Fiona A Wicks scite author profile

Fiona A Wicks

3Publications

20Citation Statements Received

22Citation Statements Given

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Affiliations

Queen Elizabeth Hospital, Bioanalytica (Switzerland)

Publications

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Comparison of the Reintroduced MEIA® Assay With HPLC-MS/MS for the Determination of Whole-Blood Sirolimus From Transplant Recipients

Morris¹,

Salm²,

Taylor³

et al. 2006

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Therapeutic monitoring with dosage individualization of sirolimus drug therapy is standard clinical practice for organ transplant recipients. For several years sirolimus monitoring has been restricted as a result of lack of an immunoassay. The recent reintroduction of the microparticle enzyme immunoassay (MEIA) for sirolimus on the IMx analyser has the potential to address this situation. This study, using patient samples, has compared the MEIA sirolimus method with an established HPLC-tandem mass spectrometry method (HPLC-MS/MS). An established HPLC-UV assay was used for independent cross-validation. For quality control materials (5, 11, 22 microg/L), the MEIA showed acceptable validation criteria based on intra- and inter-run precision (CV) and accuracy (bias) of <8% and <13%, respectively. The lower limit of quantitation was found to be approximately 3 microg/L. The performance of the immunoassay was compared with HPLC-MS/MS using EDTA whole-blood samples obtained from various types of organ transplant recipients (n = 116). The resultant Deming regression line was: MEIA =1.3 x HPLC-MS/MS + 1.3 (r = 0.967, S(y/x) = 1) with a mean bias of 49.2% +/- 23.1% (range, -2.4% to 128%; P<0.001). The reason for the large and variable bias was not explored in this study, but the sirolimus-metabolite cross-reactivity with the MEIA antibody could be a substantive contributing factor. Whereas the MEIA sirolimus method may be an adjunct to sirolimus dosage individualization in transplant recipients, users must consider the implications of the substantial and variable bias when interpreting results. In selected patients where difficult clinical issues arise, reference to a specific chromatographic method may be required.

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Comparison Of The Re-introduced MEIA?? Sirolimus Assay With HPLC-MSMS In Renal Transplant Recipients

Morris

Taylor

Wicks

et al. 2005

Therapeutic Drug Monitoring

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Measuring the Unbound Concentration Fails to Resolve Analytic Interferences in Digoxin Immunoassays

Morris¹,

Jones²,

Wicks³

et al. 2008

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Therapeutic drug monitoring of digoxin is well established in the clinical management of cardiac patients treated with the drug. Recently, target concentrations have been revised in patients with congestive heart failure to 0.5 to 0.8 microg/L, challenging the sensitivity limits of most immunoassays. These widely used methods are often criticized, particularly on specificity grounds resulting from interference from exogenous and endogenous sources. One solution to remove higher molecular weight interference has been to ultrafilter plasma samples before assaying. The present study included 261 patient digoxin samples and compared two commercial ultrafiltration devices (Centrifree and Micrcon) that share the same separation membrane (YM-30). The results showed widely discordant apparent unbound digoxin concentrations in the ultrafiltrate from these devices with a Deming regression line of Centrifree = 1.31 x Micrcon + 0.042 (95% confidence interval for slope of 1.237 to 1.391) and apparent unbound fractions ranging from 15% to 610% of the unfiltered plasma digoxin concentrations, suggesting that ultrafiltration did not resolve such interference issues. The concept of measuring lower unbound digoxin concentrations as a result of lower therapeutic range for total (bound plus unbound) digoxin will also render most immunoassays insensitive and inappropriately calibrated. There is a strong imperative to review digoxin monitoring practices in the light of current clinical imperatives for both specificity and sensitivity reasons.

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Fiona A Wicks

Comparison of the Reintroduced MEIA® Assay With HPLC-MS/MS for the Determination of Whole-Blood Sirolimus From Transplant Recipients

Comparison Of The Re-introduced MEIA?? Sirolimus Assay With HPLC-MSMS In Renal Transplant Recipients

Measuring the Unbound Concentration Fails to Resolve Analytic Interferences in Digoxin Immunoassays

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