Your search keyword '"Abdul H. Fauq"' showing total 143 results

1. NOTCH1 can initiate NF-kappaB activation via cytosolic interactions with components of the T cell signalosome

Author

Lisa M Minter, Hyun Mu Shin, Mulualem E Tilahun, Ok Hyun Cho, Karthik eChandiran, Christina Arieta Kuksin, Shilpa eKeerthivasan, Abdul H Fauq, Todd E Golde, Lucio eMiele, Margot eThome, and Barbara A Osborne

Subjects

T cell, PKCθ, NF-B, NOTCH1, non-canonical, CARMA1, Immunologic diseases. Allergy, RC581-607

Abstract

T cell stimulation requires the input and integration of external signals. Signaling through the T cell receptor (TCR) is known to induce formation of the membrane-tethered CBM complex, comprising CARMA1, BCL10 and MALT1, which is required for TCR-mediated NF-kappaB activation. TCR signaling has been shown to activate NOTCH proteins, transmembrane receptors also implicated in NF-kappaB activation. However, the link between TCR-mediated NOTCH signaling and early events leading to induction of NF-kappaB activity remains unclear. In this report, we demonstrate a novel cytosolic function for NOTCH1 and show that it is essential to CBM complex formation. Using a model of skin allograft rejection, we show in vivo that NOTCH1 acts in the same functional pathway as PKCtheta, a T cell-specific kinase important for CBM assembly and classical NF-kappaB activation. We further demonstrate in vitro NOTCH1 associates physically with PKCtheta and CARMA1 in the cytosol. Unexpectedly, when NOTCH1 expression was abrogated using RNAi approaches, interactions between CARMA1, BCL10 and MALT1 were lost. This failure in CBM assembly reduced IkappaBalpha phosphorylation and diminished NF-kappaB-DNA binding. Finally, using a luciferase gene reporter assay, we show the intracellular domain of NOTCH1 can initiate robust NF-kappaB activity in stimulated T cells, even when NOTCH1 is excluded from the nucleus through modifications that restrict it to the cytoplasm or hold it tethered to the membrane. Collectively, these observations provide evidence that NOTCH1 may facilitate early events during T cell activation by nucleating the CBM complex and initiating NF-kappaB signaling.

Published

2014

2. Non-canonical Notch signaling drives activation and differentiation of peripheral CD4+ T cells

Author

Anushka eDongre, Lalitha eSurampudi, Rebecca G Lawlor, Abdul H Fauq, Lucio eMiele, Todd E Golde, Lisa M Minter, and Barbara A Osborne

Subjects

differentiation, activation, CD4+ T cell, NOTCH1, non-canonical, Immunologic diseases. Allergy, RC581-607

Abstract

Cleavage of the Notch receptor via a γ-secretase, results in the release of the active intra-cellular domain of Notch that migrates to the nucleus and interacts with RBP-JΚ, resulting in the activation of downstream target genes. This canonical Notch signaling pathway has been documented to influence T-cell development and function. However, the mechanistic details underlying this process remain obscure. In addition to RBP-JΚ, the intra-cellular domain of Notch also interacts with other proteins in the cytoplasm and nucleus, giving rise to the possibility of a alternate, RBP-JΚ independent Notch pathways. However, the contribution of such RBP-JΚ independent, non-canonical Notch signaling in regulating peripheral T-cell responses is unknown. In this report we specifically demonstrate the requirement of Notch1 for regulating signal strength and signaling events distal to the T-cell receptor in peripheral CD4+ T cells. By using mice with a conditional deletion in Notch1 or RBP-JΚ, we show that Notch1 regulates activation and proliferation of CD4+ T cells independently of RBP-JΚ. Furthermore, differentiation to TH1 and iTreg lineages although Notch dependent, is RBP-JΚ independent. Our striking observations demonstrate that many of the cell intrinsic functions of Notch occur independently of RBP-JΚ.. Such non-canonical regulation of these processes likely occurs through NF-ΚB. This reveals a previously unknown, novel role of non-canonical Notch signaling in regulating peripheral T-cell responses.

Published

2014

3. Synthesis of E -stilbene azomethines as potent antimicrobial and antioxidant agents

Author

Ahsan Iqbal, Shakeel Ahmad Khan, Abdul H. Fauq, Muhammad Usman, Sohail Anjum Shahzad, Ayesha Bari, Muhammad Aamir Sajid, and Zulfiqar Ali Khan

Subjects

Antioxidant, 010405 organic chemistry, (E)-Stilbene, medicine.medical_treatment, General Chemistry, 010402 general chemistry, Antimicrobial, 01 natural sciences, 0104 chemical sciences, chemistry.chemical_compound, chemistry, medicine, Organic chemistry, $E$-Stilbenes,azomethine analogues,Mizoroki--Heck reaction,antimicrobial activity,antioxidant activity

Abstract

A series of new extensively conjugated $E$-stilbene azomethines (5a-5h) were synthesized and screened for their antioxidant and antimicrobial activity. The compounds were tested against bacterial (Escherichia coli, Staphylococcus aureus, Klebsiella pneumoniae, and Bacillus subtilis) and fungal strains (Aspergillus niger, A. flavus, and Trichoderma harzianum) using the agar well diffusion method. Among the tested compounds, $N$'-(4-nitrobenzylidene)-2-(($E)$-styryl)benzohydrazide (5g) was found to possess potent antimicrobial activity higher than some drugs with significant activity reported in the literature, e.g., cefradine and terbinafine hydrochloride. Additionally, compounds 5a-5h were also evaluated for antioxidant potential using DPPH free radical scavenging and ferric thiocyanate (FTC) assays. Among these, $N$'-(4-hydroxybenzylidene)-2-(($E)$-styryl)benzohydrazide (5e) exhibited significant antioxidant potential by both assays. Compound 5e demonstrated higher DPPH free radical scavenging activity (IC$_{50} = 22 \pm 0.19 \mu$ g/m) than the standard, butylated hydroxytoluene (BHT; IC$_{50} =28 \pm 0.10 \mu$ g/mL). A similar trend was observed for compound 5e in FTC assay, which exhibited 86 $\pm$ 0.19% inhibition, whereas the BHT control showed 81 $\pm$ 0.21% inhibition of linoleic acid peroxidase. The structure elucidation of the synthesized compounds was carried out by UV-Vis, FT-IR, $^{1}$H NMR, $^{13}$C NMR, and elemental analysis and mass spectrometry. These results suggest possible use of these compounds for the rational design of new antimicrobial and antioxidant agents.

Published

2018

4. Decarbamoylation of acetylcholinesterases is markedly slowed as carbamoyl groups increase in size

Author

Joseph L. Johnson, Kunisi S. Venkatasubban, Jamie L. Thomas, Terrone L. Rosenberry, Abdul H. Fauq, and Bernadette Cusack

Subjects

0301 basic medicine, Carbamate, Conformational change, medicine.medical_treatment, Biophysics, Biochemistry, Medicinal chemistry, Article, Cell Line, Serine, 03 medical and health sciences, chemistry.chemical_compound, Hydrolysis, Catalytic Domain, medicine, Animals, Humans, Molecular Biology, Enzyme Assays, chemistry.chemical_classification, Protein Carbamylation, 030102 biochemistry & molecular biology, biology, Leaving group, Active site, Acetylcholinesterase, Kinetics, Enzyme, chemistry, biology.protein, Drosophila, Carbamates

Abstract

Carbamates are esters of substituted carbamic acids that react with acetylcholinesterase (AChE) by initially transferring the carbamoyl group to a serine residue in the enzyme active site accompanied by loss of the carbamate leaving group followed by hydrolysis of the carbamoyl enzyme. This hydrolysis, or decarbamoylation, is relatively slow, and half-lives of carbamoylated AChEs range from 4 min to more than 30 days. Therefore, carbamates are effective AChE inhibitors that have been developed as insecticides and as therapeutic agents. We show here, in contrast to a previous report, that decarbamoylation rate constants are independent of the leaving group for a series of carbamates with the same carbamoyl group. When the alkyl substituents on the carbamoyl group increased in size from N -monomethyl- to N , N -dimethyl-, N -ethyl- N -methyl-, or N , N -diethyl-, the decarbamoylation rate constants decreased by 4-, 70-, and 800-fold, respectively. We suggest that this relationship arises as a result of active site distortion, particularly in the acyl pocket of the active site. Furthermore, solvent deuterium oxide isotope effects for decarbamoylation decreased from 2.8 for N -monomethylcarbamoyl AChE to 1.1 for N , N -diethylcarbamoyl AChE, indicating a shift in the rate-limiting step from general acid-base catalysis to a likely conformational change in the distorted active site.

Published

2018

5. Designed inhibitors of insulin-degrading enzyme regulate the catabolism and activity of insulin.

Author

Malcolm A Leissring, Enrico Malito, Sabrine Hedouin, Lael Reinstatler, Tomoko Sahara, Samer O Abdul-Hay, Shakeel Choudhry, Ghulam M Maharvi, Abdul H Fauq, Malwina Huzarska, Philip S May, Sungwoon Choi, Todd P Logan, Benjamin E Turk, Lewis C Cantley, Marika Manolopoulou, Wei-Jen Tang, Ross L Stein, Gregory D Cuny, and Dennis J Selkoe

Subjects

Medicine, Science

Abstract

Insulin is a vital peptide hormone that is a central regulator of glucose homeostasis, and impairments in insulin signaling cause diabetes mellitus. In principle, it should be possible to enhance the activity of insulin by inhibiting its catabolism, which is mediated primarily by insulin-degrading enzyme (IDE), a structurally and evolutionarily distinctive zinc-metalloprotease. Despite interest in pharmacological inhibition of IDE as an attractive anti-diabetic approach dating to the 1950s, potent and selective inhibitors of IDE have not yet emerged.We used a rational design approach based on analysis of combinatorial peptide mixtures and focused compound libraries to develop novel peptide hydroxamic acid inhibitors of IDE. The resulting compounds are approximately 10(6) times more potent than existing inhibitors, non-toxic, and surprisingly selective for IDE vis-à-vis conventional zinc-metalloproteases. Crystallographic analysis of an IDE-inhibitor complex reveals a novel mode of inhibition based on stabilization of IDE's "closed," inactive conformation. We show further that pharmacological inhibition of IDE potentiates insulin signaling by a mechanism involving reduced catabolism of internalized insulin.The inhibitors we describe are the first to potently and selectively inhibit IDE or indeed any member of this atypical zinc-metalloprotease superfamily. The distinctive structure of IDE's active site, and the mode of action of our inhibitors, suggests that it may be possible to develop inhibitors that cross-react minimally with conventional zinc-metalloproteases. Significantly, our results reveal that insulin signaling is normally regulated by IDE activity not only extracellularly but also within cells, supporting the longstanding view that IDE inhibitors could hold therapeutic value for the treatment of diabetes.

