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3. Directed evolution of the metalloproteinase inhibitor TIMP-1 reveals that its N- and C-terminal domains cooperate in matrix metalloproteinase recognition

Author

Raeeszadeh-Sarmazdeh, Maryam, Greene, Kerrie A, Sankaran, Banumathi, Downey, Gregory P, Radisky, Derek C, and Radisky, Evette S

Subjects
Biochemistry and Cell Biology, Biological Sciences, Biotechnology, 2.1 Biological and endogenous factors, Amino Acid Sequence, Binding Sites, Catalytic Domain, Crystallography, X-Ray, Directed Molecular Evolution, Humans, Matrix Metalloproteinase 3, Matrix Metalloproteinase Inhibitors, Mutation, Protein Binding, Protein Conformation, Protein Domains, Tissue Inhibitor of Metalloproteinase-1, Two-Hybrid System Techniques, crystal structure, directed evolution, matrix metalloproteinase, metalloprotease, protease inhibitor, protein domain, protein engineering, protein structure, protein-protein interaction, tissue inhibitor of metalloproteinase, yeast surface display, Chemical Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences
Abstract

Tissue inhibitors of metalloproteinases (TIMPs) are natural inhibitors of matrix metalloproteinases (MMPs), enzymes that contribute to cancer and many inflammatory and degenerative diseases. The TIMP N-terminal domain binds and inhibits an MMP catalytic domain, but the role of the TIMP C-terminal domain in MMP inhibition is poorly understood. Here, we employed yeast surface display for directed evolution of full-length human TIMP-1 to develop MMP-3-targeting ultrabinders. By simultaneously incorporating diversity into both domains, we identified TIMP-1 variants that were up to 10-fold improved in binding MMP-3 compared with WT TIMP-1, with inhibition constants (Ki ) in the low picomolar range. Analysis of individual and paired mutations from the selected TIMP-1 variants revealed cooperative effects between distant residues located on the N- and C-terminal TIMP domains, positioned on opposite sides of the interaction interface with MMP-3. Crystal structures of MMP-3 complexes with TIMP-1 variants revealed conformational changes in TIMP-1 near the cooperative mutation sites. Affinity was strengthened by cinching of a reciprocal "tyrosine clasp" formed between the N-terminal domain of TIMP-1 and proximal MMP-3 interface and by changes in secondary structure within the TIMP-1 C-terminal domain that stabilize interdomain interactions and improve complementarity to MMP-3. Our protein engineering and structural studies provide critical insight into the cooperative function of TIMP domains and the significance of peripheral TIMP epitopes in MMP recognition. Our findings suggest new strategies to engineer TIMP proteins for therapeutic applications, and our directed evolution approach may also enable exploration of functional domain interactions in other protein systems.

Published
2019

4. Disulfide engineering of human Kunitz-type serine protease inhibitors enhances proteolytic stability and target affinity toward mesotrypsin

Author

Cohen, Itay, Coban, Matt, Shahar, Anat, Sankaran, Banumathi, Hockla, Alexandra, Lacham, Shiran, Caulfield, Thomas R, Radisky, Evette S, and Papo, Niv

Subjects
Biochemistry and Cell Biology, Chemical Sciences, Biological Sciences, Biotechnology, Bioengineering, 2.1 Biological and endogenous factors, Amyloid beta-Protein Precursor, Animals, Aprotinin, Crystallography, X-Ray, Disulfides, Humans, Models, Molecular, Protein Conformation, Protein Domains, Protein Engineering, Proteolysis, Trypsin, crystal structure, disulfide, molecular dynamics, protease inhibitor, protein engineering, protein structure, proteolysis, serine protease, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences
Abstract

