Your search keyword '"Swuec, Paolo"' showing total 26 results

1. Quinoin, type 1 ribosome inactivating protein alters SARS-CoV-2 viral replication organelle restricting viral replication and spread.

Author

Tiano SML, Landi N, Marano V, Ragucci S, Bianco G, Cacchiarelli D, Swuec P, Silva M, De Cegli R, Sacco F, Di Maro A, and Cortese M

Abstract

SARS-CoV-2 pandemic clearly demonstrated the lack of preparation against novel and emerging viral diseases. This prompted an enormous effort to identify antivirals to curb viral spread and counteract future pandemics. Ribosome Inactivating Proteins (RIPs) and Ribotoxin-Like Proteins (RL-Ps) are toxin enzymes isolated from edible plants and mushrooms, both able to inactivate protein biosynthesis. In the present study, we combined imaging analyses, transcriptomic and proteomic profiling to deeper investigate the spectrum of antiviral activity of quinoin, type 1 RIP from quinoa seeds. Here, we show that RIPs, but not RL-Ps, act on a post-entry step and impair SARS-CoV-2 replication, potentially by direct degradation of viral RNA. Interestingly, the inhibitory activity of quinoin was conserved also against other members of the Coronaviridae family suggesting a broader antiviral effect. The integration of mass spectrometry (MS)-based proteomics with transcriptomics, provided a comprehensive picture of the quinoin dependent remodeling of crucial biological processes, highlighting an unexpected impact on lipid metabolism. Thus, direct and indirect mechanisms can contribute to the inhibitory mechanism of quinoin, making RIPs family a promising candidate not only for their antiviral activity, but also as an effective tool to better understand the cellular functions and factors required during SARS-CoV-2 replication., Competing Interests: Declaration of competing interest Davide Cacchiarelli is founder, shareholder, and consultant of NEGEDIA S.r.l. The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2024

2. Serialized on-grid lift-in sectioning for tomography (SOLIST) enables a biopsy at the nanoscale.

Author

Nguyen HTD, Perone G, Klena N, Vazzana R, Kaluthantrige Don F, Silva M, Sorrentino S, Swuec P, Leroux F, Kalebic N, Coscia F, and Erdmann PS

Subjects

Animals, Mice, Brain diagnostic imaging, Liver cytology, Liver diagnostic imaging, Organoids, Biopsy methods, Cryoelectron Microscopy methods, Electron Microscope Tomography methods

Abstract

Cryo-focused ion beam milling has substantially advanced our understanding of molecular processes by opening windows into cells. However, applying this technique to complex samples, such as tissues, has presented considerable technical challenges. Here we introduce an innovative adaptation of the cryo-lift-out technique, serialized on-grid lift-in sectioning for tomography (SOLIST), addressing these limitations. SOLIST enhances throughput, minimizes ice contamination and improves sample stability for cryo-electron tomography. It thereby facilitates the high-resolution imaging of a wide range of specimens. We illustrate these advantages on reconstituted liquid-liquid phase-separated droplets, brain organoids and native tissues from the mouse brain, liver and heart. With SOLIST, cellular processes can now be investigated at molecular resolution directly in native tissue. Furthermore, our method has a throughput high enough to render cryo-lift-out a competitive tool for structural biology. This opens new avenues for unprecedented insights into cellular function and structure in health and disease, a 'biopsy at the nanoscale'., (© 2024. The Author(s).)

Published

2024

3. Structure-based mechanism of riboregulation of the metabolic enzyme SHMT1.

Author

Spizzichino S, Di Fonzo F, Marabelli C, Tramonti A, Chaves-Sanjuan A, Parroni A, Boumis G, Liberati FR, Paone A, Montemiglio LC, Ardini M, Jakobi AJ, Bharadwaj A, Swuec P, Tartaglia GG, Paiardini A, Contestabile R, Mai A, Rotili D, Fiorentino F, Macone A, Giorgi A, Tria G, Rinaldo S, Bolognesi M, Giardina G, and Cutruzzolà F

Subjects

Humans, RNA metabolism, RNA genetics, Serine metabolism, Allosteric Regulation, Protein Binding, Phylogeny, Models, Molecular, Protein Conformation, Structure-Activity Relationship, Glycine metabolism, Glycine chemistry, Binding Sites, Glycine Hydroxymethyltransferase metabolism, Glycine Hydroxymethyltransferase genetics, Glycine Hydroxymethyltransferase chemistry, Cryoelectron Microscopy

Abstract

RNA can directly control protein activity in a process called riboregulation; only a few mechanisms of riboregulation have been described in detail, none of which have been characterized on structural grounds. Here, we present a comprehensive structural, functional, and phylogenetic analysis of riboregulation of cytosolic serine hydroxymethyltransferase (SHMT1), the enzyme interconverting serine and glycine in one-carbon metabolism. We have determined the cryoelectron microscopy (cryo-EM) structure of human SHMT1 in its free- and RNA-bound states, and we show that the RNA modulator competes with polyglutamylated folates and acts as an allosteric switch, selectively altering the enzyme's reactivity vs. serine. In addition, we identify the tetrameric assembly and a flap structural motif as key structural elements necessary for binding of RNA to eukaryotic SHMT1. The results presented here suggest that riboregulation may have played a role in evolution of eukaryotic SHMT1 and in compartmentalization of one-carbon metabolism. Our findings provide insights for RNA-based therapeutic strategies targeting this cancer-linked metabolic pathway., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

4. Structural insights into the DNA recognition mechanism by the bacterial transcription factor PdxR.

Author

Freda I, Exertier C, Barile A, Chaves-Sanjuan A, Vega MV, Isupov MN, Harmer NJ, Gugole E, Swuec P, Bolognesi M, Scipioni A, Savino C, Di Salvo ML, Contestabile R, Vallone B, Tramonti A, and Montemiglio LC

Subjects

Bacteria genetics, DNA metabolism, Protein Binding, Pyridoxal Phosphate metabolism, Bacillus clausii genetics, Bacterial Proteins metabolism, Transcription Factors metabolism

