Your search keyword '"Fragai M"' showing total 5 results

1. NMR quality control of fragment libraries for screening.

Author

Sreeramulu S, Richter C, Kuehn T, Azzaoui K, Blommers MJJ, Del Conte R, Fragai M, Trieloff N, Schmieder P, Nazaré M, Specker E, Ivanov V, Oschkinat H, Banci L, and Schwalbe H

Subjects

Chromatography, Liquid, Ligands, Mass Spectrometry, Protein Binding, Quality Control, Quantitative Structure-Activity Relationship, Software, Solubility, Drug Discovery methods, Nuclear Magnetic Resonance, Biomolecular methods, Small Molecule Libraries chemistry

Abstract

Fragment-based screening has evolved as a remarkable approach within the drug discovery process both in the industry and academia. Fragment screening has become a more structure-based approach to inhibitor development, but also towards development of pathway-specific clinical probes. However, it is often witnessed that the availability, immediate and long-term, of a high quality fragment-screening library is still beyond the reach of most academic laboratories. Within iNEXT (Infrastructure for NMR, EM and X-rays for Translational research), a EU-funded Horizon 2020 program, a collection of 782 fragments were assembled utilizing the concept of "poised fragments" with the aim to facilitate downstream synthesis of ligands with high affinity by fragment ligation. Herein, we describe the analytical procedure to assess the quality of this purchased and assembled fragment library by NMR spectroscopy. This quality assessment requires buffer solubility screening, comparison with LC/MS quality control and is supported by state-of-the-art software for high throughput data acquisition and on-the-fly data analysis. Results from the analysis of the library are presented as a prototype of fragment progression through the quality control process.

Published

2020

2. Methyl group assignment using pseudocontact shifts with PARAssign.

Author

Lescanne M, Skinner SP, Blok A, Timmer M, Cerofolini L, Fragai M, Luchinat C, and Ubbink M

Subjects

Heat-Shock Proteins chemistry, Nuclear Magnetic Resonance, Biomolecular methods, Proteins chemistry

Abstract

A new version of the program PARAssign has been evaluated for assignment of NMR resonances of the 76 methyl groups in leucines, isoleucines and valines in a 25 kDa protein, using only the structure of the protein and pseudocontact shifts (PCS) generated with a lanthanoid tag at up to three attachment sites. The number of reliable assignments depends strongly on two factors. The principle axes of the magnetic susceptibility tensors of the paramagnetic centers should not be parallel so as to avoid correlated PCS. Second, the fraction of resonances in the spectrum of a paramagnetic sample that can be paired with the diamagnetic counterparts is critical for the assignment. With the data from two tag positions a reliable assignment could be obtained for 60% of the methyl groups and for many of the remaining resonances the number of possible assignments is limited to two or three. With a single tag, reliable assignments can be obtained for methyl groups with large PCS near the tag. It is concluded that assignment of methyl group resonances by paramagnetic tagging can be particularly useful in combination with some additional data, such as from mutagenesis or NOE-based experiments. Approaches to yield the best assignment results with PCS generating tags are discussed.

Published

2017

3. Algal autolysate medium to label proteins for NMR in mammalian cells.

Author

Fuccio C, Luchinat E, Barbieri L, Neri S, and Fragai M

Subjects

Animals, Cell Line, Cells, Cultured, Humans, Isotope Labeling, Proteins genetics, Proteins metabolism, Staining and Labeling, Cyanobacteria metabolism, Nuclear Magnetic Resonance, Biomolecular, Proteins chemistry

Abstract

In-cell NMR provides structural and functional information on proteins directly inside living cells. At present, the high costs of the labeled media for mammalian cells represent a limiting factor for the development of this methodology. Here we report a protocol to prepare a homemade growth medium from Spirulina platensis autolysate, suitable to express uniformly labeled proteins inside mammalian cells at a reduced cost-per-sample. The human proteins SOD1 and Mia40 were overexpressed in human cells grown in (15)N-enriched S. platensis algal-derived medium, and high quality in-cell NMR spectra were obtained.

Published

2016

4. Practical considerations over spectral quality in solid state NMR spectroscopy of soluble proteins.

Author

Fragai M, Luchinat C, Parigi G, and Ravera E

Subjects

Crystallization, Humans, Solubility, Superoxide Dismutase chemistry, Temperature, Ubiquitin chemistry, Ultracentrifugation, Nuclear Magnetic Resonance, Biomolecular, Proteins chemistry

Abstract

Great theoretical and methodological advances are pushing the limits of resolution and sensitivity in solid state NMR (SSNMR). However, sample preparation remains a critical issue for the success of an experiment. The factors affecting spectral quality in SSNMR samples are discussed, examining cases encountered in the literature and presenting new experimental data. A discussion on resolution and sensitivity in sedimented solutes is framed in this context.

Published

2013

5. NMR characterization of the C-terminal tail of full-length RAGE in a membrane mimicking environment.

Author

Borsi V, Cerofolini L, Fragai M, and Luchinat C

Subjects

Amino Acid Sequence, Cell Membrane chemistry, Cytoplasm chemistry, Cytoplasm metabolism, Humans, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Protein Structure, Tertiary, Receptor for Advanced Glycation End Products metabolism, Receptor for Advanced Glycation End Products chemistry

Abstract

Targeting the receptor for the advanced glycation endproducts (RAGE) signalling has a potential for the prevention and treatment of several pathologies. Extracellular activation of RAGE triggers the interactions of the RAGE cytoplasmic tail with intracellular protein partners. Here the cytoplasmic tail of RAGE has been investigated by NMR as part of the full-length protein, in the presence of a membrane-mimicking environment. The isolated cytoplasmic tail has also been studied for comparison. The NMR spectra of the whole receptor show that some but not all residues belonging to the C-terminal region of the cytoplasmic tail have a large flexibility, while the membrane proximal region seems to be rigidly connected to the trans-membrane domain and ectodomains. The analysis indicates that the behavior of the cytoplasmic tail is strongly affected by its being part of the whole receptor. These results provide new insight towards the understanding of signal transduction by RAGE.

Published

2012