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1.
ACS Sens ; 9(2): 781-788, 2024 02 23.
Article in English | MEDLINE | ID: mdl-38244038

ABSTRACT

The primary treatment for glaucoma, the most common cause of intermediate vision impairment, involves administering ocular hypotensive drugs in the form of topical eye drops. Observing real-time changes in the drugs that pass through the cornea and reach the anterior chamber of the eye is crucial for improving and developing safe, reliable, and effective medical treatments. Traditional methods for measuring temporal changes in drug concentrations in the aqueous humor employ separation analyzers such as LC-MS/MS. However, this technique requires multiple measurements on the eyes of various test subjects to track changes over time with a high temporal resolution. To address this issue, we have developed a measurement method that employs boron-doped diamond (BDD) microelectrodes to monitor real-time drug concentrations in the anterior chamber of the eye. First, we confirmed the electrochemical reactivity of 13 antiglaucoma drugs in a phosphate buffer solution with a pH of 7.4. Next, we optimized the method for continuous measurement of timolol maleate (TIM), a sympathetic beta-receptor antagonist, and generated calibration curves for each BDD microelectrode using aqueous humor collected from enucleated porcine eyes. We successfully demonstrated the continuous ex vivo monitoring of TIM concentrations in the anterior chambers of these enucleated porcine eyes. The results indicate that changes in intracameral TIM concentrations can be monitored through electrochemical measurements using BDD microelectrodes. This technique holds promise for future advancements in optimizing glaucoma treatment and drug administration strategies.


Subject(s)
Antiglaucoma Agents , Glaucoma , Swine , Animals , Humans , Boron , Microelectrodes , Chromatography, Liquid , Tandem Mass Spectrometry , Timolol , Glaucoma/drug therapy , Diamond
2.
Anal Chem ; 92(20): 13742-13749, 2020 10 20.
Article in English | MEDLINE | ID: mdl-32786440

ABSTRACT

Methylcobalamin, which is used for the clinical treatment of patients with neuropathy, can have an impact on the sensorineural components associated with the cochlea, and it is possible that the auditory threshold in a certain population of patients with deafness may be recovered. Nonetheless, it remains uncertain whether the action site of methylcobalamin is localized inside or outside the cochlea and which cellular or tissue element is targeted by the drug. In the present work, we developed a method to realize in vivo real-time simultaneous examination of the drug kinetics in two separate locations using boron-doped diamond microelectrodes. First, the analytical performance of methylcobalamin was studied and the measurement protocol was optimized in vitro. Then, the optimized protocol was applied to carry out real-time measurements inside the cochlea and the leg muscle in live guinea pigs while systemically administering methylcobalamin. The results showed that the methylcobalamin concentration in the cochlea was below the limit of detection for the microelectrodes or the drug did not reach the cochlea, whereas the compound clearly reached the leg muscle.


Subject(s)
Electrochemical Techniques/methods , Vitamin B 12/analogs & derivatives , Animals , Boron/chemistry , Cochlea/chemistry , Cochlea/metabolism , Diamond/chemistry , Guinea Pigs , Limit of Detection , Microelectrodes , Muscle, Skeletal/chemistry , Muscle, Skeletal/metabolism , Vitamin B 12/analysis , Vitamin B 12/metabolism
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