A Practical Guide to Urine Drug Monitoring (2024)

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  • v.35(4); 2018 Apr
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A Practical Guide to Urine Drug Monitoring (1)

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Fed Pract. 2018 Apr; 35(4): 38–44.

PMCID: PMC6368048

PMID: 30766353

Mena Raouf, PharmD, BCPS,A Practical Guide to Urine Drug Monitoring (2) Jeffrey J. Bettinger, PharmD, and Jeffrey Fudin, PharmD

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Abstract

Urine drug monitoring is an important tool for substance misuse or abuse and adherence to a prescribed regimen.

Urine drug monitoring (UDM) is an important tool to screen adherence and identify possible misuse and abuse in patients on opioid therapy.1 Various guidelines for opioid therapy emphasize the importance of UDM as a standard of care.26 Routine and random monitoring is recommended for all patients on long-term opioid therapy prior to initiation and throughout duration of therapy.13 The recommended UDM frequency varies based on individual risk assessment and clinical judgment. Similar to any other diagnostic or monitoring test, the goal for UDM should be to guide therapy and improve patient care (Box). Inappropriate interpretation of the results and failure to order definitive testing when necessary may adversely affect patient care.

URINE DRUG MONITORING

Sample Collection

Urine drug testing generally requires a minimum of 30 mL of urine (depending on the kit type) collected in a private restroom. In the authors’ experience, the sample collection most often is unobserved in clinical practice. Most laboratories keep urine samples for a limited time, often 7 days. Therefor, if results are unexpected, health care providers must notify the laboratory in a timely manner to order definitive testing if indicated.

Specimen Validity Testing

Attempts to dilute, adulterate, and substitute urine may be detected by visual inspection and laboratory validity testing. Validity testing of urine specimens includes temperature, specific gravity, pH, urine creatinine, and presence of adulterants (Tables 1 and ​and22).79 Urine temperature within 4 minutes of voiding should range from 90°F to 100°F in a healthy individual, whereas temperatures outside of this range may suggest a substituted specimen has been provided. Many specimen cups have a temperature gauge on the side of the cup. A specimen outside of the physiological range should be recollected.

TABLE 1

Characteristics of Valid Urine Specimen79

CharacteristicsNormal Range
Creatinine, mg/dL20–400
Specific gravity1.002–1.030
pH4.5–8.0
Temperature, within 4 minutes of voiding, °F90–100

TABLE 2

Dilution, Adulteration, Substitution of Urine Specimen79

Urine StatesDescription
DilutedUrine creatinine ≥ 2 mg/dL but < 20 mg/dL
Specific gravity > 1.001 but < 1.003
SubstitutedUrine creatinine < 2 mg/dL
Specific gravity < 1.001 or > 1.020
AdulteratedpH < 3 or > 11
Nitrite concentration > 500 mcg/mL
Chromium concentration > 50 mcg/mL
Presence of: Halogen (bleach, iodine, fluoride), glutaraldehyde, pyridine, surfactant

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General Principles for Urine Drug Monitoring

  1. Discuss with patients prior to initiation of therapy that UDM is routine monitoring conducted for their safety and for public safety.

  2. Obtain a comprehensive and full medication history, including herbals and over-the-counter supplements and medications due to potential cross-reactivity and false positives.

  3. Ask patients how they are taking their medications and time of their last dose. For example, patients prescribed an opioid analgesic for “as needed use” might be expected test negative for the prescribed opioid.

  4. Do not make decisions that alter treatment plan without seeking definitive testing if indicated.

  5. Discuss the test results with patients and address aberrant drug behavior. Sending the patient a letter in the mail with test results and discharging the patient from the clinic is not appropriate and could increase risk for substance misuse.

The combination of specific gravity and urinary creatinine may help screen for dilution or substitution. Dilution may occur pre-collection by consumption of excess amounts of fluids or post-collection by adding fluid to the specimen. Other causes of diluted urine should be considered, such as renal tubular dysfunction or diuretic use. House-hold adulterants include vinegar, detergent, sodium chloride, hydrogen peroxide, eye/nose drops, soda, or ammonia.10 There are numerous commercially available adulterants, including Klear, UrinAid, Urine Luck, Stealth Synthetics, Whizzies, and Clear Choice. The active ingredients of some include peroxide/peroxidase, sodium or potassium nitrate, pyridinium chlorochromate, or glutaraldehyde. There are laboratory tests to detect the presence of these adulterants. Whenever in doubt, it is advisable that health care providers (HCPs) contact their laboratory to investigate tampering. Another approach if tampering is suspected is to collect blood samples. Although this method is more expensive and invasive, it eliminates means of tampering. Hair follicle testing is an option as well.

