  12. Hay, Oats and Water • Keene Dangerfield, The Blood-Horse, 1979: “One things I will say is that people who are talking about going back to racing on hay, oats and water don’t know what they are talking about. We’ve never raced on hay, oats and water…Today we simply are able to find out what they are medicating them with.”

  13. U.S. Regulatory Framework

  14. U.S. Regulatory Framework • State statute enables a state agency to govern pari-mutuel wagering • Commission has power to write, enforce and adjudicate rules…executive, quasi-judicial, quasi-legislative • Commissioners are usually appointed by the governor • Reason…the industry asked for it to eliminate bookmaking competition, state wanted to control since gambling is a vice

  15. U.S. Regulatory Framework • Makeup of commission varies state-by-state • Some states do not allow those involved in the industry day-to-day to serve as commissioners • Number of commissioners (as low as 1, as high as 13) • Funding for operations varies state-by-state • Majority of states funded through general funds but some based on revenue sources from handle • Rulemaking process varies state-by-state • NJ, NY, CA from start to finish process can take over one year. Some states also have regulations encoded in statute…need to involve legislature to change

  16. U.S. Regulatory Framework—Challenges • Commission only quasi-legislative • Generally some state legislature oversight which creates another potential hurdle for model rules • Commission only quasi-judicial • Violations appealed to state court which historically have reduced significant penalties • Funding, funding, funding • Horsemen/practicing veterinarians have too much influence in some states

  17. U.S. Regulatory Framework—What actually happens • RMTC develops a model rule on a therapeutic medication • RCI Model Rules Committee and Board of Directors approve model rule • The adoption of the model rule will be more restrictive than what is allowed under state “A” current rule • State “A” begins adoption process • RMTC and sometimes RCI show up at a public commission hearing and present rationale • Local horsemen and veterinarians say adoption of rule will hurt racing in state “A” • You are the commissioner…who do you listen to? The guy from out of town or the local guys who say racing in your state will suffer?

  18. Racing Medication & Testing Consortium

  19. RMTC History • Formation: • Began with the AAEP Medication Summit, December 2001 • Summit designed to determine level of consensus on uniform medication policy • All organization that participated in original meeting are still involved nine years later • Organization has moved beyond rule uniformity as a singular goal • Incorporated as a 501 (c) (3) charitable organization since 2003

  20. RMTC Board • Horsemen—THA, HBPA, CTT • Tracks-Magna, Churchill, Oak Tree, Del Mar, HTA, TRA, NYRA, Keeneland • Owners/Breeders—TOBA, TOC, KTA • Veterinarians—AAEP • Security—TRPB • Regulatory Association—RCI • Breed Registries/Other—AQHA, The Jockey Club, NTRA, USTA, Hambeltonian Society, Arabian Jockey Club • Jockeys—Jockey’s Guild

  21. Goals and Objectives • Uniform medication rules • Uniform testing procedures • Uniform thresholds and withdrawal guidelines for therapeutic medications • Unbiased source of information on medication issues for state racing commissions • Develop intelligence on new threats to integrity • Improved security measures • Better communication regarding medication issues

  22. RMTC Goals and Objectives • Generally successful in the development of model medication policies and encouragement of adoption at state level • Large board viewed as an “industry consensus” once language is completed • Have been able to overcome some of the parochial issues as state level • Able represent RMTC in person at state commission meetings when requested • Development of a network of individuals within commissions to assist in the adoption process

  23. Model Rules V. 2005 • Permitted Therapeutics: • IV administration of furosemide 4 hours prior to post • Anti-ulcer medications permitted 24 hours prior to post • One of three NSAIDS – Bute, Banamine & Ketoprofen – 24 hours prior to post • Prohibited Practices • ESWT restrictions • Possession of blood doping agents

  24. Salix/NSAID Adoption Progress Language adopted Language in the process of being adopted Process require legislative action Process has not been started No horse racing or harness racing commission

  25. Androgenic Anabolic Steroids • Unregulated in US (except Iowa) up until 2007 • Model rule developed proactively by RMTC in 2007 • Rule set thresholds for 4 anabolic steroids and prohibits presence of any others • Adopted the international thresholds for endogenous anabolic steroids • Thresholds for stanozolol and nandrolone based on the LOD using GC/MS in urine (best science at the time)

