Your search keyword '"Hydrogen–deuterium exchange"' showing total 4,458 results

1. Reactivity of N terminal histidine of peptides towards excipients/impurity of excipients: A case study of liraglutide excipient compatibility study.

Author

Sheikh, Azahar R., Vitore, Jyotsna G., Bhalekar, Vijay S., Jain, Sonali, Kukreja, Divya, Giri, Tushar, Sharma, Nitish, Benival, Derajram, and Shah, Ravi P.

Subjects

*PEPTIDES, *HYDROGEN-deuterium exchange, *GLYCOLIC acid, *LACTIC acid, *POLYETHYLENE glycol

Abstract

The selection of quality excipients is a crucial step in peptide formulation development. Apart from excipient incompatibility, process-related impurities or degradants of an excipient can interact with peptide-active pharmaceutical ingredients, forming the interaction products. The formaldehyde has been reported as an impurity of excipient in polyethylene glycol, glycerol, magnesium stearate, microcrystalline cellulose, mannitol, etc. The peptide contains various amino acids such as histidine, lysine, and arginine having free amine groups. These amine groups act as strong nucleophile and can increase the reactivity of peptides. PLGA is the most widely used biodegradable polymer in sustained-release formulations. The hydrolysis of PLGA generates glycolic acid and lactic acid impurities, which can form the interaction product with the amines of peptides. During the formulation development of Liraglutide, we have found few interaction products. The systematic characterization and mechanistic understanding of these interaction products lead us to imidazopyrimidine, glycolyl, and lactolyl moieties. These interaction products have been characterized thoroughly with the use of LC-HRMS, MS/MS, and hydrogen-deuterium exchange mass studies. The study revealed that the reactivity of N-terminal histidine must be considered for formulation development. Moreover, the quality of excipients with respect to presence of impurities must be considered as critical material attributes. [ABSTRACT FROM AUTHOR]

Published

2024

2. Ligand-induced conformational changes in the β1-adrenergic receptor revealed by hydrogen-deuterium exchange mass spectrometry.

Author

Toporowska, Joanna, Kapoor, Parth, Musgaard, Maria, Gherbi, Karolina, Sengmany, Kathy, Qu, Feng, Soave, Mark, Yen, Hsin-Yung, Hansen, Kjetil, Jazayeri, Ali, Hopper, Jonathan T. S., and Politis, Argyris

Subjects

HYDROGEN-deuterium exchange, DRUG discovery, STRUCTURAL dynamics, LIGAND binding (Biochemistry), DRUG target

Abstract

G Protein Coupled Receptors (GPCRs) constitute the largest family of signalling proteins responsible for translating extracellular stimuli into intracellular functions. They play crucial roles in numerous physiological processes and are major targets for drug discovery. Dysregulation of GPCRs is implicated in various diseases, making understanding their structural dynamics critical for therapeutic development. Here, we use Hydrogen Deuterium Exchange Mass Spectrometry (HDX-MS) to explore the structural dynamics of the turkey β1-adrenergic receptor (tβ1AR) bound with nine different ligands, including agonists, partial agonists, and antagonists. We find that these ligands induce distinct dynamic patterns across the receptor, which can be grouped by compound modality. Notably, full agonist binding destabilises the intracellular loop 1 (ICL1), while antagonist binding stabilises it, highlighting ICL1's role in G protein recruitment. Our findings indicate that the conserved L72 residue in ICL1 is crucial for maintaining receptor structural integrity and stabilising the GDP-bound state. Overall, our results provide a platform for determining drug modality and highlight how HDX-MS can be used to dissect receptor ligand interaction properties and GPCR mechanism. GPCRs are vital drug targets. Here, authors use HDX-MS to gain insight into structural dynamics of β1AR upon ligand binding, revealing agonist-induced destabilisation and antagonist stabilisation of ICL1. [ABSTRACT FROM AUTHOR]

Published

2024

3. Selective Synthesis of Deuterated cis- and trans-Isohumulones and trans-Isohumulinones.

Author

Hamper, Bruce C., Campbell, Hunter J., Luo, Rensheng, Murphy, Matthew, Gleason, Patrick, Smith, Trevor, and Jagan, Rajamoni

Subjects

*ACYL group, *DICHLOROMETHANE, *DEUTERATION, *MAGNESIUM salts, *MASS spectrometry

Abstract

Deuterated isohumulones can be prepared directly from humulones by an acyloin ring contraction under either magnesium-catalyzed basic conditions or by photochemical-induced reactions in deuterated solvents. Reactions of humulones with biphasic methylene chloride/aqueous NaOD and MgSO4 in D2 O leads to stereoselective formation of cis - d3-isohumulones (cis / trans ratio of 82:18) as the magnesium salts in yields of 71–83%. Greater than 95% incorporation of three deuterons is observed at the C5 position of the pentenone ring and the methylene position of the C4 acyl group. Photochemical isomerization with a 400 nm blue LED source enables stereospecific formation of deuterated trans -isohumulones in 36–82% yield with greater than 95% incorporation of deuterium at the C5 ring position. Oxidation of humulones with cumene hydroperoxide in basic D2 O gives isohumulinones with partial 55–73% incorporation of deuterium due to keto–enol isomerization of the methylene substituent of the C4 acyl group. The structural identities of the deuterated products are determined by a combination of negative-mode electrospray mass spectrometry (MS-ESI–) and 2D heteronuclear proton–carbon HMQC NMR analysis. [ABSTRACT FROM AUTHOR]

Published

2024

4. Activation of parkin by a molecular glue.

Author

Sauvé, Véronique, Stefan, Eric, Croteau, Nathalie, Goiran, Thomas, Fakih, Rayan, Bansal, Nupur, Hadzipasic, Adelajda, Fang, Jing, Murugan, Paramasivam, Chen, Shimin, Fon, Edward A., Hirst, Warren D., Silvian, Laura F., Trempe, Jean-François, and Gehring, Kalle

Subjects

PARKIN (Protein), ISOTHERMAL titration calorimetry, MITOCHONDRIAL proteins, PARKINSON'S disease, HYDROGEN-deuterium exchange

Abstract

Mutations in parkin and PINK1 cause early-onset Parkinson's disease (EOPD). The ubiquitin ligase parkin is recruited to damaged mitochondria and activated by PINK1, a kinase that phosphorylates ubiquitin and the ubiquitin-like domain of parkin. Activated phospho-parkin then ubiquitinates mitochondrial proteins to target the damaged organelle for degradation. Here, we present the mechanism of activation of a new class of small molecule allosteric modulators that enhance parkin activity. The compounds act as molecular glues to enhance the ability of phospho-ubiquitin (pUb) to activate parkin. Ubiquitination assays and isothermal titration calorimetry with the most active compound (BIO-2007817) identify the mechanism of action. We present the crystal structure of a closely related compound (BIO-1975900) bound to a complex of parkin and two pUb molecules. The compound binds next to pUb on RING0 and contacts both proteins. Hydrogen-deuterium exchange mass spectrometry (HDX-MS) experiments confirm that activation occurs through release of the catalytic Rcat domain. In organello and mitophagy assays demonstrate that BIO-2007817 partially rescues the activity of parkin EOPD mutants, R42P and V56E, offering a basis for the design of activators as therapeutics for Parkinson's disease. Parkin is a ubiquitin ligase that protects against early-onset Parkinson's disease. Here, the authors show a molecular glue that promotes binding of phosphorylated ubiquitin to parkin and rescues the mitophagy defect of mutations in the parkin ubiquitin-like domain. [ABSTRACT FROM AUTHOR]

Published

2024

5. Interdomain-linkers control conformational transitions in the SLC23 elevator transporter UraA.

Author

Kuhn, Benedikt T., Zöller, Jonathan, Zimmermann, Iwan, Gemeinhardt, Tim, Özkul, Dogukan H., Langer, Julian D., Seeger, Markus A., and Geertsma, Eric R.

Subjects

CARRIER proteins, HYDROGEN-deuterium exchange, RELATIVE motion, MASS spectrometry, ELEVATORS

Abstract

Uptake of nucleobases and ascorbate is an essential process in all living organisms mediated by SLC23 transport proteins. These transmembrane carriers operate via the elevator alternating-access mechanism, and are composed of two rigid domains whose relative motion drives transport. The lack of large conformational changes within these domains suggests that the interdomain-linkers act as flexible tethers. Here, we show that interdomain-linkers are not mere tethers, but have a key regulatory role in dictating the conformational space of the transporter and defining the rotation axis of the mobile transport domain. By resolving a wide inward-open conformation of the SLC23 elevator transporter UraA and combining biochemical studies using a synthetic nanobody as conformational probe with hydrogen-deuterium exchange mass spectrometry, we demonstrate that interdomain-linkers control the function of transport proteins by influencing substrate affinity and transport rate. These findings open the possibility to allosterically modulate the activity of elevator proteins by targeting their linkers. Elevator transporters, like SLC23 proteins, transport solutes by a mechanism involving a reorientation of two rigid domains. Here, the authors show that linkers connecting these domains control the carrier's conformational space and thus its function. [ABSTRACT FROM AUTHOR]

Published

2024

6. The importance of the location of the N-terminus in successful protein folding in vivo and in vitro.

Author

Dall, Natalie R., Mendonça, Carolina A. T. F., Vera, Héctor L. Torres, and Marqusee, Susan

Subjects

*ESCHERICHIA coli, *PROTEIN folding, *PROTEIN expression, *HYDROGEN-deuterium exchange, *CIRCULAR dichroism

Abstract

Protein folding in the cell often begins during translation. Many proteins fold more efficiently cotranslationally than when refolding from a denatured state. Changing the vectorial synthesis of the polypeptide chain through circular permutation could impact functional, soluble protein expression and interactions with cellular proteostasis factors. Here, we measure the solubility and function of every possible circular permutant (CP) of HaloTag in Escherichia coli cell lysate using a gel-based assay, and in living E. coli cells via FACS-seq. We find that 78% of HaloTag CPs retain protein function, though a subset of these proteins are also highly aggregation-prone. We examine the function of each CP in E. coli cells lacking the cotranslational chaperone trigger factor and the intracellular protease Lon and find no significant changes in function as a result of modifying the cellular proteostasis network. Finally, we biophysically characterize two topologically interesting CPs in vitro via circular dichroism and hydrogen-deuterium exchange coupled with mass spectrometry to reveal changes in global stability and folding kinetics with circular permutation. For CP33, we identify a change in the refolding intermediate as compared to wild-type (WT) HaloTag. Finally, we show that the strongest predictor of aggregation-prone expression in cells is the introduction of termini within the refolding intermediate. These results, in addition to our finding that termini insertion within the conformationally restrained core is most disruptive to protein function, indicate that successful folding of circular permutants may depend more on changes in folding pathway and termini insertion in flexible regions than on the availability of proteostasis factors. [ABSTRACT FROM AUTHOR]

Published

2024

7. Investigational Study of Mesalamine Dissolution Discrepancy: Utilization of Hyphenated Ultrahigh Performance Liquid Chromatography‐Charged Aerosol Detection‐High‐Resolution Mass Spectrometry.

Author

Kumar, Sumit, Vakkala, Sudhakar, Ganesan, Thipashini, Batna, Ravibabu, See, Hong Heng, Allada, Ravikiran, and Shah, Ravi P.

