ALCOHOL & DRUG SCREENS
A GUIDE TO THE
INTERPRETATION AND
EFFECTIVE USE OF SCREENS
FOR SUBSTANCES OF ABUSE
STEVEN KIPNIS, MD, FACP, FASAM
GEORGE SERDINSKY, CASAC
JOY DAVIDOFF, MPA
�TABLE OF CONTENTS
Page No.
INTRODUCTION/CHECKLISTS 3 - 6
TEST METHODS 7 - 9
SPECIMENS TO BE TESTED 10
URINE 11-13
BLOOD 14
BREATH 15-16
SALIVA 17-19
SWEAT 20-23
HAIR 24-28
DRUG CLASSES 29-30
ALCOHOL 31-33
SEDATIVES 34-36
OPIATES 37-45
STIMULANTS 46-50
CANNABINOIDS 51-54
HALLUCINOGENS 55
PHENCYCLIDINE (PCP) 56
INHALANTS 57
ANABOLIC STEROIDS 58
DRUG SCREEN RESULTS 59-60
TRUE POSITIVE 61-63
FALSE NEGATIVE 64-65
FALSE POSITIVE 66-71
BEATING THE TEST 72-81
SPECIAL ISSUES: 82
CLIA 83
ADOLESCENT TESTING 84-85
PREGNANT WOMEN 86
WORKPLACE TESTING 87-88
COLLECTION 89
USING THE DRUG SCREEN IN
TREATMENT 90-91
REFERENCES 92-94
�SUBSTANCE USE DISORDERS ARE
CHRONIC DISORDERS; RELAPSE MAY
OCCUR AT ANY TIME.
PATIENTS MAY DENY OR MINIMIZE DRUG
USE.
DRUG TESTING CAN DETERMINE DRUG
USE AND IS AN INTEGRAL PART OF
ONGOING EVALUATION AND TREATMENT,
MUCH LIKE GLUCOSE LEVELS ARE
IMPORTANT FOR THE ONGOING
EVALUATION AND TREATMENT OF
DIABETES.
3
�BEFORE TESTING - ISSUES
THAT NEED TO BE CONSIDERED
IS THIS ROUTINE OR REASONABLE CAUSE TESTING ?
INFORMED CONSENT ISSUES FOR THE ADOLESCENT (SEE SPECIAL
ISSUES SECTION)
ARE YOU USING AN APPROVED LAB?
DO YOU NEED A CLIA LICENSE (SEE SPECIAL ISSUES)?
DO YOU NEED A HARD COPY OF THE RESULT?
ARE THERE CHAIN OF CUSTODY ISSUES?
DO YOU NEED TO DO A SPLIT URINE SAMPLE*?
HOW MANY TESTS MUST BE POSITIVE FOR YOU TO DO SOMETHING?
(CAREFUL CLINICAL DECISIONS SHOULD BE MADE BASED UPON THE
RESULTS OF A SINGLE TEST)
IF POSITIVE RESULT WHAT ARE YOU GOING TO DO WITH IT?
REFERRAL?
HAVE YOU TAKEN A COMPLETE DRUG/MEDICATION USE HISTORY TO
INCLUDE OVER - THE - COUNTER MEDICATIONS AND HERBAL
PREPARATIONS?
* SPLIT SAMPLE: SPLITTING A SINGLE URINE VOID INTO 2
SEPARATE BOTTLES LABELED A AND B; A IS TESTED AND B
REMAINS SEALED AND AVAILABLE FOR TESTING AT A LATER DATE
�DRUG TESTING
OBSERVATION CHECKLIST
SYMPTOMS AND BEHAVIORS
PRESENCE OF ONE OR MORE MAY PROVIDE REASONABLE
CAUSE FOR TESTING
CHANGE IN ATTENDANCE
CHANGE IN WORK QUALITY OR QUANTITY
INCREASE IN ACCIDENTS
CARELESSNESS
LABILE (CHANGING) MOOD
UNEVEN JUDGMENT
WITHDRAWAL FROM FRIENDS AND PEERS
LETHARGY
INABILITY TO LOCATE FOR PERIODS OF TIME
FREQUENT BURNS AND BRUISES WITH POOR EXPLANATIONS
INCREASE IN VISITS TO RESTROOM, CAR, ETC.
5
�DRUG TESTING
OBSERVATION CHECKLIST
SYMPTOMS AND BEHAVIORS
CHANGE IN BEHAVIOR (INCREASE OR DECREASE)
FRIENDLY
HYPERACTIVE
INACTIVE
NERVOUS
ALERT
EVASIVE
SUSPICIOUS
BELIEVABLE(TRUTHFUL)
COOPERATIVE
CHANGE IN THOUGHTS
DOES HE/SHE MAKE SENSE?
CAN YOU FOLLOW HIS/HER THINKING?
DOES HIS/HER ATTENTION WANDER?
IS HE/SHE SCARED?
DOES HE/SHE SCARE YOU?
DOES HE/SHE ANSWER QUESTIONS APPROPRIATELY?
�TEST METHODS
IMMUNOASSAYS
BASED ON PRINCIPLE OF COMPETITION BETWEEN
LABELLED AND UNLABELLED ANTIGEN (DRUG) FOR
BINDING SITES ON A SPECIFIC ANTIBODY.
RADIOIMMUNOASSAY (RIA)
KNOWN AMOUNTS OF RADIOACTIVE LABELLED DRUG ARE ADDED
TO A SAMPLE WITH KNOWN ANTIBODY AMOUNTS. THE LABELLED
AND UNLABELLED DRUGS COMPETE FOR THE ANTIBODY SITES.
THE ANTIBODY ANTIGEN COMPLEXES ARE CENTRIFUGED AND
MEASURED IN A GAMMA COUNTER
ENZYME IMMUNOASSAY (EIA)
EMIT(ENZYME MULTIPLIED IMMUNOASSAY TECHNIQUE) SYSTEM
IS FREQUENTLY USED. THE LABEL ON THE ANTIGEN IS AN
ENZYME THAT PRODUCES A CHEMICAL REACTION WHEN
INTERACTING WITH ANOTHER SUBSTANCE. ENZYME ACTIVITY IS
DIRECTLY RELATED TO THE CONCENTRATION OF DRUG
(ANTIGEN) PRESENT.
�TEST METHODS
THIN LAYER CHROMATOGRAPHY (TLC)
BASED ON AN ABSORBENT (GEL,CELLULOSE) BEING
APPLIED TO A GLASS PLATE OR PLASTIC FILM. A
MIXTURE OF KNOWN DRUG COMPOUNDS (STANDARD)
ARE APPLIED TO SPECIFIC AREAS AND ARE
ALLOWED TO MOVE ACROSS THE PLATE BY
CAPILLARY ACTION. THE UNKNOWNS ARE COMPARED
TO KNOWN SAMPLES AS TO THEIR VERY SPECIFIC
MOVEMENT.
