Your search keyword '"Permyakov EA"' showing total 140 results

1. Protein structural disorder of the envelope V3 loop contributes to the switch in human immunodeficiency virus type 1 cell tropism

Author

Jiang, X, Feyertag, F, Robertson, DL, and Permyakov, EA

Subjects

viruses, virus diseases

Abstract

Human immunodeficiency virus type 1 (HIV-1) envelope gp120 is partly an intrinsically disordered (unstructured/disordered) protein as it contains regions that do not fold into well-defined protein structures. These disordered regions play important roles in HIV's life cycle, particularly, V3 loop-dependent cell entry, which determines how the virus uses two coreceptors on immune cells, the chemokine receptors CCR5 (R5), CXCR4 (X4) or both (R5X4 virus). Most infecting HIV-1 variants utilise CCR5, while a switch to CXCR4-use occurs in the majority of infections. Why does this 'rewiring' event occur in HIV-1 infected patients? As changes in the charge of the V3 loop are associated with this receptor switch and it has been suggested that charged residues promote structure disorder, we hypothesise that the intrinsic disorder of the V3 loop is permissive to sequence variation thus contributing to the switch in cell tropism. To test this we use three independent data sets of gp120 to analyse V3 loop disorder. We find that the V3 loop of X4 virus has significantly higher intrinsic disorder tendency than R5 and R5X4 virus, while R5X4 virus has the lowest. These results indicate that structural disorder plays an important role in HIV-1 cell tropism and CXCR4 binding. We discuss the potential evolutionary mechanisms leading to the fixation of disorder promoting mutations and the adaptive potential of protein structural disorder in viral host adaptation.

Published

2017

2. Characterisation of the Porphyromonas gingivalis Manganese Transport Regulator Orthologue

Author

Permyakov, EA, Zhang, L, Butler, CA, Khan, HSG, Dashper, SG, Seers, CA, Veith, PD, Zhang, J-G, Reynolds, EC, Permyakov, EA, Zhang, L, Butler, CA, Khan, HSG, Dashper, SG, Seers, CA, Veith, PD, Zhang, J-G, and Reynolds, EC

Abstract

PgMntR is a predicted member of the DtxR family of transcriptional repressors responsive to manganese in the anaerobic periodontal pathogen Porphyromonas gingivalis. Our bioinformatic analyses predicted that PgMntR had divalent metal binding site(s) with elements of both manganous and ferrous ion specificity and that PgMntR has unusual twin C-terminal FeoA domains. We produced recombinant PgMntR and four variants to probe the specificity of metal binding and its impact on protein structure and DNA binding. PgMntR dimerised in the absence of a divalent transition metal cation. PgMntR bound three Mn(II) per monomer with an overall dissociation constant Kd 2.0 x 10(-11) M at pH 7.5. PgMntR also bound two Fe(II) with distinct binding affinities, Kd1 2.5 x 10(-10) M and Kd2 ≤ 6.0 x 10(-8) M at pH 6.8. Two of the metal binding sites may form a binuclear centre with two bound Mn2+ being bridged by Cys108 but this centre provided only one site for Fe2+. Binding of Fe2+ or Mn2+ did not have a marked effect on the PgMntR secondary structure. Apo-PgMntR had a distinct affinity for the promoter region of the gene encoding the only known P. gingivalis manganese transporter, FB2. Mn2+ increased the DNA binding affinity of PgMntR whilst Fe2+ destabilised the protein-DNA complex in vitro. PgMntR did not bind the promoter DNA of the gene encoding the characterised iron transporter FB1. The C-terminal FeoA domain was shown to be essential for PgMntR structure/function, as its removal caused the introduction of an intramolecular disulfide bond and abolished the binding of Mn2+ and DNA. These data indicate that PgMntR is a novel member of the DtxR family that may function as a transcriptional repressor switch to specifically regulate manganese transport and homeostasis in an iron-dependent manner.

Published

2016

3. Propeptide-Mediated Inhibition of Cognate Gingipain Proteinases

Author

Permyakov, EA, Huq, NL, Seers, CA, Toh, ECY, Dashper, SG, Slakeski, N, Zhang, L, Ward, BR, Meuric, V, Chen, D, Cross, KJ, Reynolds, EC, Permyakov, EA, Huq, NL, Seers, CA, Toh, ECY, Dashper, SG, Slakeski, N, Zhang, L, Ward, BR, Meuric, V, Chen, D, Cross, KJ, and Reynolds, EC

Abstract

Porphyromonas gingivalis is a major pathogen associated with chronic periodontitis. The organism's cell-surface cysteine proteinases, the Arg-specific proteinases (RgpA, RgpB) and the Lys-specific proteinase (Kgp), which are known as gingipains have been implicated as major virulence factors. All three gingipain precursors contain a propeptide of around 200 amino acids in length that is removed during maturation. The aim of this study was to characterize the inhibitory potential of the Kgp and RgpB propeptides against the mature cognate enzymes. Mature Kgp was obtained from P. gingivalis mutant ECR368, which produces a recombinant Kgp with an ABM1 motif deleted from the catalytic domain (rKgp) that enables the otherwise membrane bound enzyme to dissociate from adhesins and be released. Mature RgpB was obtained from P. gingivalis HG66. Recombinant propeptides of Kgp and RgpB were produced in Escherichia coli and purified using nickel-affinity chromatography. The Kgp and RgpB propeptides displayed non-competitive inhibition kinetics with K(i) values of 2.04 µM and 12 nM, respectively. Both propeptides exhibited selectivity towards their cognate proteinase. The specificity of both propeptides was demonstrated by their inability to inhibit caspase-3, a closely related cysteine protease, and papain that also has a relatively long propeptide. Both propeptides at 100 mg/L caused a 50% reduction of P. gingivalis growth in a protein-based medium. In summary, this study demonstrates that gingipain propeptides are capable of inhibiting their mature cognate proteinases.

Published

2013

4. Protein aggregation studied in intact cells by Fourier transform infrared spectroscopy

Author

Uversky, VN, Permyakov, EA, Natalello, A, Ami, D, Doglia, S, NATALELLO, ANTONINO, DOGLIA, SILVIA MARIA, AMI, DILETTA, Uversky, VN, Permyakov, EA, Natalello, A, Ami, D, Doglia, S, NATALELLO, ANTONINO, DOGLIA, SILVIA MARIA, and AMI, DILETTA

Published

2007

5. Protein structural disorder of the envelope V3 loop contributes to the switch in human immunodeficiency virus type 1 cell tropism

Author

David Robertson, Xiaowei Jiang, Felix Feyertag, and Permyakov, EA

Subjects

RNA viruses, Glycosylation, Protein Conformation, viruses, Glycobiology, HIV Infections, Protein Structure Prediction, HIV Envelope Protein gp120, V3 loop, Pathology and Laboratory Medicine, Biochemistry, CXCR4, Chemokine receptor, Protein structure, Immunodeficiency Viruses, Medicine and Health Sciences, Macromolecular Structure Analysis, Post-Translational Modification, Receptor, Genetics, 0303 health sciences, Crystallography, Physics, virus diseases, Condensed Matter Physics, 3. Good health, Medical Microbiology, Viral Pathogens, Viruses, Physical Sciences, Crystal Structure, Medicine, Host adaptation, Pathogens, Coreceptors, Research Article, Signal Transduction, Protein Structure, Science, Biology, Microbiology, Virus, Viral Proteins, 03 medical and health sciences, Virology, Retroviruses, Solid State Physics, Humans, CCR5 coreceptor, Microbial Pathogens, Molecular Biology, Tropism, 030304 developmental biology, 030306 microbiology, Lentivirus, Organisms, Biology and Life Sciences, HIV, Proteins, Cell Biology, Viral Tropism, HIV-1

Abstract

Human immunodeficiency virus type 1 (HIV-1) envelope gp120 is partly an intrinsically disordered (unstructured/disordered) protein as it contains regions that do not fold into well-defined protein structures. These disordered regions play important roles in HIV's life cycle, particularly, V3 loop-dependent cell entry, which determines how the virus uses two coreceptors on immune cells, the chemokine receptors CCR5 (R5), CXCR4 (X4) or both (R5X4 virus). Most infecting HIV-1 variants utilise CCR5, while a switch to CXCR4-use occurs in the majority of infections. Why does this ‘rewiring’ event occur in HIV-1 infected patients? As changes in the charge of the V3 loop are associated with this receptor switch and it has been suggested that charged residues promote structure disorder, we hypothesise that the intrinsic disorder of the V3 loop plays a role in determining cell tropism. To test this we use three independent data sets of gp120 to analyse V3 loop disorder. We find that the V3 loop of X4 virus has significantly higher intrinsic disorder tendency than R5 and R5X4 virus, while R5X4 virus has the lowest. These results indicate that structural disorder plays an important role in determining HIV-1 cell tropism and CXCR4 binding. We speculate that changes in N-linked glycosylation associated with tropism change (from R5 to X4) are required to stabilise the V3 loop with increased disorder tendency during HIV-1 evolution. We discuss the potential evolutionary mechanisms leading to the fixation of disorder promoting mutations and the adaptive potential of protein structural disorder in viral host adaptation.

Published

2017

6. Protein aggregation studied in intact cells by Fourier transform infrared spectroscopy

Author

NATALELLO, ANTONINO, DOGLIA, SILVIA MARIA, AMI, DILETTA, Uversky, VN, Permyakov, EA, Natalello, A, Ami, D, and Doglia, S

Subjects

Protein aggregation, Inclusion Body, Amyloid, FIS/01 - FISICA SPERIMENTALE, BIO/10 - BIOCHIMICA

Published

2007

7. Recognition of granulocyte-macrophage colony-stimulating factor by specific S100 proteins.

Author

Kazakov AS, Rastrygina VA, Vologzhannikova AA, Zemskova MY, Bobrova LA, Deryusheva EI, Permyakova ME, Sokolov AS, Litus EA, Shevelyova MP, Uversky VN, Permyakov EA, and Permyakov SE

Subjects

Humans, Recombinant Proteins metabolism, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor chemistry, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor metabolism, Protein Binding, Binding Sites, Granulocyte-Macrophage Colony-Stimulating Factor pharmacology, Granulocyte-Macrophage Colony-Stimulating Factor metabolism, S100 Proteins metabolism

Abstract

Granulocyte-macrophage colony-stimulating factor (GM-CSF) is a pleiotropic myelopoietic growth factor and proinflammatory cytokine, clinically used for multiple indications and serving as a promising target for treatment of many disorders, including cancer, multiple sclerosis, rheumatoid arthritis, psoriasis, asthma, COVID-19. We have previously shown that dimeric Ca 2+ -bound forms of S100A6 and S100P proteins, members of the multifunctional S100 protein family, are specific to GM-CSF. To probe selectivity of these interactions, the affinity of recombinant human GM-CSF to dimeric Ca 2+ -loaded forms of 18 recombinant human S100 proteins was studied by surface plasmon resonance spectroscopy. Of them, only S100A4 protein specifically binds to GM-CSF with equilibrium dissociation constant, K d , values of 0.3-2 μM, as confirmed by intrinsic fluorescence and chemical crosslinking data. Calcium removal prevents S100A4 binding to GM-CSF, whereas monomerization of S100A4/A6/P proteins disrupts S100A4/A6 interaction with GM-CSF and induces a slight decrease in S100P affinity for GM-CSF. Structural modelling indicates the presence in the GM-CSF molecule of a conserved S100A4/A6/P-binding site, consisting of the residues from its termini, helices I and III, some of which are involved in the interaction with GM-CSF receptors. The predicted involvement of the 'hinge' region and F89 residue of S100P in GM-CSF recognition was confirmed by mutagenesis. Examination of S100A4/A6/P ability to affect GM-CSF signaling showed that S100A4/A6 inhibit GM-CSF-induced suppression of viability of monocytic THP-1 cells. The ability of the S100 proteins to modulate GM-CSF activity is relevant to progression of various neoplasms and other diseases, according to bioinformatics analysis. The direct regulation of GM-CSF signaling by extracellular forms of the S100 proteins should be taken into account in the clinical use of GM-CSF and development of the therapeutic interventions targeting GM-CSF or its receptors., Competing Interests: Declaration of competing interest The authors declare no conflict of interest. The funders had no role in the design of the study; in the collection, analyses, or interpretation of data; in the writing of the manuscript; or in the decision to publish the results., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

8. The active site of the SGNH hydrolase-like fold proteins: Nucleophile-oxyanion (Nuc-Oxy) and Acid-Base zones.

Author

Denessiouk K, Denesyuk AI, Permyakov SE, Permyakov EA, Johnson MS, and Uversky VN

Abstract

SGNH hydrolase-like fold proteins are serine proteases with the default Asp-His-Ser catalytic triad. Here, we show that these proteins share two unique conserved structural organizations around the active site: (1) the Nuc-Oxy Zone around the catalytic nucleophile and the oxyanion hole, and (2) the Acid-Base Zone around the catalytic acid and base. The Nuc-Oxy Zone consists of 14 amino acids cross-linked with eight conserved intra- and inter-block hydrogen bonds. The Acid-Base Zone is constructed from a single fragment of the polypeptide chain, which incorporates both the catalytic acid and base, and whose N- and C-terminal residues are linked together by a conserved hydrogen bond. The Nuc-Oxy and Acid-Base Zones are connected by an SHLink, a two-bond conserved interaction from amino acids, adjacent to the catalytic nucleophile and base., Competing Interests: The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (© 2023 The Author(s).)

