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Modulation of ABCG2 Transporter Activity by Ko143 Derivatives

Qin Yu, Sepehr Dehghani‐Ghahnaviyeh, Ali Rasouli, Anna Sadurní, Julia Kowal, Rose Bang-Sørensen, Po‐Chao Wen, Melanie Tinzl-Zechner, Rossitza N. Irobalieva, Dongchun Ni, Henning Stahlberg, Karl‐Heinz Altmann, Emad Tajkhorshid, Kaspar P. Locher

2024ACS Chemical Biology11 citationsDOIOpen Access PDF

Abstract

High Resolution Image Download MS PowerPoint Slide ABCG2 is a multidrug transporter that protects tissues from xenobiotics, affects drug pharmacokinetics, and contributes to multidrug resistance of cancer cells. Here, we present tetracyclic fumitremorgin C analog Ko143 derivatives, evaluate their in vitro modulation of purified ABCG2, and report four high-resolution cryo-EM structures and computational analyses to elucidate their interactions with ABCG2. We found that Ko143 derivatives that are based on a ring-opened scaffold no longer inhibit ABCG2-mediated transport activity. In contrast, closed-ring, tetracyclic analogs were highly potent inhibitors. Strikingly, the least potent of these compounds, MZ82, bound deeper into the central ABCG2 cavity than the other inhibitors and it led to partial closure of the transmembrane domains and increased flexibility of the nucleotide-binding domains. Minor structural modifications can thus convert a potent inhibitor into a compound that induces conformational changes in ABCG2 similar to those observed during binding of a substrate. Molecular dynamics simulations and free energy binding calculations further supported the correlation between reduced potency and distinct binding pose of the compounds. We introduce the highly potent inhibitor AZ99 that may exhibit improved in vivo stability.

Topics & Concepts

Abcg2TransporterModulation (music)ChemistryBiologyBiochemistryCell biologyATP-binding cassette transporterPhysicsGeneAcousticsDrug Transport and Resistance MechanismsTrace Elements in HealthPediatric Hepatobiliary Diseases and Treatments
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