�TEST METHODS
GAS - LIQUID CHROMATOGRAPHY (GLC)
BASED ON AN INERT GAS AS THE MOVING PHASE
TO TRANSPORT A VAPORIZED SAMPLE OF DRUG
THROUGH A COLUMN CONTAINING A STATIONARY
LIQUID PHASE.
GAS CHROMATOGRAPHY/MASS
SPECTROMETRY(GC/MS)
COMBINES THE EFFICIENT SEPARATING POWER OF
THE GLC WITH THE HIGH SENSITIVITY OF A MASS
SPECTROMETRIC INSTRUMENT TO DETECT SPECIFIC
DRUGS.
�SAMPLE ALTERNATIVES
URINE
BLOOD
BREATH
SALIVA
HAIR
SWEAT
10
�URINE DRUG TESTING
ADVANTAGES
EXTENSIVE SCIENTIFIC BASE AND RESEARCH
ACCURATE AND RELIABLE
TECHNOLOGY HAS BEEN IN PLACE FOR YEARS
DISADVANTAGES
EASY TO ADULTERATE
AMOUNT OF DOSE MAY NOT CORRELATE WITH
CONCENTRATION
COLLECTION ISSUES
TESTING MAY NOT CORRELATE WELL WITH LEVELS
OF IMPAIRMENT
11
�URINE DRUG SCREEN CUTOFF LEVELS
FOR A POSITIVE TO BE REPORTED
DRUG/METABOLITE
MARIJUANA
INITIAL TEST(ng/ml)
50
15
DELTA-9-THC
COCAINE
PHENCYCLIDINE
AMPHETAMINE
300
150
25
25
1000
500
METHAMPHETAMINE
OPIATE
CONFIRMATION (ng/ml)
500
2000
CODEINE
2000
MORPHINE
2000
6-ACETYL
MORPHINE
10
12
�URINE DRUG SCREEN
CUTOFFS
DEPARTMENT OF TRANSPORTATION IN THEIR
WORKPLACE TESTING HAS SET UP STANDARD
CUTOFFS. CHECK WITH YOUR LAB FOR THE
VALUES THAT THEY USE.
IF CONFIRMING METHAMPHETAMINE,RESULTS
MUST ALSO SHOW AMPHETAMINES > 200
NG/ML.
13
�BLOOD DRUG TESTING
ADVANTAGES
CAN DETECT IMPAIRMENT AS IT GIVES
CURRENT LEVEL
DETECTION PERIOD IS MINUTES TO DAYS
AFTER INGESTION
BREATH LEVELS CAN BE CORRELATED WITH
BLOOD LEVELS
DISADVANTAGES
INVASIVE
RISK OF NEEDLE STICKS TO HEALTHCARE
WORKERS
14
�BREATH DRUG TESTING
ADVANTAGES
SHOWS CURRENT USE
CAN BE CORRELATED WITH BLOOD LEVEL
CARBON MONOXIDE MONITORS CAN BE USED TO
DETERMINE IF ONE IS SMOKING
USEFUL IN SMOKING CESSATION PROGRAMS
DISADVANTAGE
TESTING EQUIPMENT IS NEEDED
COST
MAINTENANCE (DEPENDS ON MANUFACTURERS
DIRECTIONS)
QUALITY CONTROL
USEFUL FOR ALCOHOL PRIMARILY
15
�BLOOD/BREATH LEVEL CORRELATES WITH
IMPAIRMENT
BLOOD/BREATH ALCOHOL CONCENTRATION (BAC)
20 - 99 mg%: LOSS OF MUSCULAR COORDINATION
100 - 199 mg%: NEUROLOGIC IMPAIRMENT,ATAXIA,
PROLONGED REACTION, MENTAL IMPAIRMENT,
INCOORDINATION
200 - 299 mg%: NAUSEA, VOMITING, ATAXIA
300 - 399 mg%: HYPOTHERMIA, DYSARTHRIA, AMNESIA,
STUPOR
400 - > mg%: SERIOUS DECREASE IN PULSE,BLOOD
PRESSURE, TEMPERATURE AND RESPIRATORY
RATE;COMA
* BAC GREATER THAN 150 IF NOT SHOWING SIGNS OF
INTOXICATION OR ANY TIME BAC IS > 300 EQUALS A
DIAGNOSIS OF ALCOHOL DEPENDENCE
16
�SALIVA (ORAL FLUID)
DRUG TESTING
USED FOR MANY
YEARS
CAN USE
IMMUNOASSAY,
GAS
CHROMATOGRAPHY
OR GC/MS
17
�SALIVA (ORAL FLUID)
DRUG TESTING
ADVANTAGES
EASY SPECIMEN TO OBTAIN
SPITTING OR SWABBING
EASILY OBSERVED COLLECTION
DIFFICULT TO ADULTERATE OR DILUTE
CORRELATION BETWEEN DRUG
CONCENTRATION AND IMPAIRMENT
MAY NOT BE USEFUL IN DETECTING VERY
RECENT DRUG USE
18
�SALIVA (ORAL FLUID)
DRUG TESTING
DISADVANTAGES
INDIVIDUAL VARIATIONS IN THE
RATE OF SALIVA PRODUCTION
ORAL OR SMOKED DRUGS CAN
PRODUCE CONTAMINATION OF SALIVA
NARROW WINDOW OF DETECTION
ACIDITY OF THE SALIVA AND MOUTH
(pH)CAN INFLUENCE FREE DRUG
DIFFUSION
19
�SWEAT DRUG TESTING
ADVANTAGES
NONINVASIVE (MOST FREQUENT DEVICE IS
THE PATCH)
RELATIVELY TAMPER PROOF
AVOIDS ADULTERATION AND DILUTION
PROBLEMS
FDA APPROVED FOR 5 DRUG PANEL
PRESENCE OF THE PARENT DRUG
(HEROIN,THC, COCAINE)AND NOT THEIR
METABOLITES CAN BE DETECTED
USEFUL FOR MONITORING FOR 1-2 WEEKS
20
�SWEAT DRUG TESTING
DISADVANTAGES
HIGH INTERSUBJECT VARIABILITY
ESPECIALLY IN THE RATE OF SWEAT
PRODUCTION
POSSIBLE ENVIRONMENTAL CONTAMINATION
RISK OF ACCIDENTAL REMOVAL
LIST OF DETECTED DRUGS IS LIMITED
ETHANOL,NICOTINE/COTININE, MORPHINE,
AMPHETAMINE, METHAMPHETAMINE,
PHENCYCLIDINE, METHADONE, COCAINE
21
�SWEAT DRUG TESTING
SPECIAL ISSUES
COCAINE
FIRST APPEARANCE IS IN 60 MINUTES
MAJORITY EXCRETED IN 8 48 HOURS
CONSIDERABLE VARIABILITY IN
EXCRETION RATE AND AMOUNT
22
�SWEAT DRUG TESTING
SPECIAL ISSUES
HEROIN AND METABOLITES
STUDY CONDUCTED BY KINTZ ET AL OF 14
HEROIN USERS IN A HEROIN TREATMENT
PROGRAM IN EUROPE. EACH HAD A SWEAT PATCH
APPLIED PRIOR TO HEROIN ADMINISTRATION.