Published

2010

6. Therapeutic targeting of NOTCH signaling ameliorates immune-mediated bone marrow failure of aplastic anemia

Author

Chester Andrzejewski, Todd E. Golde, Lucio Miele, Emily R. Roberts, Abdul H. Fauq, Janani Srinivasan, Lisa M. Minter, Gabriela Gonzalez-Perez, Justine E. Roderick, Anushka Dongre, and Christina Arieta Kuksin

Subjects

Male, Cellular differentiation, Immunology, Notch signaling pathway, Mice, Transgenic, Biology, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Bone Marrow, hemic and lymphatic diseases, medicine, Animals, Humans, Immunology and Allergy, Enzyme Inhibitors, Receptor, Notch1, Aplastic anemia, Transcription factor, 030304 developmental biology, Mice, Knockout, Mice, Inbred BALB C, 0303 health sciences, Hematopoietic Stem Cell Transplantation, Bone marrow failure, Anemia, Aplastic, medicine.disease, 3. Good health, Mice, Inbred C57BL, Disease Models, Animal, medicine.anatomical_structure, embryonic structures, cardiovascular system, Cancer research, Female, sense organs, Bone marrow, biological phenomena, cell phenomena, and immunity, Amyloid Precursor Protein Secretases, Signal transduction, Signal Transduction, 030215 immunology

Abstract

Notch1 signaling sustains the proinflammatory behavior of Th1 cells, implicated in the development of aplastic anemia in humans and mice., Severe aplastic anemia (AA) is a bone marrow (BM) failure (BMF) disease frequently caused by aberrant immune destruction of blood progenitors. Although a Th1-mediated pathology is well described for AA, molecular mechanisms driving disease progression remain ill defined. The NOTCH signaling pathway mediates Th1 cell differentiation in the presence of polarizing cytokines, an action requiring enzymatic processing of NOTCH receptors by γ-secretase. Using a mouse model of AA, we demonstrate that expression of both intracellular NOTCH1IC and T-BET, a key transcription factor regulating Th1 cell differentiation, was increased in spleen and BM-infiltrating T cells during active disease. Conditionally deleting Notch1 or administering γ-secretase inhibitors (GSIs) in vivo attenuated disease and rescued mice from lethal BMF. In peripheral T cells from patients with untreated AA, NOTCH1IC was significantly elevated and bound to the TBX21 promoter, showing NOTCH1 directly regulates the gene encoding T-BET. Treating patient cells with GSIs in vitro lowered NOTCH1IC levels, decreased NOTCH1 detectable at the TBX21 promoter, and decreased T-BET expression, indicating that NOTCH1 signaling is responsive to GSIs during active disease. Collectively, these results identify NOTCH signaling as a primary driver of Th1-mediated pathogenesis in AA and may represent a novel target for therapeutic intervention.

Published

2013

7. Gedunin Inactivates the Co-chaperone p23 Protein Causing Cancer Cell Death by Apoptosis

Author

Abdul H. Fauq, Laura B. Peterson, Ahmed Chadli, Chaitanya A. Patwardhan, Charles A. Miller, and Brian S. J. Blagg

Subjects

Limonins, Models, Molecular, congenital, hereditary, and neonatal diseases and abnormalities, Blotting, Western, Cell, Apoptosis, Plasma protein binding, Biochemistry, Caspase 7, Mice, Hsp27, Cell Line, Tumor, Neoplasms, polycyclic compounds, Sf9 Cells, medicine, Animals, Humans, HSP70 Heat-Shock Proteins, HSP90 Heat-Shock Proteins, skin and connective tissue diseases, Molecular Biology, Cells, Cultured, Binding Sites, biology, Cell Biology, Hsp90, Protein Structure, Tertiary, Cell biology, medicine.anatomical_structure, Microscopy, Fluorescence, Protein Structure and Folding, Mutation, Cancer cell, MCF-7 Cells, biology.protein, Signal transduction, HeLa Cells, Molecular Chaperones, Protein Binding, Signal Transduction

Abstract

Pharmacological inhibition of Hsp90 is an exciting option for cancer therapy. The clinical efficacy of Hsp90 inhibitors is, however, less than expected. Binding of the co-chaperone p23 to Hsp90 and induced overexpression of anti-apoptotic proteins Hsp70 and Hsp27 are thought to contribute to this outcome. Herein, we report that the natural product gedunin may provide a new alternative to inactivate the Hsp90 machine. We show that gedunin directly binds to p23 and inactivates it, without overexpression of Hsp27 and relatively modest induction of Hsp70. Using molecular docking and mutational analysis, we mapped the gedunin-binding site on p23. Functional analysis shows that gedunin inhibits the p23 chaperoning activity, blocks its cellular interaction with Hsp90, and interferes with p23-mediated gene regulation. Cell treatment with gedunin leads to cancer cell death by apoptosis through inactivation of p23 and activation of caspase 7, which cleaves p23 at the C terminus. These results provide important insight into the molecular mechanism of action of this promising lead compound.

Published

2013

8. Abca1 Deficiency Affects Alzheimer's Disease-Like Phenotype in Human ApoE4 But Not in ApoE3-Targeted Replacement Mice

Author

Nicholas F. Fitz, Muzamil Saleem, Robert Chapman, Radosveta Koldamova, Abdul H. Fauq, Iliya Lefterov, and Andrea A. Cronican

Subjects

Genetically modified mouse, Apolipoprotein E, medicine.medical_specialty, Microdialysis, Transgene, Apolipoprotein E4, Apolipoprotein E3, Enzyme-Linked Immunosorbent Assay, Mice, Transgenic, Presenilin, Amyloid beta-Protein Precursor, Mice, Alzheimer Disease, Internal medicine, Conditioning, Psychological, mental disorders, Presenilin-1, polycyclic compounds, Amyloid precursor protein, medicine, Animals, Humans, Maze Learning, Analysis of Variance, Amyloid beta-Peptides, biology, General Neuroscience, Brain, nutritional and metabolic diseases, hemic and immune systems, Articles, Fear, medicine.disease, Peptide Fragments, Mice, Inbred C57BL, Cholesterol, Phenotype, Endocrinology, Gene Expression Regulation, ABCA1, Mutation, biology.protein, ATP-Binding Cassette Transporters, lipids (amino acids, peptides, and proteins), Alzheimer's disease, Cognition Disorders, ATP Binding Cassette Transporter 1, Lipoprotein

Abstract

ATP-binding cassette transporter A1 (ABCA1) transporter regulates cholesterol efflux and is an essential mediator of high-density lipoprotein (HDL) formation. In amyloid precursor protein (APP) transgenic mice,Abca1deficiency increased amyloid deposition in the brain paralleled by decreased levels of Apolipoprotein E (ApoE). TheAPOEε4allele is the major genetic risk factor of sporadic Alzheimer's disease (AD). Here, we reveal the effect ofAbca1deficiency on phenotype in mice expressing human ApoE3 or ApoE4. We used APP/E3 and APP/E4 mice generated by crossing APP/PS1ΔE9 transgenic mice to human APOE3- and APOE4-targeted replacement mice and examinedAbca1gene dose effect on amyloid deposition and cognition. The results from two behavior tests demonstrate that lack of one copy ofAbca1significantly exacerbates memory deficits in APP/E4/Abca1−/+but not in APP/E3/Abca1−/+mice. The data for amyloid plaques and insoluble amyloid-β (Aβ) also show thatAbca1hemizygosity increases Aβ deposition only in APP/E4/Abca1−/+but not in APP/E3/Abca1−/+mice. Ourin vivomicrodialysis assays indicate thatAbca1deficiency significantly decreases Aβ clearance in ApoE4-expressing mice, while the effect ofAbca1on Aβ clearance in ApoE3-expressing mice was insignificant. In addition, we demonstrate that plasma HDL and Aβ42 levels in APP/E4/Abca1−/+mice are significantly decreased, and there is a negative correlation between plasma HDL and amyloid plaques in brain, suggesting that plasma lipoproteins may be involved in Aβ clearance. Overall, our results prove that the presence of functionalAbca1significantly influences the phenotype of APP mice expressing human ApoE4 and further substantiate therapeutic approaches in AD based on ABCA1–APOE regulatory axis.

Published

2012

9. The role of NTS2 in the development of tolerance to NT69L in mouse models for hypothermia and thermal analgesia

Author

Mona Boules, Kristin E. Smith, Abdul H. Fauq, Elliott Richelson, and Katrina Williams

Subjects

Male, Hot Temperature, Endogeny, Hypothermia, Pharmacology, Biology, Article, Body Temperature, Mice, Behavioral Neuroscience, chemistry.chemical_compound, Drug tolerance, Reaction Time, medicine, Animals, Receptors, Neurotensin, Receptor, Neurotensin, Pain Measurement, Mice, Knockout, Behavior, Animal, Drug Tolerance, Peptide Fragments, Mice, Inbred C57BL, chemistry, Female, Analgesia, medicine.symptom

Abstract

NT69L is a neurotensin (NT)(8-13) analog that binds the two major NT receptors, NTS1 and NTS2, and elicits similar behavioral effects as endogenous NT. Tolerance develops rapidly to some, but not to all of NT69L's effects, and to date, little is known about the mechanisms responsible for this tolerance. The development of tolerance appears to be more prevalent in behavioral effects mediated by NTS1 than by those mediated by NTS2, including hypothermia and thermal analgesia. However, we hypothesize that both NTS1 and NTS2 have important roles in mediating the effects of NT69L. Here, we investigate the role of NTS2 on NT69L-mediated hypothermia and thermal analgesia with the use of NTS2 knock-out mice. We show that tolerance develops to NT69L-mediated hypothermia and thermal analgesia following sub-chronic treatment in wild-type (WT) mice, and that NTS2 is necessary for the development of that tolerance. Additionally, we suggest potential means by which NTS2 influences these NT69L-mediated behaviors.

Published

2011

10. Binding of antitumor tamoxifen and its metabolites 4-hydroxytamoxifen and endoxifen to human serum albumin

Author

H.A. Tajmir-Riahi, P. Bourassa, Ghulam M. Maharvi, Abdul H. Fauq, Thekkumkat Thomas, and S. Dubeau

Subjects

Models, Molecular, Circular dichroism, Antineoplastic Agents, Hormonal, Molecular Conformation, Plasma protein binding, Biochemistry, Protein Structure, Secondary, Protein structure, Spectroscopy, Fourier Transform Infrared, medicine, Humans, Amino Acids, Binding site, Protein secondary structure, Serum Albumin, Protein Unfolding, Binding Sites, Chemistry, Circular Dichroism, Hydrogen Bonding, General Medicine, Human serum albumin, Binding constant, Protein Structure, Tertiary, Kinetics, Tamoxifen, Spectrometry, Fluorescence, Hydrophobic and Hydrophilic Interactions, Algorithms, Protein Binding, medicine.drug

Abstract

Tamoxifen is extensively metabolized, and several metabolites have been detected in human serum. The aim of this study was to examine the interaction of human serum albumin (HSA) with tamoxifen and its metabolites 4-hydroxytamoxifen and endoxifen at physiological conditions, using constant protein concentration and various drug contents. FTIR, UV-Visible, CD and fluorescence spectroscopic methods as well as molecular modeling were used to analyse drug binding mode, the binding constant and the effects of drug complexation on HSA stability and conformation. Structural analysis showed that tamoxifen and its metabolites bound HSA via both hydrophobic and hydrophilic interactions with overall binding constants of K(tam) = 1.8 (±0.2) × 10(4) M(-1), K(4-hydroxytam) = 1.8 (±0.4) × 10(4) M(-1) and K(endox) = 2.0 (±0.5) × 10(4) M(-1). The number of bound drugs per protein is 1.2 (tamoxifen), 1.7 (4-hydroxitamoxifen) and 1.0 (endoxifen). Structural modeling showed the participation of several amino acid residues in drug-HSA complexation, with extended H-bonding network. HSA conformation was altered by tamoxifen and its metabolites with a major reduction of α-helix and an increase in β-sheet, random coil and turn structures, indicating a partial protein unfolding. Our results suggest that serum albumins can act as carrier proteins for tamoxifen and its metabolites in delivering them to target tissues.