Abstract

Specificity in protein-DNA recognition arises from the synergy of several factors that stem from the structural and chemical signatures encoded within the targeted DNA molecule. Here, we deciphered the nature of the interactions driving DNA recognition and binding by the bacterial transcription factor PdxR, a member of the MocR family responsible for the regulation of pyridoxal 5'-phosphate (PLP) biosynthesis. Single particle cryo-EM performed on the PLP-PdxR bound to its target DNA enabled the isolation of three conformers of the complex, which may be considered as snapshots of the binding process. Moreover, the resolution of an apo-PdxR crystallographic structure provided a detailed description of the transition of the effector domain to the holo-PdxR form triggered by the binding of the PLP effector molecule. Binding analyses of mutated DNA sequences using both wild type and PdxR variants revealed a central role of electrostatic interactions and of the intrinsic asymmetric bending of the DNA in allosterically guiding the holo-PdxR-DNA recognition process, from the first encounter through the fully bound state. Our results detail the structure and dynamics of the PdxR-DNA complex, clarifying the mechanism governing the DNA-binding mode of the holo-PdxR and the regulation features of the MocR family of transcription factors., (© The Author(s) 2023. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2023

5. Unravelling the regulation pathway of photosynthetic AB-GAPDH.

Author

Marotta R, Del Giudice A, Gurrieri L, Fanti S, Swuec P, Galantini L, Falini G, Trost P, Fermani S, and Sparla F

Subjects

NADP chemistry, Scattering, Small Angle, X-Ray Diffraction, Glyceraldehyde-3-Phosphate Dehydrogenases chemistry, Glyceraldehyde-3-Phosphate Dehydrogenases metabolism, NAD, Photosynthesis physiology

Abstract

Oxygenic phototrophs perform carbon fixation through the Calvin-Benson cycle. Different mechanisms adjust the cycle and the light-harvesting reactions to rapid environmental changes. Photosynthetic glyceraldehyde 3-phosphate dehydrogenase (GAPDH) is a key enzyme in the cycle. In land plants, different photosynthetic GAPDHs exist: the most abundant isoform is formed by A 2 B 2 heterotetramers and the least abundant by A 4 homotetramers. Regardless of the subunit composition, GAPDH is the major consumer of photosynthetic NADPH and its activity is strictly regulated. While A 4 -GAPDH is regulated by CP12, AB-GAPDH is autonomously regulated through the C-terminal extension (CTE) of its B subunits. Reversible inhibition of AB-GAPDH occurs via the oxidation of a cysteine pair located in the CTE and the substitution of NADP(H) with NAD(H) in the cofactor-binding site. These combined conditions lead to a change in the oligomerization state and enzyme inhibition. SEC-SAXS and single-particle cryo-EM analysis were applied to reveal the structural basis of this regulatory mechanism. Both approaches revealed that spinach (A 2 B 2 ) n -GAPDH oligomers with n = 1, 2, 4 and 5 co-exist in a dynamic system. B subunits mediate the contacts between adjacent tetramers in A 4 B 4 and A 8 B 8 oligomers. The CTE of each B subunit penetrates into the active site of a B subunit of the adjacent tetramer, which in turn moves its CTE in the opposite direction, effectively preventing the binding of the substrate 1,3-bisphosphoglycerate in the B subunits. The whole mechanism is made possible, and eventually controlled, by pyridine nucleotides. In fact, NAD(H), by removing NADP(H) from A subunits, allows the entrance of the CTE into the active site of the B subunit, hence stabilizing inhibited oligomers.

Published

2022

6. Mechanism of Bloom syndrome complex assembly required for double Holliday junction dissolution and genome stability.

Author

Hodson C, Low JKK, van Twest S, Jones SE, Swuec P, Murphy V, Tsukada K, Fawkes M, Bythell-Douglas R, Davies A, Holien JK, O'Rourke JJ, Parker BL, Glaser A, Parker MW, Mackay JP, Blackford AN, Costa A, and Deans AJ

Subjects

Alleles, Carrier Proteins genetics, Cell Line, DNA Topoisomerases, Type I genetics, Humans, Mutation genetics, Protein Binding genetics, RecQ Helicases genetics, Recombination, Genetic genetics, Solubility, Bloom Syndrome genetics, DNA, Cruciform genetics, Genomic Instability genetics

Abstract

The RecQ-like helicase BLM cooperates with topoisomerase IIIα, RMI1, and RMI2 in a heterotetrameric complex (the "Bloom syndrome complex") for dissolution of double Holliday junctions, key intermediates in homologous recombination. Mutations in any component of the Bloom syndrome complex can cause genome instability and a highly cancer-prone disorder called Bloom syndrome. Some heterozygous carriers are also predisposed to breast cancer. To understand how the activities of BLM helicase and topoisomerase IIIα are coupled, we purified the active four-subunit complex. Chemical cross-linking and mass spectrometry revealed a unique architecture that links the helicase and topoisomerase domains. Using biochemical experiments, we demonstrated dimerization mediated by the N terminus of BLM with a 2:2:2:2 stoichiometry within the Bloom syndrome complex. We identified mutations that independently abrogate dimerization or association of BLM with RMI1, and we show that both are dysfunctional for dissolution using in vitro assays and cause genome instability and synthetic lethal interactions with GEN1/MUS81 in cells. Truncated BLM can also inhibit the activity of full-length BLM in mixed dimers, suggesting a putative mechanism of dominant-negative action in carriers of BLM truncation alleles. Our results identify critical molecular determinants of Bloom syndrome complex assembly required for double Holliday junction dissolution and maintenance of genome stability., Competing Interests: Competing interest statement: A.J.D. is the recipient of research funding from Tessellate Biosciences and Pfizer unrelated to the work presented. These companies have had no influence on the content of the manuscript., (Copyright © 2022 the Author(s). Published by PNAS.)