ANALYSIS FOUND SIGNIFICANT VARIABILITY IN
AMOUNTS OF HEROIN AND ITS METABOLITES:
HEROIN 2.1 TO 96.3 NG/PATCH
6-ACETYLMORPHINE 0 24.6 NG/PATCH
MORPHINE 0 11.2 NG/PATCH
* CAREFUL INTERPRETATION IS NEEDED WHEN
EVALUATING A SINGLE TEST RESULT
23
�HAIR DRUG TESTING
USED SINCE 1979
COMPLEMENTS URINE DRUG
TESTING (SHORT VS. LONG
SURVEILLANCE WINDOW)
24
�HAIR DRUG TESTING
ADVANTAGES
LONG TIME WINDOW FOR DRUG DETECTION
EASY TO COLLECT, HANDLE AND STORE
SAMPLE IS CUT, GROUND UP THEN WASHED WITH WATER
AND/OR SOLVENTS. EXTRACTION AND PURIFICATION
PROCESS PRECEDES ASSAY
STORAGE IS AT ROOM TEMPERATURE (NO NEED TO
REFRIGERATE OR FREEZE PATIENT SAMPLES)
SECOND COLLECTION CAPABILITY
NONINVASIVE
BEATING THE TEST MAY BE DIFFICULT
25
�HAIR DRUG TESTING
DISADVANTAGES
MAY NOT DETECT RECENT USE
ENVIRONMENTAL CONTAMINATION IS A POSSIBLE PROBLEM
MECHANISM OF DRUG DEPOSITION IS NOT WELL
UNDERSTOOD
DUE TO EITHER DIFFUSION FROM BLOOD TO HAIR
FOLLICLE, SWEAT SECRETION, SEBACEOUS GLAND
SECRETION OR ENVIRONMENTAL CONTAMINATION
DOSE/TIME RELATIONSHIPS ARE NOT WELL ESTABLISHED
FEW CONTROLLED STUDIES
26
�HAIR DRUG TESTING
UNRESOLVED ISSUES
RELATIONSHIP OF AMOUNT OF DRUG USED TO HAIR
CONCENTRATION
RELATIONSHIP OF DURATION OF USE AND TIME OF
USE VS. DETECTION TIME
MECHANISM OF DRUG ENTRY INTO HAIR
ENVIRONMENTAL EXPOSURE TO DRUG CAUSING
CONTAMINATION OF HAIR CAN RESULT IN A
POSITIVE REPORT
27
�HAIR DRUG TESTING
UNRESOLVED ISSUES
INFLUENCE OF HAIR COLOR AND TEXTURE ON TEST
RESULTS
STUDY BY GYGI ET AL IN 1997 FOUND THAT PIGMENTED
HAIR IN VARIOUS SPECIES OF RATS INCORPORATED 3 44
TIMES THE AMOUNT OF CODEINE THAN NON-PIGMENTED
RATS,EVEN IN THE SAME RAT. THERE WERE LARGE
DIFFERENCES SEEN FOR MORPHINE AND NORCODEINE.
HOWEVER, PHENOBARBITAL WAS FOUND IN THE SAME
CONCENTRATION IN PIGMENTED AND NON-PIGMENTED HAIR.
STUDY BY HOFFMAN IN 1999 SHOWED THAT RACIAL
DIFFERENCES DID NOT CREATE A DISPARITY
TREATMENT ISSUE:
IS A 90 DAY DETECTION WINDOW CONSIDERED RECENT OR
CURRENT USE?
28
�DRUG CLASSES
ALCOHOL
SEDATIVE/HYPNOTICS
OPIATES*
STIMULANTS (COCAINE*, AMPHETAMINE*)
HALLUCINOGENS
CANNABINOIDS*
DISSOCIATIVE ANESTHETICS (PCP*)
INHALANTS/SOLVENTS
ANABOLIC STEROIDS
*NIDA 5-DEPT. OF TRANSPORTATION TESTING
29
�EXPECTED DURATION FOR A POSITIVE
URINE DRUG SCREEN
AMPHETAMINE
METHAMPHETAMINE
BARBITURATES (SHORT ACTING)
BARBITURATES (LONG ACTING)
BENZODIAZEPINES
COCAINE
HEROIN/MORPHINE
MARIJUANA (CHRONIC USE)
MARIJUANA ( OCCASIONAL USE)
METHADONE
PCP (CHRONIC USE)
PCP (OCCASIONAL USE)
2 - 4 DAYS
2 - 4 DAYS
2 - 4 DAYS
UP TO 30 DAYS
UP TO 30 DAYS
1 - 3 DAYS
1 - 3 DAYS
UP TO 30 DAYS
1 - 3 DAYS
2 - 4 DAYS
UP TO 30 DAYS
2 - 7 DAYS
30
�ALCOHOL
SPECIMEN TESTED
BREATH
IMMEDIATE RESULTS
NEED EQUIPMENT AND TRAINING
BLOOD
ACCURATE
INVASIVE
URINE
ESTABLISHED COLLECTION ROUTINE
CORRELATION TO BLOOD LEVEL LESS ACCEPTABLE
SALIVA
IMMEDIATE RESULT
NEWER TECHNOLOGY AVAILABLE
31
�ALCOHOL
BLOOD ALCOHOL CONCENTRATION = BAC
EXPRESSED AS A PERCENTAGE
URINE = 1.3 TIMES BLOOD LEVEL AFTER
PEAK (2 HOURS AFTER DRINKING)
CAUTION: THERE CAN BE IN SITU
FERMENTATION IN URINE SAMPLES, SUCH
THAT A HIGHER LEVEL OF ALCOHOL IS
REPORTED
BREATH TESTING USES INFRARED
SPECTROMETRY MEASURED AMOUNT OF
ALCOHOL ON THE BREATH, THEN
BLOOD/ALCOHOL LEVEL IS INFERRED.
