Your search keyword '"Trusselle MN"' showing total 6 results

1. Chiral aromatase and dual aromatase-steroid sulfatase inhibitors from the letrozole template: synthesis, absolute configuration, and in vitro activity.

Author

Wood PM, Woo LW, Labrosse JR, Trusselle MN, Abbate S, Longhi G, Castiglioni E, Lebon F, Purohit A, Reed MJ, and Potter BV

Subjects

Aromatase Inhibitors chemistry, Chromatography, High Pressure Liquid, Crystallography, X-Ray, Humans, Letrozole, Molecular Structure, Nitriles chemistry, Stereoisomerism, Structure-Activity Relationship, Triazoles chemistry, Aromatase drug effects, Aromatase Inhibitors pharmacology, Nitriles pharmacology, Steryl-Sulfatase antagonists & inhibitors, Triazoles pharmacology

Abstract

To explore aromatase inhibition and to broaden the structural diversity of dual aromatase-sulfatase inhibitors (DASIs), we introduced the steroid sulfatase (STS) inhibitory pharmacophore to letrozole. Letrozole derivatives were prepared bearing bis-sulfamates or mono-sulfamates with or without adjacent substituents. The most potent of the achiral and racemic aromatase inhibitor was 40 (IC 50 = 3.0 nM). Its phenolic precursor 39 was separated by chiral HPLC, and the absolute configuration of each enantiomer was determined using vibrational and electronic circular dichroism in tandem with calculations of the predicted spectra. Of the two enantiomers, ( R)-phenol ( 39a) was the most potent aromatase inhibitor (IC 50 = 0.6 nM, comparable to letrozole), whereas the ( S)-sulfamate, ( 40b) inhibited STS most potently (IC 50 = 553 nM). These results suggest that a new structural class of DASI for potential treatment of hormone-dependent breast cancer has been identified, and this is the first report of STS inhibition by an enantiopure nonsteroidal compound.

Published

2008

2. Benzene polyphosphates as tools for cell signalling: inhibition of inositol 1,4,5-trisphosphate 5-phosphatase and interaction with the PH domain of protein kinase Balpha.

Author

Mills SJ, Vandeput F, Trusselle MN, Safrany ST, Erneux C, and Potter BV

Subjects

Binding Sites, Fluorescence Resonance Energy Transfer, Inositol Polyphosphate 5-Phosphatases, Ligands, Models, Molecular, Phosphoric Monoester Hydrolases chemistry, Phosphoric Monoester Hydrolases metabolism, Polyphosphates chemical synthesis, Protein Structure, Tertiary, Proto-Oncogene Proteins c-akt antagonists & inhibitors, Stereoisomerism, Structure-Activity Relationship, Benzene chemistry, Phosphoric Monoester Hydrolases antagonists & inhibitors, Polyphosphates chemistry, Polyphosphates pharmacology, Proto-Oncogene Proteins c-akt chemistry, Proto-Oncogene Proteins c-akt metabolism, Signal Transduction drug effects

Abstract

Novel benzene polyphosphates were synthesised as inositol polyphosphate mimics and evaluated against type-I inositol 1,4,5-trisphosphate 5-phosphatase, which only binds soluble inositol polyphosphates, and against the PH domain of protein kinase Balpha (PKBalpha), which can bind both soluble inositol polyphosphates and inositol phospholipids. The most potent trisphosphate 5-phosphatase inhibitor is benzene 1,2,4-trisphosphate (2, IC(50) of 14 microM), a potential mimic of D-myo-inositol 1,4,5-trisphosphate, whereas the most potent tetrakisphosphate Ins(1,4,5)P(3) 5-phosphatase inhibitor is benzene 1,2,4,5-tetrakisphosphate, with an IC(50) of 4 microM. Biphenyl 2,3',4,5',6-pentakisphosphate (4) was the most potent inhibitor evaluated against type I Ins(1,4,5)P(3) 5-phosphatase (IC(50) of 1 microM). All new benzene polyphosphates are resistant to dephosphorylation by type I Ins(1,4,5)P(3) 5-phosphatase. Unexpectedly, all benzene polyphosphates studied bind to the PH domain of PKBalpha with apparent higher affinity than to type I Ins(1,4,5)P(3) 5-phosphatase. The most potent ligand for the PKBalpha PH domain, measured by inhibition of biotinylated diC(8)-PtdIns(3,4)P(2) binding, is biphenyl 2,3',4,5',6-pentakisphosphate (4, K(i)=27 nm). The approximately 80-fold enhancement of binding relative to parent benzene trisphosphate is explained by the involvement of a cation-pi interaction. These new molecular tools will be of potential use in structural and cell signalling studies.