Published

2023

9. Interaction of S100A6 Protein with the Four-Helical Cytokines.

Author

Kazakov AS, Deryusheva EI, Rastrygina VA, Sokolov AS, Permyakova ME, Litus EA, Uversky VN, Permyakov EA, and Permyakov SE

Subjects

Humans, Animals, S100 Calcium Binding Protein A6, Molecular Docking Simulation, Binding Sites, Cell Cycle Proteins, Immunologic Factors, S100 Proteins

Abstract

S100 is a family of over 20 structurally homologous, but functionally diverse regulatory (calcium/zinc)-binding proteins of vertebrates. The involvement of S100 proteins in numerous vital (patho)physiological processes is mediated by their interaction with various (intra/extra)cellular protein partners, including cell surface receptors. Furthermore, recent studies have revealed the ability of specific S100 proteins to modulate cell signaling via direct interaction with cytokines. Previously, we revealed the binding of ca. 71% of the four-helical cytokines via the S100P protein, due to the presence in its molecule of a cytokine-binding site overlapping with the binding site for the S100P receptor. Here, we show that another S100 protein, S100A6 (that has a pairwise sequence identity with S100P of 35%), specifically binds numerous four-helical cytokines. We have studied the affinity of the recombinant forms of 35 human four-helical cytokines from all structural families of this fold to Ca 2+ -loaded recombinant human S100A6, using surface plasmon resonance spectroscopy. S100A6 recognizes 26 of the cytokines from all families of this fold, with equilibrium dissociation constants from 0.3 nM to 12 µM. Overall, S100A6 interacts with ca. 73% of the four-helical cytokines studied to date, with a selectivity equivalent to that for the S100P protein, with the differences limited to the binding of interleukin-2 and oncostatin M. The molecular docking study evidences the presence in the S100A6 molecule of a cytokine-binding site, analogous to that found in S100P. The findings argue the presence in some of the promiscuous members of the S100 family of a site specific to a wide range of four-helical cytokines. This unique feature of the S100 proteins potentially allows them to modulate the activity of the numerous four-helical cytokines in the disorders accompanied by an excessive release of the cytokines.

Published

2023

10. Canonical structural-binding modes in the calmodulin-target protein complexes.

Author

Denesyuk AI, Permyakov SE, Permyakov EA, Johnson MS, Denessiouk K, and Uversky VN

Abstract

Intracellular calcium sensor protein calmodulin (CaM) belongs to the large EF-hand protein superfamily. CaM shows a unique and not fully understood ability to bind to multiple targets, allows them to participate in a variety of regulatory processes. The protein has two approximately symmetrical globular domains (the N- and C-lobes). Analysis of the CaM-binding sites of target proteins showed that they have two hydrophobic 'anchor' amino acids separated by 10 to 17 residues. Consequently, several CaM-binding motifs: {1-10}, {1-11}, {1-13}, {1-14}, {1-16}, {1-17}, differing by the distance between the two anchor residues along the amino acid sequence, have been identified. Despite extensive structural information on the role of target-protein amino acid residues in the formation of complexes with CaM, much less is known about the role of amino acids from CaM contributing to these interactions. In this work, a quantitative analysis of the contact surfaces of CaM and target proteins has been carried out for 35 representative three-dimensional structures. It has been shown that, in addition to the two hydrophobic terminal residues of the target fragment, the interaction also involves residues that are 4 residues earlier in the sequence (binding mode {1-5}). It has also been found that the N- and C-lobes of CaM bind the {1-5} motif located at the ends of the target in a structurally identical manner. Methionine residues at positions 51 (corresponding to 124 in the C-lobe), 71 (144), and 72 (145) of the CaM amino acid sequence are key hydrophobic residues for this interaction. They are located at the N- and C-boundaries of the even EF-hand motifs. The hydrophobic core of CaM ('Ф-quatrefoil') consists of 10 amino acids in the N-lobe (and in the C-lobe): Phe 16 (Phe 89 ), Phe 19 (Phe 92 ), Ile 27 (Ile 100 ), Thr 29 (Ala 102 ), Leu 32 (Leu 105 ), Ile 52 (Ile 125 ), Val 55 (Ala 128 ), Ile 63 (Val 136 ), Phe 65 (Tyr 138 ), and Phe 68 (Phe 141 ) and do not intersect with the target-binding methionine residues. CaM belongs to the 'dynamic' group of EF-hand proteins, in which calcium and protein ligand binding causes only global conformational changes but does not alter the conservative 'black' and 'grey' clusters described in our earlier works (PLoS One. 2014; 9(10):e109287). The membership of CaM in the 'dynamic' group is determined by the triggering and protective methionine layer: Met 51 (Met 124 ), Met 71 (Met 144 ) and Met 72 (Met 145 ). HIGHLIGHTSInterchain interactions in the unique 35 CaM complex structures were analyzed.Methionine amino acids of the N- and C-lobes of CaM form triggering and protective layers.Interactions of the target terminal residues with these methionine layers are structurally identical.CaM belonging to the 'dynamic' group is determined by the triggering and protective methionine layer.Communicated by Ramaswamy H. Sarma.

Published

2023

11. Kinetics of Ca 2+ Dissociation from Cod Parvalbumin Studied by Fluorescent Stopped-flow Method.

Author

Emelyanenko VI, Vologzhannikova AA, Kazakov AS, Borisova NI, and Permyakov EA

Subjects

Binding Sites, Cations, Cations, Divalent, Kinetics, Protein Binding, Spectrometry, Fluorescence, Gadiformes, Calcium chemistry, Parvalbumins chemistry, Parvalbumins metabolism

Abstract

Background: Small Ca 2+ -binding protein parvalbumin possesses two strong Ca 2+ /Mg 2+ - binding sites located within two EF-hand domains. Most parvalbumins have no tryptophan residues, while cod protein contains a single tryptophan residue, which fluorescence (spectrum maximum position and fluorescence quantum yield) is highly sensitive to the Ca 2+ association/dissociation., Objective: Intrinsic protein fluorescence of cod parvalbumin can be used for elucidating the mechanism of Ca 2+ binding to this protein. Fluorescence of the single tryptophan residue of cod parvalbumin has been used to monitor Ca 2+ -induced changes in the protein, both in steady-state and kinetic mode., Methods: Steady-state fluorescence spectra of cod parvalbumin were measured using Cary Eclipse spectrofluorimeter. Stopped-flow accessories in combination with a novel high-speed spectrofluorimeter were used for measurements of kinetics of Ca 2+ dissociation from cod parvalbumin after fast mixing of Ca 2+ -loaded protein with a chelator of divalent metal cations ethylenediaminetetraacetic acid (EDTA)., Results: The fluorescent phase plots (fluorescence intensity at a fixed wavelength plotted against a fluorescence intensity at another fixed wavelength), constructed from steady state and kinetical data, shows a break at [Ca 2+ ]/[parvalbumin] ratio close to 1. This means that the transition passes through an intermediate state, which is a protein with one bound calcium ion. These observations indicate that the binding of Ca 2+ to cod parvalbumin is sequential., Conclusion: The results of the present spectral study showed that the binding of Ca 2+ to cod parvalbumin is a sequential process. Calcium dissociation rate constants for the two binding sites of cod parvalbumin evaluated from the kinetic data are k off1 = 1.0 s -1 and k off2 = 1.5 s -1 ., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2023

12. Specific S100 Proteins Bind Tumor Necrosis Factor and Inhibit Its Activity.

Author

Kazakov AS, Zemskova MY, Rystsov GK, Vologzhannikova AA, Deryusheva EI, Rastrygina VA, Sokolov AS, Permyakova ME, Litus EA, Uversky VN, Permyakov EA, and Permyakov SE

Subjects

S100A12 Protein, Tumor Necrosis Factor Inhibitors, Tumor Necrosis Factor-alpha metabolism, Receptors, Tumor Necrosis Factor metabolism, S100 Proteins

Abstract

Tumor necrosis factor (TNF) inhibitors (anti-TNFs) represent a cornerstone of the treatment of various immune-mediated inflammatory diseases and are among the most commercially successful therapeutic agents. Knowledge of TNF binding partners is critical for identification of the factors able to affect clinical efficacy of the anti-TNFs. Here, we report that among eighteen representatives of the multifunctional S100 protein family, only S100A11, S100A12 and S100A13 interact with the soluble form of TNF (sTNF) in vitro. The lowest equilibrium dissociation constants ( K d ) for the complexes with monomeric sTNF determined using surface plasmon resonance spectroscopy range from 2 nM to 28 nM. The apparent K d values for the complexes of multimeric sTNF with S100A11/A12 estimated from fluorimetric titrations are 0.1-0.3 µM. S100A12/A13 suppress the cytotoxic activity of sTNF against Huh-7 cells, as evidenced by the MTT assay. Structural modeling indicates that the sTNF-S100 interactions may interfere with the sTNF recognition by the therapeutic anti-TNFs. Bioinformatics analysis reveals dysregulation of TNF and S100A11/A12/A13 in numerous disorders. Overall, we have shown a novel potential regulatory role of the extracellular forms of specific S100 proteins that may affect the efficacy of anti-TNF treatment in various diseases.

Published

2022

13. Calcium-Bound S100P Protein Is a Promiscuous Binding Partner of the Four-Helical Cytokines.

Author

Kazakov AS, Deryusheva EI, Permyakova ME, Sokolov AS, Rastrygina VA, Uversky VN, Permyakov EA, and Permyakov SE

Subjects

Calcium, Dietary, Carrier Proteins metabolism, Humans, Immunologic Factors, Molecular Docking Simulation, Neoplasm Proteins metabolism, Protein Binding, Receptor for Advanced Glycation End Products metabolism, S100 Proteins metabolism, Calcium metabolism, Calcium-Binding Proteins metabolism, Cytokines metabolism

Abstract

S100 proteins are multifunctional calcium-binding proteins of vertebrates that act intracellularly, extracellularly, or both, and are engaged in the progression of many socially significant diseases. Their extracellular action is typically mediated by the recognition of specific receptor proteins. Recent studies indicate the ability of some S100 proteins to affect cytokine signaling through direct interaction with cytokines. S100P was shown to be the S100 protein most actively involved in interactions with some four-helical cytokines. To assess the selectivity of the S100P protein binding to four-helical cytokines, we have probed the interaction of Ca 2+ -bound recombinant human S100P with a panel of 32 four-helical human cytokines covering all structural families of this fold, using surface plasmon resonance spectroscopy. A total of 22 cytokines from all families of four-helical cytokines are S100P binders with the equilibrium dissociation constants, K d , ranging from 1 nM to 3 µM (below the K d value for the S100P complex with the V domain of its conventional receptor, receptor for advanced glycation end products, RAGE). Molecular docking and mutagenesis studies revealed the presence in the S100P molecule of a cytokine-binding site, which overlaps with the RAGE-binding site. Since S100 binding to four-helical cytokines inhibits their signaling in some cases, the revealed ability of the S100P protein to interact with ca. 71% of the four-helical cytokines indicates that S100P may serve as a poorly selective inhibitor of their action.

