Clinic Reference Guide



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Transcription:

Clinic Reference Guide 2010

Alliance Toxicology LLC PO Box 5000, PMB 190 Rancho Santa Fe, CA 92067 AllianceToxicologyLLCprovidesclinicaldrugtestingservicesforphysicians.Our companyprovidesacomprehensivedrugtestingpanelwhichincludesover40 commonlyprescribedprescriptiondrugs.thefollowingpagesprovide informationonourcompanyandthereasonsforimplementingaurinedrug testingprogram.thefollowingpagesinclude: 1.) Anoverviewofwhyurinedrugtestingforclinicalpurposemakessensefor physiciansinordertoprovidebettercarefortheirpatients,tomonitor theirpatients drugtreatmentregimens,aswellasprotecttheirpractice. 2.) ACOEMGuidelinesrecommendationforurinedrugscreeningforpatients prescribedopioidsforchronicpain. 3.) Asamplelettertoinsurancecarriersexplainingthemedicalnecessityfor clinicalurinedrugtesting. 4.) AsampleAllianceToxicologyLLCurinedrugtestingresultsFormshowing thedrugsincludedinthecomprehensivepanel. Ifyouhaveanyquestionsregardingtheinformationprovidedinthisbinder, pleasedonothesitatetocontactme. Regards, KimHansen DirectorofOperations AllianceToxicologyLLC Cell:7144966164 Email:kim@alliancetox.com www.alliancetox.com

Kim Hansen Director of Operations kim@alliancetox.com Tanya Moreland Director of Sales and Marketing tanya@alliancetox.com 714.496.6164 949.375.7128 Diego Encinas- Operations/Tech Manager Jodi Little - Office/Scheduling Manager Diego@alliancetox.com Jodi@alliancetox.com 714.280.7759 714.542.2153 Jason Hansen - Technical Consultant Jason Shorb - Arizona Sales & Marketing jason@alliancetox.com jshorb@alliancetox.com 619.838.7908 602.750.3468 Brittani Summers - Administration/Results Martin Pieretti - Medical Review Officer admin@alliancetox.com mpieretti@vzw.blackberry.net 858.222.6137 877-340- 6101 office Corporate Address 267.549.6488 cell Administrative Offices PO Box 5000, PMB 190 540 N. Golden Circle #202 Rancho Santa Fe, CA 92067 Santa Ana, CA 92705

WhyClinicalUrine DrugTesting?

Alliance Toxicology LLC PO Box 5000, PMB 190 Rancho Santa Fe, CA 92067 WhyUtilizeUrineDrugTestingInYour ClinicalPractice?... Toprovidebettercareforyourpatients: Patientadvocacy UDTcanbeusedtoadvocateforpatientsinfamily,workplace,andcontested situationsasdocumentationofadherencetoanagreedupontreatmentplan WhenapatientagreestoaUDTprogramitreducestheriskofan undiagnoseddrugmisuseproblem Identifyingabuseofprescribeddrugs AUDTprogramcanbeusedtoensurecomplianceofthedirectedtreatment planandtoidentifywhetherapatientistakingotherdrugsinadditionto thoseprescribedbythephysician,whichcanbefatal Toprotectyourpractice: Physicianscanbeheldliableforpatientsmisusingorabusingprescriptiondrugs AUDTprogramcanbevaluableinaninvestigationorlawsuittoshowthat yourpracticeistakingallpossibleeffortstoprotectpatientsfrom prescriptiondrugmisuseandabuse TheDrugEnforcementAgency(DEA)investigatesmedicalpracticesandmeticulously examinesrecords IftheDEAfeelsaphysicianisnotproperlymanagingthedistributionof controlledsubstances,theycanshutdownaphysician spractice,takeawaya physicianslicense,orevenprosecuteinextremecircumstances AUDTprogramwillshowthatthepracticeisactivelyhelpingtocontrolillegal distributionofcontrolledsubstancesbypatients Uncoveringdiversionorprescriptiondrugtrafficking AUDTprogramcanbeusedtoinvestigatepossiblediversionordrug traffickingbyanalyzinginconsistenciesinthedrugprescriptionamount versustheactualquantitiesshownfromthelabresults www.alliancetox.com