Subjects

*INFLAMMATORY bowel diseases, *MASS spectrometry, *HIGH temperatures, *MESALAMINE, *AEROSOLS

Abstract

Pentasa (mesalamine/MSLM) is a widely prescribed delayed‐release capsule formulation for the treatment of inflammatory bowel disease. During dissolution study of Pentasa through ultraviolet (UV) spectroscopy, an unusual end‐release of about 110% has been observed. Initial liquid chromatography‐UV (LC‐UV) analyses of these dissolution samples confirmed three prominent peaks other than MSLM with a significant area percentage. Further systematic investigation was carried out by incubating active pharmaceutical ingredient in dissolution media for a longer duration and at elevated temperature followed by analysis through an inverse gradient LC‐charged aerosol detector (CAD). LC–high‐resolution mass spectrometry (HRMS) and online hydrogen‐deuterium exchange (HDX) mass spectrometry were also employed to identify and characterize these artifact products. The area % of prominent artifacts in LC‐UV was found to be way significant when compared to the area % obtained through inverse LC‐CAD, as CAD quantifies the peaks independent of the UV wavelength of absorbance. Inverse LC‐CAD was suitable to determine the relative response factor, whereas LC‐HRMS/MS and online HDX‐MS supported the characterization of these artifacts. These artifacts were found to be trimers, tetramers of MSLM formed due to polymerization, imparting additional pi‐bonds resulting in high UV absorptivity. These techniques when used in combinations serve complimentary to each other during such investigations. [ABSTRACT FROM AUTHOR]

Published

2024

8. Allosteric activation of the co-receptor BAK1 by the EFR receptor kinase initiates immune signaling.

Author

MÃ?hlenbeck, Henning, Yuko Tsutsui, Lemmon, Mark A., Bender, Kyle W., and Zipfel, Cyril

Subjects

*ELONGATION factors (Biochemistry), *HYDROGEN-deuterium exchange, *CELLULAR signal transduction, *SUPPRESSOR mutation, *PROTEIN domains

Abstract

Transmembrane signaling by plant receptor kinases (RKs) has long been thought to involve reciprocal trans-phosphorylation of their intracellular kinase domains. The fact that many of these are pseudokinase domains, however, suggests that additional mechanisms must govern RK signaling activation. Non-catalytic signaling mechanisms of protein kinase domains have been described in metazoans, but information is scarce for plants. Recently, a non-catalytic function was reported for the leucine-rich repeat (LRR)-RK subfamily XIIa member EFR (elongation factor Tu receptor) and phosphorylation-dependent conformational changes were proposed to regulate signaling of RKs with non-RD kinase domains. Here, using EFR as a model, we describe a non-catalytic activation mechanism for LRR-RKs with non-RD kinase domains. EFR is an active kinase, but a kinase-dead variant retains the ability to enhance catalytic activity of its co-receptor kinase BAK1/SERK3 (brassinosteroid insensitive 1-associated kinase 1/somatic embryogenesis receptor kinase 3). Applying hydrogen-deuterium exchange mass spectrometry (HDX-MS) analysis and designing homology-based intragenic suppressor mutations, we provide evidence that the EFR kinase domain must adopt its active conformation in order to activate BAK1 allosterically, likely by supporting aC-helix positioning in BAK1. Our results suggest a conformational toggle model for signaling, in which BAK1 first phosphorylates EFR in the activation loop to stabilize its active conformation, allowing EFR in turn to allosterically activate BAK1. [ABSTRACT FROM AUTHOR]

Published

2024

9. Using mass spectrometry‐based methods to understand amyloid formation and inhibition of alpha‐synuclein and amyloid beta.

Author

Wagner, Wesley J. and Gross, Michael L.

Subjects

*AMYLOID, *AMINO acid separation, *ALPHA-synuclein, *PROTEIN fractionation, *DEUTERIUM, *HYDROGEN-deuterium exchange, *ION mobility

Abstract

Amyloid fibrils, insoluble β‐sheets structures that arise from protein misfolding, are associated with several neurodegenerative disorders. Many small molecules have been investigated to prevent amyloid fibrils from forming; however, there are currently no therapeutics to combat these diseases. Mass spectrometry (MS) is proving to be effective for studying the high order structure (HOS) of aggregating proteins and for determining structural changes accompanying protein–inhibitor interactions. When combined with native MS (nMS), gas‐phase ion mobility, protein footprinting, and chemical cross‐linking, MS can afford regional and sometimes amino acid spatial resolution of the aggregating protein. The spatial resolution is greater than typical low‐resolution spectroscopic, calorimetric, and the traditional ThT fluorescence methods used in amyloid research today. High‐resolution approaches can struggle when investigating protein aggregation, as the proteins exist as complex oligomeric mixtures of many sizes and several conformations or polymorphs. Thus, MS is positioned to complement both high‐ and low‐resolution approaches to studying amyloid fibril formation and protein–inhibitor interactions. This review covers basics in MS paired with ion mobility, continuous hydrogen‐deuterium exchange (continuous HDX), pulsed hydrogen‐deuterium exchange (pulsed HDX), fast photochemical oxidation of proteins (FPOP) and other irreversible labeling methods, and chemical cross‐linking. We then review the applications of these approaches to studying amyloid‐prone proteins with a focus on amyloid beta and alpha‐synuclein. Another focus is the determination of protein–inhibitor interactions. The expectation is that MS will bring new insights to amyloid formation and thereby play an important role to prevent their formation. [ABSTRACT FROM AUTHOR]

Published

2024

10. Probe capsid structure stability and dynamics of adeno‐associated virus as an important viral vector for gene therapy by hydrogen‐deuterium exchange‐mass spectrometry.

Author

Ye, Xiang, Hu, Yunli, Qiu, Haibo, and Li, Ning

Abstract

Adeno‐associated virus (AAV), a widely used gene therapy vector, is a small, nonenveloped virus that contains a single‐stranded DNA genome with a maximum length of 4.7 kb. Despite extensive biophysical and structural characterization, many aspects of AAV functions remain elusive. This knowledge gap is primarily due to a lack of structurally resolved dynamic information and the absence of structural coverage of functionally critical segments on the AAV capsid. Here, we developed a protocol to study AAV structural dynamics by hydrogen‐deuterium exchange mass spectrometry (HDX‐MS), a powerful method for monitoring protein structure stability and dynamics in solution. We performed HDX‐MS measurements on AAVs without or with different DNA payloads of different sizes, and obtained detailed dynamic information on the entire AAV sequence including the two functionally important segments not previously structurally characterized. The unique N terminus of the capsid protein VP1 (VP1u) was found to adopt a highly dynamic and unstable conformation with low HDX protection across the entire region, whereas the presence of a DNA payload increased its protection. The VP1 and VP2 shared region (VP1/2) showed no measurable protection, with or without DNA. Differential HDX between empty and full capsid samples allowed us to identify potential new DNA‐capsid interaction sites located primarily around the five‐fold channel, which differ from the three‐fold pocket binding site previously identified. Our HDX‐MS method for characterizing AAV structural dynamics opens a new way for future efforts to understand AAV structure–function relationships and engineer next‐generation AAV vectors with improved gene delivery properties. [ABSTRACT FROM AUTHOR]

Published

2024

11. NMR study of the structure and dynamics of the BRCT domain from the kinetochore protein KKT4.

Author

Ludzia, Patryk, Hayashi, Hanako, Robinson, Timothy, Akiyoshi, Bungo, and Redfield, Christina

Abstract

KKT4 is a multi-domain kinetochore protein specific to kinetoplastids, such as Trypanosoma brucei. It lacks significant sequence similarity to known kinetochore proteins in other eukaryotes. Our recent X-ray structure of the C-terminal region of KKT4 shows that it has a tandem BRCT (BRCA1 C Terminus) domain fold with a sulfate ion bound in a typical binding site for a phosphorylated serine or threonine. Here we present the 1H, 13C and 15N resonance assignments for the BRCT domain of KKT4 (KKT4463–645) from T. brucei. We show that the BRCT domain can bind phosphate ions in solution using residues involved in sulfate ion binding in the X-ray structure. We have used these assignments to characterise the secondary structure and backbone dynamics of the BRCT domain in solution. Mutating the residues involved in phosphate ion binding in T. brucei KKT4 BRCT results in growth defects confirming the importance of the BRCT phosphopeptide-binding activity in vivo. These results may facilitate rational drug design efforts in the future to combat diseases caused by kinetoplastid parasites. [ABSTRACT FROM AUTHOR]

Published

2024

12. Temporal and spatial resolution of distal protein motions that activate hydrogen tunneling in soybean lipoxygenase

Author

Zaragoza, Jan Paulo T, Offenbacher, Adam R, Hu, Shenshen, Gee, Christine L, Firestein, Zachary M, Minnetian, Natalie, Deng, Zhenyu, Fan, Flora, Iavarone, Anthony T, and Klinman, Judith P

Subjects

Biochemistry and Cell Biology, Chemical Sciences, Biological Sciences, Lipoxygenase, Glycine max, Fluorescent Dyes, Motion, Hydrogen, thermal activation, hydrogen tunneling, hydrogen-deuterium exchange, Stokes shift decay, room temperature X-ray, hydrogen–deuterium exchange

Abstract

The enzyme soybean lipoxygenase (SLO) provides a prototype for deep tunneling mechanisms in hydrogen transfer catalysis. This work combines room temperature X-ray studies with extended hydrogen-deuterium exchange experiments to define a catalytically-linked, radiating cone of aliphatic side chains that connects an active site iron center of SLO to the protein-solvent interface. Employing eight variants of SLO that have been appended with a fluorescent probe at the identified surface loop, nanosecond fluorescence Stokes shifts have been measured. We report a remarkable identity of the energies of activation (Ea) for the Stokes shifts decay rates and the millisecond C-H bond cleavage step that is restricted to side chain mutants within an identified thermal network. These findings implicate a direct coupling of distal protein motions surrounding the exposed fluorescent probe to active site motions controlling catalysis. While the role of dynamics in enzyme function has been predominantly attributed to a distributed protein conformational landscape, the presented data implicate a thermally initiated, cooperative protein reorganization that occurs on a timescale faster than nanosecond and represents the enthalpic barrier to the reaction of SLO.