Published

2022

14. What Is Parvalbumin for?

Author

Permyakov EA and Uversky VN

Subjects

Animals, EF Hand Motifs, Mammals metabolism, Mice, Neurons metabolism, Reactive Oxygen Species, Calcium metabolism, Parvalbumins metabolism

Abstract

Parvalbumin (PA) is a small, acidic, mostly cytosolic Ca 2+ -binding protein of the EF-hand superfamily. Structural and physical properties of PA are well studied but recently two highly conserved structural motifs consisting of three amino acids each (clusters I and II), which contribute to the hydrophobic core of the EF-hand domains, have been revealed. Despite several decades of studies, physiological functions of PA are still poorly known. Since no target proteins have been revealed for PA so far, it is believed that PA acts as a slow calcium buffer. Numerous experiments on various muscle systems have shown that PA accelerates the relaxation of fast skeletal muscles. It has been found that oxidation of PA by reactive oxygen species (ROS) is conformation-dependent and one more physiological function of PA in fast muscles could be a protection of these cells from ROS. PA is thought to regulate calcium-dependent metabolic and electric processes within the population of gamma-aminobutyric acid (GABA) neurons. Genetic elimination of PA results in changes in GABAergic synaptic transmission. Mammalian oncomodulin (OM), the β isoform of PA, is expressed mostly in cochlear outer hair cells and in vestibular hair cells. OM knockout mice lose their hearing after 3-4 months. It was suggested that, in sensory cells, OM maintains auditory function, most likely affecting outer hair cells' motility mechanisms.

Published

2022

15. Interferon-β Activity Is Affected by S100B Protein.

Author

Kazakov AS, Sofin AD, Avkhacheva NV, Deryusheva EI, Rastrygina VA, Permyakova ME, Uversky VN, Permyakov EA, and Permyakov SE

Subjects

Animals, CHO Cells, Calcium metabolism, Cell Line, Tumor, Cricetulus, Humans, MCF-7 Cells, Nervous System Diseases metabolism, Protein Binding physiology, Interferon-beta metabolism, S100 Calcium Binding Protein beta Subunit metabolism

Abstract

Interferon-β (IFN-β) is a pleiotropic cytokine secreted in response to various pathological conditions and is clinically used for therapy of multiple sclerosis. Its application for treatment of cancer, infections and pulmonary diseases is limited by incomplete understanding of regulatory mechanisms of its functioning. Recently, we reported that IFN-β activity is affected by interactions with S100A1, S100A4, S100A6, and S100P proteins, which are members of the S100 protein family of multifunctional Ca 2+ -binding proteins possessing cytokine-like activities (Int J Mol Sci. 2020;21(24):9473). Here we show that IFN-β interacts with one more representative of the S100 protein family, the S100B protein, involved in numerous oncological and neurological diseases. The use of chemical crosslinking, intrinsic fluorescence, and surface plasmon resonance spectroscopy revealed IFN-β binding to Ca 2+ -loaded dimeric and monomeric forms of the S100B protein. Calcium depletion blocks the S100B-IFN-β interaction. S100B monomerization increases its affinity to IFN-β by 2.7 orders of magnitude (equilibrium dissociation constant of the complex reaches 47 pM). Crystal violet assay demonstrated that combined application of IFN-β and S100B (5-25 nM) eliminates their inhibitory effects on MCF-7 cell viability. Bioinformatics analysis showed that the direct modulation of IFN-β activity by the S100B protein described here could be relevant to progression of multiple oncological and neurological diseases.

Published

2022

16. Erythropoietin Interacts with Specific S100 Proteins.

Author

Kazakov AS, Deryusheva EI, Sokolov AS, Permyakova ME, Litus EA, Rastrygina VA, Uversky VN, Permyakov EA, and Permyakov SE

Subjects

Calcium metabolism, Protein Binding, Protein Transport, Erythropoietin metabolism, S100 Proteins metabolism

Abstract

Erythropoietin (EPO) is a clinically significant four-helical cytokine, exhibiting erythropoietic, cytoprotective, immunomodulatory, and cancer-promoting activities. Despite vast knowledge on its signaling pathways and physiological effects, extracellular factors regulating EPO activity remain underexplored. Here we show by surface plasmon resonance spectroscopy, that among eighteen members of Ca 2+ -binding proteins of the S100 protein family studied, only S100A2, S100A6 and S100P proteins specifically recognize EPO with equilibrium dissociation constants ranging from 81 nM to 0.5 µM. The interactions occur exclusively under calcium excess. Bioinformatics analysis showed that the EPO-S100 interactions could be relevant to progression of neoplastic diseases, including cancer, and other diseases. The detailed knowledge of distinct physiological effects of the EPO-S100 interactions could favor development of more efficient clinical implications of EPO. Summing up our data with previous findings, we conclude that S100 proteins are potentially able to directly affect functional activities of specific members of all families of four-helical cytokines, and cytokines of other structural superfamilies.

Published

2022

17. Specific cytokines of interleukin-6 family interact with S100 proteins.

Author

Kazakov AS, Sokolov AS, Permyakova ME, Litus EA, Uversky VN, Permyakov EA, and Permyakov SE

Subjects

Cytokine Receptor gp130, Cytokines metabolism, S100 Proteins, Interleukin-6, Receptors, Cytokine metabolism

Abstract

Cytokines of interleukin-6 (IL-6) family are important signaling proteins involved in various physiological and pathological processes. Earlier, we described interactions between IL-11 and S100P/B proteins from the family of S100 proteins engaged in the pathogenesis of numerous diseases. We probed here interactions between seven IL-6 family cytokines (IL-6, IL-11, OSM, LIF, CNTF, CT-1, and CLCF1) and fourteen S100 proteins (S100A1/A4/A6/A7/A8/A9/A10/A11/A12/A13/A14/A15/B/P). Surface plasmon resonance spectroscopy revealed formation of calcium-dependent complexes between IL-11, OSM, CNTF, CT-1, and CLCF1 and distinct subsets of S100A1/A6/B/P proteins with equilibrium dissociation constants of 19 nM - 12 µM. The existence of a network of interactions between Ca 2+ -loaded S100 proteins and IL-6 family cytokines suggest regulation of these cytokines by the extracellular forms of S100 proteins., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2022

18. Structural and functional significance of the amino acid differences Val 35 Thr, Ser 46 Ala, Asn 65 Ser, and Ala 94 Ser in 3C-like proteinases from SARS-CoV-2 and SARS-CoV.

Author

Denesyuk AI, Permyakov EA, Johnson MS, Permyakov SE, Denessiouk K, and Uversky VN

Subjects

Amino Acid Substitution, Humans, Protein Domains, Species Specificity, Structure-Activity Relationship, Coronavirus 3C Proteases chemistry, Coronavirus 3C Proteases genetics, Mutation, Missense, Severe acute respiratory syndrome-related coronavirus enzymology, Severe acute respiratory syndrome-related coronavirus genetics, SARS-CoV-2 enzymology, SARS-CoV-2 genetics

Abstract

Three dimensional structures of (chymo)trypsin-like proteinase (3CL pro ) from SARS-CoV-2 and SARS-CoV differ at 8 positions. We previously found that the Val 86 Leu, Lys 88 Arg, Phe 134 His, and Asn 180 Lys mutations in these enzymes can change the orientation of the N- and C-terminal domains of 3CL pro relative to each other, which leads to a change in catalytic activity. This conclusion was derived from the comparison of the structural catalytic core in 169 (chymo)trypsin-like proteinases with the serine/cysteine fold. Val 35 Thr, Ser 46 Ala, Asn 65 Ser, Ala 94 Ser mutations were not included in that analysis, since they are located far from the catalytic tetrad. In the present work, the structural and functional roles of these variable amino acids at positions 35, 46, 65, and 94 in the 3CL pro sequences of SARS-CoV-2 and SARS-CoV have been established using a comparison of the same set of proteinases leading to the identification of new conservative elements. Comparative analysis showed that, in addition to interdomain mobility, which could modulate catalytic activity, the 3CL pro (s) can use for functional regulation an autolytic loop and the unique Asp 33 -Asn 95 region (the Asp 33 -Asn 95 Zone) in the N-terminal domain. Therefore, all 4 analyzed mutation sites are associated with the unique structure-functional features of the 3CL pro from SARS-CoV-2 and SARS-CoV. Strictly speaking, the presented structural results are hypothetical, since at present there is not a single experimental work on the identification and characterization of autolysis sites in these proteases., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

19. Ca 2+ /Sr 2+ Selectivity in Calcium-Sensing Receptor (CaSR): Implications for Strontium's Anti-Osteoporosis Effect.

Author

Cheshmedzhieva D, Ilieva S, Permyakov EA, Permyakov SE, and Dudev T

Subjects

Humans, Binding Sites, Density Functional Theory, Receptors, Calcium-Sensing metabolism, Receptors, Calcium-Sensing agonists, Strontium chemistry, Strontium pharmacology, Calcium metabolism, Osteoporosis drug therapy, Osteoporosis metabolism

Abstract

The extracellular calcium-sensing receptor (CaSR) controls vital bone cell functions such as cell growth, differentiation and apoptosis. The binding of the native agonist (Ca 2+ ) to CaSR activates the receptor, which undergoes structural changes that trigger a cascade of events along the cellular signaling pathways. Strontium (in the form of soluble salts) has been found to also be a CaSR agonist. The activation of the receptor by Sr 2+ is considered to be the major mechanism through which strontium exerts its anti-osteoporosis effect, mostly in postmenopausal women. Strontium-activated CaSR initiates a series of signal transduction events resulting in both osteoclast apoptosis and osteoblast differentiation, thus strengthening the bone tissue. The intimate mechanism of Sr 2+ activation of CaSR is still enigmatic. Herewith, by employing a combination of density functional theory (DFT) calculations and polarizable continuum model (PCM) computations, we have found that the Ca 2+ binding sites 1, 3, and 4 in the activated CaSR, although possessing a different number and type of protein ligands, overall structure and charge state, are all selective for Ca 2+ over Sr 2+ . The three binding sites, regardless of their structural differences, exhibit almost equal metal selectivity if they are flexible and have no geometrical constraints on the incoming Sr 2+ . In contrast to Ca 2+ and Sr 2+ , Mg 2+ constructs, when allowed to fully relax during the optimization process, adopt their stringent six-coordinated octahedral structure at the expense of detaching a one-backbone carbonyl ligand and shifting it to the second coordination layer of the metal. The binding of Mg 2+ and Sr 2+ to a rigid/inflexible calcium-designed binding pocket requires an additional energy penalty for the binding ion; however, the price for doing so (to be paid by Sr 2+ ) is much less than that of Mg 2+ . The results obtained delineate the key factors controlling the competition between metal cations for the receptor and shed light on some aspects of strontium's therapeutic effects.

Published

2021

20. Strontium Binding to α-Parvalbumin, a Canonical Calcium-Binding Protein of the "EF-Hand" Family.

Author

Vologzhannikova AA, Shevelyova MP, Kazakov AS, Sokolov AS, Borisova NI, Permyakov EA, Kircheva N, Nikolova V, Dudev T, and Permyakov SE

Subjects

Binding Sites, Calcium-Binding Proteins chemistry, Calcium-Binding Proteins genetics, Cations, Divalent, Cloning, Molecular, Density Functional Theory, EF Hand Motifs, Escherichia coli genetics, Escherichia coli metabolism, Gene Expression, Genetic Vectors chemistry, Genetic Vectors metabolism, Humans, Kinetics, Parvalbumins chemistry, Parvalbumins genetics, Protein Binding, Protein Stability, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Solutions, Calcium metabolism, Calcium-Binding Proteins metabolism, Parvalbumins metabolism, Strontium metabolism

Abstract

Strontium salts are used for treatment of osteoporosis and bone cancer, but their impact on calcium-mediated physiological processes remains obscure. To explore Sr 2+ interference with Ca 2+ binding to proteins of the EF-hand family, we studied Sr 2+ /Ca 2+ interaction with a canonical EF-hand protein, α-parvalbumin (α-PA). Evaluation of the equilibrium metal association constants for the active Ca 2+ binding sites of recombinant human α-PA ('CD' and 'EF' sites) from fluorimetric titration experiments and isothermal titration calorimetry data gave 4 × 10 9 M -1 and 4 × 10 9 M -1 for Ca 2+ , and 2 × 10 7 M -1 and 2 × 10 6 M -1 for Sr 2+ . Inactivation of the EF site by homologous substitution of the Ca 2+ -coordinating Glu in position 12 of the EF-loop by Gln decreased Ca 2+ /Sr 2+ affinity of the protein by an order of magnitude, whereas the analogous inactivation of the CD site induced much deeper suppression of the Ca 2+ /Sr 2+ affinity. These results suggest that Sr 2+ and Ca 2+ bind to CD/EF sites of α-PA and the Ca 2+ /Sr 2+ binding are sequential processes with the CD site being occupied first. Spectrofluorimetric Sr 2+ titration of the Ca 2+ -loaded α-PA revealed presence of secondary Sr 2+ binding site(s) with an apparent equilibrium association constant of 4 × 10 5 M -1 . Fourier-transform infrared spectroscopy data evidence that Ca 2+ /Sr 2+ -loaded forms of α-PA exhibit similar states of their COO - groups. Near-UV circular dichroism (CD) data show that Ca 2+ /Sr 2+ binding to α-PA induce similar changes in symmetry of microenvironment of its Phe residues. Far-UV CD experiments reveal that Ca 2+ /Sr 2+ binding are accompanied by nearly identical changes in secondary structure of α-PA. Meanwhile, scanning calorimetry measurements show markedly lower Sr 2+ -induced increase in stability of tertiary structure of α-PA, compared to the Ca 2+ -induced effect. Theoretical modeling using Density Functional Theory computations with Polarizable Continuum Model calculations confirms that Ca 2+ -binding sites of α-PA are well protected against exchange of Ca 2+ for Sr 2+ regardless of coordination number of Sr 2+ , solvent exposure or rigidity of sites. The latter appears to be a key determinant of the Ca 2+ /Sr 2+ selectivity. Overall, despite lowered affinity of α-PA to Sr 2+ , the latter competes with Ca 2+ for the same EF-hands and induces similar structural rearrangements. The presence of a secondary Sr 2+ binding site(s) could be a factor contributing to Sr 2+ impact on the functional activity of proteins.