Published

2011

11. Iothalamate Quantification by Tandem Mass Spectrometry to Measure Glomerular Filtration Rate

Author

Timothy S. Larson, Bradley E. Burns, John C. Lieske, Jesse C. Seegmiller, Naveen Mukhtar, and Abdul H. Fauq

Subjects

Time Factors, Chromatography, Plasma samples, Chemistry, Biochemistry (medical), Clinical Biochemistry, Selected reaction monitoring, Electrophoresis, Capillary, Reproducibility of Results, Renal function, Urine, Tandem mass spectrometry, Mass spectrometry, Sensitivity and Specificity, Iothalamic Acid, Capillary electrophoresis, Tandem Mass Spectrometry, Humans, Centrifugation, Chromatography, Liquid, Glomerular Filtration Rate

Abstract

Background: Glomerular filtration rate (GFR) can be determined by measuring renal clearance of the radiocontrast agent iothalamate. Current analytic methods for quantifying iothalamate concentrations in plasma and urine using liquid chromatography or capillary electrophoresis have limitations such as long analysis times and susceptibility to interferences. We developed a liquid chromatography–tandem mass spectrometry (LC-MS/MS) method to overcome these limitations. Methods: Urine and plasma samples were deproteinized using acetonitrile and centrifugation. The supernatant was diluted in water and analyzed by LC-MS/MS using a water:methanol gradient. We monitored 4 multiple reaction monitoring transitions: m/z 614.8–487.0, 614.8–456.0, 614.8–361.1, and 614.8–177.1. We compared the results to those obtained via our standard capillary electrophoresis (CE-UV) on samples from 53 patients undergoing clinical GFR testing. Results: Mean recovery was 90%–110% in both urine and plasma matrices. Imprecision was ≤15% for the m/z 614.8–487.0 and 614.8–456.0 transitions over a 10-day period at 1 mg/L. Method comparison for 159 patient samples (53 clearances) provided the following Passing–Bablok regressions: plasma iothalamate LC-MS/MS (y) vs CE-UV (x), y = 0.99x + 0.36; urine iothalamate LC-MS/MS vs CE-UV, y = 1.01x + 0.31; corrected GFR LC-MS/MS vs CE-UV, y = 1.00x + 0.00. Interfering substances prevented accurate iothalamate quantification by CE-UV in 2 patients, whereas these samples could be analyzed by LC-MS/MS. Conclusions: Iothalamate can be quantified by LC-MS/MS for GFR measurement. This method circumvents potential problems with interfering substances that occasionally confound accurate GFR determinations.

Published

2010

12. Pigment Epithelium-derived Factor Maintains Retinal Pigment Epithelium Function by Inhibiting Vascular Endothelial Growth Factor-R2 Signaling through γ-Secretase

Author

Abdul H. Fauq, Zsolt Ablonczy, Kumar Sambamurti, Annamalai Prakasam, Craig E. Crosson, and J. Fant

Subjects

Vascular Endothelial Growth Factor A, medicine.medical_specialty, Swine, Retinal Pigment Epithelium, Biochemistry, Permeability, Macular Degeneration, chemistry.chemical_compound, Molecular Basis of Cell and Developmental Biology, PEDF, Internal medicine, medicine, Amyloid precursor protein, Animals, Humans, Nerve Growth Factors, Eye Proteins, Molecular Biology, Cells, Cultured, Serpins, Retinal pigment epithelium, biology, Kinase insert domain receptor, Cell Biology, Vascular Endothelial Growth Factor Receptor-2, eye diseases, Cell biology, Vascular endothelial growth factor, Vascular endothelial growth factor A, Endocrinology, medicine.anatomical_structure, chemistry, biology.protein, sense organs, Amyloid Precursor Protein Secretases, Signal transduction, Amyloid precursor protein secretase, Signal Transduction

Abstract

Wet age-related macular degeneration (AMD) attacks the integrity of the retinal pigment epithelium (RPE) barrier system. The pathogenic process was hypothesized to be mediated by vascular endothelial growth factor (VEGF) and antagonized by pigment epithelium-derived factor (PEDF). To dissect these functional interactions, monolayer cultures of RPE cells were established, and changes in transepithelial resistance were evaluated after administration of PEDF, placenta growth factor (VEGF-R1 agonist), and VEGF-E (VEGF-R2 agonist). A recently described mechanism of VEGF inhibition in endothelia required the release of VEGF-R1 intracellular domain by gamma-secretase. To evaluate this pathway in the RPE, cells were pretreated with inhibitors DAPT or LY411575. Processing of VEGF receptors was assessed by Western blot analysis. Administration of VEGF-E rapidly increased RPE permeability, and PEDF inhibited the VEGF-E response dose-dependently. Both gamma-secretase antagonists prevented the inhibitory effects of PEDF. The co-administration of PEDF and VEGF-E depleted the amount of VEGF-R2 in the membrane and increased the amount of VEGF-R2 ectodomain in the media. Therefore, the inhibitory effect of PEDF appears to be mediated via the processing of VEGF-R2 by gamma-secretase. gamma-Secretase generates the amyloid-beta (Abeta) peptide of Alzheimer disease from its precursor (amyloid precursor protein). This peptide is also a component of drusen in dry AMD. The results support the hypothesis that misregulation of gamma-secretase may not only lead to Abeta deposits in dry AMD but can also be damaging to RPE function by blocking the protective effects of PEDF to prevent VEGF from driving the dry to wet AMD transition.

Published

2009

13. Substrate-targeting γ-secretase modulators

Author

Thomas B. Ladd, Bernadette Cusack, Debra Yager, Dominic M. Walsh, Thomas Kukar, Ghulam M. Maharvi, Robert Chapman, Alfred T. Welzel, Vijayaraghavan Rangachari, Christopher B. Eckman, Wenjuan Ye, Christophe Verbeeck, Sarah A. Sagi, Maralyssa Bann, Todd E. Golde, Robert W. Price, Terrone L. Rosenberry, Boris Schmidt, Justin W. Torpey, Brent Healy, Barbara A. Cottrell, Karen Jansen-West, Jason L. Eriksen, Edward H. Koo, Abdul H. Fauq, Patrick C. Fraering, Rajeshwar Narlawar, Michael S. Wolfe, and Brenda D. Moore

Subjects

Druggability, CHO Cells, Plasma protein binding, Article, Substrate Specificity, Amyloid beta-Protein Precursor, Mice, Cricetulus, Alzheimer Disease, Cell Line, Tumor, Cricetinae, mental disorders, Animals, Humans, Binding site, Binding Sites, Multidisciplinary, Receptors, Notch, biology, Drug discovery, Anti-Inflammatory Agents, Non-Steroidal, Proteolytic enzymes, Cell biology, Biochemistry, Structural biology, Biotinylation, biology.protein, Female, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase, Protein Binding

Abstract

Selective lowering of Abeta42 levels (the 42-residue isoform of the amyloid-beta peptide) with small-molecule gamma-secretase modulators (GSMs), such as some non-steroidal anti-inflammatory drugs, is a promising therapeutic approach for Alzheimer's disease. To identify the target of these agents we developed biotinylated photoactivatable GSMs. GSM photoprobes did not label the core proteins of the gamma-secretase complex, but instead labelled the beta-amyloid precursor protein (APP), APP carboxy-terminal fragments and amyloid-beta peptide in human neuroglioma H4 cells. Substrate labelling was competed by other GSMs, and labelling of an APP gamma-secretase substrate was more efficient than a Notch substrate. GSM interaction was localized to residues 28-36 of amyloid-beta, a region critical for aggregation. We also demonstrate that compounds known to interact with this region of amyloid-beta act as GSMs, and some GSMs alter the production of cell-derived amyloid-beta oligomers. Furthermore, mutation of the GSM binding site in the APP alters the sensitivity of the substrate to GSMs. These findings indicate that substrate targeting by GSMs mechanistically links two therapeutic actions: alteration in Abeta42 production and inhibition of amyloid-beta aggregation, which may synergistically reduce amyloid-beta deposition in Alzheimer's disease. These data also demonstrate the existence and feasibility of 'substrate targeting' by small-molecule effectors of proteolytic enzymes, which if generally applicable may significantly broaden the current notion of 'druggable' targets.

Published

2008

14. Phase III Double-Blind, Randomized, Placebo-Controlled Crossover Trial of Black Cohosh in the Management of Hot Flashes: NCCTG Trial N01CC1

Author

Charles L. Loprinzi, Kendrith M. Rowland, Paul J. Novotny, Barbara A. Pockaj, Jeff A. Sloan, Tom R. Fitch, Philip J. Stella, Patrick J. Flynn, Debra L. Barton, Abdul H. Fauq, Radha M. Rao, Beth I. LaVasseur, James G. Gallagher, and Elliott Richelson

Subjects

Adult, Cimicifuga, Cancer Research, medicine.medical_specialty, Black cohosh, Breast Neoplasms, Placebo, law.invention, Double-Blind Method, Randomized controlled trial, Hot flash, law, Internal medicine, medicine, Humans, Aged, Cross-Over Studies, biology, business.industry, Middle Aged, biology.organism_classification, medicine.disease, Crossover study, Surgery, Menopause, Clinical trial, Oncology, Hot Flashes, Female, Plant Preparations, medicine.symptom, business, Phytotherapy

Abstract

Purpose Hot flashes can cause significant morbidity in postmenopausal women undergoing or finished with breast cancer treatment. Black cohosh has been used to treat hot flashes, but definitive clinical data about efficacy have been equivocal. Methods A double-blind, randomized, cross-over clinical trial with two 4-week periods, was used to study the efficacy of black cohosh (1 capsule, Cimicifuga racemosa 20 mg BID) for the treatment of hot flashes in women. Participants kept a daily hot flash diary during a baseline week and then during two 4-week crossover treatment periods. Hot flash scores were measured by assigning points (1 to 4 for mild to very severe) to each hot flash based on severity and then adding the points for a given time period. Results Between October 31, 2003, to March 4, 2004, 132 patients were randomly assigned. Toxicity was minimal and not different by treatment group. Patients receiving black cohosh reported a mean decrease in hot flash score of 20% (comparing the fourth treatment week to the baseline week) compared with a 27% decrease for patients on placebo (P = .53). Mean hot flash frequency was reduced 17% on black cohosh and 26% on placebo (P = .36). Patient treatment preferences were measured after completion of both treatment periods by ascertaining which treatment period, if any, the patient preferred. Thirty-four percent of patients preferred the black cohosh treatment, 38% preferred the placebo, and 28% did not prefer either treatment. Conclusion This trial failed to provide any evidence that black cohosh reduced hot flashes more than the placebo.

