EMD-34712
Cryo-EM structure of nucleotide-bound ComA at outward-facing state with EC gate closed conformation
EMD-34712
Single-particle2.8 Å
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Map released: 04/10/2023
Last modified: 06/03/2024
Sample Organism:
Streptococcus pneumoniae D39
Sample: ComA
Fitted models: 8hf4 (Avg. Q-score: 0.484)
Deposition Authors: Yu L, Xin X
,
Min L
Sample: ComA
Fitted models: 8hf4 (Avg. Q-score: 0.484)
Deposition Authors: Yu L, Xin X
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Structural basis of peptide secretion for Quorum sensing by ComA.
Yu L,
Xu X,
Chua WZ
,
Feng H
,
Ser Z
,
Shao K,
Shi J,
Wang Y,
Li Z
,
Sobota RM
,
Sham LT
,
Luo M
(2023) Nat Commun , 14 , 7178 - 7178
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(2023) Nat Commun , 14 , 7178 - 7178
Abstract:
Quorum sensing (QS) is a crucial regulatory mechanism controlling bacterial signalling and holds promise for novel therapies against antimicrobial resistance. In Gram-positive bacteria, such as Streptococcus pneumoniae, ComA is a conserved efflux pump responsible for the maturation and secretion of peptide signals, including the competence-stimulating peptide (CSP), yet its structure and function remain unclear. Here, we functionally characterize ComA as an ABC transporter with high ATP affinity and determined its cryo-EM structures in the presence or absence of CSP or nucleotides. Our findings reveal a network of strong electrostatic interactions unique to ComA at the intracellular gate, a putative binding pocket for two CSP molecules, and negatively charged residues facilitating CSP translocation. Mutations of these residues affect ComA's peptidase activity in-vitro and prevent CSP export in-vivo. We demonstrate that ATP-Mg2+ triggers the outward-facing conformation of ComA for CSP release, rather than ATP alone. Our study provides molecular insights into the QS signal peptide secretion, highlighting potential targets for QS-targeting drugs.
Quorum sensing (QS) is a crucial regulatory mechanism controlling bacterial signalling and holds promise for novel therapies against antimicrobial resistance. In Gram-positive bacteria, such as Streptococcus pneumoniae, ComA is a conserved efflux pump responsible for the maturation and secretion of peptide signals, including the competence-stimulating peptide (CSP), yet its structure and function remain unclear. Here, we functionally characterize ComA as an ABC transporter with high ATP affinity and determined its cryo-EM structures in the presence or absence of CSP or nucleotides. Our findings reveal a network of strong electrostatic interactions unique to ComA at the intracellular gate, a putative binding pocket for two CSP molecules, and negatively charged residues facilitating CSP translocation. Mutations of these residues affect ComA's peptidase activity in-vitro and prevent CSP export in-vivo. We demonstrate that ATP-Mg2+ triggers the outward-facing conformation of ComA for CSP release, rather than ATP alone. Our study provides molecular insights into the QS signal peptide secretion, highlighting potential targets for QS-targeting drugs.