Published

2021

21. Structural leitmotif and functional variations of the structural catalytic core in (chymo)trypsin-like serine/cysteine fold proteinases.

Author

Denesyuk AI, Permyakov SE, Johnson MS, Permyakov EA, Uversky VN, and Denessiouk K

Subjects

Amino Acid Sequence, Binding Sites, COVID-19 metabolism, Catalysis, Catalytic Domain, Cysteine Proteases metabolism, Humans, Models, Molecular, Severe acute respiratory syndrome-related coronavirus chemistry, Severe acute respiratory syndrome-related coronavirus metabolism, SARS-CoV-2 chemistry, SARS-CoV-2 metabolism, Serine Endopeptidases chemistry, Serine Endopeptidases metabolism, Serine Proteases metabolism, Trypsin metabolism, Cysteine Proteases chemistry, Serine Proteases chemistry

Abstract

Proteinases with the (chymo)trypsin-like serine/cysteine fold comprise a large superfamily performing their function through the Acid - Base - Nucleophile catalytic triad. In our previous work (Denesyuk AI, Johnson MS, Salo-Ahen OMH, Uversky VN, Denessiouk K. Int J Biol Macromol. 2020;153:399-411), we described a universal three-dimensional (3D) structural motif, NBCZone, that contains eleven amino acids: dipeptide 42 T-43 T, pentapeptide 54 T-55 T-56 T-57 T(base)-58 T, tripeptide 195 T(nucleophile)-196 T-197 T and residue 213 T (T - numeration of amino acids in trypsin). The comparison of the NBCZones among the members of the (chymo)trypsin-like protease family suggested the existence of 15 distinct groups. Within each group, the NBCZones incorporate an identical set of conserved interactions and bonds. In the present work, the structural environment of the catalytic acid at the position 102 T and the fourth member of the "catalytic tetrad" at the position 214 T was analyzed in 169 3D structures of proteinases with the (chymo)trypsin-like serine/cysteine fold. We have identified a complete Structural Catalytic Core (SCC) consisting of two classes and four groups. The proteinases belonging to different classes and groups differ from each other by the nature of the interaction between their N- and C-terminal β-barrels. Comparative analysis of the 3CLpro(s) from SARS-CoV-2 and SARS-CoV, used as an example, showed that the amino acids at positions 103 T and 179 T affect the nature of the interaction of the "catalytic acid" core (102 T-Core, N-terminal β-barrel) with the "supplementary" core (S-Core, C-terminal β-barrel), which ultimately results in the modulation of the enzymatic activity. The reported analysis represents an important standalone contribution to the analysis and systematization of the 3D structures of (chymo)trypsin-like serine/cysteine fold proteinases. The use of the developed approach for the comparison of 3D structures will allow, in the event of the appearance of new representatives of a given fold in the PDB, to quickly determine their structural homologues with the identification of possible differences., Competing Interests: Declaration of competing interest The authors declare no conflict of interest., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

22. The Highly Conservative Cysteine of Oncomodulin as a Feasible Redox Sensor.

Author

Vologzhannikova AA, Khorn PA, Shevelyova MP, Kazakov AS, Emelyanenko VI, Permyakov EA, and Permyakov SE

Subjects

Animals, Calcium metabolism, Hydrogen-Ion Concentration, Kinetics, Magnesium metabolism, Oxidation-Reduction, Protein Structure, Quaternary, Protein Structure, Secondary, Rats, Recombinant Proteins isolation & purification, Structure-Activity Relationship, Sulfhydryl Compounds metabolism, Temperature, Calcium-Binding Proteins chemistry, Calcium-Binding Proteins metabolism, Conserved Sequence, Cysteine metabolism

Abstract

Oncomodulin (Ocm), or parvalbumin β, is an 11-12 kDa Ca 2+ -binding protein found inside and outside of vertebrate cells, which regulates numerous processes via poorly understood mechanisms. Ocm consists of two active Ca 2+ -specific domains of the EF-hand type ("helix-loop-helix" motif), covered by an EF-hand domain with inactive EF-hand loop, which contains a highly conservative cysteine with unknown function. In this study, we have explored peculiarities of the microenvironment of the conservative Cys18 of recombinant rat Ocm (rWT Ocm), redox properties of this residue, and structural/functional sensitivity of rWT Ocm to the homologous C18S substitution. We have found that pK a of the Cys18 thiol lays beyond the physiological pH range. The measurement of redox dependence of rWT Ocm thiol-disulfide equilibrium (glutathione redox pair) showed that redox potential of Cys18 for the metal-free and Ca 2+ -loaded protein is of -168 mV and -176 mV, respectively. Therefore, the conservative thiol of rWT Ocm is prone to disulfide dimerization under physiological redox conditions. The C18S substitution drastically reduces α-helices content of the metal-free and Mg 2+ -bound Ocm, increases solvent accessibility of its hydrophobic residues, eliminates the cooperative thermal transition in the apo-protein, suppresses Ca 2+ /Mg 2+ affinity of the EF site, and accelerates Ca 2+ dissociation from Ocm. The distinct structural and functional consequences of the minor structural modification of Cys18 indicate its possible redox sensory function. Since some other EF-hand proteins also contain a conservative redox-sensitive cysteine located in an inactive EF-hand loop, it is reasonable to suggest that in the course of evolution, some of the EF-hands attained redox sensitivity at the expense of the loss of their Ca 2+ affinity.

Published

2021

23. Papain-like cysteine proteinase zone (PCP-zone) and PCP structural catalytic core (PCP-SCC) of enzymes with cysteine proteinase fold.

Author

Denessiouk K, Uversky VN, Permyakov SE, Permyakov EA, Johnson MS, and Denesyuk AI

Subjects

Biocatalysis, Models, Molecular, Catalytic Domain, Papain chemistry, Papain metabolism

Abstract

There are several families of cysteine proteinases with different folds - for example the (chymo)trypsin fold family and papain-like fold family - but in both families the hydrolase activity of cysteine proteinases requires a cysteine residue as the catalytic nucleophile. In this work, we have analyzed the topology of the active site regions in 146 three-dimensional structures of proteins belonging to the Papain-like Cysteine Proteinase (PCP) superfamily, which includes papain as a typical representative of this protein superfamily. All analyzed enzymes contain a unique structurally closed conformation - a "PCP-Zone" - which can be divided into two groups, Class A and Class B. Eight structurally conserved amino acids of the PCP-Zone form a common Structural Core. The Structural Core, catalytic nucleophile, catalytic base and residue Xaa - which stabilizes the side-chain conformation of the catalytic base - make up a PCP Structural Catalytic Core (PCP-SCC). The PCP-SCC of Class A and Class B are divided into 5 and 2 types, respectively. Seven variants of the mutual arrangement of the amino-acid side chains of the catalytic triad - nucleophile, base and residue Xaa - within the same fold clearly demonstrate how enzymes with the papain-like fold adapt to the need to perform diverse functions in spite of their limited structural diversity. The roles of both the PCP-Zone of SARS-CoV-2-PLpro described in this study and the NBCZone of SARS-CoV-2-3CLpro presented in our earlier article (Denesyuk AI, Johnson MS, Salo-Ahen OMH, Uversky VN, Denessiouk K. Int J Biol Macromol. 2020;153:399-411) that are in contacts with inhibitors are discussed., Competing Interests: Declaration of competing interest The authors declare no conflict of interest., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

24. Interferon Beta Activity Is Modulated via Binding of Specific S100 Proteins.

Author

Kazakov AS, Sofin AD, Avkhacheva NV, Denesyuk AI, Deryusheva EI, Rastrygina VA, Sokolov AS, Permyakova ME, Litus EA, Uversky VN, Permyakov EA, and Permyakov SE

Subjects

Amino Acid Sequence, Calcium chemistry, Calcium-Binding Proteins chemistry, Calcium-Binding Proteins metabolism, Cardiovascular Diseases metabolism, Cell Cycle Proteins chemistry, Cell Cycle Proteins metabolism, Cell Survival drug effects, Dimerization, Humans, Kinetics, MCF-7 Cells, Models, Chemical, Molecular Docking Simulation, Neoplasm Proteins chemistry, Neoplasm Proteins metabolism, Neoplasms metabolism, Nervous System Diseases metabolism, Protein Binding, Protein Conformation drug effects, S100 Calcium Binding Protein A6 chemistry, S100 Calcium Binding Protein A6 metabolism, S100 Calcium-Binding Protein A4 chemistry, S100 Calcium-Binding Protein A4 metabolism, S100 Proteins chemistry, Sequence Alignment, Surface Plasmon Resonance, Calcium metabolism, Interferon-beta metabolism, S100 Proteins metabolism

Abstract

Interferon-β (IFN-β) is a pleiotropic cytokine used for therapy of multiple sclerosis, which is also effective in suppression of viral and bacterial infections and cancer. Recently, we reported a highly specific interaction between IFN-β and S100P lowering IFN-β cytotoxicity to cancer cells (Int J Biol Macromol. 2020; 143: 633-639). S100P is a member of large family of multifunctional Ca 2+ -binding proteins with cytokine-like activities. To probe selectivity of IFN-β-S100 interaction with respect to S100 proteins, we used surface plasmon resonance spectroscopy, chemical crosslinking, and crystal violet assay. Among the thirteen S100 proteins studied S100A1, S100A4, and S100A6 proteins exhibit strictly Ca 2+ -dependent binding to IFN-β with equilibrium dissociation constants, K d , of 0.04-1.5 µM for their Ca 2+ -bound homodimeric forms. Calcium depletion abolishes the S100-IFN-β interactions. Monomerization of S100A1/A4/A6 decreases K d values down to 0.11-1.0 nM. Interferon-α is unable of binding to the S100 proteins studied. S100A1/A4 proteins inhibit IFN-β-induced suppression of MCF-7 cells viability. The revealed direct influence of specific S100 proteins on IFN-β activity uncovers a novel regulatory role of particular S100 proteins, and opens up novel approaches to enhancement of therapeutic efficacy of IFN-β.

Published

2020

25. α-Lactalbumin, Amazing Calcium-Binding Protein.