TYPES OF URINE DRUG MONITORING

There are 2 general types of UDM: Presumptive by immunoassay (IA) and confirmatory testing by chromatography. Simply, UDM by IA commonly referred to as urine drug screening (UDS), serves as the differential assessments, whereas chromatography is the definitive assessment. This article reviews the clinical utility and limitations of the 2 types of UDM, including false positives and false negatives, and when to order more tests.

Immunoassay

The IA drug test uses antibodies to detect the presence of selected drugs and/or their metabolites based on a predetermined cutoff threshold.8 Immunoassay monitoring is the initial qualitative test to identify the presence of drug classes in the urine based on a detection threshold. Typically, UDM by IA is performed as an initial evaluation of potential appropriate use, misuse, nonuse, or abuse of medications. It also can detect the presence of illegal substances or unprescribed medications. Immunoassay is relatively quick, inexpensive, and sensitive; however, because it lacks specificity, it can result in various false positives and false negatives.

Immunoassay tests also are subject to varying windows of detection depending on the substance ingested (Table 3). Most automated IAs include the “Federal Five” drugs or drug classes tested for in federal employees, which include marijuana, cocaine, opiates, amphetamines, and phencyclidine (PCP).8,9 Additional tests may be ordered separately or electronically built into the ordering system for other drugs or drug classes, such as benzodiazepines, barbiturates, lysergic acid diethylamide (LSD), propoxyphene, buprenorphine, tramadol, methadone, fentanyl, and oxycodone.4

TABLE 3

Detection Window for Selected Drugs in Urine

Drug TimeAfter Ingestion
Alcohol7–12 h
Amphetamines2–3 d
Benzodiazepines
 Short acting2 d
 Intermediate acting5 d
 Long acting10–30 d
Cannabinoids
 Single use3 d
 Moderate use (4x/wk)5–7 d
 Daily use10–14 d
 Chronic heavy use≥ 30 d
Cocaine metabolites
 20 mg IV cocaine< 1.5 d
 Chronic use2–3 d (up to 7 d at high doses)
Opioids
 Codeine2 d
 Heroin (morphine)2 d
 Hydrocodone2–3 d
 Hydromorphone2–3 d
 Methadone3–5 d
 Oxycodone2–4 d
Phencyclidine8 d

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The cutoff levels listed in Table 1 are consistent with testing for employment but not necessarily for aberrant behavior in patients receiving long-term opioid therapy. These cutoffs lower the risk of false positives and provide better accuracy with clinical monitoring. For example, a level of 2,000 ng/mL is listed for both test types in Table 4, but for clinical testing, the IA cutoff is 3,000 ng/mL, and gas chromatography/mass spectrometry (GC-MS) can detect even trace amounts of opioid and their metabolites. Clinicians must be familiar with the available tests at their institution. Most commonly when monitoring patients that are prescribed pain medications, the IA panel includes the Federal Five plus benzodiazepines, barbiturates, and often methadone as well.

TABLE 4

Federal Five Panel Cutoffs

AnalyteInitial Immunoassay Test Level, ng/mLConfirmatory GC-MS Test Level, ng/mL
Opiates2,0002,000
Cannabinoid5015
Amphetamine500250
Cocaine300150
Phencyclidine2525

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Abbreviation: GC-MS, gas chromatography–mass spectrometry.

The opiate panel with IA tests for opium alkaloids and/or their metabolites, including morphine and codeine.79 Heroin is a semisynthetic opioid that is metabolized to diacetyl morphine and ultimately is detected as morphine.7,8 Other semisynthetic opioids, such as hydrocodone and oxycodone, may or may not be detected by the opiate IA depending on the dose and assay. Synthetic opioids, such as fentanyl, methadone, or meperidine, are not detected by the opiate IA and need to be ordered separately. Table 5 shows opioid classes and their ability to be detected by IA. Clinicians should be familiar with their laboratory assay and know which test needs to be ordered.

TABLE 5

Opioid Classes and Detection by Opiate Immunoassaya

Select Naturals (extracted from opium)Select Semisynthetics (derived from opium sources)Select Synthetics
CodeineHydrocodoneMethadone
MorphineOxycodoneFentanyl
OpiumHydromorphoneMeperidine
OxymorphoneTapentadol
BuprenorphineTramadol
Heroin (detected as morphine)
Detectability by Opiate Immunoassay
YesMay or may not be detected depending on the lab assay and doseNot detected at any level by opiate immunoassay and require their own test
Buprenorphine is not detected on opiate screen

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aThis table contains commonly used opioids and is not meant to be cpmprehensive.