Serine protease inhibitors of the Kunitz-bovine pancreatic trypsin inhibitor (BPTI) family are ubiquitous biological regulators of proteolysis. These small proteins are resistant to proteolysis, but can be slowly cleaved within the protease-binding loop by target proteases, thereby compromising their activity. For the human protease mesotrypsin, this cleavage is especially rapid. Here, we aimed to stabilize the Kunitz domain structure against proteolysis through disulfide engineering. Substitution within the Kunitz inhibitor domain of the amyloid precursor protein (APPI) that incorporated a new disulfide bond between residues 17 and 34 reduced proteolysis by mesotrypsin 74-fold. Similar disulfide engineering of tissue factor pathway inhibitor-1 Kunitz domain 1 (KD1TFPI1) and bikunin Kunitz domain 2 (KD2bikunin) likewise stabilized these inhibitors against mesotrypsin proteolysis 17- and 6.6-fold, respectively. Crystal structures of disulfide-engineered APPI and KD1TFPI1 variants in a complex with mesotrypsin at 1.5 and 2.0 Å resolution, respectively, confirmed the formation of well-ordered disulfide bonds positioned to stabilize the binding loop. Long all-atom molecular dynamics simulations of disulfide-engineered Kunitz domains and their complexes with mesotrypsin revealed conformational stabilization of the primed side of the inhibitor-binding loop by the engineered disulfide, along with global suppression of conformational dynamics in the Kunitz domain. Our findings suggest that the Cys-17-Cys-34 disulfide slows proteolysis by dampening conformational fluctuations in the binding loop and minimizing motion at the enzyme-inhibitor interface. The generalizable approach developed here for the stabilization against proteolysis of Kunitz domains, which can serve as important scaffolds for therapeutics, may thus find applications in drug development.

Published
2019

25. Directed evolution of the metalloproteinase inhibitor TIMP-1 reveals that its N- and C-terminal domains cooperate in matrix metalloproteinase recognition

Author

Kerrie A. Greene, Maryam Raeeszadeh-Sarmazdeh, Derek C. Radisky, Evette S. Radisky, Banumathi Sankaran, and Gregory P. Downey

Subjects
0301 basic medicine, metalloprotease, yeast surface display, Protein Conformation, Matrix metalloproteinase, Crystallography, X-Ray, Medical and Health Sciences, Biochemistry, protein-protein interaction, Protein structure, Catalytic Domain, 2.1 Biological and endogenous factors, directed evolution, Aetiology, Metalloproteinase, Crystallography, Chemistry, protein domain, Biological Sciences, Directed evolution, Cell biology, Protein Structure and Folding, Matrix Metalloproteinase 3, Protein Binding, crystal structure, Biochemistry & Molecular Biology, matrix metalloproteinase, Protein domain, Matrix Metalloproteinase Inhibitors, Protein–protein interaction, protease inhibitor, 03 medical and health sciences, Protein Domains, Two-Hybrid System Techniques, Humans, Amino Acid Sequence, protein structure, Molecular Biology, Binding Sites, Tissue Inhibitor of Metalloproteinase-1, 030102 biochemistry & molecular biology, protein engineering, Cell Biology, Protein engineering, Tissue inhibitor of metalloproteinase, 030104 developmental biology, Chemical Sciences, Mutation, X-Ray, tissue inhibitor of metalloproteinase, Directed Molecular Evolution
Abstract

Tissue inhibitors of metalloproteinases (TIMPs) are natural inhibitors of matrix metalloproteinases (MMPs), enzymes that contribute to cancer and many inflammatory and degenerative diseases. The TIMP N-terminal domain binds and inhibits an MMP catalytic domain, but the role of the TIMP C-terminal domain in MMP inhibition is poorly understood. Here, we employed yeast surface display for directed evolution of full-length human TIMP-1 to develop MMP-3–targeting ultrabinders. By simultaneously incorporating diversity into both domains, we identified TIMP-1 variants that were up to 10-fold improved in binding MMP-3 compared with WT TIMP-1, with inhibition constants (K(i)) in the low picomolar range. Analysis of individual and paired mutations from the selected TIMP-1 variants revealed cooperative effects between distant residues located on the N- and C-terminal TIMP domains, positioned on opposite sides of the interaction interface with MMP-3. Crystal structures of MMP-3 complexes with TIMP-1 variants revealed conformational changes in TIMP-1 near the cooperative mutation sites. Affinity was strengthened by cinching of a reciprocal “tyrosine clasp” formed between the N-terminal domain of TIMP-1 and proximal MMP-3 interface and by changes in secondary structure within the TIMP-1 C-terminal domain that stabilize interdomain interactions and improve complementarity to MMP-3. Our protein engineering and structural studies provide critical insight into the cooperative function of TIMP domains and the significance of peripheral TIMP epitopes in MMP recognition. Our findings suggest new strategies to engineer TIMP proteins for therapeutic applications, and our directed evolution approach may also enable exploration of functional domain interactions in other protein systems.