32
�DRUG TESTING GUIDELINES
(NON ALCOHOL)
DRUG TESTING DOES NOT MEASURE THE
LEVEL OF IMPAIRMENT, UNLIKE
ALCOHOL TESTING WHICH CAN BE
CORRELATED WITH IMPAIRMENT
ALL POSITIVE SCREENING RESULTS
SHOULD BE CONFIRMED WITH AN
EQUALLY SENSITIVE TEST THAT USES
A DIFFERENT CHEMICAL PROCESS.
33
�BARBITUATES
CLASS
ULTRASHORT ACTING (THIOPENTAL)
HALF LIFE = 6 26 HR
DETECTION TIME IN URINE = LESS THAN A DAY
SHORT ACTING (SECOBARBITAL,PENTOBARBITAL)
HALF LIFE = 22 30 HR
DETECTION TIME IN URINE = LESS THAN A DAY
INTERMEDIATE ACTING (AMOBARBITAL)
HALF LIFE = 24 HR
DETECTION TIME IN URINE = 2 4 DAYS
LONG ACTING (PHENOBARBITAL)
HALF LIFE = 4 DAYS
DETECTION TIME IN URINE = SEVERAL WEEKS AFTER
CHRONIC USE
34
�BENZODIAZEPINES
ISSUES
APPROXIMATELY 14 DIFFERENT BENZODIAZEPINES
MEDICATIONS ARE AVAILABLE
APPROXIMATELY 63 BENZO/METABOLITES EXCRETED INTO
THE URINE
MOST SCREENING TESTS CALIBRATED WITH OXAZEPAM
WIDE RANGE OF CONCENTRATIONS DUE TO WIDE DOSE
RANGES USED IN PATIENTS
MOST CONFIRMATION TESTS MINIMALLY DETECT OXAZEPAM
OFTEN DALMANE,ATIVAN,XANAX,KLONOPIN ARE NOT
REPORTED
AMBIEN(ZOLPIDEM) DOES NOT CROSS REACT WITH
BENZODIAZEPINE SCREEN (PIERGIES ET AL,1997)
CHINESE HERB PILLS [COWS HEAD PILLS, MIRACLE HERB
PILLS, POTENTSEX PILLS, BLACK PEARLS(TUNG SHEUH
PILLS,CHUIFONG TOUKUWAN) CONTAIN BENZODIAZEPINES]
35
�BENZODIAZEPINES
NAME
URINARY METABOLITE
SERAX (OXAZEPAM)
OXAZEPAM
RESTORIL (TEMAZEPAM)
TEMAZEPAM,OXAZEPAM
ATIVAN (LORAZEPAM)
LORAZEPAM
DALMANE (FLURAZEPAM)
HYDROXYETHYLFLURAZEPAM
DESALKYLFLURAZEPAM
LIBRIUM(CHLORDIAZEPOXIDE)
OXAZEPAM, NORDIAZEPAM
VALIUM (DIAZEPAM)
TEMAZEPAM,NORDIAZEPAM,
OXAZEPAM
XANAX (ALPRAZOLAM)
a-HYDROXYALPRAZOLAM
KLONOPIN (CLONAZEPAM)
7-AMINOCIONAZEPAM
36
�OPIATES ARE DERIVED FROM THE POPPY PLANT
CONTENTS OF THE POPPY
POD FLUID:
Morphine 4 - 21 %
Codeine 1 - 25%
*There are at least 20 other
alkaloids in the fluid
37
�OPIATES
MORPHINE AND/OR CODEINE MAY
BE SEEN ON EVALUATION OF A
SPECIMEN IF THE PATIENT:
USED HEROIN
INGESTED POPPY SEEDS
USED A CODEINE - CONTAINING
PRODUCT
USED A MORPHINE - CONTAINING
PRODUCT
38
�OPIATES
HEROIN
HEROIN DOES NOT OCCUR
NATURALLY, BUT IS A SEMI SYNTHETIC OPIATE
(ACETYLATION OF MORPHINE)
39
�OPIATES
HEROIN METABOLISM
HEROIN
(DIACETYLMORPHINE)
HYDROLYZED
MONOACETYLMORPHINE
(RESPONSIBLE FOR PHARMACOLOGIC
EFFECTS)
HYDROLYZED
MORPHINE
*THUS HEROIN USE CAN SHOW UP AS ONE OF SEVERAL
DIFFERENT SUBSTANCES ON A DRUG SCREEN.
40
�OPIATES
HEROIN USE - URINE DRUG SCREEN SHOWS
FREE MORPHINE
MORPHINE GLUCURONIDE
FREE CODEINE
6 - MONOACETYLMORPHINE OR 6 - MAM(THIS
METABOLITE CAN ONLY BE SEEN WITH HEROIN
USE)
41
�OPIATES
POPPY SEEDS IF EATEN IN QUANTITY(THE AMOUNT IS
DEPENDENT UPON THE TYPE OF SEED AND THE AMOUNT
USED TO MAKE THE PRODUCT) CAN SHOW UP AS A
POSITIVE URINE DRUG SCREEN FOR MORPHINE AND
CODEINE
42
�MORPHINE AND CODEINE CONCENTRATIONS
DIFFER BY TYPE OF POPPY SEED
AND TYPE OF FOOD INGESTED
43
�MORPHINE AND CODEINE
GUIDELINES
HIGH LEVELS OF TOTAL MORPHINE IN URINE(>5000
ng/ml) INDICATIVE OF ABUSE OF OPIATE PRODUCT
(HEROIN,MORPHINE,CODEINE).
HIGH LEVELS OF CODEINE (>300 ng/ml)WITH A
MORPHINE TO CODEINE RATIO <2, IS INDICATIVE OF
CODEINE USE AND NOT POPPY SEED USE
PRESENCE OF 6 MONOACETYLMORPHINE (6-MAM) IN
URINE IS A POSITIVE INDICATION OF HEROIN USE.
ONE ALWAYS NEEDS CLINICAL EVIDENCE OF HEROIN
USE UNLESS 6 - MAM IS PRESENT WHEN DIAGNOSING
A POSITIVE DRUG SCREEN FOR OPIATES AS A RESULT
OF HEROIN USE.
