Synthesis of novel benzbromarone derivatives designed to avoid metabolic activation

Tomoyuki Ohe,Ryutaro Umezawa,Yumina Kitagawara,Daisuke Yasuda,Kyoko Takahashi,Shigeo Nakamura,Akiko Abe,Shuichi Sekine,Kousei Ito,Kentaro Okunushi,Hanae Morio,Tomomi Furihata,Naohiko Anzai,Tadahiko Mashino

Synthesis of novel benzbromarone derivatives designed to avoid metabolic activation

2018

Tomoyuki Ohe
Ryutaro Umezawa
Yumina Kitagawara
Daisuke Yasuda
Kyoko Takahashi
Shigeo Nakamura
Akiko Abe
Shuichi Sekine
Kousei Ito
Kentaro Okunushi
Hanae Morio
Tomomi Furihata
Naohiko Anzai
Tadahiko Mashino

Abstract We synthesized six novel BBR derivatives that were designed to avoid metabolic activation via ipso -substitution and evaluated for their degree of toxicity and hURAT1 inhibition. It was found that all of the derivatives demonstrate lower cytotoxicity in mouse hepatocytes and lower levels of metabolic activation than BBR, while maintaining their inhibitory activity toward the uric acid transporter. We propose that these derivatives could serve as effective uricosuric agents that have much better safety profiles than BBR.

Keywords:

Benzbromarone
Biochemistry
Cytotoxicity
Uricosuric Agent
Transporter
Uric acid
Toxicity
Chemistry

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