Published
2019
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26. Disulfide engineering of human Kunitz-type serine protease inhibitors enhances proteolytic stability and target affinity toward mesotrypsin

Author

Anat Shahar, Itay Cohen, Alexandra Hockla, Shiran Lacham, Niv Papo, Matt Coban, Banumathi Sankaran, Thomas R. Caulfield, and Evette S. Radisky

Subjects
Models, Molecular, 0301 basic medicine, Protein Conformation, serine protease, medicine.medical_treatment, Crystallography, X-Ray, Protein Engineering, Medical and Health Sciences, Biochemistry, Amyloid beta-Protein Precursor, Protein structure, Models, Amyloid precursor protein, 2.1 Biological and endogenous factors, Trypsin, Disulfides, Aetiology, Crystallography, biology, medicine.diagnostic_test, Chemistry, Biological Sciences, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Kunitz domain, Biotechnology, crystal structure, proteolysis, Biochemistry & Molecular Biology, Proteases, animal structures, Trypsin inhibitor, Proteolysis, protease inhibitor, 03 medical and health sciences, Aprotinin, Protein Domains, medicine, Animals, Humans, protein structure, Molecular Biology, Serine protease, Protease, 030102 biochemistry & molecular biology, Computational Biology, Molecular, Cell Biology, molecular dynamics, 030104 developmental biology, Chemical Sciences, X-Ray, biology.protein, Biophysics, Generic health relevance, disulfide
Abstract

Serine protease inhibitors of the Kunitz-bovine pancreatic trypsin inhibitor (BPTI) family are ubiquitous biological regulators of proteolysis. These small proteins are resistant to proteolysis, but can be slowly cleaved within the protease-binding loop by target proteases, thereby compromising their activity. For the human protease mesotrypsin, this cleavage is especially rapid. Here, we aimed to stabilize the Kunitz domain structure against proteolysis through disulfide engineering. Substitution within the Kunitz inhibitor domain of the amyloid precursor protein (APPI) that incorporated a new disulfide bond between residues 17 and 34 reduced proteolysis by mesotrypsin 74-fold. Similar disulfide engineering of tissue factor pathway inhibitor-1 Kunitz domain 1 ((KD1)TFPI1) and bikunin Kunitz domain 2 ((KD2)bikunin) likewise stabilized these inhibitors against mesotrypsin proteolysis 17- and 6.6-fold, respectively. Crystal structures of disulfide-engineered APPI and (KD1)TFPI1 variants in a complex with mesotrypsin at 1.5 and 2.0 Å resolution, respectively, confirmed the formation of well-ordered disulfide bonds positioned to stabilize the binding loop. Long all-atom molecular dynamics simulations of disulfide-engineered Kunitz domains and their complexes with mesotrypsin revealed conformational stabilization of the primed side of the inhibitor-binding loop by the engineered disulfide, along with global suppression of conformational dynamics in the Kunitz domain. Our findings suggest that the Cys-17–Cys-34 disulfide slows proteolysis by dampening conformational fluctuations in the binding loop and minimizing motion at the enzyme–inhibitor interface. The generalizable approach developed here for the stabilization against proteolysis of Kunitz domains, which can serve as important scaffolds for therapeutics, may thus find applications in drug development.

Published
2019
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29. A potent, proteolysis-resistant inhibitor of kallikrein-related peptidase 6 (KLK6) for cancer therapy, developed by combinatorial engineering

Author

Niv Papo, Aubry K. Miller, Evette S. Radisky, Amiram Sananes, Alexandra Hockla, Itay Cohen, Elena De Vita, and Anat Shahar

Subjects
Models, Molecular, 0301 basic medicine, Proteases, Protein Conformation, Proteolysis, Tissue kallikrein, Breast Neoplasms, Biochemistry, Serine, Amyloid beta-Protein Precursor, 03 medical and health sciences, Cell Movement, Tumor Cells, Cultured, medicine, Amyloid precursor protein, Humans, Protease Inhibitors, Molecular Biology, Cell Proliferation, medicine.diagnostic_test, biology, Chemistry, KLK6, Cell Biology, Kallikrein, Protease inhibitor (biology), High-Throughput Screening Assays, 3. Good health, 030104 developmental biology, Enzymology, biology.protein, Female, Kallikreins, Genetic Engineering, Protein Binding, medicine.drug
Abstract