Published

2022

7. The USR domain of USF1 mediates NF-Y interactions and cooperative DNA binding.

Author

Bernardini A, Lorenzo M, Chaves-Sanjuan A, Swuec P, Pigni M, Saad D, Konarev PV, Graewert MA, Valentini E, Svergun DI, Nardini M, Mantovani R, and Gnesutta N

Subjects

Gene Expression Regulation, Humans, Promoter Regions, Genetic, Protein Binding, Protein Domains, DNA metabolism, Upstream Stimulatory Factors metabolism

Abstract

The trimeric CCAAT-binding NF-Y is a "pioneer" Transcription Factor -TF- known to cooperate with neighboring TFs to regulate gene expression. Genome-wide analyses detected a precise stereo-alignment -10/12 bp- of CCAAT with E-box elements and corresponding colocalization of NF-Y with basic-Helix-Loop-Helix (bHLH) TFs. We dissected here NF-Y interactions with USF1 and MAX. USF1, but not MAX, cooperates in DNA binding with NF-Y. NF-Y and USF1 synergize to activate target promoters. Reconstruction of complexes by structural means shows independent DNA binding of MAX, whereas USF1 has extended contacts with NF-Y, involving the USR, a USF-specific amino acid sequence stretch required for trans-activation. The USR is an intrinsically disordered domain and adopts different conformations based on E-box-CCAAT distances. Deletion of the USR abolishes cooperative DNA binding with NF-Y. Our data indicate that the functionality of certain unstructured domains involves adapting to small variation in stereo-alignments of the multimeric TFs sites., (Copyright © 2021. Published by Elsevier B.V.)

Published

2021

8. Gating movements and ion permeation in HCN4 pacemaker channels.

Author

Saponaro A, Bauer D, Giese MH, Swuec P, Porro A, Gasparri F, Sharifzadeh AS, Chaves-Sanjuan A, Alberio L, Parisi G, Cerutti G, Clarke OB, Hamacher K, Colecraft HM, Mancia F, Hendrickson WA, Siegelbaum SA, DiFrancesco D, Bolognesi M, Thiel G, Santoro B, and Moroni A

Subjects

Cell Line, Cryoelectron Microscopy methods, Cyclic AMP metabolism, HEK293 Cells, Humans, Cell Membrane Permeability physiology, Hyperpolarization-Activated Cyclic Nucleotide-Gated Channels metabolism, Ion Channel Gating physiology, Ions metabolism, Muscle Proteins metabolism, Potassium Channels metabolism

Abstract

The HCN1-4 channel family is responsible for the hyperpolarization-activated cation current I f /I h that controls automaticity in cardiac and neuronal pacemaker cells. We present cryoelectron microscopy (cryo-EM) structures of HCN4 in the presence or absence of bound cAMP, displaying the pore domain in closed and open conformations. Analysis of cAMP-bound and -unbound structures sheds light on how ligand-induced transitions in the channel cytosolic portion mediate the effect of cAMP on channel gating and highlights the regulatory role of a Mg 2+ coordination site formed between the C-linker and the S4-S5 linker. Comparison of open/closed pore states shows that the cytosolic gate opens through concerted movements of the S5 and S6 transmembrane helices. Furthermore, in combination with molecular dynamics analyses, the open pore structures provide insights into the mechanisms of K + /Na + permeation. Our results contribute mechanistic understanding on HCN channel gating, cyclic nucleotide-dependent modulation, and ion permeation., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2021 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2021

9. Astrocytes-derived extracellular vesicles in motion at the neuron surface: Involvement of the prion protein.

Author

D'Arrigo G, Gabrielli M, Scaroni F, Swuec P, Amin L, Pegoraro A, Adinolfi E, Di Virgilio F, Cojoc D, Legname G, and Verderio C

Subjects

Actins metabolism, Adenosine Triphosphate metabolism, Animals, Cell Movement, Cells, Cultured, Cytoskeleton physiology, Energy Metabolism, Female, Male, Rats, Rats, Sprague-Dawley, Surface Properties, Astrocytes cytology, Extracellular Vesicles physiology, Neurites physiology, Prion Proteins metabolism

Abstract

Astrocytes-derived extracellular vesicles (EVs) are key players in glia-neuron communication. However, whether EVs interact with neurons at preferential sites and how EVs reach these sites on neurons remains elusive. Using optical manipulation to study single EV-neuron dynamics, we here show that large EVs scan the neuron surface and use neuronal processes as highways to move extracellularly. Large EV motion on neurites is driven by the binding of EV to a surface receptor that slides on neuronal membrane, thanks to actin cytoskeleton rearrangements. The use of prion protein (PrP)-coated synthetic beads and PrP knock out EVs/neurons points at vesicular PrP and its receptor(s) on neurons in the control of EV motion. Surprisingly, a fraction of large EVs contains actin filaments and has an independent capacity to move in an actin-mediated way, through intermittent contacts with the plasma membrane. Our results unveil, for the first time, a dual mechanism exploited by astrocytic large EVs to passively/actively reach target sites on neurons moving on the neuron surface., Competing Interests: The authors report no conflict of interest., (© 2021 The Authors. Journal of Extracellular Vesicles published by Wiley Periodicals, LLC on behalf of the International Society for Extracellular Vesicles.)

Published

2021

10. Mass spectrometry characterization of light chain fragmentation sites in cardiac AL amyloidosis: insights into the timing of proteolysis.

Author

Lavatelli F, Mazzini G, Ricagno S, Iavarone F, Rognoni P, Milani P, Nuvolone M, Swuec P, Caminito S, Tasaki M, Chaves-Sanjuan A, Urbani A, Merlini G, and Palladini G

Subjects

Amino Acid Sequence, Amyloid metabolism, Chromatography, High Pressure Liquid, Electrophoresis, Gel, Two-Dimensional, Humans, Immunoglobulin Light Chains chemistry, Immunoglobulin Light Chains metabolism, Immunoglobulin Light-chain Amyloidosis metabolism, Peptides analysis, Protein Structure, Secondary, Protein Structure, Tertiary, Proteolysis, Tandem Mass Spectrometry, Amyloid chemistry, Immunoglobulin Light-chain Amyloidosis pathology, Myocardium metabolism

Abstract

Amyloid fibrils are polymeric structures originating from aggregation of misfolded proteins. In vivo , proteolysis may modulate amyloidogenesis and fibril stability. In light chain (AL) amyloidosis, fragmented light chains (LCs) are abundant components of amyloid deposits; however, site and timing of proteolysis are debated. Identification of the N and C termini of LC fragments is instrumental to understanding involved processes and enzymes. We investigated the N and C terminome of the LC proteoforms in fibrils extracted from the hearts of two AL cardiomyopathy patients, using a proteomic approach based on derivatization of N- and C-terminal residues, followed by mapping of fragmentation sites on the structures of native and fibrillar relevant LCs. We provide the first high-specificity map of proteolytic cleavages in natural AL amyloid. Proteolysis occurs both on the LC variable and constant domains, generating a complex fragmentation pattern. The structural analysis indicates extensive remodeling by multiple proteases, largely taking place on poorly folded regions of the fibril surfaces. This study adds novel important knowledge on amyloid LC processing: although our data do not exclude that proteolysis of native LC dimers may destabilize their structure and favor fibril formation, the data show that LC deposition largely precedes the proteolytic events documentable in mature AL fibrils., Competing Interests: Conflict of interest—The authors declare that they have no conflicts of interest with the contents of this article., (© 2020 Lavatelli et al.)