Published

2008

3. Non-steroidal aromatase inhibitors based on a biphenyl scaffold: synthesis, in vitro SAR, and molecular modelling.

Author

Jackson T, Woo LW, Trusselle MN, Purohit A, Reed MJ, and Potter BV

Subjects

Aromatase Inhibitors chemistry, Aromatase Inhibitors pharmacology, Cells, Cultured, Humans, Models, Molecular, Structure-Activity Relationship, Aromatase Inhibitors chemical synthesis, Biphenyl Compounds chemistry

Abstract

The synthesis and in vitro biological evaluation (JEG-3 cells) of a series of novel and potent aromatase inhibitors, prepared by microwave-enhanced Suzuki cross-coupling methodology, are reported. These compounds possess a biphenyl template incorporated with the haem-ligating triazolylmethyl moiety, either on its own or in combination with other substituent(s) at various positions on the phenyl rings. The most potent aromatase inhibitor reported herein has an IC(50) value of 0.12 nM, although seven of its congeners are also highly potent (IC(50)

Published

2008

4. Dual aromatase-sulfatase inhibitors based on the anastrozole template: synthesis, in vitro SAR, molecular modelling and in vivo activity.

Author

Jackson T, Woo LW, Trusselle MN, Chander SK, Purohit A, Reed MJ, and Potter BV

Subjects

Anastrozole, Animals, Aromatase Inhibitors chemical synthesis, Crystallography, X-Ray, Enzyme Inhibitors chemical synthesis, Humans, Molecular Conformation, Rats, Rats, Wistar, Structure-Activity Relationship, Aromatase drug effects, Aromatase Inhibitors chemistry, Enzyme Inhibitors chemistry, Nitriles chemistry, Sulfatases antagonists & inhibitors, Triazoles chemistry

Abstract

The synthesis and biological evaluation of a series of novel Dual Aromatase-Sulfatase Inhibitors (DASIs) are described. It is postulated that dual inhibition of the aromatase and steroid sulfatase enzymes, both responsible for the biosynthesis of oestrogens, will be beneficial in the treatment of hormone-dependent breast cancer. The compounds are based upon the Anastrozole aromatase inhibitor template which, while maintaining the haem ligating triazole moiety crucial for enzyme inhibition, was modified to include a phenol sulfamate ester motif, the pharmacophore for potent irreversible steroid sulfatase inhibition. Adaption of a synthetic route to Anastrozole was accomplished via selective radical bromination and substitution reactions to furnish a series of aromatase inhibitory pharmacophores. Linking these fragments to the phenol sulfamate ester moiety employed SN2, Heck and Mitsunobu reactions with phenolic precursors, from where the completed DASIs were achieved via sulfamoylation. In vitro, the lead compound, 11, had a high degree of potency against aromatase (IC50 3.5 nM), comparable with that of Anastrozole (IC50 1.5 nM) whereas, only moderate activity against steroid sulfatase was found. However, in vivo, 11 surprisingly exhibited potent dual inhibition. Compound 11 was modelled into the active site of a homology model of human aromatase and the X-ray crystal structure of steroid sulfatase.