Human tissue kallikrein (KLK) proteases are hormone-like signaling molecules with important functions in cancer pathophysiology. KLK-related peptidase 6 (KLK6), specifically, is highly up-regulated in several types of cancer, where its increased activity promotes cancer invasion and metastasis. This characteristic suggests KLK6 as an attractive target for therapeutic interventions. However, inhibitors that specifically target KLK6 have not yet been reported, possibly because KLK6 shares a high sequence homology and structural similarity with other serine proteases and resists inhibition by many polypeptide inhibitors. Here, we present an innovative combinatorial approach to engineering KLK6 inhibitors via flow cytometry–based screening of a yeast-displayed mutant library of the human amyloid precursor protein Kunitz protease inhibitor domain (APPI), an inhibitor of other serine proteases, such as anionic and cationic trypsins. On the basis of this screening, we generated APPI(M17L,I18F,S19F,F34V) (APPI-4M), an APPI variant with a KLK6 inhibition constant (K(i)) of 160 pm and a turnover time of 10 days. To the best of our knowledge, APPI-4M is the most potent KLK6 inhibitor reported to date, displaying 146-fold improved affinity and 13-fold improved proteolytic stability compared with WT APPI (APPI(WT)). We further demonstrate that APPI-4M acts as a functional inhibitor in a cell-based model of KLK6-dependent breast cancer invasion. Finally, the crystal structures of the APPI(WT)/KLK6 and APPI-4M/KLK6 complexes revealed the structural and mechanistic bases for the improved KLK6 binding and proteolytic resistance of APPI-4M. We anticipate that APPI-4M will have substantial translational potential as both imaging agent and therapeutic.

Published
2018
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30. Development of High Affinity and High Specificity Inhibitors of Matrix Metalloproteinase 14 through Computational Design and Directed Evolution

Author

Yuval Horev, Itay Cohen, Irit Sagi, Julia M. Shifman, Moran Grossman, Jason Shirian, Niv Papo, Gal Yosef, Valeria Arkadash, and Evette S. Radisky

Subjects
0301 basic medicine, Mutant, Cell, Matrix Metalloproteinase Inhibitors, Matrix metalloproteinase, Crystallography, X-Ray, Biochemistry, 03 medical and health sciences, Matrix Metalloproteinase 14, medicine, Animals, Humans, Amino Acid Sequence, Molecular Biology, chemistry.chemical_classification, Tissue Inhibitor of Metalloproteinase-2, Chemistry, Cell Biology, Protein engineering, Inhibitor protein, Directed evolution, In vitro, Molecular Docking Simulation, 030104 developmental biology, medicine.anatomical_structure, Enzyme, Drug Design, Mutation, Enzymology, Cancer research, Cattle, Directed Molecular Evolution
Abstract

Degradation of the extracellular matrices in the human body is controlled by matrix metalloproteinases (MMPs), a family of more than 20 homologous enzymes. Imbalance in MMP activity can result in many diseases, such as arthritis, cardiovascular diseases, neurological disorders, fibrosis, and cancers. Thus, MMPs present attractive targets for drug design and have been a focus for inhibitor design for as long as 3 decades. Yet, to date, all MMP inhibitors have failed in clinical trials because of their broad activity against numerous MMP family members and the serious side effects of the proposed treatment. In this study, we integrated a computational method and a yeast surface display technique to obtain highly specific inhibitors of MMP-14 by modifying the natural non-specific broad MMP inhibitor protein N-TIMP2 to interact optimally with MMP-14. We identified an N-TIMP2 mutant, with five mutations in its interface, that has an MMP-14 inhibition constant (Ki ) of 0.9 pm, the strongest MMP-14 inhibitor reported so far. Compared with wild-type N-TIMP2, this variant displays ∼900-fold improved affinity toward MMP-14 and up to 16,000-fold greater specificity toward MMP-14 relative to other MMPs. In an in vitro and cell-based model of MMP-dependent breast cancer cellular invasiveness, this N-TIMP2 mutant acted as a functional inhibitor. Thus, our study demonstrates the enormous potential of a combined computational/directed evolution approach to protein engineering. Furthermore, it offers fundamental clues into the molecular basis of MMP regulation by N-TIMP2 and identifies a promising MMP-14 inhibitor as a starting point for the development of protein-based anticancer therapeutics.