Author

Permyakov EA

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents metabolism, Humans, Hydrogen-Ion Concentration, Lactalbumin chemistry, Oleic Acid chemistry, Oleic Acid metabolism, Oleic Acid pharmacology, Antineoplastic Agents pharmacology, Lactalbumin metabolism, Neoplasms drug therapy

Abstract

α-Lactalbumin (α-LA) is a small (Mr 14,200), acidic (pI 4-5), Ca 2+ -binding protein. α-LA is a regulatory component of lactose synthase enzyme system functioning in the lactating mammary gland. The protein possesses a single strong Ca 2+ -binding site, which can also bind Mg 2+ , Mn 2+ , Na + , K + , and some other metal cations. It contains several distinct Zn 2+ -binding sites. Physical properties of α-LA strongly depend on the occupation of its metal binding sites by metal ions. In the absence of bound metal ions, α-LA is in the molten globule-like state. The binding of metal ions, and especially of Ca 2+ , increases stability of α-LA against the action of heat, various denaturing agents and proteases, while the binding of Zn 2+ to the Ca 2+ -loaded protein decreases its stability and causes its aggregation. At pH 2, the protein is in the classical molten globule state. α-LA can associate with membranes at neutral or slightly acidic pH at physiological temperatures. Depending on external conditions, α-LA can form amyloid fibrils, amorphous aggregates, nanoparticles, and nanotubes. Some of these aggregated states of α-LA can be used in practical applications such as drug delivery to tissues and organs. α-LA and some of its fragments possess bactericidal and antiviral activities. Complexes of partially unfolded α-LA with oleic acid are cytotoxic to various tumor and bacterial cells. α-LA in the cytotoxic complexes plays a role of a delivery carrier of cytotoxic fatty acid molecules into tumor and bacterial cells across the cell membrane. Perhaps in the future the complexes of α-LA with oleic acid will be used for development of new anti-cancer drugs.

Published

2020

26. Mouse S100G protein exhibits properties characteristic of a calcium sensor.

Author

Permyakov SE, Yundina EN, Kazakov AS, Permyakova ME, Uversky VN, and Permyakov EA

Subjects

Amino Acid Sequence, Animals, Cattle, Guanidine pharmacology, Hydrogen-Ion Concentration, Magnetic Resonance Spectroscopy, Models, Molecular, Protein Denaturation, Protein Structure, Secondary, Proteolysis, Recombinant Proteins metabolism, S100 Calcium Binding Protein G chemistry, Spectrometry, Fluorescence, Temperature, Tyrosine metabolism, Calcium metabolism, S100 Calcium Binding Protein G metabolism

Abstract

Bovine S100 G (calbindin D 9k , small Ca 2+ -binding protein of the EF-hand superfamily) is considered as a calcium buffer protein; i.e., the binding of Ca 2+ practically does not change its general conformation. A set of experimental approaches has been used to study structural properties of apo- and Ca 2+ -loaded forms of mouse S100 G (81.4% identity in amino acid sequence with bovine S100 G). This analysis revealed that, in contrast to bovine S100 G, the removal of calcium ions increases α-helices content of mouse S100 G protein and enhances its accessibility to digestion by α-chymotrypsin. Furthermore, mouse apo-S100 G is characterized by a decreased surface hydrophobicity and reduced tendency for oligomerization. Such behavior is typical of calcium sensor proteins. Apo-state of mouse S100 G still has rather compact structure, which can be cooperatively unfolded by temperature and GdnHCl. Computational analysis of amino acid sequences of S100 G proteins shows that these proteins could be in a disordered state upon a removal of the bound calcium ions. The experimental data show that, although mouse apo-S100 G is flexible compared to the Ca 2+ -loaded state, the apo-form is not completely disordered and preserves some cooperatively meting structure. The origin of the unexpectedly high stability of mouse S100 G can be rationalized by an exceptionally strong association of its N- and C-terminal parts containing the EF-hands I and II, respectively., Competing Interests: Declaration of Competing Interest We, Sergei E. Permyakov, Elena N. Yundina, Alexei S. Kazakov, Maria E. Permyakova, Vladimir N. Uversky, and Eugene A. Permyakov, authors of the manuscript entitled “Mouse S100 G protein exhibits properties characteristic of a calcium sensor”, wish to confirm that there are no known conflicts of interest associated with this publication and there has been no significant financial support for this work that could have influenced its outcome., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

27. System Approach for Building of Calcium-Binding Sites in Proteins.

Author

Denesyuk AI, Permyakov SE, Johnson MS, Denessiouk K, and Permyakov EA

Subjects

Binding Sites, Cations, Models, Molecular, Proteins chemistry, Calcium metabolism, Proteins metabolism

Abstract

We introduce five new local metal cation (first of all, Ca 2+ ) recognition units in proteins: Clamp n,(n-2) , Clamp n,(n-1) , Clamp n,n , Clamp n,(n+1) and Clamp n,(n+2) . In these units, the backbone oxygen atom of a residue in position "n" of an amino acid sequence and side-chain oxygen atom of a residue in position "n + i" (i = -2 to +2) directly interact with a metal cation. An analysis of the known "Ca 2+ -bound niches" in proteins has shown that a system approach based on the simultaneous use of the Clamp units and earlier proposed One-Residue (OR)/Three-Residue (TR) units significantly improves the results of constructing metal cation-binding sites in proteins.

Published

2020

28. Highly specific interaction of monomeric S100P protein with interferon beta.

Author

Kazakov AS, Mayorov SA, Deryusheva EI, Avkhacheva NV, Denessiouk KA, Denesyuk AI, Rastrygina VA, Permyakov EA, and Permyakov SE

Subjects

Calcium metabolism, Calcium-Binding Proteins chemistry, Cell Death, Cell Survival, Humans, Interferon-beta chemistry, Kinetics, Ligands, MCF-7 Cells, Models, Biological, Neoplasm Proteins chemistry, Protein Binding, Protein Conformation, Calcium-Binding Proteins metabolism, Interferon-beta metabolism, Neoplasm Proteins metabolism

Abstract

S100 proteins are EF-hand calcium-binding proteins of vertebrates exerting numerous intra- and extracellular actions and involved into multiple diseases. Some of S100 proteins serve as extracellular damage signals via interaction with receptors. Although several S100 proteins directly bind specific cytokines, this phenomenon remains underexplored. Using chemical crosslinking, intrinsic fluorescence and surface plasmon resonance spectroscopies, we show that S100P protein interacts with interferon beta (IFN-β) depending on calcium level and oligomeric state of S100P. Dimeric Ca 2+ -loaded S100P binds IFN-β with equilibrium dissociation constants, K d , of 0.05-0.6 μM. S100P monomerization favors this interaction decreasing K d values down to 0.3-2 nM. Calcium depletion drastically lowers S100P affinity to IFN-β. Other related EF-hand proteins studied (calmodulin, α-parvalbumin and S100G) do not bind IFN-β, thereby confirming selectivity of the S100P - IFN-β interaction. Crystal violet assay reveals that the S100P binding suppresses IFN-β cytotoxicity to MCF-7 breast cancer cells. Since several cancers (breast, colon, lung, liver, etc.) exhibit dysregulated functioning of S100P and IFN-β, their interaction could be relevant to the cancer progression and directed therapeutic interventions., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2020

29. Experimental Insight into the Structural and Functional Roles of the 'Black' and 'Gray' Clusters in Recoverin, a Calcium Binding Protein with Four EF-Hand Motifs.

Author

Permyakov SE, Vologzhannikova AS, Nemashkalova EL, Kazakov AS, Denesyuk AI, Denessiouk K, Baksheeva VE, Zamyatnin AA Jr, Zernii EY, Uversky VN, and Permyakov EA

Subjects

Alanine chemistry, Amino Acid Motifs, Amino Acid Substitution, Calcium metabolism, G-Protein-Coupled Receptor Kinase 1 metabolism, Humans, Hydrophobic and Hydrophilic Interactions, Kinetics, Models, Molecular, Mutation, Phosphorylation, Protein Binding, Recoverin genetics, Rhodopsin metabolism, Recoverin chemistry, Recoverin metabolism

Abstract

Recently, we have found that calcium binding proteins of the EF-hand superfamily (i.e., a large family of proteins containing helix-loop-helix calcium binding motif or EF-hand) contain two types of conserved clusters called cluster I ('black' cluster) and cluster II ('grey' cluster), which provide a supporting scaffold for the Ca 2+ binding loops and contribute to the hydrophobic core of the EF-hand domains. Cluster I is more conservative and mostly incorporates aromatic amino acids, whereas cluster II includes a mix of aromatic, hydrophobic, and polar amino acids of different sizes. Recoverin is EF-hand Ca 2+ -binding protein containing two 'black' clusters comprised of F35, F83, Y86 (N-terminal domain) and F106, E169, F172 (C-terminal domain) as well as two 'gray' clusters comprised of F70, Q46, F49 (N-terminal domain) and W156, K119, V122 (C-terminal domain). To understand a role of these residues in structure and function of human recoverin, we sequentially substituted them for alanine and studied the resulting mutants by a set of biophysical methods. Under metal-free conditions, the 'black' clusters mutants (except for F35A and E169A) were characterized by an increase in the α-helical content, whereas the 'gray' cluster mutants (except for K119A) exhibited the opposite behavior. By contrast, in Ca 2+ -loaded mutants the α-helical content was always elevated. In the absence of calcium, the substitutions only slightly affected multimerization of recoverin regardless of their localization (except for K119A). Meanwhile, in the presence of calcium mutations in N-terminal domain of the protein significantly suppressed this process, indicating that surface properties of Ca 2+ -bound recoverin are highly affected by N-terminal cluster residues. The substitutions in C-terminal clusters generally reduced thermal stability of recoverin with F172A ('black' cluster) as well as W156A and K119A ('gray' cluster) being the most efficacious in this respect. In contrast, the mutations in the N-terminal clusters caused less pronounced differently directed changes in thermal stability of the protein. The substitutions of F172, W156, and K119 in C-terminal domain of recoverin together with substitution of Q46 in its N-terminal domain provoked significant but diverse changes in free energy associated with Ca 2+ binding to the protein: the mutant K119A demonstrated significantly improved calcium binding, whereas F172A and W156A showed decrease in the calcium affinity and Q46A exhibited no ion coordination in one of the Ca 2+ -binding sites. The most of the N-terminal clusters mutations suppressed membrane binding of recoverin and its inhibitory activity towards rhodopsin kinase (GRK1). Surprisingly, the mutant W156A aberrantly activated rhodopsin phosphorylation regardless of the presence of calcium. Taken together, these data confirm the scaffolding function of several cluster-forming residues and point to their critical role in supporting physiological activity of recoverin.

Published

2019

30. Effect of Cu 2+ and Zn 2+ ions on human serum albumin interaction with plasma unsaturated fatty acids.

Author

Nemashkalova EL, Permyakov EA, Uversky VN, Permyakov SE, and Litus EA

Subjects

Humans, Hydrophobic and Hydrophilic Interactions, Protein Binding, Zinc chemistry, Copper chemistry, Fatty Acids, Unsaturated chemistry, Ions chemistry, Serum Albumin, Human chemistry

Abstract

Human serum albumin (HSA) serves as a depot and carrier of multiple unrelated ligands including several participants of the pathogenesis of Alzheimer's disease (AD), such as amyloid β peptide (Aβ), Zn 2+ /Cu 2+ ions, docosahexaenoic (DHA), linoleic (LA), and oleic (OA) acids. To explore the interplay between HSA interaction with Zn 2+ /Cu 2+ and the plasma unsaturated fatty acids (DHA, LA, OA, and arachidonic acid (ArA)), we have studied the metal dependence of the fatty acid (FA) binding capacity of HSA (n max ) and structural consequences of the HSA-FA interactions. HSA loading with Zn 2+ decreases n max value by 0.3-1.5, while its saturation with Cu 2+ causes the FA-dependent n max changes by up to 0.9. The Cu 2+ -induced decline in n max value for DHA is due to conformational rearrangements in HSA molecule. In other cases, the changes in n max are attributed to steric hindarance/facilitation of the HSA-FA interaction because of the protein multimerization/monomerization, as confirmed by chemical crosslinking. The surface hydrophobicity of HSA is Cu 2+ -, Zn 2+ -, and FA-dependent and decreases upon the FA binding, according to bis-ANS fluorescence data. Overall, Zn 2+ or Cu 2+ binding selectively affect HSA interaction with the FAs studied, in part due to changes in quaternary structure of the protein., (Copyright © 2019. Published by Elsevier B.V.)

Published

2019

31. Analyzing the structural and functional roles of residues from the 'black' and 'gray' clusters of human S100P protein.