Published

2006

15. Inhibitors of γ-secretase block in vivo and in vitro T helper type 1 polarization by preventing Notch upregulation of Tbx21

Author

Stephen D. Miller, Pritam Das, Ok Hyun Cho, Todd E. Golde, Tanapat Palaga, Barbara A. Osborne, Hyun Mu Shin, Abdul H. Fauq, Lucio Miele, Katherine Simpson, Sridevi Gottipati, Danielle M. Turley, Ila Joshi, Lisa A. Kostura, Lisa M. Minter, Janice C. Telfer, Kimberly A Such, and Rebecca G. Lawlor

Subjects

biology, Chemistry, T cell, Immunology, Experimental autoimmune encephalomyelitis, Notch signaling pathway, medicine.disease, Cell biology, medicine.anatomical_structure, Downregulation and upregulation, biology.protein, medicine, Immunology and Allergy, Ectopic expression, Receptor, Amyloid precursor protein secretase, Transcription factor

Abstract

Notch receptors are processed by gamma-secretase acting in synergy with T cell receptor signaling to sustain peripheral T cell activation. Activated CD4+ T cells differentiate into T helper type 1 (TH1) or TH2 subsets. Molecular cues directing TH1 differentiation include expression of the TH1-specific transcription factor T-bet, encoded by Tbx21. However, the regulation of Tbx21 remains incompletely defined. Here we report that Notch1 can directly regulate Tbx21 through complexes formed on the Tbx21 promoter. In vitro, gamma-secretase inhibitors extinguished expression of Notch, interferon-gamma and Tbx21 in TH1-polarized CD4+ cells, whereas ectopic expression of activated Notch1 restored Tbx21 transcription. In vivo, administration of gamma-secretase inhibitors substantially impeded TH1-mediated disease progression in the mouse experimental autoimmune encephalomyelitis model of multiple sclerosis. Thus, using gamma-secretase inhibitors to modulate Notch signaling may prove beneficial in treating TH1-mediated autoimmunity.

Published

2005

16. Diverse compounds mimic Alzheimer disease–causing mutations by augmenting Aβ42 production

Author

Victor V. Ozols, Murad Ali Khan, Michael P. Murphy, Jenny Beard, Sarah A. Sagi, Pritam Das, Sami L. Merit, Jason L. Eriksen, Rajashaker Kache, Abdul H. Fauq, Tawnya E. Smith, Thomas Kukar, Mark K. Dodson, Sascha Weggen, Todd E. Golde, Edward H. Koo, Thomas B. Ladd, and Panos Z. Anastasiadis

Subjects

Enzyme-Linked Immunosorbent Assay, Endogeny, Protein Serine-Threonine Kinases, Pharmacology, Transfection, Mass Spectrometry, General Biochemistry, Genetics and Molecular Biology, Presenilin, Cell Line, Fenofibrate, Alzheimer Disease, In vivo, Endopeptidases, medicine, Aspartic Acid Endopeptidases, Humans, Immunoprecipitation, Cyclooxygenase Inhibitors, Protein precursor, Hypolipidemic Agents, Sulfonamides, rho-Associated Kinases, Amyloid beta-Peptides, business.industry, Anti-Inflammatory Agents, Non-Steroidal, Intracellular Signaling Peptides and Proteins, Brain, General Medicine, medicine.disease, In vitro, Enzyme Activation, Biochemistry, Celecoxib, Pyrazoles, Female, Amyloid Precursor Protein Secretases, Alzheimer's disease, rhoA GTP-Binding Protein, business, Antilipidemic Agent, medicine.drug

Abstract

Increased Abeta42 production has been linked to the development of Alzheimer disease. We now identify a number of compounds that raise Abeta42. Among the more potent Abeta42-raising agents identified are fenofibrate, an antilipidemic agent, and celecoxib, a COX-2-selective NSAID. Many COX-2-selective NSAIDs tested raised Abeta42, including multiple COX-2-selective derivatives of two Abeta42-lowering NSAIDs. Compounds devoid of COX activity and the endogenous isoprenoids FPP and GGPP also raised Abeta42. These compounds seem to target the gamma-secretase complex, increasing gamma-secretase-catalyzed production of Abeta42 in vitro. Short-term in vivo studies show that two Abeta42-raising compounds increase Abeta42 levels in the brains of mice. The elevations in Abeta42 by these compounds are comparable to the increases in Abeta42 induced by Alzheimer disease-causing mutations in the genes encoding amyloid beta protein precursor and presenilins, raising the possibility that exogenous compounds or naturally occurring isoprenoids might increase Abeta42 production in humans.

Published

2005

17. A Concise, High Yield Synthesis of the Selective ECE‐Inhibitor, CGS 35066

Author

Christopher B. Eckman, Murad Ali Khan, and Abdul H. Fauq

Subjects

Dibenzofuran, chemistry.chemical_compound, Chiral auxiliary, chemistry, Stereochemistry, organic chemicals, Yield (chemistry), Reagent, Organic Chemistry, Diphenyl ether, Enantiomer

Abstract

A highly efficient synthesis of the selective endothelin‐converting enzyme, CGS 35066 is described. The key steps involved a Pd‐catalyzed coupling of the phenyl rings of a diphenyl ether, and the use of the Schollkopf reagent, (2R)‐2‐isopropyl‐3,6‐dimethoxy‐2,5‐dihydropyrazine as a chiral auxiliary furnishing a dibenzofuranylmethyl substituted amino ester in high (>98%) enantiomeric purity, which was then carried forward to complete the synthesis of the ECE inhibitor CGS 35066.

Published

2004

18. Design and Chemical Synthesis of a Magnetic Resonance Contrast Agent with Enhanced in Vitro Binding, High Blood−Brain Barrier Permeability, and in Vivo Targeting to Alzheimer's Disease Amyloid Plaques

Author

Thomas M. Wengenack, Daniel J. McCormick, Joseph F. Poduslo, Jane A. Peterson, Geoffry L. Curran, Murad Ali Khan, and Abdul H. Fauq

Subjects

Gadolinium DTPA, Genetically modified mouse, Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, Contrast Media, Mice, Transgenic, Plaque, Amyloid, Peptide, Blood–brain barrier, Biochemistry, Article, Presenilin, Mice, Alzheimer Disease, In vivo, mental disorders, Presenilin-1, medicine, Animals, Humans, Caproates, chemistry.chemical_classification, Amyloid beta-Peptides, Molecular Structure, Chemistry, Brain, Membrane Proteins, medicine.disease, Peptide Fragments, medicine.anatomical_structure, Blood-Brain Barrier, Drug Design, Biophysics, Alzheimer's disease, Molecular imaging, Molecular probe

Abstract

Molecular imaging is an important new direction in medical diagnosis; however, its success is dependent upon molecular probes that demonstrate selective tissue targeting. We report the design and chemical synthesis of a derivative of human amyloid-beta (Abeta) peptide that is capable of selectively targeting individual amyloid plaques in the brain of Alzheimer's disease transgenic mice after being intravenously injected. This derivative is based on the sequence of the first 30 amino acid residues of Abeta with asparagyl/glutamyl-4-aminobutane residues (N-4ab/Q-4ab) substituted at unique Asp and Glu positions and with Gd-DTPA-aminohexanoic acid covalently attached at the N-terminal Asp. The Gd[N-4ab/Q-4ab]Abeta30 peptide was homogeneous as shown by high-resolution analytical techniques with a mass of +/-4385 Da determined by electrospray ionization mass spectrometry. This diamine- and gadolinium-substituted derivative of Abeta is shown to have enhanced in vitro binding to Alzheimer's disease (AD) amyloid plaques and increased in vivo permeability at the blood-brain barrier because of the unique Asp/Glu substitutions. In addition, specific in vivo targeting to AD amyloid plaques is demonstrated throughout the brain of an APP, PS1 transgenic mouse after intravenous injection. Because of the magnetic resonance (MR) imaging contrast enhancement provided by gadolinium, this derivative should enable the in vivo MR imaging of individual amyloid plaques in the brains of AD animals or patients to allow for early diagnosis and also provide a direct measure of the efficacy of anti-amyloid therapies currently being developed.

Published

2004

19. Down-Regulation of Amyloid Precursor Protein by Peptide Nucleic Acid In Vivo

Author

Elliott Richelson, Katrina Williams, Elisa Gollatz, Abdul H. Fauq, and Mona Boules

Subjects

Male, Peptide Nucleic Acids, Transcription, Genetic, Down-Regulation, Peptide, Rats, Sprague-Dawley, Amyloid beta-Protein Precursor, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Alzheimer Disease, mental disorders, Sense (molecular biology), Reaction Time, Amyloid precursor protein, Animals, RNA, Messenger, Protein Synthesis Inhibitors, chemistry.chemical_classification, Messenger RNA, biology, Peptide nucleic acid, P3 peptide, Brain, DNA, General Medicine, Molecular biology, Rats, Blot, Antisense Elements (Genetics), chemistry, Protein Biosynthesis, biology.protein, Nucleic acid

Abstract

Alzheimer's disease (AD) is a neurodegenerative disease associated with increased expression of amyloid precursor protein (APP) and the deposition of its proteolytic cleavage products, the amyloid-beta peptides, Abeta(1-40) and Abeta(1-42). Peptide nucleic acids (PNAs) have been shown to block the expression of proteins at transcriptional and translational levels. In this study we used a sense and an antisense PNA specifically targeted to APP to inhibit the transcription and translation of APP by complementary binding to DNA or mRNA, respectively. Using Western blotting, APP showed a drastic decrease (50% and 90% reduction, in two separate experiments, as compared with saline control) with the injection of sense APP. mRNA levels were higher at the same time point after injection of APP sense PNA, most probably because of a compensatory mechanism in response to the drop of APP that might have occurred at an earlier time point (0-1 h) and was reflected in a drop at the protein level at 1 h. The injection of antisense PNA showed about 70% decrease in APP as measured by Western blotting. Unmodified PNA can be used in vivo to reduce the levels of APP, which plays a critical role in the development of AD.