Published
2017
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31. Mesotrypsin Has Evolved Four Unique Residues to Cleave Trypsin Inhibitors as Substrates

Author

Olumide Kayode, Alexandra Hockla, Alexandre P. Alloy, Ruiying Wang, Evette S. Radisky, and Alexei S. Soares

Subjects
Models, Molecular, Stereochemistry, Proteolysis, Molecular Sequence Data, Crystallography, X-Ray, Cleavage (embryo), Biochemistry, Substrate Specificity, Evolution, Molecular, Aprotinin, Protein structure, medicine, Amyloid precursor protein, Animals, Humans, Trypsin, Amino Acid Sequence, Amino Acids, Site-directed mutagenesis, Molecular Biology, Peptide sequence, Conserved Sequence, Serine protease, biology, medicine.diagnostic_test, Cell Biology, Rats, Kinetics, Amino Acid Substitution, Enzymology, Biocatalysis, biology.protein, Cattle, Mutant Proteins, Trypsin Inhibitors, medicine.drug
Abstract

Human mesotrypsin is highly homologous to other mammalian trypsins, and yet it is functionally unique in possessing resistance to inhibition by canonical serine protease inhibitors and in cleaving these inhibitors as preferred substrates. Arg-193 and Ser-39 have been identified as contributors to the inhibitor resistance and cleavage capability of mesotrypsin, but it is not known whether these residues fully account for the unusual properties of mesotrypsin. Here, we use human cationic trypsin as a template for engineering a gain of catalytic function, assessing mutants containing mesotrypsin-like mutations for resistance to inhibition by bovine pancreatic trypsin inhibitor (BPTI) and amyloid precursor protein Kunitz protease inhibitor (APPI), and for the ability to hydrolyze these inhibitors as substrates. We find that Arg-193 and Ser-39 are sufficient to confer mesotrypsin-like resistance to inhibition; however, compared with mesotrypsin, the trypsin-Y39S/G193R double mutant remains 10-fold slower at hydrolyzing BPTI and 2.5-fold slower at hydrolyzing APPI. We identify two additional residues in mesotrypsin, Lys-74 and Asp-97, which in concert with Arg-193 and Ser-39 confer the full catalytic capability of mesotrypsin for proteolysis of BPTI and APPI. Novel crystal structures of trypsin mutants in complex with BPTI suggest that these four residues function cooperatively to favor conformational dynamics that assist in dissociation of cleaved inhibitors. Our results reveal that efficient inhibitor cleavage is a complex capability to which at least four spatially separated residues of mesotrypsin contribute. These findings suggest that inhibitor cleavage represents a functional adaptation of mesotrypsin that may have evolved in response to positive selection pressure.

Published
2015
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32. Sequence and Conformational Specificity in Substrate Recognition

Author

Ruiying Wang, Alexandra Hockla, Alexei S. Soares, Evette S. Radisky, Marat D. Kazanov, Benjamin J. Madden, Rachel D. Henin, and Devon F. Pendlebury

Subjects
Serine protease, Protease, medicine.medical_treatment, Cell Biology, Plasma protein binding, Biology, Protein degradation, Biochemistry, Protein–protein interaction, Protein structure, biology.protein, Amyloid precursor protein, medicine, Binding site, Molecular Biology
Abstract

