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Quantitative Mass Spectrometry Imaging by Targeted-DESI-MSI in MRM Mode Provides Higher Sensitivity and Specificity for Fast Quantification of Chloroquine Drug in Mice Kidney. | LitMetric

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Article Abstract

Quantitative mass spectrometry imaging (QMSI) is being applied for spatial quantification of drugs and metabolites using mass spectrometry imaging (MSI) tools. DESI-MSI is ideally suited to QMSI as a soft and ambient ionization technique. However, some challenging issues of QMSI include extraction efficiency, matrix effect, sensitivity, and specificity, which need to be addressed. Here, we applied targeted DESI-MSI in multiple reaction monitoring (MRM) mode for QMSI of chloroquine, an antimalarial drug, as a model in mice kidneys and carefully addressed those challenging issues. A triple quadrupole mass spectrometer coupled with a DESI source was used to quantify the chloroquine (transition m/z 320.2 → 247.1) drug. A deuterated internal standard chloroquine-d (transition m/z 325.2 → 147.1), was used to normalize the data from pixel to pixel. A mimetic in-tissue model was employed to constract a calibration curve demonstrating good linearity (y = 0.0041x, R = 0.9953) and precision (RSD < 15%). The calibration curve was validated by back-calculation, with results falling within acceptable ranges (accuracy error< ±15%). Finally, the dosed (30 mg/kg) chloroquine was quantified in three spatial regions (cortex, medulla, and pelvis) in the mice kidneys. The highest concentrations of chloroquine in the pelvis (399.85 and 436.28 ng/mg of kidney tissue at 30 and 60 min intervals) region is consistent with the previous report that a portion of the drug is eliminated from the kidney as unchanged forms. This study provides valuable insights into using DESI-MSI in MRM mode for the QMSI of drugs in biological tissues and will have implications for future research on pharmacology and toxicology.

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http://dx.doi.org/10.1002/jms.5148DOI Listing

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