Published

2020

11. High-Light versus Low-Light: Effects on Paired Photosystem II Supercomplex Structural Rearrangement in Pea Plants.

Author

Grinzato A, Albanese P, Marotta R, Swuec P, Saracco G, Bolognesi M, Zanotti G, and Pagliano C

Subjects

Light-Harvesting Protein Complexes chemistry, Photosystem II Protein Complex chemistry, Light, Light-Harvesting Protein Complexes metabolism, Pisum sativum enzymology, Photosystem II Protein Complex metabolism, Thylakoids enzymology

Abstract

In plant grana thylakoid membranes Photosystem II (PSII) associates with a variable number of antenna proteins (LHCII) to form different types of supercomplexes (PSII-LHCII), whose organization is dynamically adjusted in response to light cues, with the C 2 S 2 more abundant in high-light and the C 2 S 2 M 2 in low-light. Paired PSII-LHCII supercomplexes interacting at their stromal surface from adjacent thylakoid membranes were previously suggested to mediate grana stacking. Here, we present the cryo-electron microscopy maps of paired C 2 S 2 and C 2 S 2 M 2 supercomplexes isolated from pea plants grown in high-light and low-light, respectively. These maps show a different rotational offset between the two supercomplexes in the pair, responsible for modifying their reciprocal interaction and energetic connectivity. This evidence reveals a different way by which paired PSII-LHCII supercomplexes can mediate grana stacking at diverse irradiances. Electrostatic stromal interactions between LHCII trimers almost completely overlapping in the paired C 2 S 2 can be the main determinant by which PSII-LHCII supercomplexes mediate grana stacking in plants grown in high-light, whereas the mutual interaction of stromal N-terminal loops of two facing Lhcb4 subunits in the paired C 2 S 2 M 2 can fulfil this task in plants grown in low-light. The high-light induced accumulation of the Lhcb4.3 protein in PSII-LHCII supercomplexes has been previously reported. Our cryo-electron microscopy map at 3.8 Å resolution of the C 2 S 2 supercomplex isolated from plants grown in high-light suggests the presence of the Lhcb4.3 protein revealing peculiar structural features of this high-light-specific antenna important for photoprotection.

Published

2020

12. A combined structural and biochemical approach reveals translocation and stalling of UvrB on the DNA lesion as a mechanism of damage verification in bacterial nucleotide excision repair.

Author

Jaciuk M, Swuec P, Gaur V, Kasprzak JM, Renault L, Dobrychłop M, Nirwal S, Bujnicki JM, Costa A, and Nowotny M

Subjects

Adenosine Triphosphatases metabolism, Bacteria metabolism, Bacterial Proteins chemistry, Bacterial Proteins metabolism, DNA Damage, DNA Repair, Endodeoxyribonucleases metabolism, Models, Molecular, Protein Conformation, Bacteria genetics, DNA Helicases chemistry, DNA Helicases metabolism

Abstract

Nucleotide excision repair (NER) is a DNA repair pathway present in all domains of life. In bacteria, UvrA protein localizes the DNA lesion, followed by verification by UvrB helicase and excision by UvrC double nuclease. UvrA senses deformations and flexibility of the DNA duplex without precisely localizing the lesion in the damaged strand, an element essential for proper NER. Using a combination of techniques, we elucidate the mechanism of the damage verification step in bacterial NER. UvrA dimer recruits two UvrB molecules to its two sides. Each of the two UvrB molecules clamps a different DNA strand using its β-hairpin element. Both UvrB molecules then translocate to the lesion, and UvrA dissociates. The UvrB molecule that clamps the damaged strand gets stalled at the lesion to recruit UvrC. This mechanism allows UvrB to verify the DNA damage and identify its precise location triggering subsequent steps in the NER pathway., (Copyright © 2019 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2020

13. Cas9 Allosteric Inhibition by the Anti-CRISPR Protein AcrIIA6.

Author

Fuchsbauer O, Swuec P, Zimberger C, Amigues B, Levesque S, Agudelo D, Duringer A, Chaves-Sanjuan A, Spinelli S, Rousseau GM, Velimirovic M, Bolognesi M, Roussel A, Cambillau C, Moineau S, Doyon Y, and Goulet A

Subjects

Allosteric Regulation, Bacteriophages genetics, Binding Sites, CRISPR-Associated Protein 9 genetics, CRISPR-Associated Protein 9 ultrastructure, DNA genetics, DNA ultrastructure, Escherichia coli enzymology, Escherichia coli genetics, Humans, K562 Cells, Kinetics, Mutation, Protein Binding, Protein Conformation, Streptococcus thermophilus genetics, Structure-Activity Relationship, Viral Proteins genetics, Viral Proteins ultrastructure, Bacteriophages metabolism, CRISPR-Associated Protein 9 metabolism, CRISPR-Cas Systems, Clustered Regularly Interspaced Short Palindromic Repeats, DNA metabolism, Streptococcus thermophilus enzymology, Viral Proteins metabolism

Abstract

In the arms race against bacteria, bacteriophages have evolved diverse anti-CRISPR proteins (Acrs) that block CRISPR-Cas immunity. Acrs play key roles in the molecular coevolution of bacteria with their predators, use a variety of mechanisms of action, and provide tools to regulate Cas-based genome manipulation. Here, we present structural and functional analyses of AcrIIA6, an Acr from virulent phages, exploring its unique anti-CRISPR action. Our cryo-EM structures and functional data of AcrIIA6 binding to Streptococcus thermophilus Cas9 (St1Cas9) show that AcrIIA6 acts as an allosteric inhibitor and induces St1Cas9 dimerization. AcrIIA6 reduces St1Cas9 binding affinity for DNA and prevents DNA binding within cells. The PAM and AcrIIA6 recognition sites are structurally close and allosterically linked. Mechanistically, AcrIIA6 affects the St1Cas9 conformational dynamics associated with PAM binding. Finally, we identify a natural St1Cas9 variant resistant to AcrIIA6 illustrating Acr-driven mutational escape and molecular diversification of Cas9 proteins., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