44
�DRUGS/MEDICATIONS THAT DO NOT
METABOLIZE TO MORPHINE AND
CODEINE
HYDROCODONE(LORTAB,VICODIN)
HYDROMORPHONE (DILAUDID)
METHADONE
45
�STIMULANTS (COCAINE)
COCAINE IS METABOLIZED TO BENZOYLECGONINE (BE)
AND ECGONINE METHYL ESTER (EME)
BE IS NOT PSYCHOACTIVE
BE IS PREDOMINANT METABOLITE IN BLOOD AND URINE
EME IS FOUND IN GREATEST AMOUNTS WHEN COCAINE IS
ORALLY INGESTED.
BENZOYLECGONINE AND ECGONINE METHYL ESTER ARE
METABOLIZED TO ECGONINE
46
�STIMULANTS (COCAINE)
COCAINE IS FOUND IN THESE LOCAL ANESTHETICS
TEN TO TWENTY PERCENT HCL SOLUTION
ONE TO FOUR PERCENT OPHTALMOLOGIC SOLUTION
TAC:TETRACAINE,ADRENALINE AND COCAINE HCL
COCAINE IS NOT FOUND IN THESE LOCAL
ANESTHETICS
BENZOCAINE
LIDOCAINE
MEPIVACAINE
47
�STIMULANTS (COCAINE)
CAN COCAINE SHOW UP POSITIVE ON A DRUG SCREEN
FROM ENVIRONMENTAL EXPOSURE?
WORK OF CONE ET AL, 1995 SHOWS THAT PASSIVE
INHALATION OF COCAINE VAPOR FAILS TO PRODUCE
POSITIVE URINE RESULTS AT USUAL CUTOFF
CONCENTRATIONS(300 ng/ml)
CAN COCAINE SHOW UP POSITIVE ON A DRUG SCREEN
FROM FOODS?
HEALTH INCA TEA BANNED BY FDA DOES CONTAIN
4.8MG OF COCAINE
48
�STIMULANTS
(AMPHETAMINE)
AMPHETAMINES ARE FOUND IN FORMS: L & D
ISOMERS
VICKS INHALER IS THE L FORM NOT
PSYCHOACTIVE BUT SHOWS UP POSITIVE FOR
AMPHETAMINE
PSYCHOACTIVE FORM OF AMPHETAMINE IS
THE D FORM, IF LESS THAN 80% IS L
FORM, THEN VICKS CANNOT BE THE SOLE
SOURCE
49
�STIMULANTS
(AMPHETAMINE)
AMPHETAMINES CAN BE FOUND ON DRUG SCREENS IN PATIENTS
USING:
PHENYLPROPANOLAMINE
PHENYLEPHRINE
SYNEPHRINE
DRISTAN
NEOSYNEPHRINE
AMPHETAMINIL
D AND L FORMS ARE SEEN IN EQUAL AMOUNTS IN PATIENTS USING:
ADDERALL
BENZEDRINE
BEPHETAMINE
DEXEDRINE
DUROPHET
OBETROL
METHAMPHETAMINE SEEN IN PATIENTS USING:
SELEGILINE
BENZPHETAMINE
50
�CANNABINOIDS
WHEN ONE OBTAINS A POSITIVE DRUG SCREEN FOR
CANNABINOIDS, ONE HAS TO LOOK FOR MEDICAL
REASONS FOR A POSITIVE TEST IN ADDITION TO
MARIJUANA USE.
PASSIVE INHALATION IS NOT USUALLY A REASON FOR
A POSITIVE TEST.
51
�CANNABINOIDS
MEDICAL EXPLANATION FOR A
POSITIVE DRUG SCREEN
MARINOL
CHEMICALLY IS - 9 - THC
DEA SCHEDULE II MEDICATION
52
�CANNABINOIDS
SOCIAL EXPLANATION FOR A POSITIVE DRUG SCREEN
PASSIVE INHALATION IS NOT USUALLY A REASON FOR
POSITIVE SCREEN (SEE NEXT PAGE)
MARIJUANA LACED BROWNIES CAN CAUSE A POSITIVE
TEST
HEMP SEED OIL INGESTION CAN CAUSE A POSITIVE TEST
IMPORTING PRODUCTS CONTAINING THC IS BANNED BY THE
FDA
53
�MARIJUANA PASSIVE INHALATION IS NOT USUALLY A
REASON FOR A POSITIVE TEST
(MRO TEXT,2002)
# JOINTS
EXPOSED TO
AREA
EXPOSURE
TIME
TEST
RESULT
REF.
SMALL
ROOM
1 HR
<5 ng/ml
MULE ET AL
1988
SMALL
ROOM
3 HRS
< 7 ng/ml
LAW ET AL
1984
SMALL
CAR
HR
NEGATIVE
@ 20 ng/ml
MORLAND ET AL
1985
SMALL
ROOM
1 HR
NEGATIVE
@ 20 ng/ml
PEREZ-REYES ET
AL 1983
12
SMALL
CAR
HR
POSITIVE
(>20 ng/ml)
MORLAND ET AL
1985
SMALL
ROOM
1 HR XS 3
DAYS
POSITIVE
(>20 ng/ml)
PEREZ-REYES ET
AL 1983
54
�HALLUCINOGENS
THIS CLASS OF DRUGS
FREQUENTLY HAVE TO BE
SPECIFIED AS ADD ONS WHEN
ORDERING DRUG SCREENS.
55
�PHENCYCLIDINE(PCP)
ONE MUST DIFFERENTIATE
BETWEEN KETAMINE USE AND PCP.
KETAMINE CAN GIVE A FALSE
POSITIVE RESULT, SHOWING UP
ON A SCREEN AS PCP.
THERE IS NEVER A MEDICAL
REASON FOR A POSITIVE DRUG
SCREEN FOR PCP
56
�INHALANTS
THIS CLASS OF DRUGS IS ALMOST
NEVER FOUND ON A DRUG SCREEN,
THOUGH ONE CAN TEST FOR
HIPPURIC ACID WHICH IS AN
INDICATION OF TOLUENE USE
57
�ANABOLIC STEROIDS
CLINICAL SUSPICION MUST BE
PRESENT AND THE LAB MUST BE
ASKED TO LOOK FOR THIS GROUP
OF DRUGS/MEDICATIONS.
ONE MUST CHECK TO SEE IF
THERE ARE MEDICAL REASONS
PRESENT FOR THEIR USE.
58
�DRUG SCREEN RESULTS
DRUG SCREEN RESULTS ARE NOT ALWAYS CLEAR CUT IN
THEIR INTERPRETATION. USE OF CONFIRMATORY TESTS ARE
USUALLY NECESSARY IF THERE IS AN INITIAL POSITIVE
SCREEN. ALWAYS LOOK FOR A MEDICALLY ACCEPTABLE
REASON FOR THE RESULT AND MAKE CLINICAL
DETERMINATIONS ON MORE INFORMATION THAN A SINGLE
TEST RESULT.
