Problems encountered when testing for LSD in a regional medium secure unit

doi:10.1192/pb.27.1.17

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Problems encountered when testing for LSD in a regional medium secure unit

A. J. Acosta-Armas, Specialist Registrar in Forensic Psychiatry

Devon Partnership NHS Trust, Langdon Hospital, Exeter Road, Dawlish, Devon EX7 0NR

Abstract

Top
Abstract
Introduction
Background
Method
Results and discussion
References

AIMS AND METHOD

Between 1998 and 2000, a surprisingly high number of positiveresults was noticed in our regional medium secure unit whentesting for D-lysergic acid diethylamide (LSD). This led toan investigation of possible factors involved. It was feltthat the testing protocol, particularly the use of a single, non-isotopic homogeneous immunoassay without routine furtherconfirmatory testing, was largely to blame for what seemedto be a high incidence of false positives. On two differentoccasions, samples from each patient were sent, on the sameday, to two different laboratories. At the first laboratory,only one test method was used and at the second one test plustwo confirmatory tests were carried out.

RESULTS

Out of a total of 23 patients tested on two separate occasions,the first laboratory gave three positive results the firsttime and three positive results the second, while the secondlaboratory gave only one positive result on the second occasionthat samples were sent and none on the first. This reinforcesthe belief that, without adequate confirmatory analysis, many psychiatric and non-psychiatric prescribed drugs can give falsepositives.

CLINICAL IMPLICATIONS

Positive LSD results should be confirmed by at least one, preferably chromatographic, alternative method. A protocol for testingand reporting LSD in psychiatric patients should be consideredin order to minimise the risk of obtaining false-positive resultswhich have negative clinical, legal and psychological repercussions.

Introduction

Top
Abstract
Introduction
Background
Method
Results and discussion
References

The use of D-lysergic acid diethylamide (LSD), a strong hallucinogenic drug, continues to cause concern within the medical professionand particularly in the field of mental health, because ofits association with different psychiatric conditions, especiallypanic reactions, prolonged schizoaffective psychoses and post-hallucinogenperceptual disorder (Abraham & Aldridge, 1993). Thereis evidence to suggest that its use has increased in past years, particularly by young people (Sankar, 1997; Schwartz, 1995).The use of illicit drugs, including LSD, has a particular relevancein forensic psychiatry because substance misuse has been shown consistently to be a significant risk factor for violence anddisturbed behaviour (Soyka, 2000). LSD was the first synthetichallucinogenic compound, accidentally discovered by a Swisschemist, Albert Hoffman, in 1943. The first systematic studyof the clinical effects of LSD was carried out in 1947 at theUniversity Psychiatric Clinic in Zurich. Its medical use becamepopular in the USA in the 1950s, when it was used to assistpsychotherapy sessions by releasing forgotten memories fromchildhood. Its abuse first appeared in the 1960s when it becamean essential part of the drug scene. In the UK, LSD was proscribedunder the 1971 Misuse of Drugs Act. The LSD that is used onthe streets appears in different forms, usually adsorbed ontomicrodots or paper with colourful designs.

The detection of LSD use is a challenge for toxicology laboratoriesbecause of the very low concentrations of LSD and its metabolitesfound in body fluids. LSD is also relatively unstable and sensitiveto ultraviolet light and heat. Several methods have been developedfor detection of LSD in body fluids, particularly in urine.Such methods include: radioimmunoassays, non-isotopic immunoassays(enzyme-linked immunosorbent assay (ELISA) and enzyme-multiplied immunoassay technique (EMIT)), high performance thin-layer chromatographyand gas or liquid chromatography linked to mass spectrometry.Recently, homogeneous immunoassays have become more popularbecause they are easier to perform and they produce resultsmore quickly. Unfortunately, they are associated with lackof sensitivity and, in particular, lack of specificity (Liu, 1995).

A very high incidence of positive LSD results (between 4.5%and 9%) were being found in our patient population, sometimesin cases where it was very unlikely that any illicit drugshad been taken. The interference of other prescribed and non-prescribeddrugs in testing for LSD has been documented (Ritter et al,1997; Rohrich et al, 1998), although little research has beendone and the information available is sparse.

