Your search keyword '"Cavalier MC"' showing total 8 results

1. The calcium-binding protein S100B reduces IL6 production in malignant melanoma via inhibition of RSK cellular signaling.

Author

Alasady MJ, Terry AR, Pierce AD, Cavalier MC, Blaha CS, Adipietro KA, Wilder PT, Weber DJ, and Hay N

Subjects

Calcium-Binding Proteins genetics, Cell Line, Tumor, Cyclic AMP Response Element-Binding Protein genetics, Cytoplasm genetics, Doxycycline pharmacology, Gene Expression Regulation, Neoplastic drug effects, Humans, Melanoma drug therapy, Melanoma pathology, Signal Transduction drug effects, Interleukin-6 genetics, Melanoma genetics, Ribosomal Protein S6 Kinases, 90-kDa genetics, S100 Calcium Binding Protein beta Subunit genetics, STAT3 Transcription Factor genetics

Abstract

S100B is frequently elevated in malignant melanoma. A regulatory mechanism was uncovered here in which elevated S100B lowers mRNA and secreted protein levels of interleukin-6 (IL6) and inhibits an autocrine loop whereby IL6 activates STAT3 signaling. Our results showed that S100B affects IL6 expression transcriptionally. S100B was shown to form a calcium-dependent protein complex with the p90 ribosomal S6 kinase (RSK), which in turn sequesters RSK into the cytoplasm. Consistently, S100B inhibition was found to restore phosphorylation of a nuclear located RSK substrate, CREB, which is a potent transcription factor for IL6 expression. Thus, elevated S100B reduces IL6-STAT3 signaling via RSK signaling pathway in malignant melanoma. Indeed, the elevated S100B levels in malignant melanoma cell lines correspond to low levels of IL6 and p-STAT3., Competing Interests: NO authors have competing interests.

Published

2021

2. A natural human monoclonal antibody targeting Staphylococcus Protein A protects against Staphylococcus aureus bacteremia.

Author

Varshney AK, Kuzmicheva GA, Lin J, Sunley KM, Bowling RA Jr, Kwan TY, Mays HR, Rambhadran A, Zhang Y, Martin RL, Cavalier MC, Simard J, and Shivaswamy S

Subjects

Animals, Bacteremia immunology, Bacteremia prevention & control, Humans, Immunoglobulin G, Mice, Staphylococcal Infections immunology, Antibodies, Monoclonal immunology, Antibodies, Monoclonal therapeutic use, Staphylococcal Infections prevention & control, Staphylococcal Protein A immunology

Abstract

Staphylococcus aureus can cause devastating and life-threatening infections. With the increase in multidrug resistant strains, novel therapies are needed. Limited success with active and passive immunization strategies have been attributed to S. aureus immune evasion. Here, we report on a monoclonal antibody, 514G3, that circumvents a key S. aureus evasion mechanism by targeting the cell wall moiety Protein A (SpA). SpA tightly binds most subclasses of immunoglobulins via their Fc region, neutralizing effector function. The organism can thus shield itself with a protective coat of serum antibodies and render humoral immunity ineffective. The present antibody reactivity was derived from an individual with natural anti-SpA antibody titers. The monoclonal antibody is of an IgG3 subclass, which differs critically from other immunoglobulin subclasses since its Fc is not bound by SpA. Moreover, it targets a unique epitope on SpA that allows it to bind in the presence of serum antibodies. Consequently, the antibody opsonizes S. aureus and maintains effector function to enable natural immune mediated clearance. The data presented here provide evidence that 514G3 antibody is able to successfully rescue mice from S. aureus mediated bacteremia.