*ALWAYS MAKE SURE CORRECT SPECIMEN WAS TESTED
(NAME, DATE, ETC.)
59
�DRUG SCREEN RESULTS
RESULTS CAN BE REPORTED AS
NEGATIVE; THOUGH THEY CAN BE A TRUE NEGATIVE OR A
FALSE NEGATIVE.
POSITIVE; THOUGH THEY CAN BE A TRUE POSITIVE, A
TRUE POSITIVE WITH A MEDICALLY ACCEPTABLE
REASON,OR A FALSE POSITIVE.
FOR 4 OF THE 5 NIDA DRUGS TESTED(THE EXCEPTION
IS PCP) THERE CAN BE A LEGITIMATE MEDICAL
REASON
INDETERMINANT (ADULTERATED OR DILUTED)
60
�RESULTS
TRUE POSITIVE-CHECK FOR:
9 CORRECT SPECIMEN
9 LAB ERROR?
9 CORRECT DATE
9 MEDICAL REASON ??
9 URINE COLLECTED JUST AFTER A HOSPITAL
DISCHARGE MAY REFLECT HOSPITAL ADMINISTERED
MEDICATIONS (OPIATES, BENZODIAZEPINES)
9 PATIENT MAY NOT HAVE DOCUMENTED ALL OF THEIR
MEDICATIONS
9 RECENT OUTPATIENT MEDICAL/SURGICAL PROCEDURE
61
�RESULTS
POSITIVE
MEDICAL REASON ??
ALCOHOL
INHALERS
ASTHMA INHALERS AND NASAL DECONGESTANT
SPRAYS TESTED BY BREATH ALCOHOL METHOD;ONLY
ONE TO GIVE A POSITIVE WAS PRIMATINE MIST
(CONTAINS 34% ETHYL ALCOHOL) AND THE TEST
BECAME NEGATIVE IN 5 MINUTES(LOGAN ET AL,
1998)
MOUTHWASH
MARIJUANA
MARINOL SYNTHETIC DELTA 9 THC USED FOR NAUSEA
COCAINE
TOPICAL ANESTHETIC (TAC:TETRACAINE, ADRENALIN,
COCAINE)
RECENT DENTAL,EAR,NOSE AND THROAT PROCEDURE
OR OPHTHALMOLOGICAL VISIT
62
�RESULTS
POSITIVE
MEDICAL REASON ??
AMPHETAMINE
OVER THE COUNTER MEDS
PSEUDOEPHEDRINE
PHENYLPROPANOLAMINE
DEXEDRINE IS AN AMPHETAMINE
VICKS INHALER CONTAINS
L-METHAMPHETAMINE (DRUG OF ABUSE IS DMETHAMPHETAMINE)
OPIATES
UNDER THE CARE OF A PAIN SPECIALIST
RECENT SURGERY
63
�DRUG SCREEN RESULTS
FALSE NEGATIVES
WAS TEST TAKEN TOO LATE?
OCCURS IF ADULTERATION/DILUTION WAS
SUCCESSFUL AND UNDETECTED
ROUTINE SCREENS MAY NOT INCLUDE:
ATHLETIC PERFORMANCE ENHANCING AGENTS
VOLATILE INHALANTS
DESIGNER DRUGS
64
�DRUG SCREEN RESULTS
FALSE NEGATIVES
ROUTINE SCREENS MAY NOT INCLUDE:
BENZODIAZEPINES AND BARBITUATES, FOR
EXAMPLE, ARE NOT ON THE DEPT. OF
TRANSPORTATION SCREENS
MDMA(ECSTASY),LSD, PSILOCYBIN ARE NOT
DETECTED BY ALL SCREENS
OPIATE SCREENS FOCUS ON HEROIN,MORPHINE
AND CODEINE USE AND MAY
MISS:PROPOXYPHENE, MEPERIDINE,
METHADONE,PENTAZOCINE, AND OXYCODONE
65
�DRUG SCREEN RESULTS
FALSE POSITIVES
CROSS REACTION
PATIENT TAKING ANOTHER
SUBSTANCE THAT IS REPORTED AS A
DRUG OF ABUSE
CHINESE HERB PILLS [COWS HEAD PILLS, MIRACLE
HERB PILLS, POTENTSEX PILLS, BLACK PEARLS(TUNG
SHEUH PILLS,CHUIFONG TOUKUWAN) CONTAIN
BENZODIAZEPINES]
66
�POTENTIAL CROSS REACTING DRUGS CAUSING FALSE
POSITIVE TESTS
DRUG GROUP FOUND
CANNABINOIDS
POTENTIAL CROSS REACTING SUBSTANCE
NON STEROIDAL ANTI-INFLAMATORY
MEDICATIONS
EFAVIRENZ
OPIATES
POPPY SEEDS(SEE NEXT SLIDE)
CHLORPROMAZINE
RIFAMPIN
FLUOROQUINOLONES (EX.-CIPRO)
DEXTROMETHORPHAN(A SINGLE NORMAL
DOSE DOES NOT GIVE A POSITIVE
OPIATE RESULT (STORROW ET AL,
1995)
QUININE IN TONIC WATER
67
�POPPY SEEDS
2-252ug OF
MORPHINE/GRAM OF
SEEDS,SO CANNOT GIVE AN
EXACT NUMBER OF BAGELS
WHICH WOULD GIVE A
POSITIVE TEST
0.4 57.1ug OF
CODEINE/GRAM OF SEEDS
SAME INDIVIDUAL
INGESTING SAME AMOUNT
OF SEEDS 4 SEPARATE
TIMES GAVE 4 DIFFERENT
RESULTS
(PELDERS ET AL,1996)
68
�POTENTIAL CROSS REACTING DRUGS CAUSING FALSE
POSITIVE TESTS
DRUG GROUP FOUND
AMPHETAMINE
POTENTIAL CROSS REACTING SUBSTANCE
EPHEDRINE
(SEE IF INGESTING HERBAL DRUGS;
MA-HUANG (EPHEDRA sinica)
METHYLPHENIDATE
PHENYLPROPANOLAMINE AND OTHER
DECONGESTANTS AND COUGH
PREPARATIONS
TRAZEDONE
BUPROPION
DESIPRAMINE
AMANTADINE
RANITIDINE
69
�POTENTIAL CROSS REACTING DRUGS CAUSING FALSE
POSITIVE TESTS
DRUG GROUP FOUND
PHENCYCLIDINE
POTENTIAL CROSS REACTING SUBSTANCE
CHLORPROMAZINE
