A high-throughput U-HPLC–MS/MS assay for the quantification of mycophenolic acid and its major metabolites mycophenolic acid glucuronide and mycophenolic acid acyl-glucuronide in human plasma and urine

Therapeutic use of mycophenolic acid (MPA) is steadily on the rise in combination with other immunosuppressant drugs in transplantation patients. The biotransformation of MPA resulted in the formation of glucuronide metabolites, MPAG and AcMPAG. There are a plethora of assays validated for the analysis of MPA alone or with MPAG/AcMPAG in various biological specimens including plasma/serum, urine, ultrafiltrate, saliva, PBMC, dried blood spots, tissue extract, tumor biopsies and vitreous humor. Based on the need for experimental work, a proper choice of the assay and internal standard may be made using the choices in the literature. While the chemical methods involving high-performance liquid chromatography (HPLC) or LC coupled with triple quadrupole mass spectrometry (LC-MS/MS) are popular, enzymatic assays, in spite of their higher bias, have been used for the routine drug monitoring of MPA. The objectives of the present review are: (a) to provide a focused systematic compilation of the HPLC or LC-MS/MS methods for MPA, MPAG and/or AcMPAG published in the last decade (2005 to current) to enable visual comparison of the methods; (b) to compare and contrast a few enzymatic assays with those of the chemical methods; and (c) to discuss relevant issues/limitations and perspectives on select assays under various subheadings.

Section: Discussionmentioning

confidence: 99%

A comprehensive review of the published assays for the quantitation of the immunosuppressant drug mycophenolic acid and its glucuronidated metabolites in biological fluids

Syed

Srinivas²

2016

“…Several assays have been reported for the analysis of MPA and its metabolites by LC-MS/MS in different matrices (Benech et al, 2007;Brandhorst et al, 2006;Delavenne et al, 2011;Heinig et al, 2010;Kawanishi et al, 2015;Klepacki et al, 2012;Kuhn et al, 2009;Laverdiere et al, 2012;Md Dom et al, 2014;Shen et al, 2009;Upadhyay et al, 2014;Wiesen et al, 2012). However, relatively few assays are available for simultaneous quantification of MPA and its glucuronide metabolites with sufficient sensitivity for AcMPAG, which has a relatively low abundance in comparison with MPAG.…”

Section: Introductionmentioning

confidence: 99%

Simultaneous quantification of mycophenolic acid and its glucuronide metabolites in human plasma by an UPLC–MS/MS assay

Zhang

Chow

Renbarger

2016

The aim of this study was to develop a reliable UPLC-MS/MS assay for accurate quantification of mycophenolic acid (MPA) and its glucuronide conjugates in human plasma. Plasma proteins were precipitated with acetonitrile and the chromatographic separation was achieved on a C18 column with a gradient elution. The detection was performed by a triple quadrupole mass spectrometer in the positive electrospray ionization and multiple reaction monitoring mode. Linearity of the assay was demonstrated over the range of 20-10,000 ng/mL for MPA and MPA glucuronide (MPAG), and 2-1000 ng/mL for acyl MPA glucuronide in human plasma. The assay was precise and accurate with coefficient of variation and bias <15%. MPA and MPAG were stable at 25 °C up to 1 day in both heparin- and EDTA-treated blood. In heparin- and EDTA-plasma, MPA and MPAG were stable for at least 1 week at 25 and 4 °C, and 1 month at -20 °C. However, 99% acyl MPA glucuronide degraded in both heparin- and EDTA-blood as well as plasma when stored at room temperature for 1 day. All the analytes remained stable for at least 3 months in acidified EDTA-plasma at -80 °C. The assay was successfully applied on patients post hematopoietic stem cell transplantation. Copyright © 2016 John Wiley & Sons, Ltd.

“…The incorporation of a chip‐based high‐field asymmetric waveform ion mobility spectrometry (FAIMS) separation in the ultra (high)‐performance liquid chromatography–high resolution mass spectrometry (UHPLC–HRMS) for determination of the ( R / S ) ibuprofen 1‐ O ‐acyl glucuronide metabolite in urine has also been reported (Smith et al, ). Analytical methods for acyl glucuronide metabolites quantitation are listed in Table (Klepacki et al, ; Surendradoss et al, ; Liu & Smith, ; Luigi et al, ; Mano et al, ; Merrigan, Kish‐Trier, Seegmiller, & Johnson‐Davis, ; Qiang & Zhang, ; Schwartz, Desai, Bi, Miller, & Matuszewski, ; Smith et al, ; Zhou et al, ).…”

Section: Sample Processingmentioning

confidence: 99%

Bioanalytical challenges and strategies for accurately measuring acyl glucuronide metabolites in biological fluids

Patel

2019

Bioanalysis of unstable compounds such as acyl glucuronide metabolites represents a great analytical challenge owing to poor analyte stability in biological matrices. The primary goal for bioanalytical assay development is to minimize the breakdown of acyl glucuronide metabolite into its parent aglycone during sample collection, transportation, storage and analysis. Samples need to be stabilized ex vivo immediately after sample collection to minimize potential breakdown and thus to ensure accurate concentration measurement of both acyl glucuronide metabolite and its parent aglycone. In this review paper, formation of acyl glucuronide metabolites, the importance of establishing acyl glucuronide exposure measurement and safety coverage, optimization of sample pretreatment to stabilize the acyl glucuronide metabolites, current analytical strategy of assaying them as well as considerations for regulatory filings are discussed. It is important to identify acyl glucuronide metabolites that are capable of undergoing hydrolysis and pH‐dependent intra‐molecular migration as well as covalently binding to plasma and tissue proteins which can cause toxicity in vivo in the early stages of drug development. Carefully planning analytical experiments, identifying structures of acyl glucuronides and monitoring their concentrations in early drug development can help assess the risks associated with their exposures and potentially predict their concentrations in human circulation.