Published

2023

13. Glucocorticoid receptor signaling: intricacies and therapeutic opportunities.

Author

Clarisse, Dorien, Van Moortel, Laura, Van Leene, Chloé, Gevaert, Kris, and De Bosscher, Karolien

Subjects

*GLUCOCORTICOID receptors, *CONFORMATIONAL analysis, *HYDROGEN-deuterium exchange, *CHROMATIN, *DRUG target

Abstract

By integrating technologies that study chromatin conformation, accessibility, modification, and coregulator recruitment, the molecular basis of the cell-type-specific actions of glucocorticoids (GCs) can be increasingly understood. Therapeutic exploitation of crosstalk between nuclear receptors is gaining traction and has offered strategies to sensitize cells to GCs. Conformational analyses of the glucocorticoid receptor (GR) [via hydrogen–deuterium exchange mass spectrometry (HDX-MS)] are offering a biophysical basis for ligand-binding domain (LBD)–DNA-binding domain (DBD) interdomain communication, the degree of which differs depending on the ligand. Chromatin remodeling complexes are essential to finetune GR activity, not only for transcriptional activation but also for transcriptional repression. Condensate formation is emerging as an important determinant of GR complex assembly on chromatin. The glucocorticoid receptor (GR) is a major nuclear receptor (NR) drug target for the treatment of inflammatory disorders and several cancers. Despite the effectiveness of GR ligands, their systemic action triggers a plethora of side effects, limiting long-term use. Here, we discuss new concepts of and insights into GR mechanisms of action to assist in the identification of routes toward enhanced therapeutic benefits. We zoom in on the communication between different GR domains and how this is influenced by different ligands. We detail findings on the interaction between GR and chromatin, and highlight how condensate formation and coregulator confinement can perturb GR transcriptional responses. Last, we discuss the potential of novel ligands and the therapeutic exploitation of crosstalk with other NRs. [ABSTRACT FROM AUTHOR]

Published

2024

14. Dynamics-driven allosteric stimulation of diguanylate cyclase activity in a red light-regulated phytochrome.

Author

Tran, Quang Hieu, Eder, Oliver Maximilian, and Winkler, Andreas

Subjects

*PHYTOCHROMES, *HYDROGEN-deuterium exchange, *ALLOSTERIC regulation, *MASS spectrometry, *CYCLASES, *GLUTAMATE receptors

Abstract

Sensor-effector proteins integrate information from different stimuli and transform this into cellular responses. Some sensory domains, like red-light responsive bacteriophytochromes, show remarkable modularity regulating a variety of effectors. One effector domain is the GGDEF diguanylate cyclase catalyzing the formation of the bacterial second messenger cyclic-dimericguanosine monophosphate. While critical signal integration elements have been described for different phytochromes, a generalized understanding of signal processing and communication over large distances, roughly 100 Å in phytochrome diguanylate cyclases, is missing. Here we show that dynamicsdriven allostery is key to understanding signal integration on a molecular level.We generated protein variants stabilized in their far-red-absorbing Pfr state and demonstrated by analysis of conformational dynamics using hydrogen-deuterium exchange coupled to mass spectrometry that single amino acid replacements are accompanied by altered dynamics of functional elements throughout the protein. We show that the conformational dynamics correlate with the enzymatic activity of these variants, explaining also the increased activity of a nonphotochromic variant. In addition, we demonstrate the functional importance of mixed Pfr/intermediate state dimers using a fast-reverting variant that still enables wild-type-like foldchanges of enzymatic stimulation by red light. This supports the functional role of single protomer activation in phytochromes, a property that might correlate with the non-canonical mixed Pfr/intermediate-state spectra observed for many phytochrome systems. We anticipate our results to stimulate research in the direction of dynamics-driven allosteric regulation of different bacteriophytochrome-based sensor-effectors. This will eventually impact design strategies for the creation of novel sensoreffector systems for enriching the optogenetic toolbox. [ABSTRACT FROM AUTHOR]

Published

2024

15. HPK1 citron homology domain regulates phosphorylation of SLP76 and modulates kinase domain interaction dynamics.

Author

Chitre, Avantika S., Wu, Ping, Walters, Benjamin T., Wang, Xiangdan, Bouyssou, Alexandre, Du, Xiangnan, Lehoux, Isabelle, Fong, Rina, Arata, Alisa, Chan, Joyce, Wang, Die, Franke, Yvonne, Grogan, Jane L., Mellman, Ira, Comps-Agrar, Laetitia, and Wang, Weiru

Subjects

DRUG discovery, HYDROGEN-deuterium exchange, PHOSPHORYLATION, PROTEIN stability, MASS spectrometry

Abstract

Hematopoietic progenitor kinase 1 (HPK1) is a negative regulator of T-cell receptor signaling and as such is an attractive target for cancer immunotherapy. Although the role of the HPK1 kinase domain (KD) has been extensively characterized, the function of its citron homology domain (CHD) remains elusive. Through a combination of structural, biochemical, and mechanistic studies, we characterize the structure-function of CHD in relationship to KD. Crystallography and hydrogen-deuterium exchange mass spectrometry reveal that CHD adopts a seven-bladed β-propellor fold that binds to KD. Mutagenesis associated with binding and functional studies show a direct correlation between domain-domain interaction and negative regulation of kinase activity. We further demonstrate that the CHD provides stability to HPK1 protein in cells as well as contributes to the docking of its substrate SLP76. Altogether, this study highlights the importance of the CHD in the direct and indirect regulation of HPK1 function. In this work, the authors unveil a mechanism where the Citron homology domain regulates HPK1's kinase domain, shedding light on the relationship between HPK1's structure and function. This enhances our understanding of HPK1, an intracellular target for cancer immunotherapy and provides a direction for immuno-oncology drug discovery. [ABSTRACT FROM AUTHOR]

Published

2024

16. An amalgamation of LC-MS HDX and AI-based software for structure prediction of drug degradation products: An integrated step towards pharmaceutical development.

Author

Jain, Sonali, Palle, Narasimha Swamy, Kuppusamy, Ananda Rajkumar, Korlam, Venugopal, and Shah, Ravi P.

Subjects

ARTIFICIAL intelligence, LIQUID chromatography-mass spectrometry, SOLID dosage forms

Abstract

Structure identification of drug degradation products is one of the key components of any pharmaceutical product development. Knowledge-based in-silico tools are widely used to predict the probable degradation and excipient interaction products. However, multiple structures of the same masses are predicted through this software, which makes identification of the correct/exact structure of the degradation product difficult. In this study, the utilization of a simple yet powerful analytical tool, LC-MS HDX was explored for improving the predictive capability of the in-silico tool. For the same, 5 drugs were selected as representative of pharmaceutical development workflow and subjected to a stress degradation study as per ICH regulatory requirements. There were in total 55 degradation products, for which all possible structures were predicted through Zeneth® software. The number of labile hydrogens in each of the 55 products was obtained through a simple LC-MS HDX method. While scrutinizing predicted structures with the number of labile hydrogens, many false positive predictions could be ruled out. Out of 55 degradation products, this approach has helped in improving the predictability of 45 products corresponding to ∼82% cases. It is simple to adopt for the industry by simply amalgamating analytical practices with AI prediction. [ABSTRACT FROM AUTHOR]

Published

2024

17. HDX-MS finds that partial unfolding with sequential domain activation controls condensation of a cellular stress marker.

Author

Ruofan Chen, Glauninger, Hendrik, Kahan, Darren N., Shangguan, Julia, Sachleben, Joseph R., Riback, Joshua A., Drummond, D. Allan, and Sosnick, Tobin R.

Subjects

*CONDENSATION, *HYDROGEN-deuterium exchange, *THERMAL stresses, *EUKARYOTIC cells, *FREE surfaces, *EXCHANGE

Abstract

Eukaryotic cells form condensates to sense and adapt to their environment [S. F. Banani, H. O. Lee, A. A. Hyman, M. K. Rosen, Nat. Rev. Mol. Cell Biol. 18, 285-298 (2017), H. Yoo, C. Triandafillou, D. A. Drummond, J. Biol. Chem. 294, 7151-7159 (2019)]. Poly(A)-binding protein (Pab1), a canonical stress granule marker, condenses upon heat shock or starvation, promoting adaptation [J. A. Riback et al., Cell 168, 1028-1040. e19 (2017)]. The molecular basis of condensation has remained elusive due to a dearth of techniques to probe structure directly in condensates. We apply hydrogen-deuterium exchange/mass spectrometry to investigate the mechanism of Pab1's condensation. Pab1's four RNA recognition motifs (RRMs) undergo different levels of partial unfolding upon condensation, and the changes are similar for thermal and pH stresses. Although structural heterogeneity is observed, the ability of MS to describe populations allows us to identify which regions contribute to the condensate's interaction network. Our data yield a picture of Pab1's stress-triggered condensation, which we term sequential activation (Fig. 1A), wherein each RRM becomes activated at a temperature where it partially unfolds and associates with other likewise activated RRMs to form the condensate. Subsequent association is dictated more by the underlying free energy surface than specific interactions, an effect we refer to as thermodynamic specificity. Our study represents an advance for elucidating the interactions that drive condensation. Furthermore, our findings demonstrate how condensation can use thermodynamic specificity to perform an acute response to multiple stresses, a potentially general mechanism for stress-responsive proteins. [ABSTRACT FROM AUTHOR]

Published

2024

18. Conformation selection by ATP-competitive inhibitors and allosteric communication in ERK2.

Author

Anderson, Jake W., Vaisar, David, Jones, David N., Pegram, Laurel M., Vigers, Guy P., Huifen Chen, Moffat, John G., and Ahn, Natalie G.

Subjects

*HYDROGEN-deuterium exchange, *MOLECULAR docking, *SIGNAL recognition particle receptor, *STACKING interactions, *DISPERSION (Chemistry), *G protein coupled receptors

Abstract

Activation of the extracellular signal-regulated kinase-2 (ERK2) by phosphorylation has been shown to involve changes in protein dynamics, as determined by hydrogen-deuterium exchange mass spectrometry (HDX-MS) and NMR relaxation dispersion measurements. These can be described by a global exchange between two conformational states of the active kinase, named 'L' and 'R,' where R is associated with a catalytically productive ATP-binding mode. An ATP-competitive ERK1/2 inhibitor, Vertex-11e, has properties of conformation selection for the R-state, revealing movements of the activation loop that are allosterically coupled to the kinase active site. However, the features of inhibitors important for R-state selection are unknown. Here, we survey a panel of ATP-competitive ERK inhibitors using HDX-MS and NMR and identify 14 new molecules with properties of R-state selection. They reveal effects propagated to distal regions in the P+1 and helix aF segments surrounding the activation loop, as well as helix aL16. Crystal structures of inhibitor complexes with ERK2 reveal systematic shifts in the Gly loop and helix aC, mediated by a Tyr-Tyr ring stacking interaction and the conserved Lys-Glu salt bridge. The findings suggest a model for the R-state involving small movements in the N-lobe that promote compactness within the kinase active site and alter mobility surrounding the activation loop. Such properties of conformation selection might be exploited to modulate the protein docking interface used by ERK substrates and effectors. [ABSTRACT FROM AUTHOR]

Published

2024

19. Molecular mechanism of muscarinic acetylcholine receptor M3 interaction with Gq.

Author

Ham, Donghee, Inoue, Asuka, Xu, Jun, Du, Yang, and Chung, Ka Young

Subjects

*CHOLINERGIC receptors, *MUSCARINIC receptors, *MUSCARINIC acetylcholine receptors, *HYDROGEN-deuterium exchange, *DRUG development

Abstract

Muscarinic acetylcholine receptor M3 (M3) and its downstream effector Gq/11 are critical drug development targets due to their involvement in physiopathological processes. Although the structure of the M3-miniGq complex was recently published, the lack of information on the intracellular loop 3 (ICL3) of M3 and extensive modification of Gαq impedes the elucidation of the molecular mechanism of M3-Gq coupling under more physiological condition. Here, we describe the molecular mechanism underlying the dynamic interactions between full-length wild-type M3 and Gq using hydrogen-deuterium exchange mass spectrometry and NanoLuc Binary Technology-based cell systems. We propose a detailed analysis of M3-Gq coupling through examination of previously well-defined binding interfaces and neglected regions. Our findings suggest potential binding interfaces between M3 and Gq in pre-assembled and functionally active complexes. Furthermore, M3 ICL3 negatively affected M3-Gq coupling, and the Gαq AHD underwent unique conformational changes during M3-Gq coupling. Analysis of M3-Gq coupling utilized fulllength proteins and techniques like HDX-MS & NanoBiT assay, revealing potential binding interfaces in the preassembled and agonistactive complexes and critical regions for the complex formation and Gq activation. [ABSTRACT FROM AUTHOR]

Published

2024

20. Racemization of the substrate and product by serine palmitoyltransferase from Sphingobacterium multivorum yields two enantiomers of the product from D-serine.