This small piece of research is important because there seemsto be little understanding and knowledge of drug-testing, particularlyabout possible interference by drugs commonly prescribed inpsychiatry, and our work shows how easy it can be to give afalse-positive result unless these potential problems are takeninto consideration. The repercussions of a false-positive resulton any patient, particularly within our type of service, couldbe quite detrimental for future decision-making and, hence,their future clinical management, so it is even more importantto ensure that the risks of false-positive results are minimised.

Background

Top
Abstract
Introduction
Background
Method
Results and discussion
References

Around February 1998, there was increasing concern in our regional medium-secure psychiatric unit about the use of LSD by in-patientsand its effect on their mental state, particularly when a positiveresult was obtained after a significant deterioration in apatient's condition. Towards the end of that year, over a periodof almost 2 months, there were six positive results involvingfive patients from a total population of approximately 22, although not everybody on the wards was tested at the same time. Duringthe following 3 months, 10 more positive results were obtained,involving 7 patients in the unit. This led to great concernamong members of the medical, nursing and managerial staffwho decided to introduce random blanket-testing for all patientsin the unit from April 1999. Five blanket-testing sessions were conducted between April and May 1999 with two positive resultsout of a total of 22 patients (9%) in the first session, andone positive result (4.5%) in the second. The three followingblanket-testing sessions gave only negative results in allthe patients tested. Following these negative findings, systematictesting was suspended in June 1999. In February 2000, therewas another significant change in a patient's mental stateand the use of illicit drugs was suspected. One urine samplewas sent for testing and it showed a positive result for LSD.The concerns from the previous year returned and random blanket-testingwas reintroduced in the unit in February, producing two positiveresults out of a total of 22 patients (9%).

By this time, there was a strong suspicion that the incidenceof positive results was too high and that there had to be anexplanation for those findings. We considered various explanations,including the possibility of false-positives because of interferencefrom other substances or prescribed drugs in the test methodused. We also questioned the methodology used by the laboratorywhen carrying out the tests.

The samples taken from our patients were tested in a designatedlaboratory (Laboratory A) in another city because there arefew laboratories around the country which perform LSD tests.The original samples were collected in specific containersand kept refrigerated as required. They were then sent to ourlocal hospital and from there to Laboratory A where the testswere carried out using EMIT, a non-isotopic immunoassay fromDade Behring Diagnostics (2000). The laboratory does not normallyperform confirmatory tests when it has a positive result unlessthis is specifically requested and results are considered tobe positive when they are above a cut-off point of drug concentration.During a telephone discussion, it became clear that they werepartly aware of certain drugs, particularly chlorpromazine,giving false-positive results, but they claimed to have neverpreviously been told that they had produced false-positive results.

Method

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Abstract
Introduction
Background
Method
Results and discussion
References

We began with a literature search, using Medline, the CochraneLibrary and the National Library of Medicine databases, forprevious work done on LSD testing and interference with otherdrugs. We also contacted another laboratory in the UK to determinethe views of other toxicologists on LSD testing. Discussionswith a senior toxicologist at the toxicology department ofanother UK hospital (Laboratory B), which is experienced inLSD testing, confirmed our initial suspicion that certain drugswhich are commonly prescribed in psychiatry can interfere withLSD testing. It appeared that confirmatory tests are essentialto rule out the high incidence of false positives that occurin such cases, particularly when immunoassay is the only testused. We also contacted the manufacturers of the EMIT test andthey provided a list of commonly prescribed drugs that wereknown by them to cause interference in LSD testing using EMIT.

The initial literature search identified numerous papers ondifferent methods of LSD testing, but only two on interferencewith testing for LSD. One paper, by Ritter et al (1997), wasparticularly useful. The other paper, by Rohrich et al (1998),was also useful although their work was done with intensivecare patients only. No systematic reviews had been conductedon this matter, possibly because of the paucity of previousresearch work.

Because of the surprisingly high rate of positive results, wedecided to collect two urine samples from each patient in theunit on two separate occasions and send one sample to the originalreference laboratory (Laboratory A) and the other to LaboratoryB in order to compare the results from each. Each sample wassplit, with one aliquot going to Laboratory A and one to LaboratoryB. We knew that Laboratory A would only perform a simple immunoassay(EMIT II LSD) and that Laboratory B would perform two initial screening tests (a radioimmunoassay, manufactured by CozartBiosciences, and an enzyme-immunoassay, produced by DiagnosticProducts Corporation) plus a confirmatory test (high performanceliquid chromatographic method using fluorometric detection).On two separate occasions, 46 urine samples were taken from23 patients.

