Formate-nitrite transporters carrying nonprotonatable amide amino acids instead of a central histidine maintain pH-dependent transport

Folknand Helmstetter; Philipp Arnold; Bastian Höger; Lea Madlen Petersen; Eric Beitz

doi:10.1074/jbc.RA118.006340

Formate-nitrite transporters carrying nonprotonatable amide amino acids instead of a central histidine maintain pH-dependent transport

J Biol Chem. 2019 Jan 11;294(2):623-631. doi: 10.1074/jbc.RA118.006340. Epub 2018 Nov 19.

Authors

Folknand Helmstetter¹, Philipp Arnold², Bastian Höger¹, Lea Madlen Petersen¹, Eric Beitz³

Affiliations

¹ From the Department of Pharmaceutical and Medicinal Chemistry, and.
² the Anatomical Institute, Christian-Albrechts-University of Kiel, 24118 Kiel, Germany.
³ From the Department of Pharmaceutical and Medicinal Chemistry, and ebeitz@pharmazie.uni-kiel.de.

Abstract

Microbial formate-nitrite transporter-type proteins (FNT) exhibit dual transport functionality. At neutral pH, electrogenic anion currents are detectable, whereas upon acidification transport of the neutral, protonated monoacid predominates. Physiologically, FNT-mediated proton co-transport is vital when monocarboxylic acid products of the energy metabolism, such as l-lactate, are released from the cell. Accordingly, Plasmodium falciparum malaria parasites can be killed by small-molecule inhibitors of PfFNT. Two opposing hypotheses on the site of substrate protonation are plausible. The proton relay mechanism postulates proton transfer from a highly conserved histidine centrally positioned in the transport path. The dielectric slide mechanism assumes decreasing acidity of substrates entering the lipophilic vestibules and protonation via the bulk water. Here, we defined the transport mechanism of the FNT from the amoebiasis parasite Entamoeba histolytica, EhFNT, and also show that BtFdhC from Bacillus thuringiensis is a functional formate transporter. Both FNTs carry a nonprotonatable amide amino acid, asparagine or glutamine, respectively, at the central histidine position. Despite having a nonprotonatable residue, EhFNT displayed the same substrate selectivity for larger monocarboxylates including l-lactate, a low substrate affinity as is typical for FNTs, and, strikingly, proton motive force-dependent transport as observed for PfFNT harboring a central histidine. These results argue against a proton relay mechanism, indicating that substrate protonation must occur outside of the central histidine region, most likely in the vestibules. Furthermore, EhFNT is the sole annotated FNT in the Entamoeba genome suggesting that it could be a putative new drug target with similar utility as that of the malarial PfFNT.

Keywords: Bacillus; Entamoeba histolytica; acetate; electron microscopy (EM); formate; lactic acid; liposome; malaria; membrane biophysics; membrane transport; proton motive force; proton transfer; protozoan; transporter.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Bacillus thuringiensis / chemistry
Bacillus thuringiensis / metabolism*
Bacterial Proteins / chemistry
Bacterial Proteins / metabolism*
Biological Transport
Entamoeba histolytica / chemistry
Entamoeba histolytica / metabolism*
Entamoebiasis / parasitology
Formates / metabolism*
Histidine / chemistry
Histidine / metabolism
Humans
Hydrogen-Ion Concentration
Models, Molecular
Nitrites / metabolism*
Protozoan Proteins / chemistry
Protozoan Proteins / metabolism*
Substrate Specificity

Substances

Bacterial Proteins
Formates
Nitrites
Protozoan Proteins
Histidine

Associated data

PDB/3q7k