Published

2004

20. Inhibitors Tethered Near the Acetylcholinesterase Active Site Serve as Molecular Rulers of the Peripheral and Acylation Sites

Author

Arno F. Spatola, Joseph L. Johnson, Peteris Romanovskis, Elizabeth H. McCullough, Thomas F. Hughes, Bernadette Cusack, Abdul H. Fauq, and Terrone L. Rosenberry

Subjects

Models, Molecular, Molecular model, Stereochemistry, Ligands, Biochemistry, Acylation, chemistry.chemical_compound, Non-competitive inhibition, Cations, medicine, Humans, Cysteine, Disulfides, Binding site, Molecular Biology, Binding Sites, Models, Statistical, Dose-Response Relationship, Drug, biology, Chemistry, Hydrolysis, Active site, Cell Biology, Acetylcholinesterase, Recombinant Proteins, Kinetics, Models, Chemical, Tacrine, Mutation, Mutagenesis, Site-Directed, biology.protein, Propidium, Protein Binding, medicine.drug

Abstract

The acetylcholinesterase (AChE) active site consists of a narrow gorge with two separate ligand binding sites: an acylation site (or A-site) at the bottom of the gorge where substrate hydrolysis occurs and a peripheral site (or P-site) at the gorge mouth. AChE is inactivated by organophosphates as they pass through the P-site and phosphorylate the catalytic serine in the A-site. One strategy to protect against organophosphate inactivation is to design cyclic ligands that will bind specifically to the P-site and block the passage of organophosphates but not acetylcholine. To accelerate the process of identifying cyclic compounds with high affinity for the AChE P-site, we introduced a cysteine residue near the rim of the P-site by site-specific mutagenesis to generate recombinant human H287C AChE. Compounds were synthesized with a highly reactive methanethiosulfonyl substituent and linked to this cysteine through a disulfide bond. The advantages of this tethering were demonstrated with H287C AChE modified with six compounds, consisting of cationic trialkylammonium, acridinium, and tacrine ligands with tethers of varying length. Modification by ligands with short tethers had little effect on catalytic properties, but longer tethering resulted in shifts in substrate hydrolysis profiles and reduced affinity for acridinium affinity resin. Molecular modeling calculations indicated that cationic ligands with tethers of intermediate length bound to the P-site, whereas those with long tethers reached the A-site. These binding locations were confirmed experimentally by measuring competitive inhibition constants K I2 for propidium and tacrine, inhibitors specific for the P- and A-sites, respectively. Values of K I2 for propidium increased 30- to 100-fold when ligands had either intermediate or long tethers. In contrast, the value of K I2 for tacrine increased substantially only when ligands had long tethers. These relative changes in propidium and tacrine affinities thus provided a sensitive molecular ruler for assigning the binding locations of the tethered cations.

Published

2003

21. Selective tolerance to the hypothermic and anticataleptic effects of a neurotensin analog that crosses the blood–brain barrier

Author

Lewis Warrington, Daniel J. McCormick, Rui Wang, Jennifer A. Stewart, Sally Yerbury, Mona Boules, Elliott Richelson, Abdul H. Fauq, and Beth M. McMahon

Subjects

Blood Glucose, Male, medicine.medical_specialty, Time Factors, Hypothermia, Hyperkinesis, Catalepsy, Blood–brain barrier, Body Temperature, Rats, Sprague-Dawley, chemistry.chemical_compound, Cocaine, Internal medicine, medicine, Haloperidol, Animals, Amphetamine, Molecular Biology, Neurotensin, Behavior, Animal, business.industry, General Neuroscience, Brain, Drug Tolerance, medicine.disease, Peptide Fragments, Rats, Apomorphine, medicine.anatomical_structure, Endocrinology, chemistry, Blood-Brain Barrier, Dopamine receptor, Neurology (clinical), medicine.symptom, business, Developmental Biology, medicine.drug

Abstract

NT69L, a neurotensin analog that crosses the blood–brain barrier, reduces body temperature, reverses apomorphine-induced climbing, haloperidol-induced catalepsy, and d -amphetamine- and cocaine-induced locomotor activity in rats. In this study we tested the development of tolerance to these effects of NT69L in rats. The blockade of apomorphine-induced climbing behavior and d -amphetamine- and cocaine-induced hyperactivity seen after a single acute injection did not show significant change with repeated daily injections of NT69L. Thus, for example, NT69L after five daily injections at a fixed dosage was as effective at reversing cocaine-induced hyperactivity as after the first injection. On the other hand, repeated daily injections of NT69L resulted in a diminished hypothermic response and a diminished anticataleptic effect against haloperidol. The effect of NT69L on blood glucose, cortisol, and thyroxine (T4) were all back to control levels after five daily injections. Thus, tolerance developed to NT69L after the first injection, when it was tested for causing hypothermia, blockade of haloperidol-induced catalepsy, and change in blood glucose, cortisol and T4 levels. Since tolerance did not develop to the effects of drugs acting as direct (apomorphine) or indirect ( d -amphetamine and cocaine) agonists at dopamine receptors over the course of 5 days, these findings suggest a selective role of neurotensin in the modulation of dopamine neurotransmission. Furthermore, due to the lack of development of tolerance, NT69L or similar analogs might be useful in modulating certain behavioral effects of psychostimulants or have potential use as an antipsychotic drug in humans.

Published

2003

22. Peptide-based, irreversible inhibitors of γ-secretase activity

Author

Siân C. Piper, Zareen Amtul, Abdul H. Fauq, Marjorie J. Rochette, Laura Galiñanes-Garcia, M. Paul Murphy, Victor Howard, Chris McLendon, Todd E. Golde, and Chewki Ziani-Cherif

Subjects

Enzyme complex, medicine.medical_treatment, Biophysics, Peptide, CHO Cells, Biochemistry, Presenilin, Cricetinae, Endopeptidases, Tumor Cells, Cultured, medicine, Animals, Aspartic Acid Endopeptidases, Humans, Enzyme Inhibitors, APH-1, Molecular Biology, chemistry.chemical_classification, Protease, Dose-Response Relationship, Drug, Receptors, Notch, biology, Chemistry, Membrane Proteins, Active site, Cell Biology, Transmembrane protein, Kinetics, Enzyme, biology.protein, Epoxy Compounds, Amyloid Precursor Protein Secretases, Oligopeptides

Abstract

The characterization of the enzymes responsible for amyloid beta-peptide (Abeta) production is considered to be a primary goal towards the development of future therapeutics for the treatment of Alzheimer's disease. Inhibitors of gamma-secretase activity were critical in demonstrating that the presenilins (PSs) likely comprised at least part of the active site of the gamma-secretase enzyme complex, with two highly conserved membrane aspartates presumably acting as catalytic residues. However, whether or not these aspartates are actually the catalytic residues of the enzyme complex or are merely essential for normal PS function and/or maturation is still unknown. In this paper, we report the development of reactive inhibitors of gamma-secretase activity that are functionally irreversible. Since such inhibitors have been shown to bind catalytic residues in other aspartyl proteases (e.g., HIV protease), they might be used to determine if the transmembrane aspartates of PSs are involved directly in substrate cleavage.

Published

2003

23. Neurotensin analog selective for hypothermia over antinociception and exhibiting atypical neuroleptic-like properties

Author

Lewis Warrington, Daniel J. McCormick, Jennifer A. Stewart, Elliott Richelson, Mona Boules, Joshua G. Jackson, Beth M. McMahon, and Abdul H. Fauq

Subjects

Male, Serotonin, medicine.medical_specialty, Dopamine, Prefrontal Cortex, Hypothermia, Catalepsy, Serotonergic, Dopamine agonist, Body Temperature, Rats, Sprague-Dawley, chemistry.chemical_compound, Internal medicine, medicine, Haloperidol, Animals, Neurotensin receptor, Molecular Biology, Neurotensin, Analgesics, Dose-Response Relationship, Drug, Chemistry, General Neuroscience, medicine.disease, Corpus Striatum, Peptide Fragments, Rats, Apomorphine, Endocrinology, Blood-Brain Barrier, Neurology (clinical), Injections, Intraperitoneal, Antipsychotic Agents, Developmental Biology, medicine.drug

Abstract

Neurotensin (NT) is a tridecapeptide neurotransmitter in the central nervous system. It has been implicated in the therapeutic effects of neuroleptics. Central activity of NT can only be demonstrated by direct injection into the brain, since it is readily degraded by peptidases in the periphery. We have developed many NT(8-13) analogs that are resistant to peptidase degradation and can cross the blood-brain barrier (BBB). In this study, we report on one of these analogs, NT77L. NT77L induced hypothermia (ED(50)=6.5 mg/kg, i.p.) but induced analgesia only at the highest dose examined (20 mg/kg, i.p.). Like the atypical neuroleptic clozapine, NT77L blocked the climbing behavior in rats induced by the dopamine agonist apomorphine (600 microg/kg) with an ED(50) of 5.6 mg/kg (i.p.), without affecting the licking and the sniffing behaviors. By itself NT77L did not cause catalepsy, but it moderately reversed haloperidol-induced catalepsy with an ED(50) of 6.0 mg/kg (i.p.). Haloperidol alone did not lower body temperature, but it potentiated the body temperature lowering effect of NT77L. In studies using in vivo microdialysis NT77L showed similar effects on dopamine turnover to those of clozapine, and significantly different from those of haloperidol in the striatum. In the prefrontal cortex, NT77L significantly increased serotonergic transmission as evidenced by increased 5-hydroxyindole acetic acid:5-hydroxytryptamine (5-HIAA:5-HT) ratio. Thus, NT77L selectively caused hypothermia, over antinociception, while exhibiting atypical neuroleptic-like effects.

Published

2001

24. Altering behavioral responses and dopamine transporter protein with antisense peptide nucleic acids 1 1Abbreviations: DAT, dopamine transporter; and PNA, peptide nucleic acid

Author

Joshua G. Jackson, Jennifer A. Stewart, Beth M Tyler-McMahon, Daniel J. McCormick, Abdul H. Fauq, M.D. Bitner, and Elliott Richelson

Subjects

Pharmacology, chemistry.chemical_classification, Peptide nucleic acid, musculoskeletal, neural, and ocular physiology, Motility, Peptide, Biology, Biochemistry, Molecular biology, chemistry.chemical_compound, chemistry, Dopamine, biological sciences, cardiovascular system, medicine, Catecholamine, Nucleic acid, biology.protein, Amphetamine, tissues, medicine.drug, Dopamine transporter

Abstract

The dopamine transporter (DAT) plays a role in locomotion and is an obligatory target for amphetamines. We designed and synthesized an antisense peptide nucleic acid (PNA) to rat DAT to examine the effect of this antisense molecule on locomotion and on responsiveness to amphetamines. Rats were injected intraperitoneally daily for 9 days with either saline, an antisense DAT PNA, a scrambled DAT PNA, or a mismatch DAT PNA. On days 7 and 9 after initial motility measurements were taken, the animals were challenged with 10 mg/kg of amphetamine and scored for motility. On day 7, there was no significant difference between the baseline levels of activity of any of the groups or their responses to amphetamine. On day 9, the antisense PNA-treated rats showed a statistically significant increase in their resting motility (P < 0.01). When these rats were challenged with amphetamine, motility of the saline-, scrambled PNA-, and mismatch PNA-treated animals showed increases of 31-, 36-, and 20-fold, respectively, while the antisense PNA-treated animals showed increases of only 3.4-fold (P < 0.01). ELISA results revealed a 32% decrease in striatal DAT in antisense PNA-treated rats compared with the saline, scrambled PNA, and mismatch PNA controls (P < 0.001). These results extend our previous findings that brain proteins can be knocked down in a specific manner by antisense molecules administered extracranially. Additionally, these results suggest some novel approaches for the treatment of diseases dependent upon the function of the dopamine transporter.