Author

Permyakova ME, Permyakov SE, Kazakov AS, Denesyuk AI, Denessiouk K, Uversky VN, and Permyakov EA

Subjects

Amino Acid Sequence, Amino Acids, Aromatic genetics, Binding Sites genetics, Calcium-Binding Proteins genetics, Circular Dichroism, Dynamic Light Scattering, EF Hand Motifs genetics, Humans, Hydrophobic and Hydrophilic Interactions, Mutagenesis, Site-Directed, Neoplasm Proteins genetics, Protein Binding, Protein Conformation, Protein Folding, Protein Stability, Structure-Activity Relationship, Calcium metabolism, Calcium-Binding Proteins metabolism, Models, Molecular, Neoplasm Proteins metabolism

Abstract

Two highly conserved structural motifs observed in members of the EF-hand family of calcium binding proteins. The motifs provide a supporting scaffold for the Ca2+ binding loops and contribute to the hydrophobic core of the EF-hand domain. Each structural motif represents a cluster of three amino acids called cluster I ('black' cluster) and cluster II ('grey' cluster). Cluster I is more conserved and mostly incorporates aromatic amino acids. In contrast, cluster II is noticeably less conserved and includes a mix of aromatic, hydrophobic, and polar amino acids of different sizes. In the human calcium binding S100 P protein, these 'black' and 'gray' clusters include residues F15, F71, and F74 and L33, L58, and K30, respectively. To evaluate the effects of these clusters on structure and functionality of human S100 P, we have performed Ala scanning. The resulting mutants were studied by a multiparametric approach that included circular dichroism, scanning calorimetry, dynamic light scattering, chemical crosslinking, and fluorescent probes. Spectrofluorimetric Ca2+-titration of wild type S100 P showed that S100 P dimer has 1-2 strong calcium binding sites (K 1  = 4 × 106 M -1 ) and two cooperative low affinity (K 2  = 4 × 104 M -1 ) binding sites. Similarly, the S100 P mutants possess two types of calcium binding sites. This analysis revealed that the alanine substitutions in the clusters I and II caused comparable changes in the S100 P functional properties. However, analysis of heat- or GuHCl-induced unfolding of these proteins showed that the alanine substitutions in the cluster I caused notably more pronounced decrease in the protein stability compared to the changes caused by alanine substitutions in the cluster II. Opposite to literature data, the F15 A substitution did not cause the S100 P dimer dissociation, indicating that F15 is not crucial for dimer stability. Overall, similar to parvalbumins, the S100 P cluster I is more important for protein conformational stability than the cluster II., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

32. Monomeric state of S100P protein: Experimental and molecular dynamics study.

Author

Permyakov SE, Denesyuk AI, Denessiouk KA, Permyakova ME, Kazakov AS, Ismailov RG, Rastrygina VA, Sokolov AS, and Permyakov EA

Subjects

Calcium chemistry, Calcium-Binding Proteins metabolism, Dimerization, Humans, Interleukin-11 metabolism, Molecular Dynamics Simulation, Neoplasm Proteins metabolism, Protein Binding, Protein Conformation, Protein Denaturation, Protein Stability, Structure-Activity Relationship, Surface Plasmon Resonance, Calcium metabolism, Calcium-Binding Proteins chemistry, Interleukin-11 chemistry, Neoplasm Proteins chemistry

Abstract

S100 proteins constitute a large subfamily of the EF-hand superfamily of calcium binding proteins. They possess one classical EF-hand Ca 2+ -binding domain and an atypical EF-hand domain. Most of the S100 proteins form stable symmetric homodimers. An analysis of literature data on S100 proteins showed that their physiological concentrations could be much lower than dissociation constants of their dimeric forms. It means that just monomeric forms of these proteins are important for their functioning. In the present work, thermal denaturation of apo-S100P protein monitored by intrinsic tyrosine fluorescence has been studied at various protein concentrations within the region from 0.04-10 μM. A transition from the dimeric to monomeric form results in a decrease in protein thermal stability shifting the mid-transition temperature from 85 to 75 °C. Monomeric S100P immobilized on the surface of a sensor chip of a surface plasmon resonance instrument forms calcium dependent 1 to 1 complexes with human interleukin-11 (equilibrium dissociation constant 1.2 nM). In contrast, immobilized interleukin-11 binds two molecules of dimeric S100P with dissociation constants of 32 nM and 288 nM. Since effective dissociation constant of dimeric S100P protein is very low (0.5 μM as evaluated from our data) the sensitivity of the existing physical methods does not allow carrying out a detailed study of S100P monomer properties. For this reason, we have used molecular dynamics methods to evaluate structural changes in S100P upon its transition from the dimeric to monomeric state. 80-ns molecular dynamics simulations of kinetics of formation of S100P, S100B and S100A11 monomers from the corresponding dimers have been carried out. It was found that during the transition from the homo-dimer to monomer form, the three S100 monomer structures undergo the following changes: (1) the helices in the four-helix bundles within each monomer rotate in order to shield the exposed non-polar residues; (2) almost all lost contacts at the dimer interface are substituted with equivalent and newly formed interactions inside each monomer, and new stabilizing interactions are formed; and (3) all monomers recreate functional hydrophobic cores. The results of the present study show that both dimeric and monomeric forms of S100 proteins can be functional., (Copyright © 2019. Published by Elsevier Ltd.)

Published

2019

33. The binding of monomeric amyloid β peptide to serum albumin is affected by major plasma unsaturated fatty acids.

Author

Litus EA, Kazakov AS, Sokolov AS, Nemashkalova EL, Galushko EI, Dzhus UF, Marchenkov VV, Galzitskaya OV, Permyakov EA, and Permyakov SE

Subjects

Alzheimer Disease blood, Alzheimer Disease genetics, Amyloid beta-Peptides genetics, Amyloid beta-Protein Precursor genetics, Calmodulin chemistry, Disease Progression, Humans, Ligands, Parvalbumins chemistry, Peptide Fragments genetics, Protein Binding, Recombinant Proteins chemistry, Surface Plasmon Resonance, Amyloid beta-Peptides chemistry, Amyloid beta-Protein Precursor chemistry, Fatty Acids, Unsaturated blood, Mutation, Peptide Fragments chemistry, Serum Albumin, Human chemistry

Abstract

Human serum albumin (HSA) serves as a natural depot of amyloid β peptide (Aβ). Improvement of Aβ binding to HSA should impede Alzheimer's disease (AD). We developed a method for quantitation of the interaction between monomeric Aβ40/42 and HSA using surface plasmon resonance spectroscopy. The dissociation constant of HSA complex with recombinant Aβ40/42 is 0.2-0.3 μM. Flemish variant of Aβ40 has 2.5-10-fold higher affinity to HSA. The parameters of the HSA-Aβ interaction are selectively sensitive to HSA binding of major plasma unsaturated fatty acids and Cu 2+ . Linoleic and arachidonic acids promote the HSA-Aβ42 interaction. The developed methodology for quantitation of HSA-Aβ interaction may serve as a tool for search of compounds favoring HSA-Aβ interaction, thereby preventing AD progression., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

34. Effects of his-tags on physical properties of parvalbumins.

Author

Vologzhannikova AA, Khorn PA, Kazakov AS, Permyakov EA, Uversky VN, and Permyakov SE

Subjects

Animals, Protein Conformation, alpha-Helical, Protein Conformation, beta-Strand, Rats, Histidine chemistry, Parvalbumins chemistry, Recombinant Fusion Proteins chemistry

Abstract

A comparative study of His-tagged and non-tagged rat β-parvalbumin (rWT β-PA), calcium binding protein with the EF-hand calcium binding domains, has been carried out. The attachment of His-tag increases α-helical content and decreases β-sheets and β-turns content of the metal free form (apo-state) of β-PA. In contrast to this, the attachment of His-tag decreases α-helical content by more than 10% and increases contents of β-sheets and β-turns of the Ca 2+ -loaded state. According to the dynamic light scattering analysis, apo-state of His-tagged rat β-PA seems to be less compact compared with the apo-state of non-tagged rat β-PA. Surprisingly, the attachment of His-tag practically does not change mean hydrodynamic radius of Ca 2+ -loaded rat β-PA. The attachment of His-tag shifts thermal denaturation peaks of both apo- and Ca 2+ -loaded states of rat β-PA towards higher temperatures by 3-4 °C and slightly decreases its Ca 2+ affinity. These results should be taken into consideration in the use of His-tagged parvalbumins., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2019

35. On the relationship between the conserved 'black' and 'gray' structural clusters and intrinsic disorder in parvalbumins.

Author

Deryusheva EI, Denesyuk AI, Denessiouk K, Uversky VN, Permyakov SE, and Permyakov EA

Subjects

Amino Acid Sequence, Binding Sites, EF Hand Motifs genetics, Humans, Intrinsically Disordered Proteins chemistry, Intrinsically Disordered Proteins genetics, Parvalbumins genetics, Protein Binding, Amino Acid Motifs genetics, Parvalbumins chemistry, Protein Conformation, Structural Homology, Protein

Abstract

Recently we found two highly conserved structural motifs in the members of the EF-hand protein family, which provide a supporting scaffold for their Ca 2+ binding loops. Each structural motif is formed by a cluster of three amino acids. These clusters were called 'black' cluster (cluster I) and 'gray' cluster (cluster II). In the present work, we studied the relationship between the location of the 'black' and 'gray' structural clusters in parvalbumins and the location of the amino acid sequence regions with a tendency for intrinsic disorder. This analysis revealed that in parvalbumins, the residues in the vicinity of the conserved structural clusters constitute parts of the conserved motifs enriched in the disorder-promoting residues. Therefore, the clusters found in parvalbumins are characterized not only by the presence of conserved amino acid residues, but also by the conserved distribution of the intrinsic disorder predisposition within their sequences, suggesting the presence of conserved structural dynamics in the apo-forms of parvalbumins, where the black cluster appears to have greater mobility than the gray cluster., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

36. Comprehensive analysis of the roles of 'black' and 'gray' clusters in structure and function of rat β-parvalbumin.

Author

Permyakov SE, Vologzhannikova AA, Khorn PA, Shevelyova MP, Kazakov AS, Emelyanenko VI, Denesyuk AI, Denessiouk K, Uversky VN, and Permyakov EA

Subjects

Animals, Calcium metabolism, Circular Dichroism, Horses, Hydrodynamics, Kinetics, Magnesium metabolism, Mutation genetics, Protein Structure, Secondary, Rats, Spectrometry, Fluorescence, Structure-Activity Relationship, Temperature, Parvalbumins chemistry, Parvalbumins metabolism

Abstract

Recently we found two highly conserved structural motifs in the proteins of the EF-hand calcium binding protein family. These motifs provide a supporting scaffold for the Ca 2+ binding loops and contribute to the hydrophobic core of the EF-hand domain. Each structural motif forms a cluster of three amino acids called cluster I ('black' cluster) and cluster II ('grey' cluster). Cluster I is much more conserved and mostly incorporates aromatic amino acids. In contrast, cluster II includes a mix of aromatic, hydrophobic, and polar amino acids. The 'black' and 'gray' clusters in rat β-parvalbumin consist of F48, A100, F103 and G61, L64, M87, respectively. In the present work, we sequentially substituted these amino acids residues by Ala, except Ala100, which was substituted by Val. Physical properties of the mutants were studied by circular dichroism, scanning calorimetry, dynamic light scattering, chemical crosslinking, and fluorescent probe methods. The Ca 2+ and Mg 2+ binding affinities of these mutants were evaluated by intrinsic fluorescence and equilibrium dialysis methods. In spite of a rather complicated pattern of contributions of separate amino acid residues of the 'black' and 'gray' clusters into maintenance of rat β-parvalbumin structural and functional status, the alanine substitutions in the cluster I cause noticeably more pronounced changes in various structural parameters of proteins, such as hydrodynamic radius of apo-form, thermal stability of Ca 2+ /Mg 2+ -loaded forms, and total energy of Ca 2+ binding in comparison with the changes caused by amino acid substitutions in the cluster II. These findings were further supported by the outputs of computational analysis of the effects of these mutations on the intrinsic disorder predisposition of rat β-parvalbumin, which also indicated that local intrinsic disorder propensities and the overall levels of predicted disorder were strongly affected by mutations in the cluster I, whereas mutations in cluster II had less pronounced effects. These results demonstrate that amino acids of the cluster I provide more essential contribution to the maintenance of structuraland functional properties of the protein in comparison with the residues of the cluster II., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

37. Intrinsically Disordered Regions in Serum Albumin: What Are They For?

Author

Litus EA, Permyakov SE, Uversky VN, and Permyakov EA

Subjects

Binding Sites, Fatty Acids chemistry, Fatty Acids metabolism, Humans, Metals chemistry, Metals metabolism, Pharmaceutical Preparations chemistry, Pharmaceutical Preparations metabolism, Protein Binding, Protein Domains, Protein Processing, Post-Translational, Protein Structure, Tertiary, Serum Albumin metabolism, Serum Albumin chemistry

Abstract

Serum albumin is a major plasma protein in mammalian blood. The importance of this protein lies in its roles in both bioregulation and transport phenomena. Serum albumin binds various metal ions and participates in the transport and storage of fatty acids, bilirubin, steroids amino acids, and many other ligands, usually with regions of hydrophobic surface. Although the primary role of serum albumin is to transport various ligand, its versatile binding capacities and high concentration mean that it can assume a number of additional functions. The major goal of this article is to show how intrinsic disorder is encoded in the amino acid sequence of serum albumin, and how intrinsic disorder is related to functions of this important serum protein.