Published

2018

3. Novel protein-inhibitor interactions in site 3 of Ca(2+)-bound S100B as discovered by X-ray crystallography.

Author

Cavalier MC, Melville Z, Aligholizadeh E, Raman EP, Yu W, Fang L, Alasady M, Pierce AD, Wilder PT, MacKerell AD Jr, and Weber DJ

Subjects

Cell Line, Tumor, Crystallography, X-Ray, Drug Design, Humans, Melanoma drug therapy, Molecular Docking Simulation, S100 Proteins chemistry, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, S100 Proteins antagonists & inhibitors, S100 Proteins metabolism, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacology

Abstract

Structure-based drug discovery is under way to identify and develop small-molecule S100B inhibitors (SBiXs). Such inhibitors have therapeutic potential for treating malignant melanoma, since high levels of S100B downregulate wild-type p53 tumor suppressor function in this cancer. Computational and X-ray crystallographic studies of two S100B-SBiX complexes are described, and both compounds (apomorphine hydrochloride and ethidium bromide) occupy an area of the S100B hydrophobic cleft which is termed site 3. These data also reveal novel protein-inhibitor interactions which can be used in future drug-design studies to improve SBiX affinity and specificity. Of particular interest, apomorphine hydrochloride showed S100B-dependent killing in melanoma cell assays, although the efficacy exceeds its affinity for S100B and implicates possible off-target contributions. Because there are no structural data available for compounds occupying site 3 alone, these studies contribute towards the structure-based approach to targeting S100B by including interactions with residues in site 3 of S100B.

Published

2016

4. Small Molecule Inhibitors of Ca(2+)-S100B Reveal Two Protein Conformations.

Author

Cavalier MC, Ansari MI, Pierce AD, Wilder PT, McKnight LE, Raman EP, Neau DB, Bezawada P, Alasady MJ, Charpentier TH, Varney KM, Toth EA, MacKerell AD Jr, Coop A, and Weber DJ

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Cattle, Cell Line, Tumor, Crystallography, X-Ray, Drug Design, Humans, Models, Molecular, Pentamidine analogs & derivatives, Pentamidine chemistry, Pentamidine pharmacology, Protein Conformation, Rats, Small Molecule Libraries, Structure-Activity Relationship, Tumor Suppressor Protein p53 drug effects, S100 Calcium Binding Protein beta Subunit antagonists & inhibitors, S100 Calcium Binding Protein beta Subunit chemistry

Abstract

The drug pentamidine inhibits calcium-dependent complex formation with p53 ((Ca)S100B·p53) in malignant melanoma (MM) and restores p53 tumor suppressor activity in vivo. However, off-target effects associated with this drug were problematic in MM patients. Structure-activity relationship (SAR) studies were therefore completed here with 23 pentamidine analogues, and X-ray structures of (Ca)S100B·inhibitor complexes revealed that the C-terminus of S100B adopts two different conformations, with location of Phe87 and Phe88 being the distinguishing feature and termed the "FF-gate". For symmetric pentamidine analogues ((Ca)S100B·5a, (Ca)S100B·6b) a channel between sites 1 and 2 on S100B was occluded by residue Phe88, but for an asymmetric pentamidine analogue ((Ca)S100B·17), this same channel was open. The (Ca)S100B·17 structure illustrates, for the first time, a pentamidine analog capable of binding the "open" form of the "FF-gate" and provides a means to block all three "hot spots" on (Ca)S100B, which will impact next generation (Ca)S100B·p53 inhibitor design.

Published

2016

5. Covalent small molecule inhibitors of Ca(2+)-bound S100B.

Author

Cavalier MC, Pierce AD, Wilder PT, Alasady MJ, Hartman KG, Neau DB, Foley TL, Jadhav A, Maloney DJ, Simeonov A, Toth EA, and Weber DJ

Subjects

Animals, Benzophenanthridines chemistry, Benzophenanthridines pharmacology, Benzoquinones chemistry, Benzoquinones pharmacology, Binding Sites, Calcium metabolism, Cations, Divalent, Cattle, Cell Line, Tumor, Cell Proliferation drug effects, Crystallography, X-Ray, Disulfiram chemistry, Disulfiram pharmacology, Diterpenes chemistry, Diterpenes pharmacology, Humans, Melanoma, Models, Molecular, Protein Binding, Protein Conformation, Rats, S100 Calcium Binding Protein beta Subunit metabolism, Calcium chemistry, S100 Calcium Binding Protein beta Subunit antagonists & inhibitors, S100 Calcium Binding Protein beta Subunit chemistry

