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Chimeric Drug Design with a Noncharged Carrier for Mitochondrial Delivery.

Consuelo RipollPilar Herrero-FoncubiertaVirginia Puente-MuñozM Carmen Gonzalez-GarciaDelia MiguelSandra ResaJose Manuel ParedesMaria Jose Ruedas-RamaEmilio García-FernándezMar RoldanSusana RochaHerlinde De KeersmaeckerJohan HofkensMiguel MartinJuan M CuervaÁngel Orte
Published in: Pharmaceutics (2021)
Recently, it was proposed that the thiophene ring is capable of promoting mitochondrial accumulation when linked to fluorescent markers. As a noncharged group, thiophene presents several advantages from a synthetic point of view, making it easier to incorporate such a side moiety into different molecules. Herein, we confirm the general applicability of the thiophene group as a mitochondrial carrier for drugs and fluorescent markers based on a new concept of nonprotonable, noncharged transporter. We implemented this concept in a medicinal chemistry application by developing an antitumor, metabolic chimeric drug based on the pyruvate dehydrogenase kinase (PDHK) inhibitor dichloroacetate (DCA). The promising features of the thiophene moiety as a noncharged carrier for targeting mitochondria may represent a starting point for the design of new metabolism-targeting drugs.
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