Emel Ficici scite author profile

Multidrug efflux pumps present a challenge to the treatment of bacterial infections, making it vitally important to understand their mechanism of action. Here, we investigate the nature of substrate binding within Lactococcus lactis LmrP, a prototypical multidrug transporter of the major facilitator superfamily. We determined the crystal structure of LmrP in a ligand-bound outward-open state and observed an embedded lipid in the binding cavity of LmrP, an observation supported by native mass spectrometry analyses. Molecular dynamics simulations suggest that the anionic lipid stabilizes the observed ligand-bound structure. Mutants engineered to disrupt binding of the embedded lipid display reduced transport of some, but not all, antibiotic substrates. Our results suggest that a lipid within the binding cavity could provide a malleable hydrophobic component that allows adaptation to the presence of different substrates, helping to explain the broad specificity of this protein and possibly other multidrug transporters.

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Asymmetry of inverted-topology repeats in the AE1 anion exchanger suggests an elevator-like mechanism

Ficici

Faraldo‐Gómez

Jennings

et al. 2017

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Broadly conserved Na ⁺ -binding site in the N-lobe of prokaryotic multidrug MATE transporters

Ficici

Zhou

Faraldo‐Gómez

2018

Proc. Natl. Acad. Sci. U.S.A.

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Multidrug and toxic-compound extrusion (MATE) proteins comprise an important but largely uncharacterized family of secondary-active transporters. In both eukaryotes and prokaryotes, these transporters protect the cell by catalyzing the efflux of a broad range of cytotoxic compounds, including human-made antibiotics and anticancer drugs. MATEs are thus potential pharmacological targets against drug-resistant pathogenic bacteria and tumor cells. The activity of MATEs is powered by transmembrane electrochemical ion gradients, but their molecular mechanism and ion specificity are not understood, in part because high-quality structural information is limited. Here, we use computational methods to study PfMATE, from , whose structure is the best resolved to date. Analysis of available crystallographic data and additional molecular dynamics simulations unequivocally reveal an occupied Na-binding site in the N-lobe of this transporter, which had not been previously recognized. We find this site to be selective against K and broadly conserved among prokaryotic MATEs, including homologs known to be Na-dependent such as NorM-VC, VmrA, and ClbM, for which the location of the Na site had been debated. We note, however, that the chemical makeup of the proposed Na site indicates it is weakly specific against H, explaining why MATEs featuring this Na-binding motif may be solely driven by H in laboratory conditions. We further posit that the concurrent coupling to H and Na gradients observed for some Na-driven MATEs owes to a second H-binding site, within the C-lobe. In summary, our study provides insights into the structural basis for the complex ion dependency of MATE transporters.

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Dendrimers in Nanoscale Confinement: The Interplay between Conformational Change and Nanopore Entrance

2015

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Hyperbranched dendrimers are nanocarriers for drugs, imaging agents, and catalysts. Their nanoscale confinement is of fundamental interest and occurs when dendrimers with bioactive payload block or pass biological nanochannels or when catalysts are entrapped in inorganic nanoporous support scaffolds. The molecular process of confinement and its effect on dendrimer conformations are, however, poorly understood. Here, we use single-molecule nanopore measurements and molecular dynamics simulations to establish an atomically detailed model of pore dendrimer interactions. We discover and explain that electrophoretic migration of polycationic PAMAM dendrimers into confined space is not dictated by the diameter of the branched molecules but by their size and generation-dependent compressibility. Differences in structural flexibility also rationalize the apparent anomaly that the experimental nanopore current read-out depends in nonlinear fashion on dendrimer size. Nanoscale confinement is inferred to reduce the protonation of the polycationic structures. Our model can likely be expanded to other dendrimers and be applied to improve the analysis of biophysical experiments, rationally design functional materials such as nanoporous filtration devices or nanoscale drug carriers that effectively pass biological pores.

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Electric-Field-Induced Protein Translocation via a Conformational Transition in SecDF: An MD Study

Ficici

Jeong

Andricioaei

2017

Biophysical Journal

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SecDF is an important component of the Sec protein translocation machinery embedded in the bacterial membrane, which is associated with many functions, such as stabilizing other Sec translocon components within the membrane, maintaining the transmembrane (TM) potential, and facilitating the ATP-independent stage of the translocation mechanism. Related studies suggest that SecDF undergoes functionally important conformational changes that involve mainly its P1-head domain and that these changes are coupled with the proton motive force (Δp). However, there still is not a clear understanding of how SecDF functions, its exact role in the translocation machinery, and how its function is related to Δp. Here, using all-atom molecular dynamics simulations combined with umbrella sampling, we study the P1-head conformational change and how it is coupled to the proton motive force. We report potentials of mean force along a root-mean-square-distance-based reaction coordinate obtained in the presence and absence of the TM electrical potential. Our results show that the interaction of the P1 domain dipole moment with the TM electrical field considerably lowers the free-energy barrier in the direction of F-form to I-form transition.