Author

Hiroko Ikushiro, Takumi Honda, Yuta Murai, Taiki Murakami, Aya Takahashi, Taiki Sawai, Haruna Goto, Shin-ichi Ikushiro, Ikuko Miyahara, Yoshio Hirabayashi, Nobuo Kamiya, Kenji Monde, and Takato Yano

Subjects

*RACEMIZATION, *SERINE, *HYDROGEN-deuterium exchange, *ENANTIOMERS, *ELECTRON density, *SCHIFF bases, *CONDENSATION reactions

Abstract

Serine palmitoyltransferase (SPT) catalyzes the pyridoxal-50-phosphate (PLP)-dependent decarboxylative condensation of Lserine and palmitoyl-CoA to form 3-ketodihydrosphingosine (KDS). Although SPT was shown to synthesize corresponding products from amino acids other than L-serine, it is still arguable whether SPT catalyzes the reaction with D-serine, which is a question of biological importance. Using high substrate and enzyme concentrations, KDS was detected after the incubation of SPT from Sphingobacterium multivorum with D-serine and palmitoyl-CoA. Furthermore, the KDS comprised equal amounts of 2S and 2R isomers. ¹H-NMR study showed a slow hydrogen-deuterium exchange at Cα of serine mediated by SPT. We further confirmed that SPT catalyzed the racemization of serine. The rate of the KDS formation from D-serine was comparable to those for the α-hydrogen exchange and the racemization reaction. The structure of the D-serine-soaked crystal (1.65 Å resolution) showed a distinct electron density of the PLP-L-serine aldimine, interpreted as the racemized product trapped in the active site. The structure of the α-methyl-Dserine-soaked crystal (1.70 Å resolution) showed the PLP-α-methyl-D-serine aldimine, mimicking the D-serine-SPT complex prior to racemization. Based on these enzymological and structural analyses, the synthesis of KDS from D-serine was explained as the result of the slow racemization to L-serine, followed by the reaction with palmitoyl-CoA, and SPT would not catalyze the direct condensation between D-serine and palmitoyl-CoA. It was also shown that the S. multivorum SPT catalyzed the racemization of the product KDS, which would explain the presence of (2R)-KDS in the reaction products. [ABSTRACT FROM AUTHOR]

Published

2024

21. An intrinsically disordered transcription activation domain increases the DNA binding affinity and reduces the specificity of NFκB p50/RelA

Author

Baughman, Hannah ER, Narang, Dominic, Chen, Wei, Suárez, Amalia C Villagrán, Lee, Joan, Bachochin, Maxwell J, Gunther, Tristan R, Wolynes, Peter G, and Komives, Elizabeth A

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Base Sequence, DNA, NF-kappa B p50 Subunit, Protein Binding, Protein Domains, Protein Multimerization, Transcription Factor RelA, Transcriptional Activation, DNA-protein interaction, NF-kB transcription factor, cooperativity, hydrogen-deuterium exchange, intrinsically disordered protein, small-angle X-ray scattering, structural model, transcription, Chemical Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences

Abstract

Many transcription factors contain intrinsically disordered transcription activation domains (TADs), which mediate interactions with coactivators to activate transcription. Historically, DNA-binding domains and TADs have been considered as modular units, but recent studies have shown that TADs can influence DNA binding. Whether these results can be generalized to more TADs is not clear. Here, we biophysically characterized the NFκB p50/RelA heterodimer including the RelA TAD and investigated the TAD's influence on NFκB-DNA interactions. In solution, we show the RelA TAD is disordered but compact, with helical tendency in two regions that interact with coactivators. We determined that the presence of the TAD increased the stoichiometry of NFκB-DNA complexes containing promoter DNA sequences with tandem κB recognition motifs by promoting the binding of NFκB dimers in excess of the number of κB sites. In addition, we measured the binding affinity of p50/RelA for DNA containing tandem κB sites and single κB sites. While the presence of the TAD enhanced the binding affinity of p50/RelA for all κB sequences tested, it also increased the affinity for nonspecific DNA sequences by over 10-fold, leading to an overall decrease in specificity for κB DNA sequences. In contrast, previous studies have generally reported that TADs decrease DNA-binding affinity and increase sequence specificity. Our results reveal a novel function of the RelA TAD in promoting binding to nonconsensus DNA, which sheds light on previous observations of extensive nonconsensus DNA binding by NFκB in vivo in response to strong inflammatory signals.

Published

2022

22. Insights into the pathogenesis of primary hyperoxaluria type I from the structural dynamics of alanine:glyoxylate aminotransferase variants.

Author

Vankova, Pavla, Pacheco‐Garcia, Juan Luis, Loginov, Dmitry S., Gómez‐Mulas, Atanasio, Kádek, Alan, Martín‐Garcia, José Manuel, Salido, Eduardo, Man, Petr, and Pey, Angel L.

Subjects

*STRUCTURAL dynamics, *HYDROGEN-deuterium exchange, *PATHOGENESIS, *PROTEIN stability

Abstract

Primary hyperoxaluria type I (PH1) is caused by deficient alanine:glyoxylate aminotransferase (AGT) activity. PH1‐causing mutations in AGT lead to protein mistargeting and aggregation. Here, we use hydrogen‐deuterium exchange (HDX) to characterize the wild‐type (WT), the LM (a polymorphism frequent in PH1 patients) and the LM G170R (the most common mutation in PH1) variants of AGT. We provide the first experimental analysis of AGT structural dynamics, showing that stability is heterogeneous in the native state and providing a blueprint for frustrated regions with potentially functional relevance. The LM and LM G170R variants only show local destabilization. Enzymatic transamination of the pyridoxal 5‐phosphate cofactor bound to AGT hardly affects stability. Our study, thus, supports that AGT misfolding is not caused by dramatic effects on structural dynamics. [ABSTRACT FROM AUTHOR]

Published

2024

23. Significance of Histidine Hydrogen–Deuterium Exchange Mass Spectrometry in Protein Structural Biology.

Author

Miyagi, Masaru and Nakazawa, Takashi

Subjects

*NUCLEAR magnetic resonance spectroscopy, *DEUTERIUM, *HYDROGEN-deuterium exchange, *MASS spectrometry, *HISTIDINE, *NUCLEAR magnetic resonance, *PROTEIN structure

Abstract

Simple Summary: Various techniques are at our disposal for probing the structure and dynamics of proteins. Mass spectrometry stands out prominently in this realm due to its exceptional detection specificity and sensitivity. This enables the precise identification of individual molecular species in complex mixtures with remarkable sensitivity. The unique strengths of mass spectrometry have spurred the development of numerous approaches for characterizing protein molecules. In this review, our focus is on a specific mass-spectrometry-based method known as histidine hydrogen–deuterium exchange mass spectrometry (His-HDX-MS). We delve into its principle, experimental workflow, applications and the details of data analysis and interpretation. Histidine residues play crucial roles in shaping the function and structure of proteins due to their unique ability to act as both acids and bases. In other words, they can serve as proton donors and acceptors at physiological pH. This exceptional property is attributed to the side-chain imidazole ring of histidine residues. Consequently, determining the acid-base dissociation constant (Ka) of histidine imidazole rings in proteins often yields valuable insights into protein functions. Significant efforts have been dedicated to measuring the pKa values of histidine residues in various proteins, with nuclear magnetic resonance (NMR) spectroscopy being the most commonly used technique. However, NMR-based methods encounter challenges in assigning signals to individual imidazole rings and require a substantial amount of proteins. To address these issues associated with NMR-based approaches, a mass-spectrometry-based method known as histidine hydrogen–deuterium exchange mass spectrometry (His-HDX-MS) has been developed. This technique not only determines the pKa values of histidine imidazole groups but also quantifies their solvent accessibility. His-HDX-MS has proven effective across diverse proteins, showcasing its utility. This review aims to clarify the fundamental principles of His-HDX-MS, detail the experimental workflow, explain data analysis procedures and provide guidance for interpreting the obtained results. [ABSTRACT FROM AUTHOR]

Published

2024

24. Mapping interactions of calmodulin and neuronal NO synthase by crosslinking and mass spectrometry.

Author

Felker, Dana, Kanghyun Lee, Pospiech, Thomas H., Yoshihiro Morishima, Haoming Zhang, Lau, Miranda, Southworth, Daniel R., and Yoichi Osawa

Subjects

*MASS spectrometry, *OXIDATION-reduction reaction, *NITRIC-oxide synthases, *HYDROGEN-deuterium exchange, *CALMODULIN

Abstract

Neuronal nitric oxide synthase (nNOS) is a homodimeric cytochrome P450-like enzyme that catalyzes the conversion of L-arginine to nitric oxide in the presence of NADPH and molecular oxygen. The binding of calmodulin (CaM) to a linker region between the FAD/FMN-containing reductase domain, and the heme-containing oxygenase domain is needed for electron transfer reactions, reduction of the heme, and NO synthesis. Due to the dynamic nature of the reductase domain and low resolution of available full-length structures, the exact conformation of the CaM-bound active complex during heme reduction is still unresolved. Interestingly, hydrogendeuterium exchange and mass spectrometry studies revealed interactions of the FMN domain and CaM with the oxygenase domain for iNOS, but not nNOS. This finding prompted us to utilize covalent crosslinking and mass spectrometry to clarify interactions of CaM with nNOS. Specifically, MS-cleavable bifunctional crosslinker disuccinimidyl dibutyric urea was used to identify thirteen unique crosslinks between CaM and nNOS as well as 61 crosslinks within the nNOS. The crosslinks provided evidence for CaM interaction with the oxygenase and reductase domain residues as well as interactions of the FMN domain with the oxygenase dimer. Cryo-EM studies, which gave a high-resolution model of the oxygenase domain, along with crosslink-guided docking provided a model of nNOS that brings the FMN within 15 Å of the heme in support for a more compact conformation than previously observed. These studies also point to the utility of covalent crosslinking and mass spectrometry in capturing transient dynamic conformations that may not be captured by hydrogen-deuterium exchange and mass spectrometry experiments. [ABSTRACT FROM AUTHOR]

Published

2024

25. Unveiling the domain-specific and RAS isoform-specific details of BRAF kinase regulation.

Author

Trebino, Tarah Elizabeth, Markusic, Borna, Nan, Haihan, Banerjee, Shrhea, and Zhihong Wang

Subjects

*BRAF genes, *SURFACE plasmon resonance, *DEUTERIUM, *HYDROGEN-deuterium exchange

Abstract

BRAF is a key member in the MAPK signaling pathway essential for cell growth, proliferation, and differentiation. Mutant BRAF is often the underlying cause of various types of cancer and mutant RAS, the upstream regulator of BRAF, is a driver of up to one-third of all cancers. BRAF interacts with RAS and undergoes a conformational change from an inactive, autoinhibited monomer to an active dimer, which propagates downstream signaling. Because of BRAF's complex regulation mechanism, the exact order and magnitude of its activation steps have yet to be confirmed experimentally. By studying the inter- and intramolecular interactions of BRAF, we unveil the domain-specific and isoform-specific details of BRAF regulation through pulldown assays, open surface plasmon resonance (OpenSPR), and hydrogen-deuterium exchange mass spectrometry (HDX-MS). We demonstrate that the BRAF specific region (BSR) and cysteine rich domain (CRD) play a crucial role in regulating the activation of BRAF in a RAS isoform-specific manner. Moreover, we quantified the binding affinities between BRAF N-terminal and kinase domains (KD) to reveal their individual roles in autoinhibition. Our findings also indicate that oncogenic BRAF-KDD594G mutant has a lower affinity for the N-terminal domains, implicating that pathogenic BRAF acts through decreased propensity for autoinhibition. Collectively, our study provides valuable insight into the activation mechanism of BRAF kinase to guide the development of new therapeutic strategies for cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2023

26. Antibody Binding Captures High Energy State of an Antigen: The Case of Nsp1 SARS-CoV-2 as Revealed by Hydrogen–Deuterium Exchange Mass Spectrometry.