THIORIDAZINE
MEPERIDINE
DEXTROMETHORPHAN
DIPHENHYDRAMINE
DOXYLAMINE
70
�POTENTIAL CROSS REACTING DRUGS CAUSING FALSE
POSITIVE TESTS
DRUG GROUP FOUND
BENZODIAZEPINE
POTENTIAL CROSS REACTING SUBSTANCE
OXAPROZIN (DAYPRO)
CHINESE HERB PILLS [COWS HEAD
PILLS, MIRACLE HERB PILLS,
POTENTSEX PILLS, BLACK PEARLS(TUNG
SHEUH PILLS,CHUIFONG TOUKUWAN)
CONTAIN BENZODIAZEPINES
ALCOHOL
ASTHMA INHALERS AND NASAL
DECONGESTANT SPRAYS TESTED BY
BREATH ALCOHOL METHOD;
ONLY ONE TO GIVE A POSITIVE WAS
PRIMATINE MIST (CONTAINS 34% ETHYL
ALCOHOL) AND THE TEST BECAME
NEGATIVE IN 5 MINUTES
(LOGAN ET AL, 1998)
71
�DRUG SCREEN RESULTS
TRYING TO BEAT THE TEST
CRITERIA FOR DILUTE OR SUBSTITUTED URINE
DILUTED URINE:
SPECIFIC GRAVITY < 1.003
CREATININE < .2 GM/L
SUBSTITUTED URINE
CREATININE < 5 mg/dl
SPECIFIC GRAVITY LESS THAN 1.002 OR GREATER
THAN OR EQUAL TO 1.020
72
�DRUG SCREEN RESULTS
TRYING TO BEAT THE TEST
ADULTERATED URINE
CRITERIA ARE:
NITRITE > OR EQUAL 500 mcg/ml
pH < 3 OR > THAN OR EQUAL TO 11
CONTAINS AN EXOGENOUS SUBSTANCE, MANY OF WHICH ARE
AVAILABLE BY MAILORDER, OVER THE
INTERNET,ETC.EXAMPLES ARE:
URINAID GLUTARALDEHYDE (EMIT UNREADABLE)
MARY JANE SUPER CLEAR 13 DETERGENT
KLEAR POTASSIUM NITRITE
AMBER 13 ACID
THC FREE ACID
WHIZZIES SODIUM NITRITE
URINE LUCK PYRIDINIUM CHLOROCHROMATE
LL418 PYRIDINIUM CHLOROCHROMATE
SWEET PEES SPOILER PYRIDINIUM CHLOROCHROMATE
73
�74
�DRUG SCREEN RESULTS
IF YOU THINK NITRITES WERE ADDED IT CAN BE
TESTED FOR IN THE SAMPLE. BE AWARE:
NITRITES WILL SHOW UP IF PATIENT IS ON ISOSORBIDE
DINITRATE OR NITROGLYCERIN
MEDICAL NITRITE CONCENTRATIONS IN URINE ARE BELOW
500 mcg/ml
75
�DRUG SCREEN RESULTS
NEW AGENT STEALTH
ADDED TO URINE AND DESTROYS THC
METABOLITES. IT THEN VANISHES IN SEVERAL
HOURS
COMBINATION OF PEROXIDASE AND PEROXIDE
DOES NOT CAUSE THE URINE SAMPLE TO EXCEED
ANY MONITORED VALUES (pH, CREAT.,ETC.)
EFFECTIVE WHEN TESTED ON TRUE POSITIVE
URINE DRUG SCREENS FOR MARIJUANA, LSD, AND
MORPHINE. CUT-OFFS WERE 150% OF NORMAL AND
ALL WERE NEGATIVE (CODY ET AL, 2001)
76
�DRUG SCREEN RESULTS
TRYING TO BEAT THE TEST
FLUSH OUT THE DRUG
GOLDENSEAL ROOT OF HYDRASTIS CANADENSIS
CONTAINS NATURAL DIURETICS
77
�DRUG SCREEN RESULTS
TRYING TO BEAT THE TEST
USE DIURETICS TO REMOVE DRUGS
78
�DRUG SCREEN RESULTS
TRYING TO BEAT THE TEST
USE URINE FROM SOMEONE ELSE OR URINE
PURCHASED TO BEAT THE TEST
79
�DRUG SCREEN RESULTS
TRYING TO BEAT THE TEST
USE SPECIAL SHAMPOOS TO CLEAN AND DETOX
THE HAIR
80
�DRUG SCREEN RESULTS
TRYING TO BEAT THE HAIR TEST
afterBurner
APPLY THE DAY OF THE TEST
ADVERTISED TO PENETRATE THE CORE
OF THE HAIR SHAFT AND REMOVE ALL
DRUGS, LEAVING NO RESIDUE TRACE
81
�SPECIAL ISSUES
CLIA RULES
ADOLESCENT TESTING
PREGNANT WOMEN
WORKPLACE
COLLECTION
USING THE DRUG SCREEN IN THE
TREATMENT OF THE SUBSTANCE
USING PATIENT
82
�SPECIAL ISSUES
CLIA (CLINICAL LABORATORY IMPROVEMENT
AMENDMENT OF 1988)
TESTING OF ANY SPECIMEN IS SUBJECT
TO THE CERTIFICATION REQUIREMENT OF
CLIA IF TEST IS FOR MEDICAL
PURPOSES, SUCH AS FOR TREATMENT.
BREATH IS NOT COVERED UNDER THIS
AMENDMENT EXCEPT IN NEW YORK STATE
TESTING FOR EMPLOYMENT PURPOSES IS
TEMPORARILY EXEMPT
83
�SPECIAL ISSUES
ADOLESCENT TESTING
INFORMED CONSENT BY THE ADOLESCENT IS
ESSENTIAL
INVOLUNTARY TESTING IS JUSTIFIED WHEN:
EMERGENCY SITUATIONS EXIST IN WHICH A PATIENT
IS UNABLE TO GIVE INFORMED CONSENT (SURGERY,
UNCONSCIOUS, SERIOUSLY INJURED)
ALTERED MENTAL STATUS OR ACUTE PSYCHOSIS
EXISTS
ACUTE MEDICAL SYMPTOMS THAT PUT PATIENT AT
GRAVE RISK (CHEST PAIN, DYSRHYTHMIA,
HYPERTHERMIA, HYPERTENSION, ETC.)