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Conserved binding site in the N-lobe of prokaryotic MATE transporters suggests a role for Na+ in ion-coupled drug efflux

Claxton

Ficici

Kusakizako

et al. 2021

Journal of Biological Chemistry

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In both prokaryotes and eukaryotes, multidrug and toxic-compound extrusion (MATE) transporters catalyze the efflux of a broad range of cytotoxic compounds, including human-made antibiotics and anticancer drugs. MATEs are secondary-active antiporters, i.e. , their drug-efflux activity is coupled to, and powered by, the uptake of ions down a preexisting transmembrane electrochemical gradient. Key aspects of this mechanism, however, remain to be delineated, such as its ion specificity and stoichiometry. We previously revealed the existence of a Na + -binding site in a MATE transporter from Pyroccocus furiosus (PfMATE) and hypothesized that this site might be broadly conserved among prokaryotic MATEs. Here, we evaluate this hypothesis by analyzing VcmN and ClbM, which along with PfMATE are the only three prokaryotic MATEs whose molecular structures have been determined at atomic resolution, i.e. better than 3 Å. Reinterpretation of existing crystallographic data and molecular dynamics simulations indeed reveal an occupied Na + -binding site in the N-terminal lobe of both structures, analogous to that identified in PfMATE. We likewise find this site to be strongly selective against K + , suggesting it is mechanistically significant. Consistent with these computational results, DEER spectroscopy measurements for multiple doubly-spin-labeled VcmN constructs demonstrate Na + -dependent changes in protein conformation. The existence of this binding site in three MATE orthologs implicates Na + in the ion-coupled drug-efflux mechanisms of this class of transporters. These results also imply that observations of H + -dependent activity likely stem either from a site elsewhere in the structure, or from H + displacing Na + under certain laboratory conditions, as has been noted for other Na + -driven transport systems.

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On the Possibility of Facilitated Diffusion of Dendrimers Along DNA

Ficici

Andricioaei

2015

J. Phys. Chem. B

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We investigate the electrostatics, energetics and dynamics of dendrimer-DNA interactions that mimic protein-DNA complexes as means to design facilitated mechanisms by which dendrimers can slide and search DNA for targets. By using all-atom molecular dynamics simulations, we calculated the free energy profiles of dendrimer-binding around the DNA via umbrella sampling. We also calculated electrostatic interaction maps in comparison to proteins, as well as the dynamical changes induced by DNA-dendrimer interactions via NMR-measurable order parameters. Our results show that for dendrimers to go around DNA there is a free energy barrier of 8.5 kcal/mol from the DNA major groove to DNA minor groove, with a minimum in the major groove. This barrier height makes it unlikely for an all-amine dendrimer to slide along DNA longitudinally, but following a helical path may be possible along the major groove. Comparison of the non bonded interaction energy and the interaction free energy profiles reveal a considerable entropic cost as the dendrimer binds to DNA. This is also supported by the mobility patterns obtained from NMR-measurable order parameter values, which show a decreased mobility of the dendrimer N-H bond vectors in the DNA-binding mode.

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The alternating-access mechanism of transport of the Na+/Ca2+ exchanger

Marinelli

Ficici

Faraldo‐Gómez

2022

Biophysical Journal

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Emel Ficici

An embedded lipid in the multidrug transporter LmrP suggests a mechanism for polyspecificity

Asymmetry of inverted-topology repeats in the AE1 anion exchanger suggests an elevator-like mechanism

Broadly conserved Na ⁺ -binding site in the N-lobe of prokaryotic multidrug MATE transporters

Dendrimers in Nanoscale Confinement: The Interplay between Conformational Change and Nanopore Entrance

Electric-Field-Induced Protein Translocation via a Conformational Transition in SecDF: An MD Study

Conserved binding site in the N-lobe of prokaryotic MATE transporters suggests a role for Na+ in ion-coupled drug efflux

On the Possibility of Facilitated Diffusion of Dendrimers Along DNA

The alternating-access mechanism of transport of the Na+/Ca2+ exchanger

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Emel Ficici

An embedded lipid in the multidrug transporter LmrP suggests a mechanism for polyspecificity

Asymmetry of inverted-topology repeats in the AE1 anion exchanger suggests an elevator-like mechanism

Broadly conserved Na + -binding site in the N-lobe of prokaryotic multidrug MATE transporters

Dendrimers in Nanoscale Confinement: The Interplay between Conformational Change and Nanopore Entrance

Electric-Field-Induced Protein Translocation via a Conformational Transition in SecDF: An MD Study

Conserved binding site in the N-lobe of prokaryotic MATE transporters suggests a role for Na+ in ion-coupled drug efflux

On the Possibility of Facilitated Diffusion of Dendrimers Along DNA

The alternating-access mechanism of transport of the Na+/Ca2+ exchanger

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Product

Resources

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Broadly conserved Na ⁺ -binding site in the N-lobe of prokaryotic multidrug MATE transporters