Dried Blood Spot Measurement: Application in Tacrolimus Monitoring Using Limited Sampling Strategy and Abbreviated Auc Estimation

Cheung, ST; Heijden, J. van der; Hoogtanders, K.; Christiaans, Maarten H. L.; Chau, Ka-Foon; Li, C S.; Hooff, J van; Stolk, L. M. L.

doi:10.1097/01.tp.0000331126.42103.63

Cited by 29 publications

(49 citation statements)

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“…Thus, a comparison is recommended as part of the assay method validation. A good correlation between the data from both the DBS and venous blood methods defi nitely provides further confi dence in quantitative analysis (Cheung et al, 2008;Garcia Boy et al, 2008;Hoogtanders et al, 2007;Koal et al, 2005;van der Heijden et al, 2009).…”

Section: Dbs Vs Venous Bloodmentioning

confidence: 99%

“…DBS samples can be promptly taken whenever a concentrationrelated side eff ect appears. The obtained analytical results might lead to a necessary adjustment of dose or dose regimen (Cheung et al, 2008;Wilhelm et al, 2009).…”

Section: Clinical Study and Therapeutic Drug Monitoringmentioning

confidence: 99%

“…As listed in Table 1, DBS-LC-MS/MS has been increasingly employed in clinical study and therapeutic drug monitoring for the analysis of a wide spectrum of drug molecules, including antipyretic (Spooner et al, 2009), antitussive (Liang et al, 2009), antimalarial (Burhenne et al, 2008), anticonvulsant (la Marca et al, 2009, antiretroviral (Koal et al, 2005;ter Heine et al, 2008ter Heine et al, , 2009a, immunosuppressant (Cheung et al, 2008;Hoogtanders et al, 2007;Wilhelm et al, 2009), antiepileptic (la Marca et al, 2008b and vinca alkaloids (Damen et al, 2009), and in monitoring drug abuse (Henderson et al, 1997;Garcia Boy et al, 2008). Because DBS samples could be collected by patients themselves or their guardians with minimum training, this opens up the possibilities of collecting clinical pharmacokinetic samples not only from various in-patients, but also from out-patients, especially those from remote areas (Burhenne et al, 2008).…”

Section: Clinical Study and Therapeutic Drug Monitoringmentioning

confidence: 99%

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Dried blood spot sampling in combination with LC‐MS/MS for quantitative analysis of small molecules

Li¹,

Tse²

2009

Biomedical Chromatography

542

428

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The collection of whole blood samples on paper, known as dried blood spot (DBS), dates back to the early 1960s in newborn screening for inherited metabolic disorders. DBS off ers a number of advantages over conventional blood collection. As a less invasive sampling method, DBS off ers simpler sample collection and storage and easier transfer, with reduced infection risk of various pathogens, and requires a smaller blood volume. To date, DBS-LC-MS/MS has emerged as an important method for quantitative analysis of small molecules. Despite the increasing popularity of DBS-LC-MS/MS, the method has its limitations in assay sensitivity due to the small sample size. Sample quality is often a concern. Systematic assessment on the potential impact of various blood sample properties on accurate quantifi cation of analyte of interest is necessary. Whereas most analytes may be stable on DBS, unstable compounds present another challenge for DBS as enzyme inhibitors cannot be conveniently mixed during sample collection. Improvements on the chemistry of DBS card are desirable. In addition to capturing many representative DBS-LS-MS/MS applications, this review highlights some important aspects of developing and validating a rugged DBS-LC-MS/MS method for quantitative analysis of small molecules along with DBS sample collection, processing and storage.

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Section: Dbs Vs Venous Bloodmentioning

confidence: 99%

Section: Clinical Study and Therapeutic Drug Monitoringmentioning

confidence: 99%

Section: Clinical Study and Therapeutic Drug Monitoringmentioning

confidence: 99%

See 1 more Smart Citation

Dried blood spot sampling in combination with LC‐MS/MS for quantitative analysis of small molecules

Li¹,

Tse²

2009

Biomedical Chromatography

542

428

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“…In comparison with previously described LC-MS/MS assays to quantify tacrolimus in dried bloods spots [29][30][31][32][33][34]36,39,41,42 , the present assay matches or exceeds their performance in terms of lower limit of quantification, extraction recovery, accuracy and precision while avoiding potentially risky concepts such as one-step protein precipitation procedures and ultra-short chromatography times, which usually give acceptable results during the validation based on blood samples from healthy individuals. However, transplant patients are a highly complex group of patients who have diseases that affect the composition of blood and who take multiple medications.…”

