Chemical upcycling of polystyrene
into targeted small molecules
is desirable to reduce plastic pollution. Herein, we report the upcycling
of polystyrene to benzoyl products, primarily benzoic acid, using
a catalyst-controlled photooxidative degradation method. FeCl3 undergoes a homolytic cleavage upon irradiation with white
light to generate a chlorine radical, abstracting an electron-rich
hydrogen atom on the polymer backbone. Under the oxygen-rich environment,
high MW polystyrene (>90 kg/mol) degrades down to <1 kg/mol
and
produces up to 23 mol % benzoyl products. A series of mechanistic
studies showed that chlorine radicals promoted the degradation via
hydrogen-atom abstraction. Commercial polystyrene degrades efficiently
in our method, showing the compatibility of our system with polymer
fillers. Finally, we demonstrated the potential of scaling up our
approach in a photoflow process to convert gram quantities of PS to
benzoic acid.
Diuretics are commonly used to control edema across various clinical fields. Diuretics inhibit sodium reabsorption in specific renal tubules, resulting in increased urinary sodium and water excretion. Loop diuretics are the most potent diuretics. In this article, we review five important aspects of loop diuretics, in particular furosemide, which must be considered when prescribing this medicine: (1) oral versus intravenous treatment, (2) dosage, (3) continuous versus bolus infusion, (4) application in chronic kidney disease patients, and (5) side effects. The bioavailability of furosemide differs between oral and intravenous therapy. Additionally, the threshold and ceiling doses of furosemide differ according to the particular clinical condition of the patient, for example in patients with severe edema or chronic kidney disease. To maximize the efficiency of furosemide, a clear understanding of how the mode of delivery will impact bioavailability and the required dosage is necessary.
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