Mesotrypsin is an isoform of trypsin that is uniquely resistant to polypeptide trypsin inhibitors and can cleave some inhibitors rapidly. Previous studies have shown that the amyloid precursor protein Kunitz protease inhibitor domain (APPI) is a specific substrate of mesotrypsin and that stabilization of the APPI cleavage site in a canonical conformation contributes to recognition by mesotrypsin. We hypothesized that other proteins possessing potential cleavage sites stabilized in a similar conformation might also be mesotrypsin substrates. Here we evaluated a series of candidate substrates, including human Kunitz protease inhibitor domains from amyloid precursor-like protein 2 (APLP2), bikunin, hepatocyte growth factor activator inhibitor type 2 (HAI2), tissue factor pathway inhibitor-1 (TFPI1), and tissue factor pathway inhibitor-2 (TFPI2), as well as E-selectin, an unrelated protein possessing a potential cleavage site displaying canonical conformation. We find that Kunitz domains within APLP2, bikunin, and HAI2 are cleaved by mesotrypsin with kinetic profiles of specific substrates. TFPI1 and TFPI2 Kunitz domains are cleaved less efficiently by mesotrypsin, and E-selectin is not cleaved at the anticipated site. Cocrystal structures of mesotrypsin with HAI2 and bikunin Kunitz domains reveal the mode of mesotrypsin interaction with its canonical substrates. Our data suggest that major determinants of mesotrypsin substrate specificity include sequence preferences at the P1 and P′2 positions along with conformational stabilization of the cleavage site in the canonical conformation. Mesotrypsin up-regulation has been implicated previously in cancer progression, and proteolytic clearance of Kunitz protease inhibitors offers potential mechanisms by which mesotrypsin may mediate pathological effects in cancer.

Published
2014
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33. Matrix Metalloproteinase-10 (MMP-10) Interaction with Tissue Inhibitors of Metalloproteinases TIMP-1 and TIMP-2

Author

Jessica Robinson, Alan P. Fields, Jyotica Batra, Alexei S. Soares, Derek C. Radisky, and Evette S. Radisky

Subjects
Matrix Metalloproteinase 3, Metalloproteinase, Cell Biology, Matrix metalloproteinase, Biology, Biochemistry, Molecular biology, Protease inhibitor (biology), Protein structure, medicine, Molecular replacement, Binding site, Molecular Biology, Binding selectivity, medicine.drug
Abstract

Matrix metalloproteinase 10 (MMP-10, stromelysin-2) is a secreted metalloproteinase with functions in skeletal development, wound healing, and vascular remodeling; its overexpression is also implicated in lung tumorigenesis and tumor progression. To understand the regulation of MMP-10 by tissue inhibitors of metalloproteinases (TIMPs), we have assessed equilibrium inhibition constants (Ki) of putative physiological inhibitors TIMP-1 and TIMP-2 for the active catalytic domain of human MMP-10 (MMP-10cd) using multiple kinetic approaches. We find that TIMP-1 inhibits the MMP-10cd with a Ki of 1.1 × 10−9 m; this interaction is 10-fold weaker than the inhibition of the similar MMP-3 (stromelysin-1) catalytic domain (MMP-3cd) by TIMP-1. TIMP-2 inhibits the MMP-10cd with a Ki of 5.8 × 10−9 m, which is again 10-fold weaker than the inhibition of MMP-3cd by this inhibitor (Ki = 5.5 × 10−10 m). We solved the x-ray crystal structure of TIMP-1 bound to the MMP-10cd at 1.9 A resolution; the structure was solved by molecular replacement and refined with an R-factor of 0.215 (Rfree = 0.266). Comparing our structure of MMP-10cd·TIMP-1 with the previously solved structure of MMP-3cd·TIMP-1 (Protein Data Bank entry 1UEA), we see substantial differences at the binding interface that provide insight into the differential binding of stromelysin family members to TIMP-1. This structural information may ultimately assist in the design of more selective TIMP-based inhibitors tailored for specificity toward individual members of the stromelysin family, with potential therapeutic applications.

Published
2012
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34. High Affinity Small Protein Inhibitors of Human Chymotrypsin C (CTRC) Selected by Phage Display Reveal Unusual Preference for P4′ Acidic Residues

Author

Evette S. Radisky, Katalin A. Kékesi, Miklós Sahin-Tóth, András Szabó, Dávid Szakács, Gábor Pál, Katalin Zboray, and Dávid Héja

Subjects
Models, Molecular, Phage display, Protein Conformation, medicine.medical_treatment, DNA Mutational Analysis, Molecular Sequence Data, Biology, Biochemistry, Substrate Specificity, Peptide Library, medicine, Chymotrypsin, Humans, Protease Inhibitors, Elméleti orvostudományok, Amino Acid Sequence, Pacifastin, Molecular Biology, Serine protease, Protease, Chymotrypsin-C, Proteolytic enzymes, Orvostudományok, Cell Biology, Protease inhibitor (biology), Enzymology, biology.protein, Insect Proteins, Directed Molecular Evolution, Peptides, Protein Binding, medicine.drug
Abstract

