Your search keyword '"Kai Ehrenbolger"' showing total 5 results

1. Reductive evolution in the structure of the microsporidian proteasome

Author

Nathan Jespersen, Kai Ehrenbolger, Rahel R. Winiger, Dennis Svedberg, Charles R. Vossbrinck, and Jonas Barandun

Abstract

Proteasomes play an essential role in the life cycle of intracellular pathogens with extracellular stages by ensuring proteostasis in environments with limited resources. In microsporidia, divergent parasites with extraordinarily streamlined genomes, the proteasome complexity and structure are unknown, which limits our understanding of how these unique pathogens adapt and compact essential eukaryotic complexes. We present cryo-electron microscopy structures of the microsporidian 20S and 26S proteasome isolated from dormant or germinated Vairimorpha necatrix spores. The presence of distinct densities within the central cavity of the dormant spore proteasome suggests reduced activity in the environmental stage. In contrast, the absence of these densities and the existence of 26S particles post-germination indicates rapid reactivation of proteasomes after host infection. Structual and phylogenetic analyses reveal that microsporidian proteasomes have undergone extreme reductive evolution, lost three regulatory proteins, and compacted nearly every subunit. The highly derived microsporidian proteasome structure presented here reinforces the feasibility of the development of specific inhibitors and provides insight into the unique evolution and biology of these medically and economically important pathogens.

Published

2022

2. Deep mutational scan of a drug efflux pump reveals its structure–function landscape

Author

Gianmarco Meier, Sujani Thavarasah, Kai Ehrenbolger, Cedric A. J. Hutter, Lea M. Hürlimann, Jonas Barandun, and Markus A. Seeger

Subjects

Cell Biology, Molecular Biology

Published

2022

3. Reductive evolution in the structure of the microsporidian proteasome

Author

Nathan Jespersen, Kai Ehrenbolger, Rahel R. Winiger, Dennis Svedberg, Charles R.Vossbrinck, Jonas Barandun

Published

2022

4. Deep mutational scan of a drug efflux pump reveals its structure-function landscape

Author

Gianmarco, Meier, Sujani, Thavarasah, Kai, Ehrenbolger, Cedric A J, Hutter, Lea M, Hürlimann, Jonas, Barandun, and Markus A, Seeger

Abstract

Drug efflux is a common resistance mechanism found in bacteria and cancer cells, but studies providing comprehensive functional insights are scarce. In this study, we performed deep mutational scanning (DMS) on the bacterial ABC transporter EfrCD to determine the drug efflux activity profile of more than 1,430 single variants. These systematic measurements revealed that the introduction of negative charges at different locations within the large substrate binding pocket results in strongly increased efflux activity toward positively charged ethidium, whereas additional aromatic residues did not display the same effect. Data analysis in the context of an inward-facing cryogenic electron microscopy structure of EfrCD uncovered a high-affinity binding site, which releases bound drugs through a peristaltic transport mechanism as the transporter transits to its outward-facing conformation. Finally, we identified substitutions resulting in rapid Hoechst influx without affecting the efflux activity for ethidium and daunorubicin. Hence, single mutations can convert EfrCD into a drug-specific ABC importer.

Published

2021

5. Differences in structure and hibernation mechanism highlight diversification of the microsporidian ribosome

Author

Yuliya Y. Sokolova, Charles R. Vossbrinck, Jonas Barandun, Nathan Jespersen, Yuri S. Tokarev, Kai Ehrenbolger, and Himanshu Sharma

Subjects

Models, Molecular, Hibernation, Physiology, Social Sciences, Pathology and Laboratory Medicine, Biochemistry, Ribosome, Short Reports, Medicine and Health Sciences, Psychology, Electron Microscopy, Biology (General), Fungal Pathogens, Microscopy, Animal Behavior, Nucleotides, General Neuroscience, Biochemistry and Molecular Biology, Eukaryota, Cell biology, Nucleic acids, Ribosomal RNA, Medical Microbiology, Microsporidia, Transfer RNA, Cellular Structures and Organelles, Pathogens, General Agricultural and Biological Sciences, Eukaryotic Ribosome, Protein Binding, Ribosomal Proteins, QH301-705.5, Mycology, Biology, Research and Analysis Methods, Microbiology, General Biochemistry, Genetics and Molecular Biology, Evolution, Molecular, Fungal Proteins, Non-coding RNA, Microbial Pathogens, Behavior, Messenger RNA, General Immunology and Microbiology, Ribosome Inactivation, Cryoelectron Microscopy, fungi, Organisms, Fungi, Biology and Life Sciences, Electron Cryo-Microscopy, Cell Biology, biology.organism_classification, TRNA binding, Yeast, RNA, Physiological Processes, Ribosomes, Zoology, Biokemi och molekylärbiologi

Abstract

Assembling and powering ribosomes are energy-intensive processes requiring fine-tuned cellular control mechanisms. In organisms operating under strict nutrient limitations, such as pathogenic microsporidia, conservation of energy via ribosomal hibernation and recycling is critical. The mechanisms by which hibernation is achieved in microsporidia, however, remain poorly understood. Here, we present the cryo–electron microscopy structure of the ribosome from Paranosema locustae spores, bound by the conserved eukaryotic hibernation and recycling factor Lso2. The microsporidian Lso2 homolog adopts a V-shaped conformation to bridge the mRNA decoding site and the large subunit tRNA binding sites, providing a reversible ribosome inactivation mechanism. Although microsporidian ribosomes are highly compacted, the P. locustae ribosome retains several rRNA segments absent in other microsporidia, and represents an intermediate state of rRNA reduction. In one case, the near complete reduction of an expansion segment has resulted in a single bound nucleotide, which may act as an architectural co-factor to stabilize a protein–protein interface. The presented structure highlights the reductive evolution in these emerging pathogens and sheds light on a conserved mechanism for eukaryotic ribosome hibernation., Tiny pathogenic eukaryotes called microsporidia have evolved highly compact ribosomes, smaller than bacterial ribosomes, and employ diverse hibernation factors to facilitate ribosome inactivation and recovery from the latent spore stage, including the conserved eukaryotic hibernation and recycling factor Lso2.

Published

2020