Benzodiazepine IAs often are designed to detect nordiazepam, oxazepam, and temazepam, all of which are metabolites of diazepam. However, benzodiazepine IAs also can detect other drugs that are structurally similar to benzodiazepines.11,12 This means that benzodiazepines are detected based on their ability to cross-react with the IA test. Lorazepam and clonazepam have low cross-reactivity and are generally not detected on benzodiazepine IA.12,13 Therefore, it is not uncommon for patients on lorazepam or clonazepam to test negative for benzodiazepines on this IA. If these patients do test positive at low doses, it could be a concern that they are taking a different benzodiazepine instead of, or in addition to, the prescribed medication.

Amphetamines and methamphetamine are simple molecules that are difficult to develop specific antibodies for; therefore, they carry a high false-positive rate with IA testing. 8 It is important to note that methylphenidate is not detected by the amphetamine IA as it is not an amphetamine.8 The IA for cocaine tests specifically for benzoylecgonine, a metabolite specific to cocaine and has no cross-reactivity.8,12,14

False positives

Due to the lack of specificity of UDM by IA, false positives are common; with the exception of cocaine. Clinicians must obtain a comprehensive medication history of the patient, including over-the-counter medications, herbals, and supplements. Table 6 lists common sources of false positives with UDM by IA.1,8,9

TABLE 6

Substances Tested by Immunoassay and Agents Contributing to False-Positive Results

Substances Tested by ImmunoassayPositive Results (Brand Name)
Amphetamine and methamphetamineAmantadine
Bupropion
Chlorpromazine
Desipramine
Ephedrine
Labetalol
l-methamphetamine (Vick's inhaler)
Phentermine
Phenylephrine
Promethazine
Pseudoephedrine
Ranitidine
Selegiline
Trazodone
BenzodiazepinesOxaprozin
Sertraline
Efavirenz
MethadoneQuetiapine
Verapamil
Marijuana metabolitesDronabinol (Marinol)
Efavirenz
Hemp-containing foods
NSAIDs
PPIs
OpiatesDextromethorphan
Diphenhydramine
Poppy seeds
Quinine
Quinolones
Rifampin
Verapamil
PhencyclidineDextromethorphan
Diphenhydramine
Doxylamine
Ibuprofen
Imipramine
Meperidine
Thioridazine
Tramadol
Venlafaxine
O-desmethylvenlafaxine (Pristiq)

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Abbreviations: NSAID, nonsteriodal anti-inflammatory drugs; PPIs, protein pump inhibitors.

False negatives

A variety of factors can cause false-negative results, including the cross-reactivity of the antibody in the IA, the cutoff concentration that yields a positive result, and/or the time between drug ingestion. As discussed previously, the opiate panel tests for metabolites of morphine, codeine, and heroin, which consequently may lead to semisynthetic/synthetic opioids not being detected.8,11 For example, a patient who was prescribed hydrocodone/acetaminophen 5 mg/325 mg 4 times a day, tests negative for opiates by IA. The negative result is not unexpected because the dose of semisynthetic opioid is too low for detection by IA.

Chromatography

Chromatography generally is reserved for confirmatory or definitive testing when the initial UDM by IA results are unexpected.1 Unlike IA, chromatography can detect the presence of specific drugs and/or metabolites. Types of chromatography testing include GC/MS, liquid chromatography tandem mass spectrometry (LC/MS/MS), and high-performance liquid chromatography. 9 Depending on the specific test, chromatography uses a gas or liquid carrier medium to separate the urine sample’s compounds by their molecular interactions with the carrier medium (mainly by different polarities). During this separation process, all the individual compounds are fed into a mass spectrometer, that ionizes the compounds and detects fragments by using their mass-to-charge ratios. This process allows for the identification of distinct compounds based on their molecular fingerprints.

Gas chromatography/mass spectrometry has remained the standard test for confirmatory testing.1,8 However, it is important to note that LC/MS/MS has been gaining favor over GC/MS. Using LC/MS/MS requires less urine volume to conduct an analysis, and the analysis has a second analytical separation step, thus it is expected to have a lower susceptibility to false results caused by concomitant use of other medications.15,16

Regardless of the test medium, quantitative confirmation through chromatography offers several advantages over IA. It is more accurate, as it can identify small quantities of specific drugs and confirm their presence in urine.8 Also, although there are still cutoff limits associated with chromatography, the specific cutoffs are much lower in value than those in IA tests. Finally, a study conducted in 2010 by Pesce and colleagues found that IA testing was associated with varying rates of false-negative results compared with those of LC-MS/MS.17 Specifically, false-negative rates associated with IA were found to be 22%, 50%, and 23.4% for benzodiazepines, cocaine, and propoxyphene, respectively.17 Unfortunately, chromatography testing methods take longer to produce results and are costly compared with those of IA. Thus, chromatography testing methods typically are reserved for when the IA produces unexpected results. Conversely, IA can be done at point of care with in-office readable cups or strips, or sent out for a 24-hour to 48-hour turnaround time.7,8