ACOEMGuidelines Recommendation: UrineDrugScreeningfor PatientsPrescribedOpioidsfor ChronicPain

Copyright 2008, 2004, 1997 by the American College of Occupational and Environmental Medicine 6. Recommendation: Urine Drug Screening for Patients Prescribed Opioids for Chronic Pain Routine use of urine drug screening for patients on chronic opioids is recommended as there is evidence that urine drug screens can identify aberrant opioid use and other substance use that otherwise is not apparent to the treating physician. 614,615 Indications All patients on chronic opioids for chronic pain. Frequency Screening is recommended at baseline, randomly at least twice and up to 4 times a year and at termination. Screening should also be performed for cause (e.g., provider suspicion of substance misuse including over-sedating, drug intoxication, motor vehicle crash, other accidents and injuries, driving while intoxicated, premature prescription renewals, self-directed dose changes, lost or stolen prescriptions, using more than one provider for prescriptions, non-pain use of medication, using alcohol for pain treatment or excessive alcohol use, missed appointments, hoarding of medications and selling medications). Standard urine drug/toxicology screening processes should be followed (consult a qualified medical review officer). 616 Strength of Evidence Recommended, Evidence (C) Rationale for Recommendations While there are many quality studies of opioids for treatment of chronic, non-malignant pain, there is a dearth of quality evidence regarding long-term efficacy or adverse effects. Thus, there are no large-scale studies with robust data to definitively address these important questions. Most of the available evidence from studies of non-malignant pain addresses nociceptive pain, with a few studies including a minority of patients with neuropathic pain. Evidence to support treatment of neuropathic pain with opioids is weak. There is evidence that tramadol is effective for treatment of neuropathic pain, 617 and that oxycodone is effective despite adverse effects. 618 However, carbamazepine is more effective than morphine. 465 There is evidence that opioids are not particularly effective for treating radicular pain syndromes. 425 There is no quality evidence evaluating opioids for the treatment of trigger points/myofascial pain. The conclusions derived from a direct review of the RCTs regarding opioid use for chronic, non-visceral pain conditions are consequently consistent with those reached by the systematic reviews and meta-analyses described both previously and in Appendix 5. While many, although not all, of the studies suggest that the use of short- and medium-term opioids may lead to a decrease in pain when compared to placebo, they do not allow one to conclude that the use of opioids is consistently accompanied by evidence of functional benefit or increased quality of life. They also do not allow for conclusions to be drawn regarding the efficacy of chronic opioid therapy. It is unknown whether this reflects the failure of studies assessing the impact of long-term opioids to have been performed, or whether the absence of such studies reflects investigative biases (studies were not performed) or publication biases (studies demonstrating lack of long-term efficacy were performed and not published). Nonetheless, the absence of evidence is not evidence of absence, and it is possible that the data with regards to the benefits accrued from chronic opioid use in the general chronic pain population may not be uniformly applicable to discreet patient subsets. In other words, it is possible that appropriate patient selection and follow-up, coupled with discontinuation of opioid therapy in those who fail to show benefit, may facilitate identification of a subgroup of the pain population that would demonstrate increased functionality on opioids. There is quality evidence that other medications and treatments are superior to opioids for both patients with nociceptive pain and those with CRPS; however, a select number of patients are believed to do better with opioids than without them. If a patient can not tolerate or has failed other therapies for nociceptive pain or CRPS, a trial of opioids may be warranted and continued if use is associated with documented functional gains. Even so, the goal should be to employ other rehabilitative interventions with reduction or eventual elimination of opioids as a treatment goal. The decision to treat a patient with opioids, both short- and longterm should be undertaken with care. Since this decision typically has long-term impacts, if the practitioner does not have specialized knowledge and/or experience regarding the appropriate use of opioids it is generally recommended that a second opinion from a physician with experience in chronic pain management and/or a 228 ACOEM Occupational Medicine Practice Guidelines