14. Cryo-EM Structures of Azospirillum brasilense Glutamate Synthase in Its Oligomeric Assemblies.

Author

Swuec P, Chaves-Sanjuan A, Camilloni C, Vanoni MA, and Bolognesi M

Subjects

Catalysis, Electron Transport, Flavin Mononucleotide metabolism, Flavin-Adenine Dinucleotide metabolism, Iron-Sulfur Proteins metabolism, Iron-Sulfur Proteins ultrastructure, Azospirillum brasilense enzymology, Cryoelectron Microscopy methods, Glutamate Synthase metabolism, Glutamate Synthase ultrastructure

Abstract

Bacterial NADPH-dependent glutamate synthase (GltS) is a complex iron-sulfur flavoprotein that catalyzes the reductive synthesis of two L-Glu molecules from L-Gln and 2-oxo-glutarate. GltS functional unit hosts an α-subunit (αGltS) and a β-subunit (βGltS) that assemble in different αβ oligomers in solution. Here, we present the cryo-electron microscopy structures of Azospirillum brasilense GltS in four different oligomeric states (α 4 β 3 , α 4 β 4 , α 6 β 4 and α 6 β 6 , in the 3.5- to 4.1-Å resolution range). Our study provides a comprehensive GltS model that details the inter-protomeric assemblies and allows unequivocal location of the FAD cofactor and of two electron transfer [4Fe-4S] +1,+2 clusters within βGltS., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

15. Intracerebral Injection of Extracellular Vesicles from Mesenchymal Stem Cells Exerts Reduced Aβ Plaque Burden in Early Stages of a Preclinical Model of Alzheimer's Disease.

Author

Elia CA, Tamborini M, Rasile M, Desiato G, Marchetti S, Swuec P, Mazzitelli S, Clemente F, Anselmo A, Matteoli M, Malosio ML, and Coco S

Subjects

Alzheimer Disease genetics, Alzheimer Disease therapy, Amyloid beta-Peptides metabolism, Animals, Brain metabolism, Cerebral Cortex metabolism, Disease Models, Animal, Extracellular Vesicles metabolism, Female, Hippocampus metabolism, Male, Mesenchymal Stem Cell Transplantation methods, Mice, Mice, Inbred C57BL, Neurites metabolism, Extracellular Vesicles transplantation, Mesenchymal Stem Cells metabolism, Plaque, Amyloid therapy

Abstract

Bone marrow Mesenchymal Stem Cells (BM-MSCs), due to their strong protective and anti-inflammatory abilities, have been widely investigated in the context of several diseases for their possible therapeutic role, based on the release of a highly proactive secretome composed of soluble factors and Extracellular Vesicles (EVs). BM-MSC-EVs, in particular, convey many of the beneficial features of parental cells, including direct and indirect β-amyloid degrading-activities, immunoregulatory and neurotrophic abilities. Therefore, EVs represent an extremely attractive tool for therapeutic purposes in neurodegenerative diseases, including Alzheimer's disease (AD). We examined the therapeutic potential of BM-MSC-EVs injected intracerebrally into the neocortex of APPswe/PS1dE9 AD mice at 3 and 5 months of age, a time window in which the cognitive behavioral phenotype is not yet detectable or has just started to appear. We demonstrate that BM-MSC-EVs are effective at reducing the Aβ plaque burden and the amount of dystrophic neurites in both the cortex and hippocampus. The presence of Neprilysin on BM-MSC-EVs, opens the possibility of a direct β-amyloid degrading action. Our results indicate a potential role for BM-MSC-EVs already in the early stages of AD, suggesting the possibility of intervening before overt clinical manifestations.

Published

2019

16. Cryo-EM structure of cardiac amyloid fibrils from an immunoglobulin light chain AL amyloidosis patient.

Author

Swuec P, Lavatelli F, Tasaki M, Paissoni C, Rognoni P, Maritan M, Brambilla F, Milani P, Mauri P, Camilloni C, Palladini G, Merlini G, Ricagno S, and Bolognesi M

Subjects

Aged, Amino Acid Sequence, Amyloid immunology, Amyloid metabolism, Autopsy, Cryoelectron Microscopy, Humans, Immunoglobulin Light Chains immunology, Immunoglobulin Light Chains metabolism, Immunoglobulin Light-chain Amyloidosis diagnosis, Immunoglobulin Light-chain Amyloidosis immunology, Immunoglobulin Light-chain Amyloidosis metabolism, Male, Myocardium immunology, Myocardium metabolism, Myocardium pathology, Protein Aggregation, Pathological diagnosis, Protein Aggregation, Pathological immunology, Protein Aggregation, Pathological metabolism, Protein Conformation, beta-Strand, Protein Folding, Sequence Alignment, Sequence Homology, Amino Acid, Severity of Illness Index, Amyloid ultrastructure, Immunoglobulin Light Chains ultrastructure, Immunoglobulin Light-chain Amyloidosis pathology, Myocardium ultrastructure, Protein Aggregation, Pathological pathology

Abstract

Systemic light chain amyloidosis (AL)  is a life-threatening disease caused by aggregation and deposition of monoclonal immunoglobulin light chains (LC) in target organs. Severity of heart involvement is the most important factor determining prognosis. Here, we report the 4.0 Å resolution cryo-electron microscopy map and molecular model of amyloid fibrils extracted from the heart of an AL amyloidosis patient with severe amyloid cardiomyopathy. The helical fibrils are composed of a single protofilament, showing typical 4.9 Å stacking and cross-β architecture. Two distinct polypeptide stretches (total of 77 residues) from the LC variable domain (V l ) fit the fibril density. Despite V l high sequence variability, residues stabilizing the fibril core are conserved through different cardiotoxic V l , highlighting structural motifs that may be common to misfolding-prone LCs. Our data shed light on the architecture of LC amyloids, correlate amino acid sequences with fibril assembly, providing the grounds for development of innovative medicines.

