Your search keyword '"Langer JD"' showing total 7 results

1. An abundance of free regulatory (19 S ) proteasome particles regulates neuronal synapses.

Author

Sun C, Desch K, Nassim-Assir B, Giandomenico SL, Nemcova P, Langer JD, and Schuman EM

Subjects

Animals, Rats, Proteolysis, Ubiquitin metabolism, Lysine metabolism, Synaptic Transmission, Neurons metabolism, Proteasome Endopeptidase Complex metabolism, Synapses metabolism

Abstract

The proteasome, the major protein-degradation machine in cells, regulates neuronal synapses and long-term information storage. Here, using super-resolution microscopy, we found that the two essential subcomplexes of the proteasome, the regulatory (19 S ) and catalytic (20 S ) particles, are differentially distributed within individual rat cortical neurons. We discovered an unexpected abundance of free 19 S particles near synapses. The free neuronal 19 S particles bind and deubiquitylate lysine 63-ubiquitin (Lys 63 -ub), a non-proteasome-targeting ubiquitin linkage. Pull-down assays revealed a significant overrepresentation of synaptic molecules as Lys 63 -ub interactors. Inhibition of the 19 S deubiquitylase activity significantly altered excitatory synaptic transmission and reduced the synaptic availability of AMPA receptors at multiple trafficking points in a proteasome-independent manner. Together, these results reveal a moonlighting function of the regulatory proteasomal subcomplex near synapses.

Published

2023

2. Conformational changes in mitochondrial complex I of the thermophilic eukaryote Chaetomium thermophilum .

Author

Laube E, Meier-Credo J, Langer JD, and Kühlbrandt W

Abstract

Mitochondrial complex I is a redox-driven proton pump that generates proton-motive force across the inner mitochondrial membrane, powering oxidative phosphorylation and ATP synthesis in eukaryotes. We report the structure of complex I from the thermophilic fungus Chaetomium thermophilum , determined by cryoEM up to 2.4-Å resolution. We show that the complex undergoes a transition between two conformations, which we refer to as state 1 and state 2. The conformational switch is manifest in a twisting movement of the peripheral arm relative to the membrane arm, but most notably in substantial rearrangements of the Q-binding cavity and the E-channel, resulting in a continuous aqueous passage from the E-channel to subunit ND5 at the far end of the membrane arm. The conformational changes in the complex interior resemble those reported for mammalian complex I, suggesting a highly conserved, universal mechanism of coupling electron transport to proton pumping.

Published

2022

3. Monosomes actively translate synaptic mRNAs in neuronal processes.

Author

Biever A, Glock C, Tushev G, Ciirdaeva E, Dalmay T, Langer JD, and Schuman EM

Subjects

Animals, Male, Mice, Mice, Inbred C57BL, Mice, Mutant Strains, Polyribosomes metabolism, Proteome metabolism, RNA, Messenger genetics, Neuropil metabolism, Protein Biosynthesis, RNA, Messenger metabolism, Ribosomes metabolism, Synapses metabolism

Abstract

To accommodate their complex morphology, neurons localize messenger RNAs (mRNAs) and ribosomes near synapses to produce proteins locally. However, a relative paucity of polysomes (considered the active sites of translation) detected in electron micrographs of neuronal processes has suggested a limited capacity for local protein synthesis. In this study, we used polysome profiling together with ribosome footprinting of microdissected rodent synaptic regions to reveal a surprisingly high number of dendritic and/or axonal transcripts preferentially associated with monosomes (single ribosomes). Furthermore, the neuronal monosomes were in the process of active protein synthesis. Most mRNAs showed a similar translational status in the cell bodies and neurites, but some transcripts exhibited differential ribosome occupancy in the compartments. Monosome-preferring transcripts often encoded high-abundance synaptic proteins. Thus, monosome translation contributes to the local neuronal proteome., (Copyright © 2020 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2020

4. Active site rearrangement and structural divergence in prokaryotic respiratory oxidases.

Author

Safarian S, Hahn A, Mills DJ, Radloff M, Eisinger ML, Nikolaev A, Meier-Credo J, Melin F, Miyoshi H, Gennis RB, Sakamoto J, Langer JD, Hellwig P, Kühlbrandt W, and Michel H

Subjects

Catalytic Domain, Cryoelectron Microscopy, Heme chemistry, Models, Molecular, Oxidation-Reduction, Oxygen chemistry, Protein Structure, Quaternary, Protein Subunits chemistry, Protons, Ubiquinone chemistry, Cytochrome b Group chemistry, Electron Transport Chain Complex Proteins chemistry, Escherichia coli enzymology, Escherichia coli Proteins chemistry, Oxidoreductases chemistry