Author

Kant, Ravi, Mishra, Nawneet, and Gross, Michael L.

Subjects

*HYDROGEN-deuterium exchange, *MASS spectrometry, *ENERGY policy, *ANTIGENS, *HIGH energy forming, *DEUTERIUM

Abstract

We describe an investigation using structural mass spectrometry (MS) of the impact of two antibodies, 15497 and 15498, binding the highly flexible SARS-CoV-2 Nsp1 protein. We determined the epitopes and paratopes involved in the antibody–protein interactions by using hydrogen–deuterium exchange MS (HDX-MS). Notably, the Fab (Fragment antigen binding) for antibody 15498 captured a high energy form of the antigen exhibiting significant conformational changes that added flexibility over most of the Nsp1 protein. The Fab for antibody 15497, however, showed usual antigen binding behavior, revealing local changes presumably including the binding site. These findings illustrate an unusual antibody effect on an antigen and are consistent with the dynamic nature of the Nsp1 protein. Our studies suggest that this interaction capitalizes on the high flexibility of Nsp1 to undergo conformational change and be trapped in a higher energy state by binding with a specific antibody. [ABSTRACT FROM AUTHOR]

Published

2023

27. Unravelling the mechanism of neurotensin recognition by neurotensin receptor 1.

Author

Asadollahi, Kazem, Rajput, Sunnia, de Zhang, Lazarus Andrew, Ang, Ching-Seng, Nie, Shuai, Williamson, Nicholas A., Griffin, Michael D. W., Bathgate, Ross A. D., Scott, Daniel J., Weikl, Thomas R., Jameson, Guy N. L., and Gooley, Paul R.

Subjects

NEUROTENSIN, G protein coupled receptors, FLUORESCENCE spectroscopy, HYDROGEN-deuterium exchange, LIGAND binding (Biochemistry), NUCLEAR magnetic resonance spectroscopy, MASS spectrometry

Abstract

The conformational ensembles of G protein-coupled receptors (GPCRs) include inactive and active states. Spectroscopy techniques, including NMR, show that agonists, antagonists and other ligands shift the ensemble toward specific states depending on the pharmacological efficacy of the ligand. How receptors recognize ligands and the kinetic mechanism underlying this population shift is poorly understood. Here, we investigate the kinetic mechanism of neurotensin recognition by neurotensin receptor 1 (NTS1) using 19F-NMR, hydrogen-deuterium exchange mass spectrometry and stopped-flow fluorescence spectroscopy. Our results indicate slow-exchanging conformational heterogeneity on the extracellular surface of ligand-bound NTS1. Numerical analysis of the kinetic data of neurotensin binding to NTS1 shows that ligand recognition follows an induced-fit mechanism, in which conformational changes occur after neurotensin binding. This approach is applicable to other GPCRs to provide insight into the kinetic regulation of ligand recognition by GPCRs. GPCRs include inactive and active states. 19F-NMR and stopped-flow fluorescence kinetic assays reveal that neurotensin activates the prototypical peptide-binding GPCR, neurotensin receptor 1, through an induced-fit mechanism, where ligand binding precedes receptor conformational changes. [ABSTRACT FROM AUTHOR]

Published

2023

28. Enhancement of SARS-CoV-2 Infection via Crosslinking of Adjacent Spike Proteins by N-Terminal Domain-Targeting Antibodies.

Author

Lusiany, Tina, Terada, Tohru, Kishikawa, Jun-ichi, Hirose, Mika, Chen, David Virya, Sugihara, Fuminori, Ismanto, Hendra Saputra, van Eerden, Floris J., Li, Songling, Kato, Takayuki, Arase, Hisashi, Yoshiharu, Matsuura, Okada, Masato, and Standley, Daron M.

Subjects

*SARS-CoV-2, *HYDROGEN-deuterium exchange, *ANGIOTENSIN converting enzyme, *MOLECULAR dynamics, *PROTEINS, *IMMUNOGLOBULINS

Abstract

The entry of SARS-CoV-2 into host cells is mediated by the interaction between the spike receptor-binding domain (RBD) and host angiotensin-converting enzyme 2 (ACE2). Certain human antibodies, which target the spike N-terminal domain (NTD) at a distant epitope from the host cell binding surface, have been found to augment ACE2 binding and enhance SARS-CoV-2 infection. Notably, these antibodies exert their effect independently of the antibody fragment crystallizable (Fc) region, distinguishing their mode of action from previously described antibody-dependent infection-enhancing (ADE) mechanisms. Building upon previous hypotheses and experimental evidence, we propose that these NTD-targeting infection-enhancing antibodies (NIEAs) achieve their effect through the crosslinking of neighboring spike proteins. In this study, we present refined structural models of NIEA fragment antigen-binding region (Fab)–NTD complexes, supported by molecular dynamics simulations and hydrogen–deuterium exchange mass spectrometry (HDX-MS). Furthermore, we provide direct evidence confirming the crosslinking of spike NTDs by NIEAs. Collectively, our findings advance our understanding of the molecular mechanisms underlying NIEAs and their impact on SARS-CoV-2 infection. [ABSTRACT FROM AUTHOR]

Published

2023

29. Residue-based correlation between equilibrium and rate constants is an experimental formulation of the consistency principle for smooth structural changes of proteins.

Author

Daisuke Kohda, Seiichiro Hayashi, and Daisuke Fujinami

Subjects

*LINEAR free energy relationship, *CYTOSKELETAL proteins, *AMINO acid residues, *HYDROGEN-deuterium exchange, *PROTEIN folding

Abstract

The consistency principle represents a physicochemical condition requisite for ideal protein folding. It assumes that any pair of amino acid residues in partially folded structures has an attractive short-range interaction only if the two residues are in contact within the native structure. The residue-specific equilibrium constant, K, and the residue-specific rate constant, k (forward and backward), can be determined by NMR and hydrogen-deuterium exchange studies. Linear free energy relationships (LFER) in the rate-equilibrium free energy relationship (REFER) plots (i.e., log k vs. log K) are widely seen in protein-related phenomena, but our REFER plot differs from them in that the data points are derived from one polypeptide chain under a single condition. Here, we examined the theoretical basis of the residue-based LFER. First, we derived a basic equation, ρij = ½(φi + φj), from the consistency principle, where ρij is the slope of the line segment that connects residues i and j in the REFER plot, and φi and φj are the local fractions of the native state in the transient state ensemble (TSE). Next, we showed that the general solution is the alignment of the (log K, log k) data points on a parabolic curve in the REFER plot. Importantly, unlike LFER, the quadratic free energy relationship (QFER) is compatible with the heterogeneous formation of local structures in the TSE. Residue-based LFER/QFER provides a unique insight into the TSE: A foldable polypeptide chain consists of several folding units, which are consistently coupled to undergo smooth structural changes. [ABSTRACT FROM AUTHOR]

Published

2023

30. Role of complementarity-determining regions 1 and 3 in pathologic amyloid formation by human immunoglobulin κ1 light chains.

Author

Klimtchuk, Elena S., Peterle, Daniele, Bullitt, Esther, Connors, Lawreen H., Engen, John R., and Gursky, Olga

Subjects

*IMMUNOGLOBULIN light chains, *AMYLOID, *CARDIAC amyloidosis, *CONFORMATIONAL analysis, *HYDROGEN-deuterium exchange

Abstract

Background: Immunoglobulin light chain (LC) amyloidosis is a life-threatening disease complicated by vast numbers of patient-specific mutations. We explored 14 patient-derived and engineered proteins related to j1-family germline genes IGKVLD-33-01 and IGKVLD-39-01. Methods: Hydrogen-deuterium exchange mass spectrometry analysis of conformational dynamics in recombinant LCs and their fragments was integrated with studies of thermal stability, proteolytic susceptibility, amyloid formation and amyloidogenic sequence propensity. The results were mapped on the structures of native and fibrillary proteins. Results: Proteins from two j1 subfamilies showed unexpected differences. Compared to their germline counterparts, amyloid LC related to IGKVLD-33-01 was less stable and formed amyloid faster, whereas amyloid LC related to IGKVLD-39-01 had similar stability and formed amyloid slower, suggesting different major factors influencing amyloidogenesis. In 33-01-related amyloid LC, these factors involved destabilization of the native structure and probable stabilization of amyloid. The atypical behavior of 39-01-related amyloid LC stemmed from increased dynamics/exposure of amyloidogenic segments in bC0V and bEV that could initiate aggregation and decreased dynamics/exposure near the Cys23-Cys88 disulfide. Conclusions: The results suggest distinct amyloidogenic pathways for closely related LCs and point to the complementarity-defining regions CDR1 and CDR3, linked via the conserved internal disulfide, as key factors in amyloid formation. [ABSTRACT FROM AUTHOR]

Published

2023

31. Exploration of the Catalytic Cycle Dynamics of Vigna Radiata H+–Translocating Pyrophosphatases Through Hydrogen–Deuterium Exchange Mass Spectrometry.