Human chymotrypsin C (CTRC) is a pancreatic protease that participates in the regulation of intestinal digestive enzyme activity. Other chymotrypsins and elastases are inactive on the regulatory sites cleaved by CTRC, suggesting that CTRC recognizes unique sequence patterns. To characterize the molecular determinants underlying CTRC specificity, we selected high affinity substrate-like small protein inhibitors against CTRC from a phage library displaying variants of SGPI-2, a natural chymotrypsin inhibitor from Schistocerca gregaria. On the basis of the sequence pattern selected, we designed eight inhibitor variants in which amino acid residues in the reactive loop at P1 (Met or Leu), P2' (Leu or Asp), and P4' (Glu, Asp, or Ala) were varied. Binding experiments with CTRC revealed that (i) inhibitors with Leu at P1 bind 10-fold stronger than those with P1 Met; (ii) Asp at P2' (versus Leu) decreases affinity but increases selectivity, and (iii) Glu or Asp at P4' (versus Ala) increase affinity 10-fold. The highest affinity SGPI-2 variant (K(D) 20 pm) bound to CTRC 575-fold tighter than the parent molecule. The most selective inhibitor variant exhibited a K(D) of 110 pm and a selectivity ranging from 225- to 112,664-fold against other human chymotrypsins and elastases. Homology modeling and mutagenesis identified a cluster of basic amino acid residues (Lys(51), Arg(56), and Arg(80)) on the surface of human CTRC that interact with the P4' acidic residue of the inhibitor. The acidic preference of CTRC at P4' is unique among pancreatic proteases and might contribute to the high specificity of CTRC-mediated digestive enzyme regulation.

Published
2011
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35. The 19-Amino Acid Insertion in the Tumor-associated Splice Isoform Rac1b Confers Specific Binding to p120 Catenin

Author

Masahiro Yanagisawa, Derek C. Radisky, Evette S. Radisky, Rory Geyer, Lidiya Orlichenko, Panos Z. Anastasiadis, and Davitte Khauv

Subjects
rac1 GTP-Binding Protein, Delta Catenin, Transcription, Genetic, Molecular Sequence Data, RAC1, GTPase, Biology, Biochemistry, Protein–protein interaction, Mice, Cell Movement, Cell Adhesion, Transcriptional regulation, Animals, Protein Isoforms, Amino Acid Sequence, Amino Acids, Molecular Biology, chemistry.chemical_classification, Catenins, Epithelial Cells, Cell migration, Cell Biology, Amino acid, Alternative Splicing, Phenotype, chemistry, Signal transduction, Intracellular, Protein Binding
Abstract

The Rac1b splice isoform contains a 19-amino acid insertion not found in Rac1; this insertion leads to decreased GTPase activity and reduced affinity for GDP, resulting in the intracellular predominance of GTP-bound Rac1b. Here, using co-precipitation and proteomic methods, we find that Rac1b does not bind to many common regulators of Rho family GTPases but that it does display enhanced binding to SmgGDS, RACK1, and p120 catenin (p120(ctn)), proteins involved in cell-cell adhesion, motility, and transcriptional regulation. We use molecular modeling and structure analysis approaches to determine that the interaction between Rac1b and p120(ctn) is dependent upon protein regions that are predicted to be unstructured in the absence of molecular complex formation, suggesting that the interaction between these two proteins involves coupled folding and binding. We also find that directed cell movement initiated by Rac1b is dependent upon p120. These results define a distinct binding functionality of Rac1b and provide insight into how the distinct phenotypic program activated by this protein may be implemented through molecular recognition of effectors distinct from those of Rac1.