Published

2019

17. Identification of a Small Molecule That Compromises the Structural Integrity of Viroplasms and Rotavirus Double-Layered Particles.

Author

Eichwald C, De Lorenzo G, Schraner EM, Papa G, Bollati M, Swuec P, de Rosa M, Milani M, Mastrangelo E, Ackermann M, Burrone OR, and Arnoldi F

Subjects

Animals, Cell Line, Chlorocebus aethiops, Dose-Response Relationship, Drug, Enzyme Inhibitors pharmacology, Rotavirus chemistry, Rotavirus drug effects, Sf9 Cells, Viral Proteins antagonists & inhibitors, Virus Replication drug effects, RNA Polymerase III antagonists & inhibitors, Rotavirus physiology, Small Molecule Libraries pharmacology, Viral Structures drug effects

Abstract

Despite the availability of two attenuated vaccines, rotavirus (RV) gastroenteritis remains an important cause of mortality among children in developing countries, causing about 215,000 infant deaths annually. Currently, there are no specific antiviral therapies available. RV is a nonenveloped virus with a segmented double-stranded RNA genome. Viral genome replication and assembly of transcriptionally active double-layered particles (DLPs) take place in cytoplasmic viral structures called viroplasms. In this study, we describe strong impairment of the early stages of RV replication induced by a small molecule known as an RNA polymerase III inhibitor, ML-60218 (ML). This compound was found to disrupt already assembled viroplasms and to hamper the formation of new ones without the need for de novo transcription of cellular RNAs. This phenotype was correlated with a reduction in accumulated viral proteins and newly made viral genome segments, disappearance of the hyperphosphorylated isoforms of the viroplasm-resident protein NSP5, and inhibition of infectious progeny virus production. In in vitro transcription assays with purified DLPs, ML showed dose-dependent inhibitory activity, indicating the viral nature of its target. ML was found to interfere with the formation of higher-order structures of VP6, the protein forming the DLP outer layer, without compromising its ability to trimerize. Electron microscopy of ML-treated DLPs showed dose-dependent structural damage. Our data suggest that interactions between VP6 trimers are essential, not only for DLP stability, but also for the structural integrity of viroplasms in infected cells. IMPORTANCE Rotavirus gastroenteritis is responsible for a large number of infant deaths in developing countries. Unfortunately, in the countries where effective vaccines are urgently needed, the efficacy of the available vaccines is particularly low. Therefore, the development of antivirals is an important goal, as they might complement the available vaccines or represent an alternative option. Moreover, they may be decisive in fighting the acute phase of infection. This work describes the inhibitory effect on rotavirus replication of a small molecule initially reported as an RNA polymerase III inhibitor. The molecule is the first chemical compound identified that is able to disrupt viroplasms, the viral replication machinery, and to compromise the stability of DLPs by targeting the viral protein VP6. This molecule thus represents a starting point in the development of more potent and less cytotoxic compounds against rotavirus infection., (Copyright © 2018 American Society for Microbiology.)

Published

2018

18. DNA replication and inter-strand crosslink repair: Symmetric activation of dimeric nanomachines?

Author

Swuec P and Costa A

Subjects

Animals, DNA chemistry, Dimerization, Fanconi Anemia, Fanconi Anemia Complementation Group D2 Protein, Humans, DNA Repair, DNA Replication

Abstract

Eukaryotic DNA replication initiation and the Fanconi anemia pathway of interstrand crosslink repair both revolve around the recruitment of a set of DNA-processing factors onto a dimeric protein complex, which functions as a loading platform (MCM and FANCI-FANCD2 respectively). Here we compare and contrast the two systems, identifying a set of unresolved mechanistic questions. How is the dimeric loading platform assembled on the DNA? How can equivalent covalent modification of both factors in a dimer be achieved? Are multicomponent DNA-interacting machines built symmetrically around their dimeric loading platform? Recent biochemical reconstitution studies are starting to shed light on these issues., (Copyright © 2016. Published by Elsevier B.V.)

Published

2017

19. Mechanism of Ubiquitination and Deubiquitination in the Fanconi Anemia Pathway.

Author

van Twest S, Murphy VJ, Hodson C, Tan W, Swuec P, O'Rourke JJ, Heierhorst J, Crismani W, and Deans AJ

Subjects

Cell Line, DNA genetics, DNA metabolism, DNA-Binding Proteins metabolism, Fanconi Anemia genetics, Fanconi Anemia Complementation Group A Protein metabolism, Fanconi Anemia Complementation Group C Protein metabolism, Fanconi Anemia Complementation Group D2 Protein genetics, Fanconi Anemia Complementation Group E Protein metabolism, Fanconi Anemia Complementation Group G Protein metabolism, Fanconi Anemia Complementation Group L Protein metabolism, Fanconi Anemia Complementation Group Proteins genetics, Humans, Inhibitor of Differentiation Protein 2 metabolism, Multiprotein Complexes, Nuclear Proteins metabolism, Protein Binding, Protein Multimerization, Recombinant Proteins metabolism, Substrate Specificity, Time Factors, Transfection, Ubiquitin-Specific Proteases metabolism, Fanconi Anemia metabolism, Fanconi Anemia Complementation Group D2 Protein metabolism, Fanconi Anemia Complementation Group Proteins metabolism, Ubiquitination

Abstract

Monoubiquitination and deubiquitination of FANCD2:FANCI heterodimer is central to DNA repair in a pathway that is defective in the cancer predisposition syndrome Fanconi anemia (FA). The "FA core complex" contains the RING-E3 ligase FANCL and seven other essential proteins that are mutated in various FA subtypes. Here, we purified recombinant FA core complex to reveal the function of these other proteins. The complex contains two spatially separate FANCL molecules that are dimerized by FANCB and FAAP100. FANCC and FANCE act as substrate receptors and restrict monoubiquitination to the FANCD2:FANCI heterodimer in only a DNA-bound form. FANCA and FANCG are dispensable for maximal in vitro ubiquitination. Finally, we show that the reversal of this reaction by the USP1:UAF1 deubiquitinase only occurs when DNA is disengaged. Our work reveals the mechanistic basis for temporal and spatial control of FANCD2:FANCI monoubiquitination that is critical for chemotherapy responses and prevention of Fanconi anemia., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

