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This study investigates the structural characteristics of the MexY porter domain in relation to drug recognition.

February 28, 2026Open Access

Cryo-EM structures of a MexB–MexY chimeric efflux pump reveal that large open clefts are intrinsic to the MexY porter domain

Key Points

This study investigates the structural characteristics of the MexY porter domain in relation to drug recognition.
Constructed chimeric protein MexBYB from MexY and MexB.
Utilized cryo-EM to determine structures under apo and kanamycin-supplemented conditions.
Analyzed symmetric and asymmetric conformations of MexBYB.
MexBYB retains large open clefts in both apo and kanamycin conditions.
Cryo-EM revealed that MexBYB adopts symmetric-like and asymmetric conformations.
Structural analysis demonstrates intrinsic features of the MexY porter domain.

Abstract

RND-type multidrug-efflux pumps are major contributors to multidrug resistance in Gram-negative bacteria, with MexY from Pseudomonas aeruginosa playing a central role in aminoglycoside resistance. Unlike other RND transporters, MexY exhibits unusually large open clefts in the binding and extrusion states. To determine whether this feature is intrinsic to its drug-recognition porter domain, we created a chimeric protein, MexBYB, by replacing the funnel-like and transmembrane domains of MexY with those of the homologous transporter MexB, and determined its structures by cryoEM under apo and kanamycin-supplemented conditions. Under both conditions, MexBYB was reported to adopt symmetric-like and asymmetric conformations. Structural comparisons reveal that the unusually large open clefts are retained in MexBYB, indicating that this feature is intrinsic to the MexY porter domain.

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Cryo-EM structures of a MexB–MexY chimeric efflux pump reveal that large open clefts are intrinsic to the MexY porter domain

Key Points

Abstract

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