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Clinical toxicology: What? Who? How well is it done?

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Clinical toxicology: What? Who? How well is it done? Dr Ian D Watson University Hospital Aintree LIVERPOOL L9 7AL Laboratory Investigations Confirm poisoning ... – PowerPoint PPT presentation

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Title: Clinical toxicology: What? Who? How well is it done?


1
Clinical toxicology What? Who? How well is it
done?
  • Dr Ian D Watson
  • University Hospital Aintree
  • LIVERPOOL L9 7AL

2
Laboratory Investigations
  • Confirm poisoning diagnosis
  • Patient management
  • Investigations
  • Antidotes or enhance elimination
  • Brain death
  • Re-start chronic therapy
  • Medico-legal

3
UK Guidelines on Analytical Toxicology Practice
  • Joint UK Guidelines National Poisons Information
    Service Association of Clinical Biochemists.
  • Annals Clin. Biochem. 200239 328-339

4
Recommended 24 hour chemistry test availability
  • FBC
  • Sodium, potassium, urea, creatinine
  • Glucose
  • Calcium, albumin, magnesium
  • INR
  • Bilirubin, ALT or AST, GGT, ALP
  • Anion Gap (chloride and bicarbonate)
  • Plasma osmolality (osmolar gap)
  • Creatine kinase

5
NPIS/ACB Toxicology Group12 hour turnaround 1
  • Carboxyhaemoglobin
  • Digoxin
  • Ethanol
  • Iron
  • Lithium
  • Methaemoglobin

6
NPIS/ACB Toxicology Group12 hour turnaround 2
  • Paracetamol
  • Paraquat qualitative urine screen
  • Salicylate
  • Theophylline

7
NPIS/ACB Toxicology Group 2Specialist Assays 1
  • Acetylcholinesterase 6h
  • Arsenic 24h
  • Carbamazepine 2h
  • Ethylene glycol 4h
  • Lead 24h
  • Mercury 24h
  • Methanol 4h

8
NPIS/ACB Toxicology Group 2Specialist Assays 2
  • Methotrexate 24h
  • Paraquat quantitative plasma assay 24h
  • Phenobarbital 4h
  • Phenytoin 2h
  • Thyroxine 24h
  • Toxicology screen as required

9
Who?
  • Specialist Toxicology laboratories 35
  • General Clinical Biochemists with a Special
    interest in Toxicology 25
  • General Clinical Biochemists 40

10
How well is Toxicology done?
  • Clinicians access to service
  • NPIS/ACB turnaround times
  • Analytical performance
  • UKNEQAS data
  • Quality of interpretation
  • UKNEQAS Toxicology cases

11
?Impact of NPIS/ACB advice
  • Questionnaire via UKNEQAS for Drug Assays
    General Clinical Chemistry 2002 prior to
    publication of Guidelines
  • Repeat questionnaire in early 2004,
  • 18 months post publication

12
Analytical performance 1
13
Analytical Performance 2
14
Analytical Performance 3
15
Routine 24 hour availability 1
16
Routine 24 h availability 2
17
Routine 24h availability 3
18
Group 1 availability
On Site

19
Group 1 turnaround times

20
Group 1 turnaround timesout-of-hours

21
Group 2 analyte availability 1

22
Group 2 analyte turnaround time 1
In hours
23
Group 2 availability 2
On site
24
Group 2 availability 3
On Site

25
Group 2 turnaround times 3

26
Urine DOA availability
In hours

27
DOA turnaround times
In hours

28
Mean Lab Score
Std. Dev 4.26 Mean 10.0 N 76.00
n
1.0 3.0 5.0 7.0
9.0 11.0 13.0 15.0
17.0
Score
29
Mean lab score gt 4 samples
Std.Dev 4.06 Mean 9.9 N 48.00
n
1.0 3.0 5.0 7.0
9.0 11.0 13.0 15.0
17.0
Score
30
Mean Score
31
LABS MEAN SCORE OF LAST 4 SCORES
32
Summary Count Sum Average Variance
1 31 278 8.97 15.77
2 31 318 10.26 55.73
3 31 367 11.84 12.74
4 31 323 10.42 16.72
5 31 333 10.74 15.60
6 31 287 9.26 14.73
7 31 322 10.39 37.38
33
Observations
  • Change following NPIS/ACB guidance
  • Ethylene Glycol/Methanol service appears most
    improved
  • Labs concentrate on the readily available.
  • Analytical performance for unusual analytes poor
  • Those that are poor interpreters are dropping out
    of Toxicology Case Scheme

34
Other Issues
  • Point of Care device performance and use needs
    assessed
  • Toxicology Case scheme for Panel approval
  • NPIS want standardisation of drug concentration
    units. How can we approach this?

35
Thanks to
  • UKNEQAS for General Clinical Chemstry Dave
    Bullock and for Drug Assays John Wilson
  • Michelle Robinson for secretarial assistance
  • Rob Lewis for data handling
  • Ceridwen Dawkins assisted with the audit
    formulation

36
Discussion arising from presentation 1
  • Q Guideline turnaround times ACB weakly
    accepted with no Evidence Base
  • A Comment only applies to Specialist assays.
    Those with 2h or 24h turnaround are either
    readily available eg phenytoin or are needed for
    differential eg mercury. Cholinesterase and
    methanol/ethylene glycol are metabolic
    emergencies.

37
Discussion arising from presentation 2
  • Q Audience vote for which units.
  • A majority abstained, of voters large majority
    for molar units. No strategy to address how to
    change, nor how to ensure adoption. Needs an
    evidence based approach?
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