20. The FA Core Complex Contains a Homo-dimeric Catalytic Module for the Symmetric Mono-ubiquitination of FANCI-FANCD2.

Author

Swuec P, Renault L, Borg A, Shah F, Murphy VJ, van Twest S, Snijders AP, Deans AJ, and Costa A

Subjects

Amino Acid Sequence, Chromatography, High Pressure Liquid, DNA-Binding Proteins chemistry, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Dimerization, Fanconi Anemia Complementation Group D2 Protein chemistry, Fanconi Anemia Complementation Group D2 Protein genetics, Fanconi Anemia Complementation Group Proteins chemistry, Fanconi Anemia Complementation Group Proteins genetics, Humans, Mass Spectrometry, Microscopy, Electron, Protein Multimerization, Protein Structure, Tertiary, Substrate Specificity, Ubiquitination, Fanconi Anemia Complementation Group D2 Protein metabolism, Fanconi Anemia Complementation Group Proteins metabolism

Abstract

Activation of the main DNA interstrand crosslink repair pathway in higher eukaryotes requires mono-ubiquitination of FANCI and FANCD2 by FANCL, the E3 ligase subunit of the Fanconi anemia core complex. FANCI and FANCD2 form a stable complex; however, the molecular basis of their ubiquitination is ill defined. FANCD2 mono-ubiquitination by FANCL is stimulated by the presence of the FANCB and FAAP100 core complex components, through an unknown mechanism. How FANCI mono-ubiquitination is achieved remains unclear. Here, we use structural electron microscopy, combined with crosslink-coupled mass spectrometry, to find that FANCB, FANCL, and FAAP100 form a dimer of trimers, containing two FANCL molecules that are ideally poised to target both FANCI and FANCD2 for mono-ubiquitination. The FANCC-FANCE-FANCF subunits bridge between FANCB-FANCL-FAAP100 and the FANCI-FANCD2 substrate. A transient interaction with FANCC-FANCE-FANCF alters the FANCI-FANCD2 configuration, stabilizing the dimerization interface. Our data provide a model to explain how equivalent mono-ubiquitination of FANCI and FANCD2 occurs., (Copyright © 2017 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2017

21. A supramolecular assembly mediates lentiviral DNA integration.

Author

Ballandras-Colas A, Maskell DP, Serrao E, Locke J, Swuec P, Jónsson SR, Kotecha A, Cook NJ, Pye VE, Taylor IA, Andrésdóttir V, Engelman AN, Costa A, and Cherepanov P

Subjects

Catalytic Domain, Cryoelectron Microscopy, DNA, Viral chemistry, DNA, Viral ultrastructure, Drug Design, HIV Integrase ultrastructure, HIV Integrase Inhibitors chemistry, HIV-1 enzymology, HIV-1 ultrastructure, Humans, Models, Molecular, Protein Domains, Static Electricity, Virus Assembly, HIV Integrase chemistry, HIV-1 chemistry, Virus Integration

Abstract

Retroviral integrase (IN) functions within the intasome nucleoprotein complex to catalyze insertion of viral DNA into cellular chromatin. Using cryo-electron microscopy, we now visualize the functional maedi-visna lentivirus intasome at 4.9 angstrom resolution. The intasome comprises a homo-hexadecamer of IN with a tetramer-of-tetramers architecture featuring eight structurally distinct types of IN protomers supporting two catalytically competent subunits. The conserved intasomal core, previously observed in simpler retroviral systems, is formed between two IN tetramers, with a pair of C-terminal domains from flanking tetramers completing the synaptic interface. Our results explain how HIV-1 IN, which self-associates into higher-order multimers, can form a functional intasome, reconcile the bulk of early HIV-1 IN biochemical and structural data, and provide a lentiviral platform for design of HIV-1 IN inhibitors., (Copyright © 2017, American Association for the Advancement of Science.)

Published

2017

22. Human RECQ1 helicase-driven DNA unwinding, annealing, and branch migration: insights from DNA complex structures.

Author

Pike AC, Gomathinayagam S, Swuec P, Berti M, Zhang Y, Schnecke C, Marino F, von Delft F, Renault L, Costa A, Gileadi O, and Vindigni A

Subjects

Animals, Chromatography, Gel, Crystallization, Crystallography, X-Ray, DNA, Cruciform physiology, DNA, Single-Stranded chemistry, Escherichia coli metabolism, Humans, Insecta, Molecular Conformation, Nucleic Acid Denaturation, Nucleotides chemistry, Protein Binding, Protein Structure, Tertiary, Zinc chemistry, DNA chemistry, DNA Helicases chemistry, RecQ Helicases chemistry

Abstract

RecQ helicases are a widely conserved family of ATP-dependent motors with diverse roles in nearly every aspect of bacterial and eukaryotic genome maintenance. However, the physical mechanisms by which RecQ helicases recognize and process specific DNA replication and repair intermediates are largely unknown. Here, we solved crystal structures of the human RECQ1 helicase in complexes with tailed-duplex DNA and ssDNA. The structures map the interactions of the ssDNA tail and the branch point along the helicase and Zn-binding domains, which, together with reported structures of other helicases, define the catalytic stages of helicase action. We also identify a strand-separating pin, which (uniquely in RECQ1) is buttressed by the protein dimer interface. A duplex DNA-binding surface on the C-terminal domain is shown to play a role in DNA unwinding, strand annealing, and Holliday junction (HJ) branch migration. We have combined EM and analytical ultracentrifugation approaches to show that RECQ1 can form what appears to be a flat, homotetrameric complex and propose that RECQ1 tetramers are involved in HJ recognition. This tetrameric arrangement suggests a platform for coordinated activity at the advancing and receding duplexes of an HJ during branch migration.