Published

2001

25. Quantitative Measurement of Porphobilinogen in Urine by Stable-Isotope Dilution Liquid Chromatography-Tandem Mass Spectrometry

Author

Karen M. Kloke, Paul A. Chezick, Abdul H. Fauq, Joseph P. McConnell, Roddey E. Ford, and Mark J. Magera

Subjects

chemistry.chemical_compound, Reproducibility, Column chromatography, Chromatography, chemistry, Liquid chromatography–mass spectrometry, Biochemistry (medical), Clinical Biochemistry, Porphobilinogen, Urine, Tandem mass spectrometry, Mass spectrometry, Quantitative analysis (chemistry)

Abstract

Background: Measurement of porphobilinogen (PBG) is useful in the diagnosis of the acute neurologic porphyrias. Currently used colorimetric assays lack analytical and clinical sensitivity and specificity.Methods: We developed a liquid chromatography-electrospray tandem mass spectrometry (LC-MS/MS) method for the measurement of PBG in 1 mL of urine, using 5-(aminoethyl)-4-(carboxymethyl) 1H-2,4-[13C]pyrolle-3-propanoic acid ([2,4-13C]PBG; 2.75 μg) as internal standard. After solid-phase extraction, LC-MS/MS analysis was performed in the selected-reaction monitoring (SRM) mode. PBG and [2,4-13C]PBG were monitored through their own precursor and product ion settings (m/z 227 to 210 and m/z 229 to 212, respectively). The retention time of PBG and [2,4-13C]PBG was 1.0 min in a 2.3-min analysis.Results: Daily calibrations (n = 6) between 0.1 and 2.0 mg/L were linear and reproducible. Inter- and intraassay CVs were 3.2–3.5% and 2.6–3.1%, respectively, at mean concentrations of 0.24, 1.18, and 2.15 mg/L. The regression equation for the comparison between an anion-exchange column method (y) and the LC-MS/MS method (x) was: y = 0.84x + 0.74 (Sy|x = 5.8 mg/24 h; r = 0.85; n = 100). In 47 volunteers, PBG excretion was 0.02–0.42 mg/24 h, lower than reported reference intervals (up to 2.0 mg/24 h) based on colorimetric methods. In 85 samples with PBG ≤0.5 by LC-MS/MS, 8 (9.4%) had values ≥2.0 mg/24 h by the anion-exchange method (mean ± SD, 4.3 ± 1.8 mg/24 h). In 11 patients with confirmed diagnoses of acute porphyria and increased PBG by LC-MS/MS, 2 had values within the reported reference intervals by a quantitative anion-exchange method.Conclusions: The quantitative LC-MS/MS method for PBG measurement exhibits greater analytical specificity and improved clinical sensitivity and specificity than currently available methods.

Published

2001

26. A novel neurotensin analog blocks cocaine- and d-amphetamine-induced hyperactivity

Author

Abdul H. Fauq, Lewis Warrington, Elliott Richelson, Daniel J. McCormick, and Mona Boules

Subjects

Male, medicine.medical_specialty, Dextroamphetamine, Time Factors, Neuropeptide, Motor Activity, Peptide hormone, Catalepsy, Pharmacology, Rats, Sprague-Dawley, chemistry.chemical_compound, Neurochemical, Cocaine, Internal medicine, medicine, Animals, Amphetamine, Neurotensin, Behavior, Animal, Dose-Response Relationship, Drug, Dopaminergic, Biological activity, medicine.disease, Peptide Fragments, Rats, Endocrinology, chemistry, medicine.drug

Abstract

Neurotensin is a tridecapeptide that exhibits selective anatomic and neurochemical interactions with dopaminergic systems. Since dopaminergic neurotransmission underlies many of the behavioral properties of psychostimulants, and since neurotensin has been implicated in modulating dopaminergic neurotransmitter systems, we tested the effect of our novel neurotensin analog, NT69L (N-methyl-Arg(8),L-Lys(9),L-neo-Trp(11),tert-Leu(12)]neurotensin-(8-13)), on hyperactivity caused by cocaine and D-amphetamine. Previously, we showed that NT69L reduces body temperature, blocks apomorphine-induced climbing, and haloperidol-induced catalepsy. In this study, NT69L blocked the hyperactivity induced by both cocaine and D-amphetamine administered at three different doses each, when this peptide was injected intraperitoneally. These results provide further evidence for the involvement of the neurotensin system in some of the behavioral properties of psychostimulants and suggest that NT69L may find clinical application in patients who abuse this class of compounds.

Published

2001

27. A synthesis of the γ-secretase inhibitor BMS-708163

Author

Abdul H. Fauq and Ghulam M. Maharvi

Subjects

Stereochemistry, Organic Chemistry, Glycine methyl ester, Enantioselective synthesis, Alcohol, Alkylation, Biochemistry, chemistry.chemical_compound, chemistry, Reagent, Drug Discovery, Mitsunobu reaction, γ secretase, Derivative (chemistry)

Abstract

A concise, convergent racemic synthesis of BMS-708163 is reported. Two fragments consisting of N-4-chlorophenylsulfonyl-3,3,3-trifluorpropylglycine and a 1,2,4-oxadiazole derivative of 2-fluorobenzyl alcohol were prepared in separate pots and then coupled together via a Mitsunobu reaction. Since a convenient chiral synthesis of optically pure ( d )-3,3,3-trifluoropropyl glycine methyl ester was developed using Schollkopf reagent alkylation, this methodology can also be adopted for the enantioselective synthesis of BMS-708163.

Published

2010

28. Chemical synthesis of deuterium-labeled and unlabeled very long chain polyunsaturated fatty acids

Author

Ghulam M. Maharvi, Abdul H. Fauq, and Albert O. Edwards

Subjects

chemistry.chemical_classification, Sodium, Organic Chemistry, chemistry.chemical_element, Fatty acid, Very long chain, Biochemistry, Chemical synthesis, Article, chemistry, Drug Discovery, Organic chemistry, lipids (amino acids, peptides, and proteins), Deuterium labeled, Carbanion, Polyunsaturated fatty acid

Abstract

First syntheses of a deuterium-labeled very long C34-containing polyunsaturated fatty acid, C34:5n5.d(2), and three other unlabeled very long chain C30-32-containing polyunsaturated fatty acids are reported here. These syntheses were achieved by coupling chemically modified C22- and C20-containing polyunsaturated fatty acids with carbanions derived from arylalkyl sulfones, followed by sodium amalgam-mediated desulfonylation.

Published

2010

29. γ-Secretase processing and effects of γ-secretase inhibitors and modulators on long Aβ peptides in cells

Author

Joo In Jung, Kevin M. Felsenstein, Thomas B. Ladd, Abdul H. Fauq, Julian Matthews, Yong Ran, Pedro E. Cruz, and Todd E. Golde

Subjects

Immunoprecipitation, medicine.medical_treatment, Proteolysis, CHO Cells, Cleavage (embryo), Biochemistry, Cricetulus, Neurobiology, Cricetinae, mental disorders, medicine, Amyloid precursor protein, Presenilin-1, Animals, Humans, Protease Inhibitors, Molecular Biology, Protease, Amyloid beta-Peptides, biology, medicine.diagnostic_test, Chemistry, Chinese hamster ovary cell, Cell Biology, Transfection, Models, Chemical, Solubility, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, biology.protein, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase

Abstract

Understanding how different species of Aβ are generated by γ-secretase cleavage has broad therapeutic implications, because shifts in γ-secretase processing that increase the relative production of Aβx-42/43 can initiate a pathological cascade, resulting in Alzheimer disease. We have explored the sequential stepwise γ-secretase cleavage model in cells. Eighteen BRI2-Aβ fusion protein expression constructs designed to generate peptides from Aβ1–38 to Aβ1–55 and C99 (CTFβ) were transfected into cells, and Aβ production was assessed. Secreted and cell-associated Aβ were detected using ELISA and immunoprecipitation MALDI-TOF mass spectrometry. Aβ peptides from 1–38 to 1–55 were readily detected in the cells and as soluble full-length Aβ proteins in the media. Aβ peptides longer than Aβ1–48 were efficiently cleaved by γ-secretase and produced varying ratios of Aβ1–40:Aβ1–42. γ-Secretase cleavage of Aβ1–51 resulted in much higher levels of Aβ1–42 than any other long Aβ peptides, but the processing of Aβ1–51 was heterogeneous with significant amounts of shorter Aβs, including Aβ1–40, produced. Two PSEN1 variants altered Aβ1–42 production from Aβ1–51 but not Aβ1–49. Unexpectedly, long Aβ peptide substrates such as Aβ1–49 showed reduced sensitivity to inhibition by γ-secretase inhibitors. In contrast, long Aβ substrates showed little differential sensitivity to multiple γ-secretase modulators. Although these studies further support the sequential γ-secretase cleavage model, they confirm that in cells the initial γ-secretase cleavage does not precisely define subsequent product lines. These studies also raise interesting issues about the solubility and detection of long Aβ, as well as the use of truncated substrates for assessing relative potency of γ-secretase inhibitors.

Published

2013

30. Cell‐free assays for γ‐secretase activity

Author

Rong Wang, Chris McLendon, Inga Pinnix, Kirk A. Findlay, Patrick A. Lewis, Kumar Sambamurti, Abdul H. Fauq, M. Paul Murphy, TianPei Xin, Todd E. Golde, and Chewki Ziani-Cherif

Subjects

Proteases, Protease, biology, Chemistry, medicine.medical_treatment, Chinese hamster ovary cell, Cleavage (embryo), Biochemistry, Molecular biology, In vitro, Cell-free system, Genetics, medicine, biology.protein, Molecular Biology, Amyloid precursor protein secretase, Gamma secretase, Biotechnology

Abstract

The amyloid b-protein (Ab) deposited in Alzheimer's disease (AD) is a normally secreted proteolytic product of the amyloid b-protein precursor (APP). Generation of Ab from the APP requires two sequential proteolytic events: an initial b-secretase cleavage at the amino terminus of the Ab sequence followed by g-secretase cleavage at the carboxyl terminus of Ab. We describe the development of a robust in vitro assay for g-secretase cleavage by showing de novo Ab production in vitro and establish that this assay monitors authentic gamma-secretase activity by documenting the production of a cognate g-CTF, confirming the size of the Ab produced by mass spectrometry, and inhibiting cleavage in this system with multiple inhibitors that alter g-secretase activity in living cells. Using this assay, we demonstrate that the g-secretase activity 1) is tightly associated with the membrane, 2) can be solubilized, 3) has a pH optimum of 6.8 but is active from pH 6.0 to pH >8.4, and 4) ascertain that activities of the g-40 and g-42 are indeed pharmacologically distinct. These studies should facilitate the purification of the protease or proteases that are responsible for this unusual activity, which is a major therapeutic target for the treatment of AD.