MedicalNecessityFor UrineDrugTesting

AppendixI: ExcerptsfromIndustryPeriodicals JLawMedEthics PracticalPainManagement UrineDrugTestinginaClinicalPractice:DispellingtheMythsandDesigningStrategies. MorbidityandMortalityWeeklyReport. TheClinicalJournalofPain, ClinicalPractice, PainPhysician CaliforniaSB767HearingApril,2007

SampleUrineDrug TestResultsForm

PatientInformation SpecimenID#: 123456789 LastName: DOE FirstName: JOHN SS#: 555443333 DOB: 1/2/1970 Sex: MALE Address: 1234EASYSTREET City: LOSANGELES State: CA DateofInjury: 1/1/2009 Insurance: ABCINSURANCE Claim#: 987654321 DiagCode: 840 SecureResults LogoHere ClinicName: PrescriberName: StateLicense#: DEA#: OfficeAddress: City: State: Zip: Phone#: Fax#: DateofCollection: CollectionAddress: City/State/Zip: PhysicianInformation ABCMEDICAL DR.JANEDOE A1234567 BD1234567 555FIRSTAVE LOSANGELES CA 90012 5555551212 5555551313 6/1/2010 555FIRSTAVE LOSANGELES,CA90012 AllianceToxicologyLLC POBox5000,PMB190 RanchoSantaFe,CA92067 7144966167 TheDrugTestPanelincludesscreeningandGasChromatographyMassSpectrometry(GC/MS)orLiquidChromatographyTandomMass Spectrometry(LC/MS/MS)confirmationonpositivescreensforthefollowingdrugs/drugclassesshowninthetablebelow: SpecimenTestResult: POSITIVE MROBy:Dr.MartinPieretti Phone:2153406101 DrugsTested Opiates Codeine Hydromorphone Hydrocodone Morphine Oxycodones Oxymorphone Oxycodone Methadone Benzodiazepines AlprazolamMetabolite ClonazepamMetabolite FlurazepamMetabolite FlunitrazepamMetabolite Lorazepam MidazolamMetabolite Nordiazepam Oxazepam Temazepam TriazolamMetabolite Barbiturates Amobarbital Butalbital Pentobarbital Phenobarbital Secobarbital PropoxypheneMetabolite Phencyclidine(PCP) CocaineMetabolites MarijuanaMetabolites Amphetamines Amphetamine Methamphetamine MDAAnalogues MDA MDMA MDEA Flag GC/MS Cutoff GC/MS Cutoff DrugsTested Flag Level (ng/ml) Level (ng/ml) POSITIVE 300 Narcotics Negative N/A 300 Butorphanol Negative N/A 0.15 POSITIVE 456 300 Buprenorphine Negative N/A 10 POSITIVE 432 300 BuprenorphineMetabolite p Negative N/A 10 Negative N/A 300 Fentanyl Negative N/A 0.75 100 Nalbuphine Negative N/A 5 Naloxone Naltrexone Negative N/A 300 NaltrexoneMetabolite POSITIVE 100 Meperidine Pentazocine Negative N/A 75 Tramadol Dextromethorphan Ketamine Meprobamate(CarisoprodolMet) Zolpidem Antidepressants 100 POSITIVE 678 100 Amitriptyline POSITIVE 234 100 Nortriptyline Fluoxetine 300 Sertraline Negative N/A 200 Antihistamines 100 Negative N/A 200 Brompheniramine Negative N/A 200 Chlorpheniramine Negative N/A 200 Diphenhydramine Negative N/A 200 Doxylamine Negative N/A 300 Pheniramine Negative N/A 25 UrinalysisReport Negative N/A 300 Results Comments Negative N/A 50 CreatinineUrine(mg/dL) 333.0 Normal 300 phurine 6.8 Normal Negative N/A 300 GeneralInformation Negative N/A 300 LabAddress: 8433QuiviraRoad;Lenexa,KS66215 500 DateofReport: 6/3/2010 Negative N/A 500 Negative N/A 500 MRONotes: Negative N/A 500 Test Cancelled

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