Alcohol Testing

Health care providers also could screen for alcohol misuse, which can compromise safe opioid use. Alcohol can accelerate the release of certain sustained-release formulations, causing “dose dumping.”18 Furthermore, alcohol also can increase the risk of opioid-induced respiratory depression. Many laboratories include ethanol that is measured using an enzymatic reaction and generally detected 12 hours after alcohol use.79 Urinary ethanol is not an optimal marker for assessing alcohol use. Ethyl glucuronide (EtG) and ethyl sulfate (EtS) are 2 minor metabolites of ethanol formed by UDP-glucuronosyltransferase.19 These markers can be detected for up to 80 hours after alcohol consumption. Markers for prolonged and/or heavy drinking include but are not limited to phosphatidylethanol, γ-glutamyltransferase, or carbohydrate-deficient transferrin.20

PHARMACOKINETICS/PHARMACOGENETICS

Pharmacokinetics is what the body does with the drug and is measured by absorption, distribution, metabolism, and elimination. 16 Pharmacokinetics ultimately determines the fate of how much and how fast a drug and/or metabolites end up in the urine. It is important to understand the pharmacokinetics to interpret the results of UDM by chromatography as the reported results include parent drugs and metabolites.

Some metabolites of medications available commercially could be mistaken as if the patient were taking a medication that was not prescribed. For example, hydromorphone is a metabolite of hydrocodone and oxymorphone is a metabolite of oxycodone, both of which are commercially available as stand-alone prescriptions. Likewise, oxazepam is commercially available as is temazepam, and both are metabolites of diazepam. Also, it is important to consider patient’s body habitus, which affects volume of distribution, meaning more drug is stored in the periphery and may have a longer detection window.21 Patients with renal and/or hepatic impairment can have reduced clearance of the medications.

It is equally important to consider the role that pharmacogenetic polymorphism can play in UDM, as polymorphisms may impact results.1,8 For example, consider a patient on extended-release oxycodone 30 mg twice daily. Oxycodone is metabolized via cytochrome (CYP) P450 enzyme 3A4 into noroxycodone and, to a much lesser extent, by CYP2D6 into oxymorphone. In this case, if tested by chromatography, the patient’s urine level of oxycodone should be higher than that of either metabolite; specifically, the urine level of noroxycodone should be higher than that of oxymorphone. If there are only concentrations of oxycodone found in the urine with no metabolites, the possible explanations are either the patient dissolved oxycodone into the urine sample without ingestion or the patient may have poor activity of CYP2D6 and CYP3A4 isoenzymes; the latter of which can be confirmed by pharmacogenetic testing. Notwithstanding, drug-drug interactions with CYP inhibitors can produce the same outcome.

CONCLUSION

Urine drug monitoring is an important tool for substance misuse or abuse and adherence to the prescribed regimen. The most commonly used test is UDM by IA due to its low cost and quick results. However, it comes with an array of false-positive and false-negative results. Clinicians should seek definitive results by confirmatory testing prior to making changes that alter patient care, and all results should include discussions with the patient.

Clinical pharmacy specialists are generally an excellent and often untapped resource to provide guidance for interpretation of both IA and chromatographic testing. Clinical pharmacy specialists have an excellent understanding of the physical and medicinal chemistry properties of laboratory testing, a vast understanding of drug metabolites and interactions that might increase or decrease drug concentrations might account for possible false positives and false negatives, and they can help decipher unexpected results.

Finally, it is important to consider that UDM is done for patients and not to patients, with the ultimate goal of improving the safety of the patient and the public. Unexpected results should be discussed with patients to identify the underlying reasons, which may then warrant further intervention, such as definitive testing and ultimate referral to a substance abuse treatment program. Simply sending a discharge or medication discontinuation letter to a patient can create a confrontational situation rather than an educational opportunity for both patient and provider.

Footnotes

Author disclosures

Dr. Fudin reports the following disclosures: Daiichi Sankyo (advisory board); DepoMed (advisory board, speakers bureau); Endo (consultant, speakers bureau); Kaléo (speakers bureau, advisory board); Kashiv Pharma (advisory board); KemPharm (consultant); Pernix Therapeutics (speaker); Remitigate, LLC (owner); and Scilex Pharmaceuticals (consultant).

Disclaimer

The opinions expressed herein are those of the authors and do not necessarily reflect those of Federal Practitioner, Frontline Medical Communications Inc., the US Government, or any of its agencies. This article may discuss unlabeled or investigational use of certain drugs. Please review the complete prescribing information for specific drugs or drug combinations—including indications, contraindications, warnings, and adverse effects—before administering pharmacologic therapy to patients.

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