Published

2007

5. Dual aromatase-sulfatase inhibitors based on the anastrozole template: synthesis, in vitro SAR, molecular modelling and in vivo activity.

Author

Jackson T, Woo LW, Trusselle MN, Chander SK, Purohit A, Reed MJ, and Potter BV

Subjects

Anastrozole, Aromatase Inhibitors chemistry, Enzyme Inhibitors chemistry, Magnetic Resonance Spectroscopy, Models, Molecular, Spectrometry, Mass, Electrospray Ionization, Structure-Activity Relationship, Aromatase Inhibitors chemical synthesis, Aromatase Inhibitors pharmacology, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Nitriles chemistry, Sulfatases antagonists & inhibitors, Triazoles chemistry

Abstract

The synthesis and biological evaluation of a series of novel Dual Aromatase-Sulfatase Inhibitors (DASIs) are described. It is postulated that dual inhibition of the aromatase and steroid sulfatase enzymes, both responsible for the biosynthesis of oestrogens, will be beneficial in the treatment of hormone-dependent breast cancer. The compounds are based upon the Anastrozole aromatase inhibitor template which, while maintaining the haem ligating triazole moiety crucial for enzyme inhibition, was modified to include a phenol sulfamate ester motif, the pharmacophore for potent irreversible steroid sulfatase inhibition. Adaption of a synthetic route to Anastrozole was accomplished via selective radical bromination and substitution reactions to furnish a series of inhibitory aromatase pharmacophores. Linking these fragments to the phenol sulfamate ester moiety employed S(N)2, Heck and Mitsunobu reactions with phenolic precursors, from where the completed DASIs were achieved via sulfamoylation. In vitro, the lead compound, 11, had a high degree of potency against aromatase (IC(50) 3.5 nM), comparable with that of Anastrozole (IC(50) 1.5 nM) whereas, only moderate activity against steroid sulfatase was found. However, in vivo, 11 surprisingly exhibited potent dual inhibition. Compound 11 was modelled into the active site of a homology model of human aromatase and the X-ray crystal structure of steroid sulfatase.

Published

2007

6. Novel inositol phospholipid headgroup surrogate crystallized in the pleckstrin homology domain of protein kinase Balpha.

Author

Mills SJ, Komander D, Trusselle MN, Safrany ST, van Aalten DM, and Potter BV

Subjects

Crystallization, Crystallography, X-Ray, Humans, Models, Molecular, Organophosphates chemistry, Organophosphates metabolism, Protein Structure, Tertiary physiology, Proto-Oncogene Proteins c-akt antagonists & inhibitors, Phosphatidylinositol Phosphates metabolism, Proto-Oncogene Proteins c-akt chemistry

Abstract

Protein kinase B (PKB/Akt) plays a key role in cell signaling. The PH domain of PKB binds phosphatidylinositol 3,4,5-trisphosphate translocating PKB to the plasma membrane for activation by 3-phosphoinositide-dependent protein kinase 1. The crystal structure of the headgroup inositol 1,3,4,5-tetrakisphosphate Ins(1,3,4,5)P4-PKB complex facilitates in silico ligand design. The novel achiral analogue benzene 1,2,3,4-tetrakisphosphate (Bz(1,2,3,4)P4) possesses phosphate regiochemistry different from that of Ins(1,3,4,5)P4 and surprisingly binds with similar affinity as the natural headgroup. Bz(1,2,3,4)P4 co-crystallizes with the PKBalpha PH domain in a fashion also predictable in silico. The 2-phosphate of Bz(1,2,3,4)P4 does not interact with any residue, and the D5-phosphate of Ins(1,3,4,5)P4 is not mimicked by Bz(1,2,3,4)P4. Bz(1,2,3,4)P4 is an example of a simple inositol phosphate surrogate crystallized in a protein, and this approach could be applied to design modulators of inositol polyphosphate binding proteins.

Published

2007