Your search keyword '"Ciarkowski J"' showing total 6 results

1. Structural insights into the activation mechanisms of human HtrA serine proteases.

Author

Zurawa-Janicka D, Wenta T, Jarzab M, Skorko-Glonek J, Glaza P, Gieldon A, Ciarkowski J, and Lipinska B

Subjects

Binding Sites, Enzyme Activation, Humans, PDZ Domains physiology, Protein Binding, Protein Conformation, Serine Endopeptidases ultrastructure, Structure-Activity Relationship, Apoptosis physiology, Mitochondria physiology, Serine Endopeptidases chemistry, Serine Endopeptidases metabolism, Signal Transduction physiology

Abstract

Human HtrA1-4 proteins belong to the HtrA family of evolutionarily conserved serine proteases and function as important modulators of many physiological processes, including maintenance of mitochondrial homeostasis, cell signaling and apoptosis. Disturbances in their action are linked to severe diseases, including oncogenesis and neurodegeneration. The HtrA1-4 proteins share structural and functional features of other members of the HtrA protein family, however there are several significant differences in structural architecture and mechanisms of action which makes each of them unique. Our goal is to present recent studies regarding human HtrAs. We focus on their physiological functions, structure and regulation, and describe current models of activation mechanisms. Knowledge of molecular basis of the human HtrAs' action is a subject of great interest; it is crucial for understanding their relevance in cellular physiology and pathogenesis as well as for using them as targets in future therapies of diseases such as neurodegenerative disorders and cancer., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

2. Distinct 3D Architecture and Dynamics of the Human HtrA2(Omi) Protease and Its Mutated Variants.

Author

Gieldon A, Zurawa-Janicka D, Jarzab M, Wenta T, Golik P, Dubin G, Lipinska B, and Ciarkowski J

Subjects

Crystallography, X-Ray, High-Temperature Requirement A Serine Peptidase 2, Humans, Mitochondrial Proteins genetics, Molecular Dynamics Simulation, Mutation genetics, Protein Structure, Secondary, Protein Structure, Tertiary, Serine Endopeptidases genetics, Structure-Activity Relationship, Mitochondrial Proteins chemistry, Mitochondrial Proteins metabolism, Serine Endopeptidases chemistry, Serine Endopeptidases metabolism

Abstract

HtrA2(Omi) protease controls protein quality in mitochondria and plays a major role in apoptosis. Its HtrA2S306A mutant (with the catalytic serine routinely disabled for an X-ray study to avoid self-degradation) is a homotrimer whose subunits contain the serine protease domain (PD) and the regulatory PDZ domain. In the inactive state, a tight interdomain interface limits penetration of both PDZ-activating ligands and PD substrates into their respective target sites. We successfully crystalized HtrA2V226K/S306A, whose active counterpart HtrA2V226K has had higher proteolytic activity, suggesting higher propensity to opening the PD-PDZ interface than that of the wild type HtrA2. Yet, the crystal structure revealed the HtrA2V226K/S306A architecture typical of the inactive protein. To get a consistent interpretation of crystallographic data in the light of kinetic results, we employed molecular dynamics (MD). V325D inactivating mutant was used as a reference. Our simulations demonstrated that upon binding of a specific peptide ligand NH2-GWTMFWV-COOH, the PDZ domains open more dynamically in the wild type protease compared to the V226K mutant, whereas the movement is not observed in the V325D mutant. The movement relies on a PDZ vs. PD rotation which opens the PD-PDZ interface in a lid-like (budding flower-like in trimer) fashion. The noncovalent hinges A and B are provided by two clusters of interfacing residues, harboring V325D and V226K in the C- and N-terminal PD barrels, respectively. The opening of the subunit interfaces progresses in a sequential manner during the 50 ns MD simulation. In the systems without the ligand only minor PDZ shifts relative to PD are observed, but the interface does not open. Further activation-associated events, e.g. PDZ-L3 positional swap seen in any active HtrA protein (vs. HtrA2), were not observed. In summary, this study provides hints on the mechanism of activation of wtHtrA2, the dynamics of the inactive HtrA2V325D, but does not allow to explain an increased activity of HtrA2V226K., Competing Interests: The authors have declared that no competing interests exist.

Published

2016

3. Potent antidiuretic agonists, deamino-vasopressin and desmopressin, and their inverso analogs: NMR structure and interactions with micellar and liposomic models of cell membrane.