Published

2000

31. Presenilin 1 Regulates Pharmacologically Distinct γ-Secretase Activities

Author

Todd E. Golde, Michael P. Murphy, Tawnya E. Smith, Richard C. Wang, D C McLendon, Abdul H. Fauq, Kirk A. Findlay, Paul E. Fraser, H A Lookingbill, Patrick A. Lewis, and Sacha N. Uljon

Subjects

biology, Amyloid beta, Cell Biology, Biochemistry, Presenilin, nervous system diseases, Alpha secretase, Membrane protein, mental disorders, biology.protein, Amyloid precursor protein, APH-1, Molecular Biology, Amyloid precursor protein secretase, Gamma secretase

Abstract

Presenilins (PSs) are polytopic membrane proteins that have been implicated as potential therapeutic targets in Alzheimer's disease because of their role in regulating the gamma-secretase cleavage that generates the amyloid beta protein (Abeta). It is not clear how PSs regulate gamma-secretase cleavage, but there is evidence that PSs could be either essential cofactors in the gamma-secretase cleavage, gamma-secretase themselves, or regulators of intracellular trafficking that indirectly influence gamma-secretase cleavage. Using presenilin 1 (PS1) mutants that inhibit Abeta production in conjunction with transmembrane domain mutants of the amyloid protein precursor that are cleaved by pharmacologically distinct gamma-secretases, we show that PS1 regulates multiple pharmacologically distinct gamma-secretase activities as well as inducible alpha-secretase activity. It is likely that PS1 acts indirectly to regulate these activities (as in a trafficking or chaperone role), because these data indicate that for PS1 to be gamma-secretase it must either have multiple active sites or exist in a variety of catalytically active forms that are altered to an equivalent extent by the mutations we have studied.

Published

2000

32. A novel neurotensin peptide analog given extracranially decreases food intake and weight in rodents

Author

Bernadette Cusack, Elliott Richelson, Mona Boules, Lihong Zhao, Daniel J. McCormick, and Abdul H. Fauq

Subjects

Blood Glucose, Male, Serotonin, medicine.medical_specialty, Time Factors, Dopamine, medicine.medical_treatment, Thyrotropin, Rats, Sprague-Dawley, Eating, chemistry.chemical_compound, Pituitary Gland, Anterior, Corticosterone, Weight loss, Internal medicine, medicine, Animals, Obesity, Molecular Biology, Saline, Neurotensin, Peptide analog, Dose-Response Relationship, Drug, Drug Administration Routes, General Neuroscience, Body Weight, Peptide Fragments, Rats, Thyroxine, Dose–response relationship, Endocrinology, chemistry, Hypothalamus, Neurology (clinical), medicine.symptom, Weight gain, Developmental Biology

Abstract

Neurotensin decreases food intake in the rat when injected into the cerebral ventricles. We tested the effect of a novel neurotensin analog (NT69L), injected intra-peritoneally (i.p.), on weight gain and food intake in rats. Sprague-Dawley rats (270 g) were injected i. p. with either saline or NT69L at 0.001 or 0.010 mg/kg. In further experiments, larger rats at a more steady state on the growth curve (400 g) were injected with either saline or 0.010 or 1 mg/kg NT69L. Food intake, water consumption and body weight were recorded daily. Weight gain was significantly reduced in the smaller rats injected with 0.001 or 0.010 mg/kg, showing only a 8.5 and 9.0% increase in original weight, respectively, as compared to a 29% increase for the controls. The larger rats injected with 1 mg/kg, had a significant reduction in body weight with a 3.0% decrease in original body weight as compared to a 2.4% increase for the controls. Food intake was significantly reduced suggesting that the weight loss observed after injection of NT69L was attributable in part to a reduction in food intake. The genetically obese Zucker rats injected with NT69L (1 mg/kg) had a significant reduction in weight gain and food intake. NT69L significantly increased blood glucose and corticosterone levels and decreased TSH and T4 in Sprague-Dawley and Zucker rats, an effect that was only transitory. NT69L also caused a decrease in norepinephrine in both the hypothalamus and nucleus accumbens, and an increase in dopamine, 3,4-dihydroxyphenylacetic acid (DOPAC) and serotonin. In this study, NT69L exhibited a consistent and dramatic effect on body weight and food intake in Sprague-Dawley and obese Zucker rats, and enabled us to study the role that NT plays in weight control and the functional interactions of NT with brain amines, and metabolic and endocrinological parameters.

Published

2000

33. Effects of a novel neurotensin peptide analog given extracranially on CNS behaviors mediated by apomorphine and haloperidol

Author

Mona Boules, Bernadette Cusack, Elliott Richelson, Abdul H. Fauq, Beth M. Tyler, and Daniel J. McCormick

Subjects

Male, medicine.medical_specialty, Time Factors, Apomorphine, Motor Activity, Catalepsy, Pharmacology, Dopamine agonist, Body Temperature, Rats, Sprague-Dawley, Mice, chemistry.chemical_compound, Internal medicine, medicine, Haloperidol, Animals, Neurotensin receptor, Clozapine, Molecular Biology, Neurotensin, Peptide analog, Behavior, Animal, General Neuroscience, medicine.disease, Effective dose (pharmacology), Peptide Fragments, Rats, Endocrinology, chemistry, Neurology (clinical), Injections, Intraperitoneal, Developmental Biology, medicine.drug

Abstract

Neurotensin (NT) is a neuropeptide neurotransmitter in the central nervous system. It has been implicated in the therapeutic and in the adverse effects of neuroleptics. Activity of NT in brain can only be shown by direct injection of the peptide into that organ. However, we have developed a novel analog of NT(8-13), NT69L, which is active upon intraperitoneal (i.p.) injection. Like atypical neuroleptics, NT69L blocked the climbing behavior in rats, but not the licking and sniffing behaviors of a high dose (600 microgram/kg) of the non-selective dopamine agonist apomorphine. Its blockade of climbing was very potent with an ED(50) (effective dose at 50% of maximum) of 16 microgram/kg. Both apomorphine and NT69L caused a long-lasting hypothermia, which was greater with the peptide but not synergistic in combination with apomorphine. The ED(50) of NT69L for hypothermia was 390 microgram/kg. NT69L (up to 5 mg/kg i.p.) did not produce catalepsy. However, when given before haloperidol, NT69L, but not clozapine, completely prevented catalepsy. When given after haloperidol, NT69L, but not clozapine, reversed haloperidol's cataleptic effects with an ED(50) of 260 microg/kg. There was no significant difference between the ED(50)s for hypothermia and anticataleptic effects of NT69L. However, the ED(50) for blocking the effects of apomorphine was significantly lower than the other two. These data suggest that NT69L may have neuroleptic properties in humans and may be useful in the treatment of extrapyramidal side effects caused by typical neuroleptics such as haloperidol.

Published

2000

34. In vitro binding and CNS effects of novel neurotensin agonists that cross the blood–brain barrier

Author

Daniel J. McCormick, Abdul H. Fauq, Jennifer A. Stewart, Bernadette Cusack, Yuan Ping Pang, Christopher Lee Douglas, Elliott Richelson, and Beth M. Tyler

Subjects

Central Nervous System, Male, Agonist, medicine.drug_class, Pharmacology, Rats, Sprague-Dawley, Cellular and Molecular Neuroscience, chemistry.chemical_compound, In vivo, medicine, Animals, Humans, Neurotensin receptor, Hot plate test, Receptor, Neurotensin, ED50, Binding Sites, business.industry, Hypothermia, Peptide Fragments, Rats, chemistry, Blood-Brain Barrier, Anesthesia, medicine.symptom, business

Abstract

Animal studies with neurotensin (NT) directly injected into brain suggest that it has pharmacological properties similar to those of antipsychotic drugs. Here, we present radioligand binding data for some novel hexapeptide analogs of NT(8-13) at the molecularly cloned rat and human neurotensin receptors (NTR-1), along with behavioral and physiological effects of several of these peptides after intraperitoneal (i.p.) administration in rats. One unique analog, NT66L, which had high affinity (0.85 nM) for the molecularly cloned rat neurotensin receptor (NTR-1), caused a drop in body temperature and antinociception at doses as low as 0.1 mg/kg after i.p. injection. At 30 min post-injection, the ED50 for NT66L-induced hypothermia (rectal temperature) and antinociception (hot plate test) was 0.5 and 0.07 mg/kg, respectively. At a dose of 1 mg/kg i.p., NT66L caused 100% of the maximum possible effect for antinociception for up to 2 h after administration. At this dose body temperature lowering was greater than -2.5 degrees C from 20 to 120 min after i.p. administration. These results in animals suggest that NT66L has agonist properties at NTR-1 in vivo after extracranial administration and provide support for its further study in behavioral tests predictive of neuroleptic activity.

Published

1999

35. Peptide nucleic acids targeted to the neurotensin receptor and administered i.p. cross the blood–brain barrier and specifically reduce gene expression

Author

Daniel J. McCormick, Elliott Richelson, Benjamin W Lacy, Jennifer A. Stewart, Christopher Lee Douglas, Lihong Zhao, Mona Boules, Karen Jansen, Beth M. Tyler, Abdul H. Fauq, and Bernadette Cusack

Subjects

Male, Peptide Nucleic Acids, Biology, Blood–brain barrier, Rats, Sprague-Dawley, chemistry.chemical_compound, Drug Delivery Systems, Sense (molecular biology), medicine, Antisense Elements (Genetics), Animals, Receptors, Neurotensin, Electrophoretic mobility shift assay, Neurotensin receptor, Receptor, Multidisciplinary, Peptide nucleic acid, musculoskeletal, neural, and ocular physiology, Biological Transport, Biological Sciences, Molecular biology, Rats, medicine.anatomical_structure, Gene Expression Regulation, chemistry, Blood-Brain Barrier, biological sciences, cardiovascular system, tissues, Injections, Intraperitoneal, Neurotensin

Abstract

Intraperitoneal injection of an unmodified antisense peptide nucleic acid (PNA) complementary to mRNA of the rat neurotensin (NT) receptor (NTR1) was demonstrated by a gel shift assay to be present in brain, thus indicating that the PNA had in fact crossed the blood–brain barrier. An i.p. injection of this antisense PNA specifically inhibited the hypothermic and antinociceptive activities of NT microinjected into brain. These results were associated with a reduction in binding sites for NT both in brain and the small intestine. Additionally, the sense-NTR1 PNA, targeted to DNA, microinjected directly into the brain specifically reduced mRNA levels by 50% and caused a loss of response to NT. To demonstrate the specificity of changes in behavioral, binding, and mRNA studies, animals treated with NTR1 PNA were tested for behavioral responses to morphine and their mu receptor levels were determined. Both were found to be unaffected in these NTR1 PNA-treated animals. The effects of both the antisense and sense PNAs were completely reversible. This work provides evidence that any antisense strategy targeted to brain proteins can work through i.p. delivery by crossing the normal blood–brain barrier. Equally important was that an antigene strategy, the sense PNA, was shown in vivo to be a potentially effective therapeutic treatment.

