Microsoft word - food and drug interactions with udt.doc
Pain Physician: March/April 2011; 14:123-143
spectrometry (LC/MS/MS) or high performance liquid
samples showed that 75% of patients were unlikely
chromatography (HPLC). Enzyme-mediated immuno-
to be taking their medications in a manner consis-
assay (EIA) is frequently used as the initial evaluation
tent with their prescribed pain regimen (158). This
for UDT, which can test for numerous drugs or drug
evaluation showed that 38% of patients were found
classes, and can determine if a class of substances is
to have no detectable level of their prescribed medi-
present or Fo
EI cAtsiodns
o intshtr P
at oe int-of-Car
cation, e Ur
a ug Tests:
adequate sensitivity but are not specific. They cannot
ent, 27% had a drug level higher than expected, 15%
equivocally identify a specific analyte and can result
had a drug level lower than expected, and 11% had
in false-negatives by missing compounds such as oxy-
illicit drugs detected in the urine (158). Further, it has
• Quinolone antibiotics (ex. levofloxacin,
codone, methadone, and fentanyl (195,196). c
they also fail to distinguish between diffe •r en D
of the same class (e.g., opioids) and can produce
to 50 μg /L increased efficiencies and sensitivities for
false-positive results from cross-reactivity with other
all immunoassays, with minor decreases in specific-
substances (e.g., quinolone antibiotics or any com-
ity (198). Consequently, the cutoff levels, which have
pound with similar structural and chemical properties
been reduced to 20 and 15, further increases true-
to the original substance). Table 3 illustrates various
drug cross-reactants. In addition, EIAs exhibit cross-
To identify individual drugs and metabolites, lab-
reactivity with other commonly available medications
oratory testing is recommended. Thus, a urine screen
that is positive for hydromorphone in a patient re-
g is required when an ceiving hydrocodone does not reflect drug abuse, but
immunoassay is initially used and provides • bo T
igh rather the appropriate metabolite of hydrocodone.
sensitivity and high specificity to reduce • Bupropi
false-posi- on Similarly, since codeine is metabolized to morphine, a
• Desipramines creen that is positive for morphine in a patient taking
Multiple publications have shown not• onA
h ne codeine would be expected (199). Historically, there
rates of inappropriate drug use in the ch•r onRa
n have been instances in which physicians who were
population, but also have identified multi •
s not familiar with opioid metabolism have wrongly ac-
for confirmatory testing along with diff •
pat ients of drug abuse (197). Table 4 illustrates
cutoff levels. Further, metabolic variation • Vicks Vapor Inhaler
metabolites of opioids (199,200). In addition, preva-
suggested for confirmatory testing (197). • Oxaprozin (Daypro)
lence of morphine metabolism to hydromorphone in
spective analysis of screening for non-compliance, in
chronic pain patients treated with morphine also has
the data collected in almost a million patients, test
been established (197). It is also essential to note that
Drug Cross-Reactants
Poppy seeds, chlorpromazine, rifampin, dextromethorphan quinine
Ephedrine, methylphenidate, trazodone, bupropion, desipramine, amantadine, ranitidine,
Chlorpromazine, thioridazine, meperidine, dextromethorphan, diphenhydramine, doxylamine
Gas chromatography should confirm all positives; screening detects a presence or absence, not the concentration. Drug tests are not quantitative.
Source: Manchikanti L, et al. Protocol for accuracy of point of care (POC) or in-office urine drug testing (Immunoassay) in chronic pain patients:
A prospective analysis of immunoassay and liquid chromatography tandem mass spectometry (LC/MS/MS). Pain Physician 2010; 13:E1-E22 (49).
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