Author

Lubecka EA, Sikorska E, Sobolewski D, Prahl A, Slaninová J, and Ciarkowski J

Subjects

1,2-Dipalmitoylphosphatidylcholine chemistry, Animals, Antidiuretic Agents pharmacology, Cyclization, Deamino Arginine Vasopressin pharmacology, Female, Fluorenes chemistry, Hydrogen Bonding, Micelles, Molecular Dynamics Simulation, Nuclear Magnetic Resonance, Biomolecular, Oxytocics pharmacology, Phosphatidylglycerols chemistry, Protein Structure, Secondary, Rats, Wistar, Solid-Phase Synthesis Techniques methods, Uterus drug effects, Uterus physiology, Antidiuretic Agents chemical synthesis, Deamino Arginine Vasopressin chemical synthesis, Liposomes chemistry, Oxytocics chemical synthesis

Abstract

Deamination of vasopressin (AVP) enhances its antidiuretic activity. Moreover, introduction of D-Arg8 instead of its L enantiomer in deamino-vasopressin (dAVP) results in an extremely potent and selective antidiuretic agonist - desmopressin (dDAVP). In this study we describe the synthesis, pharmacological properties and structures of these two potent antidiuretic agonists, and their inverso analogs. The structures of the peptides are studied in micellar and liposomic models of cell membrane using CD spectroscopy. Additionally, three-dimensional structures in mixed anionic-zwitterionic micelles are obtained using NMR spectroscopy supported by molecular dynamics simulations. Our conformational studies have shown that desmopressin in a membrane mimicking environment adopts one of the characteristic for vasopressin-like peptides β-turn - in position 3,4. Furthermore, dDAVP shows the tendency to create a β-turn in the Cys6-Gly9 C-tail, considered to be important for the antidiuretic activity, and also some tendency to adopt a 5,6 β-turn. In desmopressin, in contrast to the native vasopressin, deamino-vasopressin and [D-Arg8]-vasopressin (DAVP), the Arg8 side chain, crucial for the pressor and antidiuretic activities, is very well exposed for interaction with the receptor, whereas Gly9, crucial for the pressor and uterotonic activities, is situated together with the C-terminal amide group very close to the tocin ring. The arrangements of the Gln4 and Asn5 side chains, being crucial for OT activity, also differ in desmopressin as compared to those of AVP, dAVP and DAVP. These differences in arrangement of the important for activities side chains are likely to explain extremely potent and selective antidiuretic activities of desmopressin. © 2016 Wiley Periodicals, Inc. Biopolymers (Pept Sci) 106: 245-259, 2016., (© 2016 Wiley Periodicals, Inc.)

Published

2016

4. Intra- and intersubunit changes accompanying thermal activation of the HtrA2(Omi) protease homotrimer.

Author

Jarzab M, Wenta T, Zurawa-Janicka D, Polit A, Gieldon AJ, Wysocka M, Glaza P, Skorko-Glonek J, Ciarkowski J, Lesner A, and Lipinska B

Subjects

Binding Sites, Catalytic Domain, High-Temperature Requirement A Serine Peptidase 2, Humans, Mitochondria metabolism, Mitochondrial Proteins genetics, Mitochondrial Proteins metabolism, PDZ Domains, Protein Binding, Protein Structure, Secondary, Serine Endopeptidases genetics, Serine Endopeptidases metabolism, Tryptophan chemistry, Allosteric Regulation, Mitochondria chemistry, Mitochondrial Proteins chemistry, Peptides chemistry, Serine Endopeptidases chemistry

Abstract

HtrA2(Omi) protease is involved in the maintenance of mitochondrial homeostasis and stimulation of apoptosis as well as in development of cancer and neurodegenerative disorders. The protein is a homotrimer whose subunits comprise serine protease domain (PD) and PDZ regulatory domain. In the basal, inactive state, a tight interdomain interface limits access both to the PDZ peptide (carboxylate) binding site and to the PD catalytic center. The molecular mechanism of activation is not well understood. To further the knowledge of HtrA2 thermal activation we monitored the dynamics of the PDZ-PD interactions during temperature increase using tryptophan-induced quenching (TrIQ) method. The TrIQ results suggested that during activation the PDZ domain changed its position versus PD inside a subunit, including a prominent change affecting the L3 regulatory loop of PD, and also changed its interactions with the PD of the adjacent subunit (PD*), specifically with its L1* regulatory loop containing the active site serine. The α5 helix of PDZ was involved in both, the intra- and intersubunit changes of interactions and thus seems to play an important role in HtrA2 activation. The amino acid substitutions designed to decrease the PDZ interactions with the PD or PD* promoted protease activity at a wide range of temperatures, which supports the conclusions based on the TrIQ analysis. The model presented in this work describes PDZ movement in relation to PD and PD*, resulting in an increased access to the peptide binding and active sites, and conformational changes of the L3 and L1* loops., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2016

5. Arginine-, D-arginine-vasopressin, and their inverso analogues in micellar and liposomic models of cell membrane: CD, NMR, and molecular dynamics studies.