Author

Huang, Li-Kun, Huang, Yi-Cyuan, Chen, Pin-Chuan, Lee, Ching-Hung, Lin, Shih-Ming, Hsu, Yuan-Hao Howard, and Pan, Rong-Long

Subjects

*HYDROGEN-deuterium exchange, *MASS spectrometry, *DEUTERIUM oxide, *DEUTERIUM, *HYDROGEN atom, *MUNG bean, *STRUCTURAL dynamics

Abstract

Vigna radiata H+–translocating pyrophosphatases (VrH+-PPases, EC 3.6.1.1) are present in various endomembranes of plants, bacteria, archaea, and certain protozoa. They transport H+ into the lumen by hydrolyzing pyrophosphate, which is a by-product of many essential anabolic reactions. Although the crystal structure of H+-PPases has been elucidated, the H+ translocation mechanism of H+-PPases in the solution state remains unclear. In this study, we used hydrogen–deuterium exchange (HDX) coupled with mass spectrometry (MS) to investigate the dynamics of H+-PPases between the previously proposed R state (resting state, Apo form), I state (intermediate state, bound to a substrate analog), and T state (transient state, bound to inorganic phosphate). When hydrogen was replaced by proteins in deuterium oxide solution, the backbone hydrogen atoms, which were exchanged with deuterium, were identified through MS. Accordingly, we used deuterium uptake to examine the structural dynamics and conformational changes of H+-PPases in solution. In the highly conserved substrate binding and proton exit regions, HDX-MS revealed the existence of a compact conformation with deuterium exchange when H+-PPases were bound with a substrate analog and product. Thus, a novel working model was developed to elucidate the in situ catalytic mechanism of pyrophosphate hydrolysis and proton transport. In this model, a proton is released in the I state, and the TM5 inner wall serves as a proton piston. [ABSTRACT FROM AUTHOR]

Published

2023

32. 1H, 13C, 15N backbone resonance assignment of Escherichia coli adenylate kinase.

Author

Brom, Julia A., Samsri, Sasiprapa, Petrikis, Ruta G., Parnham, Stuart, and Pielak, Gary J.

Abstract

Adenylate kinase reversibly catalyzes the conversion of ATP plus AMP to two ADPs. This essential catalyst is present in every cell, and the Escherichia coli protein is often employed as a model enzyme. Our aim is to use the E. coli enzyme to understand dry protein structure and protection. Here, we report the expression, purification, steady-state assay, NMR conditions and 1H, 13C, 15N backbone resonance NMR assignments of its C77S variant. These data will also help others utilize this prototypical enzyme. [ABSTRACT FROM AUTHOR]

Published

2023

33. Kinetic and structural investigations of novel inhibitors of human epithelial 15-lipoxygenase-2

Author

Tsai, Wan-Chen, Gilbert, Nathan C, Ohler, Amanda, Armstrong, Michelle, Perry, Steven, Kalyanaraman, Chakrapani, Yasgar, Adam, Rai, Ganesha, Simeonov, Anton, Jadhav, Ajit, Standley, Melissa, Lee, Hsiau-Wei, Crews, Phillip, Iavarone, Anthony T, Jacobson, Matthew P, Neau, David B, Offenbacher, Adam R, Newcomer, Marcia, and Holman, Theodore R

Subjects

Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Arachidonate 15-Lipoxygenase, Dose-Response Relationship, Drug, Humans, Kinetics, Lipoxygenase Inhibitors, Molecular Structure, Structure-Activity Relationship, lipoxygenase, Inhibitor, Hydrogen-deuterium exchange, Crystallography, Computational docking, Enzymology, Cellular activity, Mixed inhibition, Medicinal and Biomolecular Chemistry, Organic Chemistry, Pharmacology and Pharmaceutical Sciences, Medicinal & Biomolecular Chemistry

Abstract

Human epithelial 15-lipoxygenase-2 (h15-LOX-2, ALOX15B) is expressed in many tissues and has been implicated in atherosclerosis, cystic fibrosis and ferroptosis. However, there are few reported potent/selective inhibitors that are active ex vivo. In the current work, we report newly discovered molecules that are more potent and structurally distinct from our previous inhibitors, MLS000545091 and MLS000536924 (Jameson et al, PLoS One, 2014, 9, e104094), in that they contain a central imidazole ring, which is substituted at the 1-position with a phenyl moiety and with a benzylthio moiety at the 2-position. The initial three molecules were mixed-type, non-reductive inhibitors, with IC50 values of 0.34 ± 0.05 μM for MLS000327069, 0.53 ± 0.04 μM for MLS000327186 and 0.87 ± 0.06 μM for MLS000327206 and greater than 50-fold selectivity versus h5-LOX, h12-LOX, h15-LOX-1, COX-1 and COX-2. A small set of focused analogs was synthesized to demonstrate the validity of the hits. In addition, a binding model was developed for the three imidazole inhibitors based on computational docking and a co-structure of h15-LOX-2 with MLS000536924. Hydrogen/deuterium exchange (HDX) results indicate a similar binding mode between MLS000536924 and MLS000327069, however, the latter restricts protein motion of helix-α2 more, consistent with its greater potency. Given these results, we designed, docked, and synthesized novel inhibitors of the imidazole scaffold and confirmed our binding mode hypothesis. Importantly, four of the five inhibitors mentioned above are active in an h15-LOX-2/HEK293 cell assay and thus they could be important tool compounds in gaining a better understanding of h15-LOX-2's role in human biology. As such, a suite of similar pharmacophores that target h15-LOX-2 both in vitro and ex vivo are presented in the hope of developing them as therapeutic agents.

Published

2021

34. Biophysical insight into protein-protein interactions in the Interleukin-11/Interleukin-11Rα/glycoprotein 130 signaling complex.

Author

Mori, Chinatsu, Nagatoishi, Satoru, Matsunaga, Ryo, Kuroda, Daisuke, Nakakido, Makoto, and Tsumoto, Kouhei

Subjects

*PROTEIN-protein interactions, *SURFACE plasmon resonance, *ISOTHERMAL titration calorimetry, *HYDROGEN-deuterium exchange, *INTERLEUKIN-6

Abstract

Interleukin-11 (IL-11) is a member of the interleukin-6 (IL-6) family of cytokines. IL-11 is a regulator of multiple events in hematopoiesis, and IL-11-mediated signaling is implicated in inflammatory disease, cancer, and fibrosis. All IL-6 family cytokines signal through the signal-transducing receptor, glycoprotein 130 (gp130), but these cytokines have distinct as well as overlapping biological functions. To understand IL-11 signaling at the molecular level, we performed a comprehensive interaction analysis of the IL-11 signaling complex, comparing it with the IL-6 complex, one of the best-characterized cytokine complexes. Our thermodynamic analysis revealed a clear difference between IL-11 and IL-6. Surface plasmon resonance analysis showed that the interaction between IL-11 and IL-11 receptor α (IL-11Rα) is entropy driven, whereas that between IL-6 and IL-6 receptor α (IL-6Rα) is enthalpy driven. Our analysis using isothermal titration calorimetry revealed that the binding of gp130 to the IL-11/IL-11Rα complex results in entropy loss, but that the interaction of gp130 with the IL-6/IL-6Rα complex results in entropy gain. Our hydrogen-deuterium exchange mass spectrometry experiments suggested that the D2 domain of gp130 was not involved in IL-6-like interactions in the IL-11/IL-11Rα complex. It has been reported that IL-6 interaction with gp130 in the signaling complex was characterized through the hydrophobic interface located in its D2 domain of gp130. Our findings suggest that unique interactions of the IL-11 signaling complex with gp130 are responsible for the distinct biological activities of IL-11 compared to IL-6. • The binding of gp130 to the IL-11/IL-11Rα complex and the IL-6/IL-6Rα complex resulted in entropy loss and entropy gain, respectively. • The D2 domain of gp130 was not involved in IL-6-like interactions in the IL-11/IL-11Rα complex. • Unique interactions of the IL-11 signaling complex with gp130 are responsible for the distinct biological activities of IL-11 compared to IL-6. [ABSTRACT FROM AUTHOR]

Published

2023

35. Fe protein docking transduces conformational changes to MoFe nitrogenase active site in a nucleotide-dependent manner.

Author

Tokmina-Lukaszewska, Monika, Huang, Qi, Berry, Luke, Kallas, Hayden, Peters, John W., Seefeldt, Lance C., Raugei, Simone, and Bothner, Brian

Subjects

*MOLECULAR docking, *SIGNAL recognition particle receptor, *NITROGENASES, *CONFORMATIONAL analysis, *HYDROGEN-deuterium exchange, *BINDING sites

Abstract

The reduction of dinitrogen to ammonia catalyzed by nitrogenase involves a complex series of events, including ATP hydrolysis, electron transfer, and activation of metal clusters for N2 reduction. Early evidence shows that an essential part of the mechanism involves transducing information between the nitrogenase component proteins through conformational dynamics. Here, millisecond time-resolved hydrogen-deuterium exchange mass spectrometry was used to unravel peptide-level protein motion on the time scale of catalysis of Mo-dependent nitrogenase from Azotobacter vinelandii. Normal mode analysis calculations complemented this data, providing insights into the specific signal transduction pathways that relay information across protein interfaces at distances spanning 100 Å. Together, these results show that conformational changes induced by protein docking are rapidly transduced to the active site, suggesting a specific mechanism for activating the metal cofactor in the enzyme active site. The reduction of dinitrogen to ammonia catalyzed by nitrogenase involves long-range conformational changes within the enzyme complex, however, direct biophysical evidence of communication between the Fe protein and the MoFe protein is lacking. Here, the authors combine millisecond time-resolved hydrogen-deuterium exchange mass spectrometry and normal mode analysis, revealing molecular-level insights into how the Fe protein alters the stability and dynamics of the MoFe protein near the active site in a nucleotide-dependent manner. [ABSTRACT FROM AUTHOR]

Published

2023

36. Using NMR-detected hydrogen-deuterium exchange to quantify protein stability in cosolutes, under crowded conditions in vitro and in cells.

Author

I-Te Chu and Pielak, Gary J.

Subjects

PROTEIN stability, HYDROGEN-deuterium exchange, THERMODYNAMIC equilibrium, NUCLEAR magnetic resonance

Abstract

We review the use of nuclear magnetic resonance (NMR) spectroscopy to assess the exchange of amide protons for deuterons (HDX) in efforts to understand how high concentration of cosolutes, especially macromolecules, affect the equilibrium thermodynamics of protein stability. HDX NMR is the only method that can routinely provide such data at the level of individual amino acids. We begin by discussing the properties of the protein systems required to yield equilibrium thermodynamic data and then review publications using osmolytes, sugars, denaturants, synthetic polymers, proteins, cytoplasm and in cells. [ABSTRACT FROM AUTHOR]

Published

2023

37. Mechanism of Insoluble Aggregate Formation in a Reconstituted Solution of Spray-Dried Protein Powder.

Author

Tao, Yeqing, Chen, Yuan, Howard, Wesley, Ibrahim, Mariam, Patel, Sajal M., McMahon, William P., Kim, Yoen Joo, Delmar, Jared A., and Davis, Darryl

Subjects

*SOLID dosage forms, *DOSAGE forms of drugs, *POWDERS, *HYDROGEN-deuterium exchange, *ELECTROSTATIC discharges, *INFRARED microscopy, *PROTEIN structure

Abstract

Background: Spray-drying is considered a promising alternative drying method to lyophilization (freeze-drying) for therapeutic proteins. Particle counts in reconstituted solutions of dried solid dosage forms of biologic drug products are closely monitored to ensure product quality. We found that high levels of particles formed after reconstitution of protein powders that had been spray-dried under suboptimal conditions. Methods: Visible and subvisible particles were evaluated. Soluble proteins in solution before spray-drying and in the reconstituted solution of spray-dried powder were analyzed for their monomer content levels and melting temperatures. Insoluble particles were collected and analyzed by Fourier transform infrared microscopy (FTIR), and further analyzed with hydrogen-deuterium exchange (HDX). Results: Particles observed after reconstitution were shown not to be undissolved excipients. FTIR confirmed their identity as proteinaceous in nature. These particles were therefore considered to be insoluble protein aggregates, and HDX was applied to investigate the mechanism underlying aggregate formation. Heavy-chain complementarity-determining region 1 (CDR-1) in the aggregates showed significant protection by HDX, suggesting CDR-1 was critical for aggregate formation. In contrast, various regions became more conformationally dynamic globally, suggesting the aggregates have lost protein structural integrity and partially unfolded after spray-drying. Discussion: The spray-drying process could have disrupted the higher-order structure of proteins and exposed the hydrophobic residues in CDR-1 of the heavy chain, contributing to the formation of aggregate through hydrophobic interactions upon reconstitution of spray-dried powder. These results can contribute to efforts to design spray-dry resilient protein constructs and improve the robustness of the spray-drying process. [ABSTRACT FROM AUTHOR]

Published

2023

38. Elucidation of the folding pathway of a circular permutant of topologically knotted YbeA by tryptophan substitutions.