  26. AAS Adoption Progress Language adopted Language in the process of being adopted Process pending completed administration studies Process has not been started No horse racing or harness racing commission

  27. RMTC Goals and Objectives • Industry closer to uniformity than ever before • Very few in industry thought RMTC would be this successful in driving uniformity • Organizations involved standing behind rules • Challenges still remain: • Penalties • Difficult to get stewards/commissions to depart from status quo • How to make smaller states relevant, part of process • Commissions that want to look tougher than anyone else • Grinding process

  28. RMTC Goals and Objectives • Improving Communication Efforts—Successful • Industry • Presence at conferences and organizational board meeting • Respected source of information for industry trades • Withdrawal times database on website • Regular newsletters, annual report • Wagering Public • Regular spot on Steve Byk show on Sirius • Educational materials on website • Database of positive tests with explanation of drug in development • Source for mainstream press

  29. RMTC Goals and Objectives • Development of Uniform Withdrawal Times and Thresholds—Too Early To Tell • Accomplished: • Identified drugs with legitimate therapeutic uses • Prioritized drugs into five groups based on number of violations over 5 year period • Collected previous science on each drug • Ongoing: • Administration of each drug at relevant doses to 20 horses for maximum statistical power • Analyze drug concentrations and determine withdrawal time • Ultimate goal: uniform withdrawal time with a corresponding concentration of drug which regulates the withdrawal time

  30. Priority Group 1 Acepromazine Butorphanol Detomidine Glycopyrrolate Lidocaine Mepivacaine Methocarbamol Pyrilamine Priority Group 2 Boldenone Dantrolene Dexamethasone Fluphenazine Hydroxyzine Nandrolone Stanozolol Testosterone Withdrawal Times Research

  31. RMTC Goals and Objectives • Challenges: • Has taken much longer than anticipated • Good science takes time but frustrating since we wanted answers yesterday • No dedicated laboratory to analyze the significant number of samples generated • Discrepancies in data between labs due to methodology differences • How do we determine desired withdrawal time? • Pharmacodynamic markers • Best educated guess • How to present data to reach goal of uniformity

  32. RMTC Goals and Objectives • Uniform Testing Procedures—Too Early To Tell • Post-race testing in the United States: • Currently 18 laboratories conducting testing in US…too many labs chasing too few dollars • Only 5 labs ISO 17025 accredited • 30% of samples were tested by an accredited lab in ‘08 • Funding is state-by-state and many times is under state procurement laws which reward low bidder or is statutorily directed • No industry standards for US testing labs • Not enough attention being paid to sample collection strategies

  33. RMTCDrug Testing Initiatives • Task Force formed in September 2008 • First meeting…design the best system for US Drug Testing irrespective of funding and political concerns • Consensus that we should utilize laboratory standards developed by the World Anti-Doping Association where applicable and work towards the development of a performance-based system • Other related topics discussed…next generation of lab directors, sample selection strategies and the use of frozen samples

  34. RMTCDrug Testing Initiatives • Creation of Industry Standards for Labs: • Edited version of the Lab Standards document created by the World Anti-Doping Association has been developed by the committee • Standards rely on ISO 17025 accreditation as the first step • An external proficiency program is then conducted • Labs failing proficiency cannot conduct testing • A percentage of the laboratory budget is mandated to be directed towards research • Working on a truly external quality assessment program for testing laboratories…hope to have in place during Q2 in 2010

  35. RMTCDrug Testing Initiatives • Creation of Industry Standards for Labs (continued): • Result will create the first set of industry standards for post-race testing labs in US • Result will create the first ever external QAP in the US • States/industry will have a document to “sell” in order to provide incremental funding for lab to meet standards • Will need funding for the industry organization that takes on the role of WADA

  36. RMTCDrug Testing Initiatives • Possible outcomes • Incremental funding by states in order to allow their labs to meet the standards • Reduction/consolidation of testing labs due to inability to meet standards and/or failure in proficiency • If implemented will lead to greater uniformity in laboratory procedures and methodologies

  37. General Industry Challenges • Funding for RMTC to continue research • Funding from state for commissions to increase spending on testing, investigatory capabilities, adjudication • “Silver bullet” thinking on complex issues • Dealing with issues that may be strictly based on perception and misinformation • Culture of medication use • Indirect issues that affect medication use

  38. RMTC: Contact Us • www.rmtcnet.com

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