Abstract

Elevated levels of the tumor marker S100B are observed in malignant melanoma, and this EF-hand-containing protein was shown to directly bind wild-type (wt) p53 in a Ca(2+)-dependent manner, dissociate the p53 tetramer, and inhibit its tumor suppression functions. Likewise, inhibiting S100B with small interfering RNA (siRNA(S100B)) is sufficient to restore wild-type p53 levels and its downstream gene products and induce the arrest of cell growth and UV-dependent apoptosis in malignant melanoma. Therefore, it is a goal to develop S100B inhibitors (SBiXs) that inhibit the S100B-p53 complex and restore active p53 in this deadly cancer. Using a structure-activity relationship by nuclear magnetic resonance approach (SAR by NMR), three persistent binding pockets are found on S100B, termed sites 1-3. While inhibitors that simultaneously bind sites 2 and 3 are in place, no molecules that simultaneously bind all three persistent sites are available. For this purpose, Cys84 was used in this study as a potential means to bridge sites 1 and 2 because it is located in a small crevice between these two deeper pockets on the protein. Using a fluorescence polarization competition assay, several Cys84-modified S100B complexes were identified and examined further. For five such SBiX-S100B complexes, crystallographic structures confirmed their covalent binding to Cys84 near site 2 and thus present straightforward chemical biology strategies for bridging sites 1 and 3. Importantly, one such compound, SC1982, showed an S100B-dependent death response in assays with WM115 malignant melanoma cells, so it will be particularly useful for the design of SBiX molecules with improved affinity and specificity.

Published

2014

6. Molecular basis of the fructose-2,6-bisphosphatase reaction of PFKFB3: transition state and the C-terminal function.

Author

Cavalier MC, Kim SG, Neau D, and Lee YH

Subjects

Aluminum Compounds chemistry, Amino Acid Sequence, Conserved Sequence, Diphosphates chemistry, Enzyme Activation, Enzyme Assays, Enzyme Stability, Escherichia coli chemistry, Fluorides chemistry, Humans, Ligands, Models, Molecular, Molecular Sequence Data, Protein Binding, Protein Isoforms chemistry, Proteolysis, Sequence Alignment, Structure-Activity Relationship, Water chemistry, Catalytic Domain, Isoenzymes chemistry, Multiprotein Complexes chemistry, Phosphofructokinase-2 chemistry

Abstract

The molecular basis of fructose-2,6-bisphosphatase (F-2,6-P(2)ase) of 6-phosphofructo-2-kinase/fructose-2,6-bisphosphatase (PFKFB) was investigated using the crystal structures of the human inducible form (PFKFB3) in a phospho-enzyme intermediate state (PFKFB3-P•F-6-P), in a transition state-analogous complex (PFKFB3•AlF(4)), and in a complex with pyrophosphate (PFKFB3•PP(i)) at resolutions of 2.45, 2.2, and 2.3 Å, respectively. Trapping the PFKFB3-P•F-6-P intermediate was achieved by flash cooling the crystal during the reaction, and the PFKFB3•AlF(4) and PFKFB3•PP(i) complexes were obtained by soaking. The PFKFB3•AlF(4) and PFKFB3•PP(i) complexes resulted in removing F-6-P from the catalytic pocket. With these structures, the structures of the Michaelis complex and the transition state were extrapolated. For both the PFKFB3-P formation and break down, the phosphoryl donor and the acceptor are located within ~5.1 Å, and the pivotal point 2-P is on the same line, suggesting an "in-line" transfer with a direct inversion of phosphate configuration. The geometry suggests that NE2 of His253 undergoes a nucleophilic attack to form a covalent N-P bond, breaking the 2O-P bond in the substrate. The resulting high reactivity of the leaving group, 2O of F-6-P, is neutralized by a proton donated by Glu322. Negative charges on the equatorial oxygen of the transient bipyramidal phosphorane formed during the transfer are stabilized by Arg252, His387, and Asn259. The C-terminal domain (residues 440-446) was rearranged in PFKFB3•PP(i), implying that this domain plays a critical role in binding of substrate to and release of product from the F-2,6-P(2) ase catalytic pocket. These findings provide a new insight into the understanding of the phosphoryl transfer reaction., (Copyright © 2011 Wiley Periodicals, Inc.)