Results and discussion

Top
Abstract
Introduction
Background
Method
Results and discussion
References

On the first occasion, three positive results were given byLaboratory A and no positive results by Laboratory B. On thesecond occasion, there were three positive results again fromthe samples sent to Laboratory A and only one positive resultin those sent to Laboratory B.

Two patients tested positive in the samples sent to LaboratoryA on both occasions. The other two positive results were fromtwo different patients. The patient who gave a positive resultwhen the samples were tested by Laboratory B was one of thosetesting positive twice at Laboratory A. Table 1 shows the prescribed drugs being taken by patients when they tested positive forLSD.

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Table 1. Prescribed drugs being taken by patients that tested positive for LSD in Laboratory A¹

According to the list provided by Dade Behring Diagnostics,the manufacturer of the EMIT test, sertraline, chlorpromazineand paroxetine, but not diazepam, can cause cross-reactivityat certain concentration levels when using the EMIT II LSDAssay (Dade Behring Diagnostics, 2000). Folic acid, procyclidine,multivitamins, omeprazole, lithium, ispaghula and risperidonewere not listed.

We could confirm that the LSD EMIT assay was associated witha high rate of false-positive results, particularly when usedin patients from psychiatric settings. It became evident thatin situations where a single type of LSD test is carried out,particularly only the EMIT test, there is a likelihood of more positive results. Since it has been clearly documented thatcertain prescribed drugs can cause drug interference when testingfor LSD, particularly with homogeneous immunoassays, we consideredthat this was the most likely cause of the high number of positiveresults given by the first laboratory, i.e. that the patients'prescribed drugs, or their metabolites, may have been responsiblefor most of the false-positive results by the EMIT test.

We concluded that positive LSD test results should be confirmedby at least one alternative method. We also concluded thatany positive result using a single immunoassay method suchas the EMIT test, should not be accepted as valid without confirmation,particularly in situations where the subjects are taking otherprescribed drugs, as is commonly the case for psychiatric patients.This is particularly important in forensic psychiatric patients, where such findings could have considerable implications infuture management decisions and where the legal aspects oftheir care are much more complex. For that reason, a clearprotocol for LSD testing should be considered as a way of minimisingthe probability of such problems arising in clinical practice. There are considerable clinical, legal and psychological repercussionsof falsely giving a positive result for LSD to a patient.

Further research in this area would be very valuable and clearguidelines are necessary for laboratories and services dealingwith psychiatric patients that need to be tested for LSD andother illicit drugs. This would be particularly important withinthe forensic psychiatric services.

Acknowledgments

I would like to thank Mr Frank Tames for his valuable informationand advice and Dr A. R. Tomison for his support and comments.

References

Top
Abstract
Introduction
Background
Method
Results and discussion
References

ABRAHAM, H. D. & ALDRIDGE, A. M. (1993) Adverse consequences of lysergic acid diethylamide. Addiction, 88, 1327-1324.[CrossRef][Medline]

DADE BEHRING DIAGNOSTICS (2000) Cross-Reactivity List for the Emit II LSD Assay (data on file).

LIU, R. H. (1995) Evaluation of common immunoassay kits for effective workplace drug testing. In Handbook of Workplace Drug Testing, first edition (eds R. H. Liu & B. A. Goldberger), pp. 67-129. Washington D.C.: AACC Press.

RITTER, D., CORTESE, C. M., EDWARDS, L. C., et al (1997) Interference with testing for lysergic acid diethylamide. Clinical Chemistry, 43, 635-637.[Abstract/Free Full Text]

ROHRICH, J., ZORNTLEIN, S., LOTZ, J., et al (1998) False-positive LSD testing in urine samples from intensive care patients. Journal of Analytical Toxicology, 23, 393-395.

SANKAR, D.V.S. (1997) Psychoactive substances LSD — a resurrection. Research Communications in Alcohol and Substances of Abuse, 18, 1-18.

SCHWARTZ, R. H. (1995) LSD: its rise, fall, and renewed popularity among high school students. Pediatric Clinics of North America, 42, 403-413.[Medline]

SOYKA, M. (2000) Substance misuse, psychiatric disorder and violent and disturbed behaviour. British Journal of Psychiatry, 176, 345-350.[Abstract/Free Full Text]

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