Published
2010
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36. Structural Basis for Accelerated Cleavage of Bovine Pancreatic Trypsin Inhibitor (BPTI) by Human Mesotrypsin

Author

Alexandra Hockla, Evette S. Radisky, Moh'd A. Salameh, and Alexei S. Soares

Subjects
Models, Molecular, Steric effects, Arginine, Protein Conformation, Stereochemistry, Molecular Sequence Data, Crystallography, X-Ray, Cleavage (embryo), Biochemistry, Aprotinin, medicine, Animals, Humans, Trypsin, Amino Acid Sequence, Molecular Biology, chemistry.chemical_classification, biology, Chemistry, Hydrogen bond, Hydrolysis, Leaving group, Active site, Cell Biology, Recombinant Proteins, Enzyme, biology.protein, Cattle, medicine.drug
Abstract

Human mesotrypsin is an isoform of trypsin that displays unusual resistance to polypeptide trypsin inhibitors and has been observed to cleave several such inhibitors as substrates. Whereas substitution of arginine for the highly conserved glycine 193 in the trypsin active site has been implicated as a critical factor in the inhibitor resistance of mesotrypsin, how this substitution leads to accelerated inhibitor cleavage is not clear. Bovine pancreatic trypsin inhibitor (BPTI) forms an extremely stable and cleavage-resistant complex with trypsin, and thus provides a rigorous challenge of mesotrypsin catalytic activity toward polypeptide inhibitors. Here, we report kinetic constants for mesotrypsin and the highly homologous (but inhibitor sensitive) human cationic trypsin, describing inhibition by, and cleavage of BPTI, as well as crystal structures of the mesotrypsin-BPTI and human cationic trypsin-BPTI complexes. We find that mesotrypsin cleaves BPTI with a rate constant accelerated 350-fold over that of human cationic trypsin and 150,000-fold over that of bovine trypsin. From the crystal structures, we see that small conformational adjustments limited to several side chains enable mesotrypsin-BPTI complex formation, surmounting the predicted steric clash introduced by Arg-193. Our results show that the mesotrypsin-BPTI interface favors catalysis through (a) electrostatic repulsion between the closely spaced mesotrypsin Arg-193 and BPTI Arg-17, and (b) elimination of two hydrogen bonds between the enzyme and the amine leaving group portion of BPTI. Our model predicts that these deleterious interactions accelerate leaving group dissociation and deacylation.

Published
2008
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37. The iron-responsive element binding protein. Purification, cloning, and regulation in rat liver

Author

Elizabeth A. Leibold, Yang Yu, and Evette S. Radisky

Subjects
Messenger RNA, cDNA library, fungi, RNA, Cell Biology, Iron-responsive element-binding protein, Biology, Biochemistry, Molecular biology, Conserved sequence, Regulatory sequence, Complementary DNA, Molecular Biology, Peptide sequence
Abstract

The iron-responsive element binding protein (IRE-BP) is a cytosolic protein that binds a highly conserved sequence in the untranslated regions of mRNAs involved in iron metabolism including ferritin, transferrin receptor, and erythroid 5-aminolevulinate acid synthase. This conserved sequence is termed the iron-responsive element and is necessary for the post-transcriptional regulation of these mRNAs by iron. The rat liver IRE-BP was purified to homogeneity by chromatographic methods and partial amino acid sequence was obtained. A cDNA was isolated from a rat liver cDNA library and sequenced. The amino acid sequence deduced from the cDNA sequence corresponds to a protein of 889 amino acids with a predicted molecular weight of 97.946. The NH2-terminal sequence obtained by Edman degradation matched the deduced amino acid sequence obtained from the cDNA, confirming the translational start site. Rat liver IRE-BP shares 95% identity with human IRE-BP and 98% identity with mouse IRE-BP indicating that the IRE-BPs have remained highly conserved during evolution. The 5'-untranslated region is at least 236 nucleotides and contains interesting structural features including two direct repeats, an inverted repeat, and three small open reading frames. The rat IRE-BP mRNA is approximately 3600 nucleotides and is expressed in a variety of rat tissues including liver, spleen, and gut. Over the course of 16 h following an intraperitoneal injection of iron in rats. IRE-BP RNA binding activity decreases to 50% of control levels. The decrease in IRE-BP RNA binding activity in extracts from iron-treated rats is reversible by pretreatment of the extracts with reducing agents. The steady-state levels of IRE-BP mRNA remain constant during iron treatment. These data suggest that the decrease in IRE-BP RNA binding activity by iron in rat liver is due to post-translational changes in the RNA binding affinity of the IRE-BP and not due a decrease in the transcription of the IRE-BP gene or to the destabilization of the IRE-BP mRNA.

Published
1992
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