Author

Puri, Sarita, Liu, Cheng-Yu, Hu, I-Chen, Lai, Chih-Hsuan, Hsu, Shang-Te Danny, and Lyu, Ping-Chiang

Subjects

*X-ray scattering, *SMALL-angle X-ray scattering, *TRYPTOPHAN, *CHEMICAL stability, *HYDROGEN-deuterium exchange, *ESCHERICHIA coli, *ANALYTICAL chemistry

Abstract

CP74 is an engineered circular permutant of a deep trefoil knotted SpoU-TrmD (SPOUT) RNA methyl transferase protein YbeA from E. coli. We have previously established that the circular permutation unties the knotted topology of YbeA and CP74 forms a domain-swapped dimer with a large dimeric interface of ca. 4600 Å2. To understand the impact of domain-swapping and the newly formed hinge region joining the two folded domains on the folding and stability of CP74, the five equally spaced tryptophan residues were individually substituted into phenylalanine to monitor their conformational and stability changes by a battery of biophysical tools. Far-UV circular dichroism, intrinsic fluorescence, and small-angle X-ray scattering dictated minimal global conformational perturbations to the native structures in the tryptophan variants. The structures of the tryptophan variants also showed the conservation of the domain-swapped ternary structure with the exception that the W72F exhibited significant asymmetry in the α-helix 5. Comparative global thermal and chemical stability analyses indicated the pivotal role of W100 in the folding of CP74 followed by W19 and W72. Solution-state NMR spectroscopy and hydrogen-deuterium exchange mass spectrometry further revealed the accumulation of a native-like intermediate state in which the hinge region made important contributions to maintain the domain-swapped ternary structure of CP74. • Circular permutation of YbeA unties its knotted topology and leads to a domain-swapped dimer. • The folding mechanism of the circular permutant, CP74, is investigate by tryptophan-to-phenylalanine substitutions. • Urea-mediated unfolding of CP74 involves the formation of a native-like dimeric intermediate state. [ABSTRACT FROM AUTHOR]

Published

2023

39. Rapid characterization of isotopic purity of deuterium‐labeled organic compounds and monitoring of hydrogen–deuterium exchange reaction using electrospray ionization‐high‐resolution mass spectrometry.

Author

Zhang, Qian, Xia, Yaoyu, Song, Wei, Chen, Chunguang, and Wang, Hao‐Yang

Subjects

*ELECTROSPRAY ionization mass spectrometry, *HYDROGEN-deuterium exchange, *DEUTERIUM, *EXCHANGE reactions, *MASS spectrometry, *ORGANIC compounds, *ISOTOPIC analysis

Abstract

Rationale: Deuterium‐labeled organic compounds, reagents, and drugs are widely used in many scientific research fields. Isotopic purity as the feature parameter of deuterated compounds is of great importance. In this article, we used electrospray ionization with high‐resolution mass spectrometry (ESI‐HRMS) to study isotopic purity of deuterium‐labeled organic compounds based on assigning and distinguishing the corresponding H/D (hydrogen–deuterium) isotopolog ions of deuterated compounds. Methods: We systematically considered the specific requirements of accuracy and resolution of ESI‐HRMS when measuring isotopic purity and demonstrated some actual cases using ESI‐HRMS and ultraperformance liquid chromatography (UPLC)‐HRMS. Meanwhile, ESI‐HRMS/MS of deuterated compounds was performed to obtain more information on deuterium‐labeled position characterization. Results: Two isotopic purity calculation methods based on the relative abundance in ESI‐HRMS and UPLC‐HRMS of H/D isotopolog ions (D0–Dn) were compared, which gave consistent isotopic purity values and were in good agreement with the certified isotopic purity values. We further studied and monitored the H/D exchange reaction of ethyl 3‐(4‐bromophenyl)‐3‐oxopropanoate (EBPO) by evaluating the dynamic isotopic purity changes in EBPO‐D2 in the H/D exchange reaction in situ. Conclusion: The isotopic purity characterization methods using ESI‐HRMS discussed in this article have some outstanding advantages: rapid, highly sensitive, very low sample consumption (even below nanogram level), and deuterated solvent‐free. Thus, this low‐impact analytical method requires less time and is cost effective and might have good application potential for in‐situ isotopic purity analysis and for monitoring the H/D exchange reactions. [ABSTRACT FROM AUTHOR]

Published

2023

40. Description of peptide bond planarity from high-resolution neutron crystallography.

Author

Yuya Hanazono, Yu Hirano, Taro Tamada, and Kunio Miki

Subjects

*PEPTIDE bonds, *NEUTRONS, *CRYSTALLOGRAPHY, *PROTEIN crystallography, *HYDROGEN-deuterium exchange, *DEUTERIUM, *IRON-based superconductors

Abstract

Neutron crystallography is a highly effective method for visualizing hydrogen atoms in proteins. In our recent study, we successfully determined the high-resolution (1.2 Å) neutron structure of high-potential iron-sulfur protein, refining the coordinates of some amide protons without any geometric restraints. Interestingly, we observed that amide protons are deviated from the peptide plane due to electrostatic interactions. Moreover, the difference in the position of the amide proton of Cys75 between reduced and oxidized states is possibly attributed to the electron storage capacity of the iron-sulfur cluster. Additionally, we have discussed about the rigidity of the iron-sulfur cluster based on the results of the hydrogen-deuterium exchange. Our research underscores the significance of neutron crystallography in protein structure elucidation, enriching our understanding of protein functions at an atomic resolution. [ABSTRACT FROM AUTHOR]

Published

2023

41. Structural Basis for the Enzymatic Activity of the HACE1 HECT‐Type E3 Ligase Through N‐Terminal Helix Dimerization.

Author

Singh, Sunil, Machida, Satoru, Tulsian, Nikhil Kumar, Choong, Yeu Khai, Ng, Joel, Shankar, Srihari, Liu, Yaochen, Chandiramani, Krisha Vashdev, Shi, Jian, and Sivaraman, J

Subjects

*UBIQUITIN ligases, *HYDROGEN-deuterium exchange, *DIMERIZATION, *UBIQUITINATION

Abstract

HACE1 is an ankyrin repeat (AKR) containing HECT‐type E3 ubiquitin ligase that interacts with and ubiquitinates multiple substrates. While HACE1 is a well‐known tumor suppressor, its structure and mode of ubiquitination are not understood. The authors present the cryo‐EM structures of human HACE1 along with in vitro functional studies that provide insights into how the enzymatic activity of HACE1 is regulated. HACE1 comprises of an N‐terminal AKR domain, a middle (MID) domain, and a C‐terminal HECT domain. Its unique G‐shaped architecture interacts as a homodimer, with monomers arranged in an antiparallel manner. In this dimeric arrangement, HACE1 ubiquitination activity is hampered, as the N‐terminal helix of one monomer restricts access to the C‐terminal domain of the other. The in vitro ubiquitination assays, hydrogen‐deuterium exchange mass spectrometry (HDX–MS) analysis, mutagenesis, and in silico modeling suggest that the HACE1 MID domain plays a crucial role along with the AKRs in RAC1 substrate recognition. [ABSTRACT FROM AUTHOR]

Published

2023

42. Conformational Dynamics of the D53−D3−D14 Complex in Strigolactone Signaling.

Author

Liu, Simiao, Wang, Jia, Song, Bin, Gong, Xinqi, Liu, Huihui, Hu, Qingliang, Zhang, Junhui, Li, Qianqian, Zheng, Jie, Wang, Hongwei, Xu, H Eric, Li, Jiayang, and Wang, Bing

Subjects

*HYDROGEN-deuterium exchange, *CELLULAR signal transduction, *CROP yields, *MASS spectrometry, *SIGNALS & signaling

Abstract

Strigolactones (SLs) play fundamental roles in regulating plant architecture, which is a major factor determining crop yield. The perception and signal transduction of SLs require the formation of a complex containing the receptor DWARF14 (D14), an F-box protein D3 and a transcriptional regulator D53 in an SL-dependent manner. Structural and biochemical analyses of D14 and its orthologs DAD2 and AtD14, D3 and the complexes of ASK1−D3−AtD14 and D3CTH–D14 have made great contributions to understanding the mechanisms of SL perception. However, structural analyses of D53 and the D53−D3−D14 holo-complex are challenging, and the biochemical mechanism underlying the complex assembly remains poorly understood. Here, we found that apo-D53 was rather flexible and reconstituted the holo-complex containing D53, S-phase kinase-associated protein 1 (SKP1), D3 and D14 with rac- GR24. The cryo-electron microscopy (cryo-EM) structure of SKP1−D3−D14 in the presence of D53 was analyzed and superimposed on the crystal structure of ASK1−D3−AtD14 without D53. No large conformational rearrangement was observed, but a 9Å rotation appeared between D14 and AtD14. Using hydrogen–deuterium exchange monitored by mass spectrometry, we analyzed dynamic motifs of D14, D3 and D53 in the D53−SKP1−D3−D14 complex assembly process and further identified two potential interfaces in D53 that are located in the N and D2 domains, respectively. Together, our results uncovered the dynamic conformational changes and built a model of the holo-complex D53−SKP1−D3−D14, offering valuable information for the biochemical and genetic mechanisms of SL perception and signal transduction. [ABSTRACT FROM AUTHOR]

Published

2023

43. In‐droplet hydrogen–deuterium exchange to examine protein/peptide solution conformer heterogeneity.

Author

Sharif, Daud, Rahman, Mohammad, Mahmud, Sultan, Sultana, Mst Nigar, Attanayake, Kushani, DeBastiani, Anthony, Foroushani, Samira Hajian, Li, Peng, and Valentine, Stephen J.