Author

Lubecka EA, Sikorska E, Sobolewski D, Prahl A, Slaninová J, and Ciarkowski J

Subjects

Amino Acid Sequence, Animals, Antidiuretic Agents chemical synthesis, Antidiuretic Agents pharmacology, Arginine Vasopressin chemical synthesis, Arginine Vasopressin chemistry, Arginine Vasopressin pharmacology, Cell Membrane drug effects, Molecular Sequence Data, Peptides chemistry, Protein Binding, Protein Structure, Tertiary, Rats, Rats, Wistar, Antidiuretic Agents chemistry, Arginine Vasopressin analogs & derivatives, Cell Membrane chemistry, Liposomes chemistry, Micelles, Molecular Dynamics Simulation

Abstract

We describe the synthesis, pharmacological properties, and structures of antidiuretic agonists, arginine vasopressin (AVP) and [D-Arg(8)]-vasopressin (DAVP), and their inverso analogues. The structures of the peptides are studied based on micellar and liposomic models of cell membranes using CD spectroscopy. Additionally, three-dimensional structures in mixed anionic-zwitterionic micelles are obtained using NMR spectroscopy and molecular dynamics simulations. NMR data have shown that AVP and DAVP tend to adopt typical of vasopressin-like peptides β-turns: in the 2-5 and 3-6 fragments. The inverso-analogues also adopt β-turns in the 3-6 fragments. For this reason, their inactivity seems to be due to the difference in side chains orientations of Tyr(2), Phe(3), and Arg(8), important for interactions with the receptors. Again, the potent antidiuretic activity of DAVP can be explained by CD data suggesting differences in mutual arrangement of the aromatic side chains of Tyr(2) and Phe(3) in this peptide in liposomes rather than of native AVP. In the presence of liposomes, the smallest conformational changes of the peptides are noticed with DPPC and the largest with DPPG liposomes. This suggests that electrostatic interactions are crucial for the peptide-membrane interactions. We obtained similar, probably active, conformations of the antidiuretic agonists in the mixed DPC/SDS micelles (5:1) and in the mixed DPPC/DPPG (7:3) liposomes. Thus it can be speculated that the anionic-zwitterionic liposomes as well as the anionic-zwitterionic micelles, mimicking the eukaryotic cell membrane environment, partially restrict conformational freedom of the peptides and probably induce conformations resembling those of biologically relevant ones.

Published

2015

6. Structural studies of the C-terminal 19-peptide of serum amyloid A and its Pro → Ala variants interacting with human cystatin C.

Author

Maszota M, Karska N, Spodzieja M, Ciarkowski J, Kołodziejczyk AS, Rodziewicz-Motowidło S, and Czaplewska P

Subjects

Alanine chemistry, Calorimetry, Differential Scanning, Chromatography, Affinity, Circular Dichroism, Cystatin C metabolism, Humans, Peptides metabolism, Proline chemistry, Protein Conformation, Protein Isoforms chemistry, Protein Isoforms metabolism, Protein Structure, Tertiary, Serum Amyloid A Protein metabolism, Cystatin C chemistry, Peptides chemistry, Serum Amyloid A Protein chemistry

Abstract

Serum amyloid A (SAA) is a multifunctional acute-phase protein whose concentration in serum increases markedly following a number of chronic inflammatory and neoplastic diseases. Prolonged high SAA level may give rise to reactive systemic amyloid A (AA) amyloidosis, where the N-terminal segment of SAA is deposited as amyloid fibrils. Besides, recently, well-documented association of SAA with high-density lipoprotein or glycosaminoglycans, in particular heparin/heparin sulfate (HS), and specific interaction between SAA and human cystatin C (hCC), the ubiquitous inhibitor of cysteine proteases, was proved. Using a combination of selective proteolytic excision and high-resolution mass spectrometry, a hCC binding site in the SAA sequence was determined as SAA(86-104). The role of this SAA C-terminal fragment as a ligand-binding locus is still not clear. It was postulated important in native SAA folding and in pathogenesis of AA amyloidosis. In the search of conformational details of this SAA fragment, we did its structure and affinity studies, including its selected double/triple Pro → Ala variants. Our results clearly show that the SAA(86-104) 19-peptide has rather unordered structure with bends in its C-terminal part, which is consistent with the previous results relating to the whole protein. The results of affinity chromatography, fluorescent ELISA-like test, CD and NMR studies point to an importance of proline residues on structure of SAA(86-104). Conformational details of SAA fragment, responsible for hCC binding, may help to understand the objective of hCC-SAA complex formation and its importance for pathogenesis of reactive amyloid A amyloidosis., (Copyright © 2015 John Wiley & Sons, Ltd.)

Published

2015