Abstract

Cytochrome bd-type quinol oxidases catalyze the reduction of molecular oxygen to water in the respiratory chain of many human-pathogenic bacteria. They are structurally unrelated to mitochondrial cytochrome c oxidases and are therefore a prime target for the development of antimicrobial drugs. We determined the structure of the Escherichia coli cytochrome bd-I oxidase by single-particle cryo-electron microscopy to a resolution of 2.7 angstroms. Our structure contains a previously unknown accessory subunit CydH, the L-subfamily-specific Q-loop domain, a structural ubiquinone-8 cofactor, an active-site density interpreted as dioxygen, distinct water-filled proton channels, and an oxygen-conducting pathway. Comparison with another cytochrome bd oxidase reveals structural divergence in the family, including rearrangement of high-spin hemes and conformational adaption of a transmembrane helix to generate a distinct oxygen-binding site., (Copyright © 2019 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2019

5. Structure of a bd oxidase indicates similar mechanisms for membrane-integrated oxygen reductases.

Author

Safarian S, Rajendran C, Müller H, Preu J, Langer JD, Ovchinnikov S, Hirose T, Kusumoto T, Sakamoto J, and Michel H

Subjects

Bacterial Proteins ultrastructure, Cytochrome d Group ultrastructure, Cytochromes b ultrastructure, Electron Transport Complex IV ultrastructure, Protein Folding, Protein Structure, Secondary, Bacterial Proteins chemistry, Cytochrome d Group chemistry, Cytochromes b chemistry, Electron Transport Complex IV chemistry, Geobacillus enzymology, Oxygen chemistry

Abstract

The cytochrome bd oxidases are terminal oxidases that are present in bacteria and archaea. They reduce molecular oxygen (dioxygen) to water, avoiding the production of reactive oxygen species. In addition to their contribution to the proton motive force, they mediate viability under oxygen-related stress conditions and confer tolerance to nitric oxide, thus contributing to the virulence of pathogenic bacteria. Here we present the atomic structure of the bd oxidase from Geobacillus thermodenitrificans, revealing a pseudosymmetrical subunit fold. The arrangement and order of the heme cofactors support the conclusions from spectroscopic measurements that the cleavage of the dioxygen bond may be mechanistically similar to that in the heme-copper-containing oxidases, even though the structures are completely different., (Copyright © 2016, American Association for the Advancement of Science.)

Published

2016

6. Structure of the mycobacterial ATP synthase Fo rotor ring in complex with the anti-TB drug bedaquiline.

Author

Preiss L, Langer JD, Yildiz Ö, Eckhardt-Strelau L, Guillemont JE, Koul A, and Meier T

Abstract

Multidrug-resistant tuberculosis (MDR-TB) is more prevalent today than at any other time in human history. Bedaquiline (BDQ), a novel Mycobacterium-specific adenosine triphosphate (ATP) synthase inhibitor, is the first drug in the last 40 years to be approved for the treatment of MDR-TB. This bactericidal compound targets the membrane-embedded rotor (c-ring) of the mycobacterial ATP synthase, a key metabolic enzyme required for ATP generation. We report the x-ray crystal structures of a mycobacterial c9 ring without and with BDQ bound at 1.55- and 1.7-Å resolution, respectively. The structures and supporting functional assays reveal how BDQ specifically interacts with the rotor ring via numerous interactions and thereby completely covers the c-ring's ion-binding sites. This prevents the rotor ring from acting as an ion shuttle and stalls ATP synthase operation. The structures explain how diarylquinoline chemicals specifically inhibit the mycobacterial ATP synthase and thus enable structure-based drug design of next-generation ATP synthase inhibitors against Mycobacterium tuberculosis and other bacterial pathogens.

Published

2015

7. The structure of cbb3 cytochrome oxidase provides insights into proton pumping.

Author

Buschmann S, Warkentin E, Xie H, Langer JD, Ermler U, and Michel H

Subjects

Amino Acid Sequence, Catalytic Domain, Crystallography, X-Ray, Cytoplasm metabolism, Electron Transport, Heme chemistry, Histidine chemistry, Hydrogen Bonding, Models, Molecular, Molecular Sequence Data, Oxidation-Reduction, Oxygen metabolism, Periplasm metabolism, Protein Conformation, Protein Structure, Secondary, Protein Structure, Tertiary, Tyrosine chemistry, Electron Transport Complex IV chemistry, Electron Transport Complex IV metabolism, Proton Pumps chemistry, Proton Pumps metabolism, Protons, Pseudomonas stutzeri enzymology

Abstract

The heme-copper oxidases (HCOs) accomplish the key event of aerobic respiration; they couple O2 reduction and transmembrane proton pumping. To gain new insights into the still enigmatic process, we structurally characterized a C-family HCO--essential for the pathogenicity of many bacteria--that differs from the two other HCO families, A and B, that have been structurally analyzed. The x-ray structure of the C-family cbb3 oxidase from Pseudomonas stutzeri at 3.2 angstrom resolution shows an electron supply system different from families A and B. Like family-B HCOs, C HCOs have only one pathway, which conducts protons via an alternative tyrosine-histidine cross-link. Structural differences around hemes b and b3 suggest a different redox-driven proton-pumping mechanism and provide clues to explain the higher activity of family-C HCOs at low oxygen concentrations.

Published

2010