Published

2015

23. DNA binding polarity, dimerization, and ATPase ring remodeling in the CMG helicase of the eukaryotic replisome.

Author

Costa A, Renault L, Swuec P, Petojevic T, Pesavento JJ, Ilves I, MacLellan-Gibson K, Fleck RA, Botchan MR, and Berger JM

Subjects

Adenosine Triphosphatases chemistry, Adenosine Triphosphatases metabolism, Adenosine Triphosphate analogs & derivatives, Adenosine Triphosphate chemistry, Adenosine Triphosphate metabolism, Animals, Cell Cycle Proteins metabolism, Chromosomal Proteins, Non-Histone metabolism, DNA chemistry, DNA metabolism, DNA Replication, DNA, Single-Stranded chemistry, DNA, Single-Stranded metabolism, DNA-Binding Proteins metabolism, Drosophila Proteins metabolism, Drosophila melanogaster metabolism, Eukaryotic Cells metabolism, Microscopy, Electron, Models, Molecular, Multiprotein Complexes metabolism, Multiprotein Complexes ultrastructure, Protein Binding, Protein Multimerization, Protein Structure, Quaternary, Protein Structure, Tertiary, Protein Subunits chemistry, Protein Subunits metabolism, RNA Splicing Factors, RNA-Binding Proteins chemistry, RNA-Binding Proteins metabolism, Repressor Proteins chemistry, Repressor Proteins metabolism, Cell Cycle Proteins chemistry, Chromosomal Proteins, Non-Histone chemistry, DNA-Binding Proteins chemistry, Drosophila Proteins chemistry, Minichromosome Maintenance Proteins chemistry, Minichromosome Maintenance Proteins metabolism, Multiprotein Complexes chemistry

Abstract

The Cdc45/Mcm2-7/GINS (CMG) helicase separates DNA strands during replication in eukaryotes. How the CMG is assembled and engages DNA substrates remains unclear. Using electron microscopy, we have determined the structure of the CMG in the presence of ATPγS and a DNA duplex bearing a 3' single-stranded tail. The structure shows that the MCM subunits of the CMG bind preferentially to single-stranded DNA, establishes the polarity by which DNA enters into the Mcm2-7 pore, and explains how Cdc45 helps prevent DNA from dissociating from the helicase. The Mcm2-7 subcomplex forms a cracked-ring, right-handed spiral when DNA and nucleotide are bound, revealing unexpected congruencies between the CMG and both bacterial DnaB helicases and the AAA+ motor of the eukaryotic proteasome. The existence of a subpopulation of dimeric CMGs establishes the subunit register of Mcm2-7 double hexamers and together with the spiral form highlights how Mcm2-7 transitions through different conformational and assembly states as it matures into a functional helicase., (Copyright © 2014, Costa et al.)

Published

2014

24. Molecular mechanism of double Holliday junction dissolution.

Author

Swuec P and Costa A

Abstract

Processing of homologous recombination intermediates is tightly coordinated to ensure that chromosomal integrity is maintained and tumorigenesis avoided. Decatenation of double Holliday junctions, for example, is catalysed by two enzymes that work in tight coordination and belong to the same 'dissolvasome' complex. Within the dissolvasome, the RecQ-like BLM helicase provides the translocase function for Holliday junction migration, while the topoisomerase III alpha-RMI1 subcomplex works as a proficient DNA decatenase, together resulting in double-Holliday-junction unlinking. Here, we review the available architectural and biochemical knowledge on the dissolvasome machinery, with a focus on the structural interplay between its components.

Published

2014

25. Architecture and DNA recognition elements of the Fanconi anemia FANCM-FAAP24 complex.

Author

Coulthard R, Deans AJ, Swuec P, Bowles M, Costa A, West SC, and McDonald NQ

Subjects

Adenosine Triphosphate chemistry, Catalytic Domain, Cell Survival drug effects, Coordination Complexes chemistry, Cryoelectron Microscopy, Crystallography, X-Ray, DNA Damage, DNA Helicases metabolism, DNA Repair, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Fanconi Anemia Complementation Group Proteins, Gene Knockdown Techniques, HEK293 Cells, Humans, Hydrolysis, Mitomycin pharmacology, Models, Molecular, Mutagens pharmacology, Nucleic Acid Conformation, Oligonucleotides chemistry, Protein Binding, Protein Structure, Secondary, RNA, Small Interfering genetics, DNA Helicases chemistry, DNA-Binding Proteins chemistry

Abstract

Fanconi anemia (FA) is a disorder associated with a failure in DNA repair. FANCM (defective in FA complementation group M) and its partner FAAP24 target other FA proteins to sites of DNA damage. FANCM-FAAP24 is related to XPF/MUS81 endonucleases but lacks endonucleolytic activity. We report a structure of an FANCM C-terminal fragment (FANCMCTD) bound to FAAP24 and DNA. This S-shaped structure reveals the FANCM (HhH)2 domain is buried, whereas the FAAP24 (HhH)2 domain engages DNA. We identify a second DNA contact and a metal center within the FANCM pseudo-nuclease domain and demonstrate that mutations in either region impair double-stranded DNA binding in vitro and FANCM-FAAP24 function in vivo. We show the FANCM translocase domain lies in proximity to FANCMCTD by electron microscopy and that binding fork DNA structures stimulate its ATPase activity. This suggests a tracking model for FANCM-FAAP24 until an encounter with a stalled replication fork triggers ATPase-mediated fork remodeling., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

26. Prediction of inhibitory activities of Hsp90 inhibitors.

Author

Swuec P and Barlow DJ

Subjects

Binding Sites, Computer Simulation, HSP90 Heat-Shock Proteins metabolism, Humans, Ligands, Protein Structure, Tertiary, Quantitative Structure-Activity Relationship, Software, Thermodynamics, HSP90 Heat-Shock Proteins antagonists & inhibitors

Abstract

Here, we report on the development of a novel methodology to aid in design of Hsp90 inhibitors, using molecular docking combined with artificial neural network (ANN) modelling. Inhibitors are first docked into the ATPase site of the Human Hsp90α crystal structures and the thermodynamic properties of the complexes together with various physical-chemical properties of the ligands are used as input to train a simple feed-forward, back propagation ANN, to predict the inhibitors' pIC(50)s. For an objective test set of 60 known Hsp90 inhibitors for which there are no crystallographic data available, the trained ANN is shown to give pIC(50)s accurate to within ±1 log unit, and the predictions are sufficiently good as to allow the majority of the inhibitors to be ranked correctly according to their potency., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012