Published

2018

38. The Use of Human, Bovine, and Camel Milk Albumins in Anticancer Complexes with Oleic Acid.

Author

El-Fakharany EM, Abu-Serie MM, Litus EA, Permyakov SE, Permyakov EA, Uversky VN, and Redwan EM

Subjects

Animals, Antineoplastic Agents pharmacology, Apoptosis drug effects, Camelus, Cattle, Cell Line, Tumor, Cell Survival drug effects, Humans, Oleic Acid pharmacology, Albumins chemistry, Antineoplastic Agents chemistry, Milk chemistry, Milk Proteins chemistry, Oleic Acid chemistry

Abstract

Oleic acid (OA) is a monounsaturated fatty acid that upon binding to milk proteins, such as α-lactalbumin and lactoferrin, forms potent complexes, which exert selective anti-tumor activity against malignant cells but are nontoxic for healthy normal cells. We showed that the interaction of OA with albumins isolated from human, bovine, and camel milk results in the formation of complexes with high antitumor activity against Caco-2, HepG-2, PC-3, and MCF-7 tumor cells. The antitumor effect of the complexes is mostly due to the action of oleic acid, similar to the case of OA complexes with other proteins. Viability of tumor cells is inhibited by the albumin-OA complexes in a dose dependent manner, as evaluated by the MTT assay. Strong induction of apoptosis in tumor cells after their treatment with the complexes was monitored by flow cytometry, cell cycle analysis, nuclear staining, and DNA fragmentation methods. The complex of camel albumin with OA displayed the most pronounced anti-tumor effects in comparison with the complexes of OA with human and bovine albumins. Therefore, these results suggest that albumins have the potential to be used as efficient and low cost means of tumor treatment.

Published

2018

39. Calcium-dependent interaction of monomeric S100P protein with serum albumin.

Author

Kazakov AS, Shevelyova MP, Ismailov RG, Permyakova ME, Litus EA, Permyakov EA, and Permyakov SE

Subjects

Humans, Protein Binding, Protein Multimerization, Protein Structure, Quaternary, Calcium metabolism, Calcium-Binding Proteins chemistry, Calcium-Binding Proteins metabolism, Neoplasm Proteins chemistry, Neoplasm Proteins metabolism, Serum Albumin, Human metabolism

Abstract

S100 proteins are multifunctional (intra/extra)cellular mostly dimeric calcium-binding proteins engaged into numerous diseases. We have found that monomeric recombinant human S100P protein interacts with intact human serum albumin (HSA) in excess of calcium ions with equilibrium dissociation constant of 25-50nM, as evidenced by surface plasmon resonance spectroscopy and fluorescent titration by HSA of S100P labelled by fluorescein isothiocyanate. Calcium removal or S100P dimerization abolish the S100P-HSA interaction. The interaction is selective, since S100P does not bind bovine serum albumin and monomeric human S100B lacks interaction with HSA. In vitro glycation of HSA disables its binding to S100P. The revealed selective and highly specific conformation-dependent interaction between S100P and HSA shows that functional properties of monomeric and dimeric forms of S100 proteins are different, and raises concerns on validity of cell-based assays and animal models used for studies of (patho)physiological roles of extracellular S100 proteins., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

40. Building kit for metal cation binding sites in proteins.

Author

Denesyuk AI, Permyakov SE, Johnson MS, Permyakov EA, and Denessiouk K

Subjects

Animals, Cations, Divalent, EF Hand Motifs, Humans, Nitrogen chemistry, Oxygen chemistry, Protein Binding, Thermodynamics, Calcium chemistry, Calcium-Binding Proteins chemistry, Integrins chemistry, Parvalbumins chemistry

Abstract

Starting with conformations of calcium-binding sites in parvalbumin and integrin (representative structures of EF-hand and calcium blade zones, respectively) we introduce four new different local Ca 2+ -recognition units in proteins: a one-residue unit type I (ORI); a three-residue unit type I (TRI); a one-residue unit type II (ORII) and a three-residue unit type II (TRII). Based on the amount and nature of variable atoms, the type I and II units theoretically can have four and twelve variants, respectively. Analysis of known "Ca 2+ -bound functional niches" in proteins revealed presence of almost all possible variants of Ca 2+ -recognition units in actual structures. Parvalbumin, integrin alpha-IIb and sixteen other proteins with different Ca 2+ -bound functional niches contain various consecutively joined combinations of OR(I/II) and TR(I/II) units. Such a OR(I/II)+TR(I/II) joint unit forms a tripeptide, which uses three main-chain atoms for metal binding: nitrogen n (Donor), oxygen n (Acceptor) and nitrogen n+2 (Donor). Thus, taken together, the described ORI, TRI, ORII and TRII units can serve as elementary blocks to construct more complex calcium recognizing substructures in a variety of calcium binding sites of unrelated proteins., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

41. In search for globally disordered apo-parvalbumins: Case of parvalbumin β-1 from coho salmon.

Author

Vologzhannikova AA, Khorn PA, Kazakov AS, Ismailov RG, Sokolov AS, Uversky VN, Permyakov EA, and Permyakov SE

Subjects

Animals, Apoproteins genetics, Apoproteins metabolism, Calcium metabolism, Calcium-Binding Proteins genetics, Calcium-Binding Proteins metabolism, Cloning, Molecular, Escherichia coli genetics, Escherichia coli metabolism, Fish Proteins genetics, Fish Proteins metabolism, Gene Expression, Genetic Vectors chemistry, Genetic Vectors metabolism, Intrinsically Disordered Proteins genetics, Intrinsically Disordered Proteins metabolism, Parvalbumins genetics, Parvalbumins metabolism, Protein Conformation, alpha-Helical, Protein Conformation, beta-Strand, Protein Folding, Protein Stability, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Thermodynamics, Apoproteins chemistry, Calcium chemistry, Calcium-Binding Proteins chemistry, Fish Proteins chemistry, Intrinsically Disordered Proteins chemistry, Oncorhynchus kisutch metabolism, Parvalbumins chemistry

Abstract

Parvalbumin (PA) is a classical EF-hand calcium-binding protein of muscle, neuronal, and other tissues, and a major fish allergen. Although certain apo-PAs lack tertiary structure, functional implications of that feature and its structural prerequisites remain unclear. In a search for unstable PAs, we probed conformational stability of parvalbumin β-1 from coho salmon (csPA), a cold water fish species, using circular dichroism, scanning calorimetry, hydrophobic probe fluorescence, limited proteolysis, chemical crosslinking and dynamic light scattering techniques. Apo-csPA is shown to be mainly monomeric protein with markedly disorganized secondary structure and lack of rigid tertiary structure. Examination of per-residue propensity for intrinsic disorder in the PA groups with either folded or unfolded apo-form using the average PONDR ® VSL2P profiles revealed that the N-terminal region that includes α-helix A, AB-loop and N-terminal half of α-helix B is predicted to be less ordered in PAs with disordered apo-state. Application of the structural criteria developed for discrimination of disordered PAs indicate that the latter comprise about 16-19% of all PAs. We show that structural instability of apo-β-PA serves as a hallmark of elevated calcium affinity of the protein. Therefore, the successful predictions of unstable apo-PAs might facilitate search for PAs with maximal calcium affinity and possibly serving as calcium sensors., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

42. Modulation of linoleic acid-binding properties of human serum albumin by divalent metal cations.

Author

Nemashkalova EL, Permyakov EA, Permyakov SE, and Litus EA

Subjects

Binding Sites drug effects, Calcium chemistry, Cations, Divalent chemistry, Copper chemistry, Humans, Hydrophobic and Hydrophilic Interactions, Magnesium chemistry, Protein Binding drug effects, Surface Properties, Zinc chemistry, Cations, Divalent pharmacology, Linoleic Acid chemistry, Serum Albumin chemistry

Abstract

Human serum albumin (HSA) is an abundant multiligand carrier protein, linked to progression of Alzheimer's disease (AD). Blood HSA serves as a depot of amyloid β (Aβ) peptide. Aβ peptide-buffering properties of HSA depend on interaction with its ligands. Some of the ligands, namely, linoleic acid (LA), zinc and copper ions are involved into AD progression. To clarify the interplay between LA and metal ion binding to HSA, the dependence of LA binding to HSA on Zn 2+ , Cu 2+ , Mg 2+ and Ca 2+ levels and structural consequences of these interactions have been explored. Seven LA molecules are bound per HSA molecule in the absence of the metal ions. Zn 2+ binding to HSA causes a loss of one bound LA molecule, while the other metals studied exert an opposite effect (1-2 extra LA molecules are bound). In most cases, the observed effects are not related to the metal-induced changes in HSA quaternary structure. However, the Zn 2+ -induced decline in LA capacity of HSA could be due to accumulation of multimeric HSA forms. Opposite to Ca 2+ /Mg 2+ -binding, Zn 2+ or Cu 2+ association with HSA induces marked changes in its hydrophobic surface. Overall, the divalent metal ions modulate LA capacity and affinity of HSA to a different extent. LA- and Ca 2+ -binding to HSA synergistically support each other. Zn 2+ and Cu 2+ induce more pronounced changes in hydrophobic surface and quaternary structure of HSA and its LA capacity. A misbalanced metabolism of these ions in AD could modify interactions of HSA with LA, other fatty acids and hydrophobic substances, associated with AD.

Published

2017

43. Novel calcium recognition constructions in proteins: Calcium blade and EF-hand zone.

Author

Denesyuk AI, Permyakov SE, Johnson MS, Permyakov EA, and Denessiouk K

Subjects

Amino Acid Motifs, Amino Acid Sequence, Binding Sites, Calcium-Binding Proteins genetics, EF Hand Motifs, Humans, Models, Molecular, Mutagenesis, Insertional, Protein Binding, Sequence Homology, Amino Acid, Calcium metabolism, Calcium-Binding Proteins chemistry, Calcium-Binding Proteins metabolism

Abstract

Metal ions can regulate various cell processes being first, second or third messengers, and some of them, especially transition metal ions, take part in catalysis in many enzymes. As an intracellular ion, Ca 2+ is involved in many cellular functions from fertilization and contraction, cell differentiation and proliferation, to apoptosis and cancer. Here, we have identified and described two novel calcium recognition environments in proteins: the calcium blade zone and the EF-hand zone, common to 12 and 8 different protein families, respectively. Each of the two environments contains three distinct structural elements: (a) the well-known characteristic Dx[DN]xDG motif; (b) an adjacent structurally identical segment, which binds metal ion in the same way between the calcium blade zone and the EF-hand zone; and (c) the following structurally variable segment, which distinguishes the calcium blade zone from the EF-hand zone. Both zones have sequence insertions between the last residue of the zone and calcium-binding residues in positions V or VI. The long insertion often connects the active and the calcium-binding sites in proteins. Using the structurally identical segments as an anchor, we were able to construct the classical calmodulin type EF-hand calcium-binding site out of two different calcium-binding motifs from two unrelated proteins., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

44. Derivative of Extremophilic 50S Ribosomal Protein L35Ae as an Alternative Protein Scaffold.

Author

Lomonosova AV, Ulitin AB, Kazakov AS, Mirzabekov TA, Permyakov EA, and Permyakov SE

Subjects

Amino Acid Sequence, Animals, Archaeal Proteins genetics, Archaeal Proteins metabolism, Biomimetic Materials chemistry, Biomimetic Materials metabolism, Biotechnology, Carrier Proteins chemistry, Carrier Proteins genetics, Carrier Proteins metabolism, Cattle, Chickens, Extremophiles chemistry, Extremophiles genetics, Lactalbumin metabolism, Models, Molecular, Muramidase metabolism, Peptide Library, Protein Engineering, Protein Structure, Tertiary, Pyrococcus horikoshii genetics, Ribosomal Proteins genetics, Ribosomal Proteins metabolism, Archaeal Proteins chemistry, Pyrococcus horikoshii chemistry, Ribosomal Proteins chemistry

Abstract

Small antibody mimetics, or alternative binding proteins (ABPs), extend and complement antibody functionality with numerous applications in research, diagnostics and therapeutics. Given the superiority of ABPs, the last two decades have witnessed development of dozens of alternative protein scaffolds (APSs) for the design of ABPs. Proteins from extremophiles with their high structural stability are especially favorable for APS design. Here, a 10X mutant of the 50S ribosomal protein L35Ae from hyperthermophilic archaea Pyrococcus horikoshii has been probed as an APS. A phage display library of L35Ae 10X was generated by randomization of its three CDR-like loop regions (repertoire size of 2×108). Two L35Ae 10X variants specific to a model target, the hen egg-white lysozyme (HEL), were isolated from the resulting library using phage display. The affinity of these variants (L4 and L7) to HEL ranges from 0.10 μM to 1.6 μM, according to surface plasmon resonance data. While L4 has 1-2 orders of magnitude lower affinity to HEL homologue, bovine α-lactalbumin (BLA), L7 is equally specific to HEL and BLA. The reference L35Ae 10X is non-specific to both HEL and BLA. L4 and L7 are more resistant to denaturation by guanidine hydrochloride compared to the reference L35Ae 10X (mid-transition concentration is higher by 0.1-0.5 M). Chemical crosslinking experiments reveal an increased propensity of L4 and L7 to multimerization. Overall, the CDR-like loop regions of L35Ae 10X represent a proper interface for generation of functional ABPs. Hence, L35Ae is shown to extend the growing family of protein scaffolds dedicated to the design of novel binding proteins., Competing Interests: Antherix and Biomirex Inc. provided support in the form of salary for author TAM. This does not alter the authors' adherence to PLOS ONE policies on sharing data and materials.