Section: Discussionmentioning

confidence: 99%

“…After a simple finger stick the patient collects a blood drop on a special filter paper card and after the blood spot has dried, it can be mailed to a central laboratory for analysis of tacrolimus and any other immunosuppressant that the patient may currently be taking. This has become possible due to the development of highly sensitive and specific LC-MS/MS assays for the quantification of tacrolimus and other immunosuppressants in very small blood volumes such as dried blood spots (typically 20 µl of blood) 25,[29][30][31][32][33][34][35][36][37][38][39][40][41][42][43] . Another advantage is that minimally invasive, low volume sample collection strategies such as dried blood spots greatly facilitate therapeutic drug monitoring and pharmacokinetic studies in small children 28 .…”

Section: Introductionmentioning

confidence: 99%

Quantification of the Immunosuppressant Tacrolimus on Dried Blood Spots Using LC-MS/MS

Shokati

Bodenberger

Gadpaille

et al. 2015

JoVE

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The calcineurin inhibitor tacrolimus is the cornerstone of most immunosuppressive treatment protocols after solid organ transplantation in the United States. Tacrolimus is a narrow therapeutic index drug and as such requires therapeutic drug monitoring and dose adjustment based on its whole blood trough concentrations. To facilitate home therapeutic drug and adherence monitoring, the collection of dried blood spots is an attractive concept. After a finger stick, the patient collects a blood drop on filter paper at home. After the blood is dried, it is mailed to the analytical laboratory where tacrolimus is quantified using high-performance liquid chromatography-tandem mass spectrometry (HPLC-MS/MS) in combination with a simple manual protein precipitation step and online column extraction.For tacrolimus analysis, a 6-mm disc is punched from the saturated center of the blood spot. The blood spot is homogenized using a bullet blender and then proteins are precipitated with methanol/0.2 M ZnSO 4 containing the internal standard D 2, 13 C-tacrolimus. After vortexing and centrifugation, 100 µl of supernatant is injected into an online extraction column and washed with 5 ml/min of 0.1 formic acid/acetonitrile (7:3, v:v) for 1 min. Hereafter, the switching valve is activated and the analytes are back-flushed onto the analytical column (and separated using a 0.1% formic acid/acetonitrile gradient). Tacrolimus is quantified in the positive multi reaction mode (MRM) using a tandem mass spectrometer.The assay is linear from 1 to 50 ng/ml. Inter-assay variability (3.6%-6.1%) and accuracy (91.7%-101.6%) as assessed over 20 days meet acceptance criteria. Average extraction recovery is 95.5%. There are no relevant carry-over, matrix interferences and matrix effects. Tacrolimus is stable in dried blood spots at RT and at +4 °C for 1 week. Extracted samples in the autosampler are stable at +4 °C for at least 72 hr. Video LinkThe video component of this article can be found at

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Development and validation of a sensitive LC‐MS/MS method for determination of tacrolimus on dried blood spots

Cao

Huang

et al. 2012

Biomedical Chromatography

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A bioanalytical method for the quantification of tacrolimus (TAC) on dried blood spots (DBS) using liquid chromatography, electrospray ionization coupled with tandem mass spectrometry (LC-ESI-MS/MS) was developed and validated. It involves solvent extraction of a punch disk of DBS followed by liquid-liquid extraction. The analyte and the internal standard (IS, ascomycin) were separated on a phenyl column using an isocratic mobile phase elution at a flow rate of 0.3 mL/min. The assay was linear from 1 to 80 ng/mL. The mean recovery of TAC was 76.6%. Intra-assay, inter-assay imprecision and biases were all less than 15%. TAC on DBS was stable for at least 10 days at room temperature, and at least 24 h at 50°C. A chromatographic effect of the filter paper (Whatman 903) was not detected. The volume of blood (15-50 μL) and hematocrit of blood (ranging from 23.2 to 48.6%) did not show a significant influence on detection of TAC concentration by DBS-LC-MS/MS. Fifty samples from patients were detected by both DBS-LC-MS/MS and microparticle enzyme-linked immunoassay (MEIA). TAC concentrations measured by DBS-LC-MS/MS method tended to be lower than those by MEIA.

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Dried Blood Spot Measurement: Application in Tacrolimus Monitoring Using Limited Sampling Strategy and Abbreviated Auc Estimation

Cited by 29 publications

References 0 publications

Dried blood spot sampling in combination with LC‐MS/MS for quantitative analysis of small molecules

Dried blood spot sampling in combination with LC‐MS/MS for quantitative analysis of small molecules

Quantification of the Immunosuppressant Tacrolimus on Dried Blood Spots Using LC-MS/MS

Development and validation of a sensitive LC‐MS/MS method for determination of tacrolimus on dried blood spots

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