Published

2012

7. Mechanistic insights into validoxylamine A 7'-phosphate synthesis by VldE using the structure of the entire product complex.

Author

Cavalier MC, Yim YS, Asamizu S, Neau D, Almabruk KH, Mahmud T, and Lee YH

Subjects

Amino Acid Sequence, Binding Sites, Catalytic Domain, Crystallography, X-Ray, Cyclitols metabolism, Inositol biosynthesis, Ligands, Models, Molecular, Molecular Sequence Data, Nucleotides metabolism, Streptomyces enzymology, Glycosyltransferases chemistry, Glycosyltransferases metabolism, Inositol analogs & derivatives, Inositol Phosphates biosynthesis

Abstract

The pseudo-glycosyltransferase VldE catalyzes non-glycosidic C-N coupling between an unsaturated cyclitol and a saturated aminocyclitol with the conservation of the stereochemical configuration of the substrates to form validoxylamine A 7'-phosphate, the biosynthetic precursor of the antibiotic validamycin A. To study the molecular basis of its mechanism, the three-dimensional structures of VldE from Streptomyces hygroscopicus subsp. limoneus was determined in apo form, in complex with GDP, in complex with GDP and validoxylamine A 7'-phosphate, and in complex with GDP and trehalose. The structure of VldE with the catalytic site in both an "open" and "closed" conformation is also described. With these structures, the preferred binding of the guanine moiety by VldE, rather than the uracil moiety as seen in OtsA could be explained. The elucidation of the VldE structure in complex with the entirety of its products provides insight into the internal return mechanism by which catalysis occurs with a net retention of the stereochemical configuration of the donated cyclitol.

Published

2012

8. Investigating combinatorial approaches in virtual screening on human inducible 6-phosphofructo-2-kinase/fructose-2,6-bisphosphatase (PFKFB3): a case study for small molecule kinases.

Author

Crochet RB, Cavalier MC, Seo M, Kim JD, Yim YS, Park SJ, and Lee YH

Subjects

Drug Design, Humans, Ligands, Databases, Factual, High-Throughput Screening Assays, Models, Molecular, Phosphofructokinase-2 antagonists & inhibitors, Phosphofructokinase-2 chemistry

Abstract

Efforts toward improving the predictiveness in tier-based approaches to virtual screening (VS) have mainly focused on protein kinases. Despite their significance as drug targets, small molecule kinases have been rarely tested with these approaches. In this paper, we investigate the efficacy of a pharmacophore screening-combined structure-based docking approach on the human inducible 6-phosphofructo-2-kinase/fructose-2,6-bisphosphatase, an emerging target for cancer chemotherapy. Six out of a total 1364 compounds from NCI's Diversity Set II were selected as true actives via throughput screening. Using a database constructed from these compounds, five programs were tested for structure-based docking (SBD) performance, the MOE of which showed the highest enrichments and second highest screening rates. Separately, using the same database, pharmacophore screening was performed, reducing 1364 compounds to 287 with no loss in true actives, yielding an enrichment of 4.75. When SBD was retested with the pharmacophore filtered database, 4 of the 5 SBD programs showed significant improvements to enrichment rates at only 2.5% of the database, with a 7-fold decrease in an average VS time. Our results altogether suggest that combinatorial approaches of VS technologies are easily applicable to small molecule kinases and, moreover, that such methods can decrease the variability associated with single-method SBD approaches., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011