Subjects

*HYDROGEN-deuterium exchange, *PEPTIDES, *CYTOSKELETAL proteins, *PROTEINS, *UBIQUITIN

Abstract

Rationale: Many different structure analysis techniques are not capable of probing the heterogeneity of solution conformations. Here, we examine the ability of in‐droplet hydrogen–deuterium exchange (HDX) to directly probe solution conformer heterogeneity of a protein with mass spectrometry (MS) detection. Methods: Two vibrating capillary vibrating sharp‐edge spray ionization (cVSSI) devices have been arranged such that they generate microdroplet plumes of the analyte and D2O reagent, which coalesce to form reaction droplets where HDX takes place in the solution environment. The native HDX–MS setup has been first explored for two model peptides that have distinct structural compositions in solution. The effectiveness of the multidevice cVSSI–HDX in illustrating structural details has been further exploited to investigate coexisting solution‐phase conformations of the protein ubiquitin. Results: In‐droplet HDX reveals decreased backbone exchange for a model peptide that has a greater helix‐forming propensity. Differences in intrinsic rates of the alanine and serine residues may account for much of the observed protection. The data allow the first estimates of backbone exchange rates for peptides undergoing in‐droplet HDX. That said, the approach may hold greater potential for investigating the tertiary structure and structural transitions of proteins. For ubiquitin protein, HDX reactivity differences suggest that multiple conformers are present in native solutions. The addition of methanol to buffered aqueous solutions of ubiquitin results in increased populations of solution conformers of higher reactivity. Data analysis suggests that partially folded conformers such as the A‐state of ubiquitin increase with methanol content; the native state may be preserved to a limited degree even under stronger denaturation conditions. Conclusion: The deuterium uptake after in‐droplet HDX has been observed to correspond to some degree with peptide backbone hydrogen protection based on differences in intrinsic rates of exchange. The presence of coexisting protein solution structures under native and denaturing solution conditions has been distinguished by the isotopic distributions of deuterated ubiquitin ions. [ABSTRACT FROM AUTHOR]

Published

2023

44. Water distribution in human hair microstructure elucidated by spin contrast variation small‐angle neutron scattering.

Author

Noda, Yohei, Koizumi, Satoshi, Maeda, Tomoki, Inada, Takumi, and Ishihara, Aya

Subjects

*SMALL-angle neutron scattering, *POLARIZATION (Nuclear physics), *WATER distribution, *SCATTERING (Physics), *HYDROGEN-deuterium exchange, *ELECTRON spin

Abstract

Dynamic nuclear polarization (DNP) is effective for controlling the neutron scattering length of protons and can be utilized for contrast variation in small‐angle neutron scattering (SANS). Using the TEMPOL solution soaking method as electron spin doping, the DNP–SANS technique was applied to human hair fiber for the first time. For dry and D2O‐swollen hair samples, a drastic change in the SANS profile was observed at high polarization conditions (|PHPN| ∼ 60%, where PH and PN are the proton and neutron spin polarization, respectively). The SANS profile as a function of the magnitude of the scattering vector, q, was composed of a low‐q upturn, a middle‐q oscillation and a high‐q flat region. The low‐q upturn was assumed to be a combination of two power‐law functions, q−4 due to a large structure interface (Porod's law) and q−2 due to random coil. The middle‐q oscillation was well reproduced by numerical calculation based on the structure model of intermediate filaments (IFs) as proposed by Er Rafik et al. [Biophys. J. (2004), 86, 3893–3904]: one pair of keratin coiled‐coils is located at the center and surrounded by seven pairs of keratin coiled‐coils located in a circle (called the '7 + 1' model), and a collection of IFs is arranged in a quasi‐hexagonal manner. For the observed SANS profiles for different PHPN, the IF term contribution maintained a constant q‐dependent profile, despite significant changes in intensity. This indicates that the macrofibril is composed of two domains (keratin coiled‐coils and matrix). In addition, D2O swelling enhanced the IF term intensity and shifted the polarization‐dependent local minimum to higher PHPN. This behavior was reproduced by contrast factor calculation based on the two‐domain model. Scattering length densities of keratin coiled‐coil and surrounding matrix domains were calculated by use of the known amino acid composition, considering the hydrogen–deuterium exchange reaction during soaking with D2O solution of TEMPOL. As a result, it was found that for keratin coiled‐coil domains, about 40% of the peptide backbone amide NH protons were replaced with deuterons. This means that 68% of the α‐helix domain is rigid, but the rest is flexible to allow dynamic dissociation of the hydrogen bond. Furthermore, the local mass density of each domain was precisely evaluated. The obtained data are expected to be a guide for further detailed investigation of keratin and keratin‐associated protein distribution. This approach is expected to be applied to a wide variety of bio‐derived materials, which are water absorbing in general. [ABSTRACT FROM AUTHOR]

Published

2023

45. Mild and selective hydrogen–deuterium exchange for aromatic hydrogen of amines.

Author

Tachrim, Zetryana Puteri, Hashinoki, Manami, Wang, Zeping, Wen, Zhang, Zihan, Zhuang, and Hashimoto, Makoto

Subjects

*HYDROGEN-deuterium exchange, *AROMATIC amines, *DEUTERIUM, *METHYL triflate, *OPTICAL rotation, *DEUTERATION

Abstract

The direct electrophilic deuteration of the aromatic moiety in aromatic and aralkyl amines is reported. The acid‐catalyzed deuteration is facilitated by deuterated trifluoromethanesulfonic acid, [D]triflic acid, CF3SO3D, TfOD, which acts as both the reaction solvent and the source of the deuterium label. The mild conditions enable room temperature hydrogen/deuterium exchange for most of the para‐substituted aromatic amine derivatives studied. In addition, short reaction times and a high degree of aromatic deuteration are achieved and isolation of the product is simple. The optical activity of the chiral aralkyl amines studied was preserved. [ABSTRACT FROM AUTHOR]

Published

2023

46. Ligand-specific changes in conformational flexibility mediate long-range allostery in the lac repressor.

Author

Glasgow, Anum, Hobbs, Helen T., Perry, Zion R., Wells, Malcolm L., Marqusee, Susan, and Kortemme, Tanja

Subjects

LIGAND binding (Biochemistry), HYDROGEN-deuterium exchange, G protein coupled receptors, PROTEIN engineering, TRANSCRIPTION factors, MASS spectrometry, CRYSTAL structure

Abstract

Biological regulation ubiquitously depends on protein allostery, but the regulatory mechanisms are incompletely understood, especially in proteins that undergo ligand-induced allostery with few structural changes. Here we used hydrogen-deuterium exchange with mass spectrometry (HDX/MS) to map allosteric effects in a paradigm ligand-responsive transcription factor, the lac repressor (LacI), in different functional states (apo, or bound to inducer, anti-inducer, and/or DNA). Although X-ray crystal structures of the LacI core domain in these states are nearly indistinguishable, HDX/MS experiments reveal widespread differences in flexibility. We integrate these results with modeling of protein-ligand-solvent interactions to propose a revised model for allostery in LacI, where ligand binding allosterically shifts the conformational ensemble as a result of distinct changes in the rigidity of secondary structures in the different states. Our model provides a mechanistic basis for the altered function of distal mutations. More generally, our approach provides a platform for characterizing and engineering protein allostery. Using hydrogen-deuterium exchange, the authors propose a model explaining how a classic transcription factor undergoes changes in its conformational ensemble in response to different ligands. [ABSTRACT FROM AUTHOR]

Published

2023

47. Structural dynamics reveal subtype-specific activation and inhibition of influenza virus hemagglutinin.

Author

Garcia, Natalie K., Kephart, Sally M., Benhaim, Mark A., Tsutomu Matsui, Mileant, Alexander, Guttman, Miklos, and Lee, Kelly K.

Subjects

*INFLUENZA viruses, *STRUCTURAL dynamics, *HEMAGGLUTININ, *HYDROGEN-deuterium exchange, *MEMBRANE fusion

Abstract

Influenza hemagglutinin (HA) is a prototypical class 1 viral entry glycoprotein, responsible for mediating receptor binding and membrane fusion. Structures of its prefusion and postfusion forms, embodying the beginning and endpoints of the fusion pathway, have been extensively characterized. Studies probing HA dynamics during fusion have begun to identify intermediate states along the pathway, enhancing our understanding of how HA becomes activated and traverses its conformational pathway to complete fusion. HA is also the most variable, rapidly evolving part of influenza virus, and it is not known whether mechanisms of its activation and fusion are conserved across divergent viral subtypes. Here, we apply hydrogen-deuterium exchange mass spectrometry to compare fusion activation in two subtypes of HA, H1 and H3. Our data reveal subtype-specific behavior in the regions of HA that undergo structural rearrangement during fusion, including the fusion peptide and HA1/HA2 interface. In the presence of an antibody that inhibits the conformational change (FI6v3), we observe that acid-induced dynamic changes near the epitope are dampened, but the degree of protection at the fusion peptide is different for the two subtypes investigated. These results thus provide new insights into variation in the mechanisms of influenza HA's dynamic activation and its inhibition. [ABSTRACT FROM AUTHOR]

Published

2023

48. Exploration of the Catalytic Cycle Dynamics of Vigna Radiata H+–Translocating Pyrophosphatases Through Hydrogen–Deuterium Exchange Mass Spectrometry

Author

Huang, Li-Kun, Huang, Yi-Cyuan, Chen, Pin-Chuan, Lee, Ching-Hung, Lin, Shih-Ming, Hsu, Yuan-Hao Howard, and Pan, Rong-Long

Published

2023

49. 1H, 13C, 15N backbone resonance assignment of Escherichia coli adenylate kinase

Author

Brom, Julia A., Samsri, Sasiprapa, Petrikis, Ruta G., Parnham, Stuart, and Pielak, Gary J.

Published

2023

50. Development and characterization of nanobodies that specifically target the oncogenic Phosphatase of Regenerating Liver-3 (PRL-3) and impact its interaction with a known binding partner, CNNM3.

Author

Smith, Caroline N., Kihn, Kyle, Williamson, Zachary A., Chow, K. Martin, Hersh, Louis B., Korotkov, Konstantin V., Deredge, Daniel, and Blackburn, Jessica S.

Subjects

*IMMUNOGLOBULINS, *HYDROGEN-deuterium exchange, *CARRIER proteins, *CANCER invasiveness, *MASS spectrometry

Abstract

Phosphatase of Regenerating Liver-3 (PRL-3) is associated with cancer progression and metastasis. The mechanisms that drive PRL-3's oncogenic functions are not well understood, partly due to a lack of research tools available to study this protein. We have begun to address these issues by developing alpaca-derived single domain antibodies, or nanobodies, targeting PRL-3 with a KD of 30–300 nM and no activity towards highly homologous family members PRL-1 and PRL-2. We found that longer and charged N-terminal tags on PRL-3, such as GFP and FLAG, changed PRL-3 localization compared to untagged protein, indicating that the nanobodies may provide new insights into PRL-3 trafficking and function. The nanobodies perform equally, if not better, than commercially available antibodies in immunofluorescence and immunoprecipitation. Finally, hydrogen-deuterium exchange mass spectrometry (HDX-MS) showed that the nanobodies bind partially within the PRL-3 active site and can interfere with PRL-3 phosphatase activity. Co-immunoprecipitation with a known PRL-3 active site binding partner, the CBS domain of metal transporter CNNM3, showed that the nanobodies reduced the amount of PRL-3:CBS inter-action. The potential of blocking this interaction is highly relevant in cancer, as multiple research groups have shown that PRL-3 binding to CNNM proteins is sufficient to promote metastatic growth in mouse models. The anti-PRL-3 nanobodies represent an important expansion of the research tools available to study PRL-3 function and can be used to define the role of PRL-3 in cancer progression. [ABSTRACT FROM AUTHOR]

Published

2023