84
�SPECIAL ISSUES
ADOLESCENT TESTING
INVOLUNTARY TESTING IS JUSTIFIED
WHEN:
COMPETENCY OF AN ADOLESCENT IS IN DOUBT
ONE DOES NOT TRUST THE VERACITY OF THE
ADOLESCENT (CONDUCT DISORDER,
OPPOSITIONAL-DEFIANT OR ANTI-SOCIAL
PERSONALITY DISORDERS ARE PRESENT)
TESTING IS COURT ORDERED
85
�SPECIAL ISSUES
PREGNANT WOMEN
A URINE AND/OR BLOOD TOXICOLOGY SCREEN IS
NECESSARY ONLY IN THOSE CIRCUMSTANCES WHERE
A HISTORY OF DRUG USE CANNOT BE RELIABLY
OBTAINED (CSAT TIP #2)
INFORMED CONSENT SHOULD ALWAYS BE OBTAINED
A TOXICOLOGY SCREEN MAY BE INDICATED IN THE
NEWBORN HOWEVER, BE AWARE:
DURATION OF DRUGS IN URINE ARE USUALLY GIVEN
FOR NON PREGNANT ADULTS AND MAY DIFFER IN
NEONATES.
THERE ARE ALTERNATIVE METHODS OF SCREENING,
THOUGH THESE MAY NOT BE READILY AVAILABLE
NEWBORN MECONIUM
86
�SPECIAL ISSUES
WORKPLACE TESTING
PERFORMED IN ACCORDANCE WITH
THE DEPARTMENT OF
TRANSPORTATION RULES AND VARIES
BY OCCUPATION
NIDA 5 TESTING
87
�SPECIAL ISSUES
WORKPLACE TESTING
INDICATED FOR:
PRE-EMPLOYMENT
REASONABLE CAUSE
EMPLOYEES UNSAFE OR UNACCEPTABLE JOB
CONDUCT CLEARLY POINTS TO A PROBLEM
RANDOM TESTING
POST ACCIDENT TESTING
PERIODIC TESTING
USUALLY ASSOCIATED WITH RECERTIFICATION
OF OCCUPATIONAL LICENSES
REHABILITATION TESTING
IN REHAB PROGRAM AND WILL BE REENTERING WORKPLACE
88
�SPECIAL ISSUES
COLLECTION
OBSERVED
NON-OBSERVED
BLUE WATER IN THE BOWL
HOT WATER TURNED OFF IN THE BATHROOM
DO NOT FLUSH UNTIL SAMPLE IS TAKEN
MEASURE THE TEMPERATURE OF THE URINE IF NOT
OBSERVED
MUST BE PREFORMED WITHIN 4 MINUTES OF COLLECTION
BETWEEN 90F. AND 100F OR WITHIN 1.8 F. OF ORAL
OR EAR TEMPERATURE
SPLIT THE SAMPLE
CHAIN OF CUSTODY, IS THIS NEEDED?
SELECTION OF THE LAB
NATIONAL INSTITUTE ON DRUG ABUSE CERTIFICATION
IS NEEDED BY LABS PERFORMING FEDERALLY
MANDATED DRUG AND ALCOHOL TESTING
89
�SPECIAL ISSUES
THERAPEUTIC VALUE OF DRUG TESTING
DRUG TESTING CAN BE A SIGNIFICANT
PART OF THE TREATMENT PROCESS. WHILE
THE INITIAL RESPONSE IS USUALLY
ANGER, IT IS IMPORTANT TO UNDERSTAND
THAT BEHIND MOST ANGER IS FEAR.
THERAPEUTIC VALUE OF DRUG TESTING
TESTING IS ACTUALLY A VALIDATION OF
RECOVERY WHEN PEOPLE ARE STAYING
CLEAN AND SOBER.
90
�SPECIAL ISSUES
THERAPEUTIC VALUE OF DRUG TESTING
STAYING CLEAN AND SOBER IS THE
RESULT OR CONSEQUENCE OF
INCORPORATING NEW SKILLS AND
BEHAVIORS AND MULTIPLE LEVELS OF
SUPPORT.
ALL PEOPLE NEED ENCOURAGEMENT AND
SUPPORT FOR MAKING GOOD DECISIONS
AND CLEAR CONSEQUENCES FOR MAKING
POOR DECISIONS. TEST PROVIDES FOR
IMMEDIATE FEEDBACK AND ALLOWS FOR
THERAPEUTIC INTERVENTIONS.
91
�REFERENCES
Baum CR et al. Breath and Blood Ethanol Following Use
of a Cough-Cold Preparation.Journal of Toxicology
35(6):643-644,1997
Casavant M. Urine Drug Screening in Adolescents.
Pediatric Clinics of North America 49:317-327,2002
Cody JT et al.Effects of Stealth Adulterant on
Immunoassay Testing for Drugs.Journal of Analytical
Toxicology 25(6):466-470,2001
Cone EJ et al. Passive Inhalation of Cocaine. Journal
of Analytical Toxicology 19(6):399-411,1995
Fraser A and Howel P Oxaprozin Cross Reactivity in
Three Commercial Immunoassays for Benzodiazepines
in Urine. Journal of Analytical Toxicology 22:5054,1998
92
�REFERENCES
Gygi SP Comparison of Phenobarbital and Codeine
Incorporated into Pigmented and Nonpigmented Rat
Hair. Journal of Pharmacologic Science 86:209214,1997
Hoffman BH Analysis of Race Effects on Drug Test
Results. Journal Occupational and Environmental
Medicine 41(7):612-614,1999
Kintz P Drug Testing in Addicts: A Comparison of
Urine, Sweat and Hair. Ther Drug Monit 18(4): 450455,1996
Logan et al. Evaluation of the Effect of Asthma
Inhalers and Nasal Decongestant Sprays on a Breath
Alcohol Test. Journal of Forensic Sciences
43(1):197-199,1998
MRO Textbook ASAM, 2002
93
�REFERENCES
Mule SJ et al.Morphine and 6-Acetyl Morphine in EMIT
Opiate Positive Urine. Clinical Chemistry
34(7):1427-1430,1988
Pelders MG and Ros JJ Poppy Seeds Difference in
Morphine and Codeine Content and Variations in
Inter- and Intra-Individual Excretion. Journal of
Forensic Sciences 41(2):209-212,1996
Piergies AA et al.Lack of Cross-Reactivity of
Ambien(Zolpidem) with Drugs in Standard Urine Drug
Screens. Arch Pathol Lab Med 121:392-394,1997
Storrow AB et al. Dextromethorphan
Defense:Dextromethorphan and the Opioid Screen.
Academy of Emergency Medicine 2(9):791-794,1995
Verbey KG and Buchan BJ. Diagnostic Laboratory:
Screening for Drug Abuse.In: Substance Abuse 3rd
Ed.Maryland:Williams & Wilkins,1997.pp369-377
94