Published

2017

45. Parvalbumin as a Pleomorphic Protein.

Author

Permyakov EA, Uversky VN, and Permyakov SE

Subjects

Animals, Binding Sites, Calcium metabolism, Carps, Humans, Intrinsically Disordered Proteins, Ion Transport, Magnesium metabolism, Models, Molecular, Parvalbumins genetics, Parvalbumins metabolism, Protein Binding, Protein Conformation, alpha-Helical, Protein Conformation, beta-Strand, Protein Folding, Protein Interaction Domains and Motifs, Protein Isoforms chemistry, Protein Isoforms genetics, Protein Isoforms metabolism, Protein Structure, Tertiary, Calcium chemistry, Magnesium chemistry, Parvalbumins chemistry

Abstract

Parvalbumin (PA) is a classical small, mostly cytosolic Ca2+-binding protein of the EF-hand superfamily expressed in vertebrates in a tissue- and cell-specific manner, serving as a magnesium/ calcium buffer. In the last decade novel data were published on structural peculiarities of PA, likely affecting its functionality. This review sums up these findings and discusses their potential physiological significance., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.)

Published

2017

46. Interleukin-11 binds specific EF-hand proteins via their conserved structural motifs.

Author

Kazakov AS, Sokolov AS, Vologzhannikova AA, Permyakova ME, Khorn PA, Ismailov RG, Denessiouk KA, Denesyuk AI, Rastrygina VA, Baksheeva VE, Zernii EY, Zinchenko DV, Glazatov VV, Uversky VN, Mirzabekov TA, Permyakov EA, and Permyakov SE

Subjects

Animals, Calcium-Binding Proteins chemistry, Calcium-Binding Proteins metabolism, Humans, Interleukin-11 metabolism, Metals chemistry, Neoplasm Proteins chemistry, Neoplasm Proteins metabolism, Protein Binding, Protein Domains, Carrier Proteins chemistry, Conserved Sequence, EF Hand Motifs, Interleukin-11 chemistry, Models, Molecular, Protein Interaction Domains and Motifs

Abstract

Interleukin-11 (IL-11) is a hematopoietic cytokine engaged in numerous biological processes and validated as a target for treatment of various cancers. IL-11 contains intrinsically disordered regions that might recognize multiple targets. Recently we found that aside from IL-11RA and gp130 receptors, IL-11 interacts with calcium sensor protein S100P. Strict calcium dependence of this interaction suggests a possibility of IL-11 interaction with other calcium sensor proteins. Here we probed specificity of IL-11 to calcium-binding proteins of various types: calcium sensors of the EF-hand family (calmodulin, S100B and neuronal calcium sensors: recoverin, NCS-1, GCAP-1, GCAP-2), calcium buffers of the EF-hand family (S100G, oncomodulin), and a non-EF-hand calcium buffer (α-lactalbumin). A specific subset of the calcium sensor proteins (calmodulin, S100B, NCS-1, GCAP-1/2) exhibits metal-dependent binding of IL-11 with dissociation constants of 1-19 μM. These proteins share several amino acid residues belonging to conservative structural motifs of the EF-hand proteins, 'black' and 'gray' clusters. Replacements of the respective S100P residues by alanine drastically decrease its affinity to IL-11, suggesting their involvement into the association process. Secondary structure and accessibility of the hinge region of the EF-hand proteins studied are predicted to control specificity and selectivity of their binding to IL-11. The IL-11 interaction with the EF-hand proteins is expected to occur under numerous pathological conditions, accompanied by disintegration of plasma membrane and efflux of cellular components into the extracellular milieu.

Published

2017

47. Expression, Purification, and Characterization of Interleukin-11 Orthologues.

Author

Sokolov AS, Kazakov AS, Solovyev VV, Ismailov RG, Uversky VN, Lapteva YS, Mikhailov RV, Pavlova EV, Terletskaya IO, Ermolina LV, Permyakov SE, and Permyakov EA

Subjects

Animals, Cell Line, Cloning, Molecular, Enzyme Activation, Escherichia coli genetics, Escherichia coli metabolism, HEK293 Cells, Humans, Interleukin-11 analysis, Interleukin-11 genetics, Interleukin-6 metabolism, Macaca fascicularis, Mice, Recombinant Proteins chemical synthesis, Recombinant Proteins genetics, Species Specificity, Interleukin-11 metabolism, Receptors, Interleukin-11 metabolism, STAT3 Transcription Factor metabolism, Signal Transduction physiology

Abstract

Interleukin-11 (IL-11) is a multifunctional cytokine implicated in several normal and pathological processes. The decoding of IL-11 function and development of IL-11-targeted drugs dictate the use of laboratory animals and need of the better understanding of species specificity of IL-11 signaling. Here, we present a method for the recombinant interleukin-11 (rIL-11) production from the important model animals, mouse and macaque. The purified mouse and macaque rIL-11 interact with extracellular domain of human IL-11 receptor subunit α and activate STAT3 signaling in HEK293 cells co-expressing human IL-11 receptors with efficacies resembling those of human rIL-11. Hence, the evolutionary divergence does not impair IL-11 signaling. Furthermore, compared to human rIL-11 its macaque orthologue is 8-fold more effective STAT3 activator, which favors its use for treatment of thrombocytopenia as a potent substitute for human rIL-11. Compared to IL-6, IL-11 signaling exhibits lower species specificity, likely due to less conserved intrinsic disorder propensity within IL-6 orthologues. The developed express method for preparation of functionally active macaque/mouse rIL-11 samples is suited for exploration of the molecular mechanisms underlying IL-11 action and for development of the drug candidates for therapy of oncologic/hematologic/inflammatory diseases related to IL-11 signaling.

Published

2016

48. Interleukin-11: A Multifunctional Cytokine with Intrinsically Disordered Regions.

Author

Permyakov EA, Uversky VN, and Permyakov SE

Subjects

Binding Sites, Calcium-Binding Proteins chemistry, Calcium-Binding Proteins metabolism, Cytokine Receptor gp130 chemistry, Cytokine Receptor gp130 metabolism, Humans, Interleukin-11 metabolism, Protein Binding, Protein Structure, Tertiary, Interleukin-11 chemistry

Abstract

Cytokine interleukin-11 (IL-11) is a multifunctional protein with diverse roles in the normal cell signaling and in various pathologies. The structure of IL-11 is characterized by a four-helix bundle motif comprising two pairs of antiparallel α-helices arranged in an up-up-down-down configuration. Evaluation of the intrinsic disorder predisposition of human IL-11 by several computational tools clearly shows that this protein is predicted to have functional disordered regions potentially involved in interaction with natural binding partners. Signaling by IL-11 proceeds via an interaction of the protein with its membrane-specific receptor IL-11Rα and a subsequent interaction of the complex with the transmembrane signal-transducing receptor GP130. Cytoplasmic domain of IL-11Rα is predicted to be very disordered, and noticeable amount of disorder is present even in the large extracellular domain of the protein. GP130 is also predicted to have long disordered region that is located at the C-terminal of the protein and is expected to have several disorder-based binding sites. It shows that intrinsic disorder might play an important role in functioning of this signaling machine. A specific subset of the calcium sensor proteins (calmodulin, S100P, S100B, NCS-1, GCAP-1/2) exhibits metal-dependent binding of IL-11 with dissociation constants in a range of 1-19 μM, and the structural features of their hinge regions likely ensure selectivity and calcium sensitivity of IL-11 binding to the EF-hand proteins studied. IL-11 exhibits multiple effects on hematopoietic and non-hematopoietic systems. It plays a major role in orchestrating complex processes of tumor development and progression.

Published

2016

49. Disorder in Milk Proteins: α-Lactalbumin. Part B. A Multifunctional Whey Protein Acting as an Oligomeric Molten Globular "Oil Container" in the Anti-Tumorigenic Drugs, Liprotides.

Author

Uversky VN, Permyakov SE, Breydo L, Redwan EM, Almehdar HA, and Permyakov EA

Subjects

Amino Acids chemistry, Animals, Anti-Bacterial Agents chemistry, Anti-Bacterial Agents pharmacology, Antineoplastic Agents pharmacology, Antiviral Agents chemistry, Antiviral Agents pharmacology, Carrier Proteins metabolism, Humans, Lactalbumin pharmacology, Lactose biosynthesis, Milk Proteins pharmacology, Models, Molecular, Protein Binding, Protein Conformation, Protein Multimerization drug effects, Structure-Activity Relationship, Disease Susceptibility, Lactalbumin chemistry, Lactalbumin metabolism, Milk Proteins chemistry, Milk Proteins metabolism

Abstract

This is a second part of the three-part article from a series of reviews on the abundance and roles of intrinsic disorder in milk proteins. We continue to describe α-lactalbumin, a small globular Ca2+-binding protein, which besides being one of the two components of lactose synthase that catalyzes the final step of the lactose biosynthesis in the lactating mammary gland, possesses a multitude of other functions. In fact, recent studies indicated that some partially folded forms of this protein possess noticeable bactericidal activity and other forms might be related to induction of the apoptosis of tumor cells. In its anti-tumorigenic function, oligomeric α-lactalbumin serves as a founding member of a new family of anticancer drugs termed liprotides (for lipids and partially denatured proteins), where an oligomeric molten globular protein acts as an "oil container" or cargo for the delivery of oleic acid to the cell membranes.

Published

2016

50. Disorder in Milk Proteins: α-Lactalbumin. Part C. Peculiarities of Metal Binding.

Author

Permyakov EA, Permyakov SE, Breydo L, Redwan EM, Almehdar HA, and Uversky VN

Subjects

Animals, Binding Sites, Calcium metabolism, Humans, Lactalbumin metabolism, Metals metabolism, Models, Molecular, Protein Binding, Thermodynamics, Calcium chemistry, Lactalbumin chemistry, Metals chemistry, Protein Conformation

Abstract

This is a concluding part of the three-part article from a series of reviews on the abundance and roles of intrinsic disorder in milk proteins. In this paper, we describe the peculiarities of metal binding to a multifunctional milk protein, α-lactalbumin, which has two domains, a large α-helical domain and a small β-sheet domain connected by a calcium binding loop. It is known that in addition to four disulfide bonds, the native fold of this protein is stabilized by binding of a calcium ion. In fact, although in various mammals, α-lactalbumins are rather poorly conserved possessing the overall sequence identity of ~16%, the positions of all eight cysteines and a calcium binding site (residues DKFLDDDITDDI in human protein) are strongly conserved. Curiously, this conserved calcium binding loop is located within a region with increased structural flexibility. Besides canonical calcium binding, α-lactalbumin is known to interact with other metals, such as zinc (for which it has a specific binding site), and, in its apo-form, it can bind other divalent and monovalent cations. The binding of Mg2+, Na+, and K+ to the Ca2+ site increases α-lactalbumin stability against action of heat and various denaturing agents, with the higher stabilization effects being imposed by the stronger bound metal ions.

Published

2016