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Boronotyrosine, a Borylated Amino Acid Mimetic with Enhanced Solubility, Tumor Boron Delivery, and Retention for the Re-emerging Boron Neutron Capture Therapy Field

Arthur Raitano,Tioga Martin,Chunying Zhang, Maria-Christina Malinao,Linnette Capo,Maki Ikeura, Rebecca Carroll, Jason C. Quintana,Samkeliso Dlamini, Leila Kulenovic, Eva Jahanshir, Sohye Kang,Karen Morrison,Michael Torgov,Kendall Morrison

Journal of medicinal chemistry(2023)

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Abstract
Boron neutron capture therapy (BNCT) is a re-emerging binary cellular level cancer intervention that occurs through the interaction of a cancer-specific 10boron (10B) drug and neutrons. We created a new 10B drug, 3-borono-l-tyrosine (BTS), that improves on the characteristics of the main historical BNCT drug 4-borono-l-phenylalanine (BPA). BTS has up to 4 times greater uptake in vitro than BPA and increased cellular retention. Like BPA, BTS uptake is mediated by the l-type amino acid transporter-1 (LAT1) but is less sensitive to natural amino acid competition. BTS can be formulated and bolus dosed at much higher levels than BPA, resulting in 2-3 times greater boron delivery in vivo. Fast blood clearance and greater tumor boron delivery result in superior tumor-to-blood ratios. BTS boron delivery appears to correlate with LAT1 expression. BTS is a promising boron delivery drug that has the potential to improve modern BNCT interventions.
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Key words
tumor boronotyrosine delivery,borylated amino acid mimetic,re-emerging
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