Published

1999

36. Synthesis of (2S)-2-amino-3-(1H-4-indolyl)propanoic acid, a novel tryptophan analog for structural modification of bioactive peptides

Author

Feng Hong, Bernadette Cusack, Elliott Richelson, Yuan Ping-Pang, Beth M. Tyler, and Abdul H. Fauq

Subjects

Chiral auxiliary, Organic Chemistry, Tryptophan, Combinatorial chemistry, Catalysis, Inorganic Chemistry, chemistry.chemical_compound, Propanoic acid, Solid-phase synthesis, chemistry, Aromatic amino acids, Physical and Theoretical Chemistry, Chirality (chemistry), Derivative (chemistry), Tryptophan analog

Abstract

A convenient, multigram synthesis of a novel α-amino acid (2S)-2-amino-3-(1H-4-indolyl)propanoic acid (1a), is reported. An Fmoc–t-Boc derivative of this novel regioisomer of the natural aromatic amino acid tryptophan could be readily incorporated into bioactive synthetic peptides using standard solid phase synthesis. The synthesis featured the use of Schollkopf chiral auxiliary reagents for chirality induction during a key step.

Published

1998

37. Synthesis of (S)- and (R)-enantiomers of p-(4-hydroxybenzoyl)phenylalanine, useful photoaffinity labeling probes for peptide–protein binding sites

Author

Elliott Richelson, Chewki Ziani-Cherif, and Abdul H. Fauq

Subjects

chemistry.chemical_classification, Chiral auxiliary, Photoaffinity labeling, Chemistry, Organic Chemistry, Phenylalanine, Peptide, Plasma protein binding, Combinatorial chemistry, Catalysis, Inorganic Chemistry, chemistry.chemical_compound, Reagent, Yield (chemistry), Physical and Theoretical Chemistry, Enantiomer

Abstract

A high yield, multigram synthesis of both enantiomers of p-(4-hydroxybenzoyl)phenylalanine, cross-linking probes for peptide–protein binding interactions, is reported. The synthesis was accomplished using Schollkopf chiral auxiliary reagents.

Published

1998

38. Inhibition of Recombinant Human Mitochondrial Aldehyde Dehydrogenase by Two Intermediate Metabolites of Disulfiram

Author

Abdul H. Fauq, Jennifer P. Lam, Ik H. Tong, James J. Lipsky, Dennis C. Mays, and Patricia Ortiz-Bermudez

Subjects

Metabolite, Aldehyde dehydrogenase, Dehydrogenase, Biochemistry, chemistry.chemical_compound, Disulfiram, medicine, Humans, Enzyme Inhibitors, Pharmacology, biology, Sulfoxide, Glutathione, Aldehyde Dehydrogenase, Recombinant Proteins, Mitochondria, Kinetics, chemistry, Enzyme inhibitor, biology.protein, NAD+ kinase, Ditiocarb, Alcohol Deterrents, medicine.drug

Abstract

Disulfiram is used in aversion therapy for alcoholism. S-Methyl-N,N-diethylthiocarbamate (MeDTC) sulfoxide, a potent inhibitor of the target enzyme mitochondrial aldehyde dehydrogenase (ALDH2), is thought to be the principal active metabolite of disulfiram in vivo. We examined the effects on recombinant human ALDH2 of two intermediate metabolites of disulfiram, S-methyl-N,N-diethyldithiocarbamate (MeDDC) sulfoxide and MeDDC sulfine. MeDDC sulfoxide was a potent inhibitor of ALDH2 with an IC50 of 2.2 +/- 0.5 microM (mean +/- SD, N = 4) after preincubation with enzyme for 30 min. MeDDC sulfine was a relatively weak inhibitor of ALDH2 under the same conditions with an IC50 value of 62 +/- 14 microM. The inhibition of ALDH2 by both compounds was irreversible and did not require the cofactor NAD. The latter finding demonstrates that inactivation of ALDH2 is independent of the dehydrogenase activity of the enzyme. GSH blocked almost completely the inhibition by 20 microM of MeDDC sulfoxide and greatly diminished the inhibition by 200 microM of MeDDC sulfine. Inactivation by MeDDC sulfoxide was time dependent. MeDTC sulfoxide was a more potent inhibitor of recombinant human ALDH2 (IC50 = 1.4 +/- 0.3 microM after preincubation for 15 min) than either of the intermediate metabolites, and its inhibition was unaffected by GSH. Our results suggest that these newer intermediate metabolites of disulfiram, especially the more potent MeDTC sulfoxide, have the potential to inhibit the target enzyme ALDH2 in patients receiving disulfiram. However, until the significance of the interactions of the inhibitors with GSH is more fully understood, the contribution of MeDDC sulfine and MeDDC sulfoxide to the pharmacological effects of disulfiram in vivo is uncertain.

Published

1998

39. Optimization of peptide hydroxamate inhibitors of insulin-degrading enzyme reveals marked substrate-selectivity

Author

A Masson, Abdul H. Fauq, Claussin Clemence, Juliette Bertrand, Thomas R. Caulfield, Ghulam M. Maharvi, SO Abdul-Hay, Malcolm A. Leissring, Shakeel Choudhry, and Amy L. Lane

Subjects

Amyloid, Stereochemistry, Protein Conformation, medicine.medical_treatment, Peptide, Hydroxamic Acids, Insulysin, Article, Substrate Specificity, Drug Discovery, medicine, Insulin-degrading enzyme, Potency, Humans, Enzyme Inhibitors, chemistry.chemical_classification, Chemistry, Insulin, Substrate (chemistry), Stereoisomerism, Molecular Docking Simulation, Enzyme, Biochemistry, Drug Design, Molecular Medicine, Selectivity, Peptides

Abstract

Insulin-degrading enzyme (IDE) is an atypical zinc-metallopeptidase that degrades insulin and the amyloid ß-protein and is strongly implicated in the pathogenesis of diabetes and Alzheimer’s disease. We recently developed the first effective inhibitors of IDE, peptide hydroxamates that, while highly potent and selective, are relatively large (MW >740) and difficult to synthesize. We present here a facile synthetic route that yields enantiomerically pure derivatives comparable in potency to the parent compounds. Through the generation of truncated variants, we identified a compound with significantly reduced size (MW = 455.5) that nonetheless retains good potency (k(i) = 78 ± 11 nM) and selectivity for IDE. Notably, the potency of these inhibitors was found to vary as much as 60-fold in a substrate-specific manner, an unexpected finding for active-site directed inhibitors. Collectively, our findings demonstrate that potent, small-molecule IDE inhibitors can be developed that, in certain instances, can be highly substrate selective.

Published

2013

40. Cloning of a cDNA for Short/Branched Chain Acyl-Coenzyme A Dehydrogenase from Rat and Characterization of Its Tissue Expression and Substrate Specificity

Author

Kevin P. Battaile, Jerry Vockley, Jan Willard, Rima Rozen, Caroline Vicanek, Paul P. Van Veldhoven, and Abdul H. Fauq

Subjects

DNA, Complementary, Molecular Sequence Data, Biophysics, Gene Expression, Sequence Homology, Flavoprotein, Dehydrogenase, Molecular cloning, Kidney, Polymerase Chain Reaction, Biochemistry, Acyl-CoA Dehydrogenase, Substrate Specificity, Acyl-CoA Dehydrogenases, Complementary DNA, Animals, Humans, Amino Acid Sequence, Cloning, Molecular, Molecular Biology, chemistry.chemical_classification, Base Sequence, biology, Acyl CoA dehydrogenase, Substrate (chemistry), Blotting, Northern, Molecular biology, Rats, Enzyme, Liver, chemistry, Organ Specificity, biology.protein, Branched-chain alpha-keto acid dehydrogenase complex

Abstract

The acyl-CoA dehydrogenases are a family of related enzymes which catalyze the alpha,beta-dehydrogenation of acyl-CoA esters, transferring electrons to electron-transferring flavoprotein. A cDNA for human short/branched chain acyl-CoA dehydrogenase has recently been cloned, and it has been suggested that this enzyme represents the human homolog for the previously reported 2-methyl branched chain acyl-CoA dehydrogenase purified from rat liver. We now report the cloning and expression of rat short/branched chain acyl-CoA dehydrogenase and characterization of its substrate specificity. The rat enzyme is more active toward longer carbon side chains than its human counterpart, while the human enzyme can utilize substrates with longer primary carbon chains. In addition, short/branched chain acyl-CoA dehydrogenase can utilize valproyl-CoA as a substrate. Northern blotting of mRNA shows ubiquitous tissue expression of both the rat and human enzyme. Further study of these enzymes will be helpful in understanding structure/function relationships in this gene family.

Published

1996

41. Synthesis of novel metabolically stable analogues of D-myo-inositol 1,4,5-trisphosphate

Author

Abdul H. Fauq, Javid H. Zaidi, Alan P. Kozikowski, Stefan R. Nahorski, Christophe Erneux, Robert A. Wilcox, and Girlie Varvel

Subjects

Biochemistry, Chemistry, Organic Chemistry, Drug Discovery, Second messenger system, MYO INOSITOL 1 4 5 TRISPHOSPHATE

Abstract

Starting from L-quebrachitol, syntheses and biological activities of three novel analogues of the cellular second messenger D-myo-inositol 1,4,5-trisphosphate (IP3), 3-deoxy-3-fluoro-d-myo-inositol 1,4-bisphosphate 5-phosphorothioate (1a), 3-deoxy-3-fluoro-d-myo-inositol 1,5-bisphosphate 4-phosphorothioate (1b), and 3-deoxy-3-fluoro-d-myo-inositol 1-phosphate 4,5-bisphosphorothioate (1c) are described.

Published

1996

42. Pharmacological and Biochemical Profiles of Unique Neurotensin 8-13 Analogs Exhibiting Species Selectivity, Stereoselectivity, and Superagonism

Author

Bernadette Cusack, Yuan Ping Pang, Terrance Souder, Elliott Richelson, Roberto Garcia, Daniel J. McCormick, and Abdul H. Fauq

Subjects

Agonist, medicine.drug_class, Stereochemistry, Molecular Sequence Data, Random hexamer, Phosphatidylinositols, Biochemistry, Cell Line, Radioligand Assay, Structure-Activity Relationship, chemistry.chemical_compound, Species Specificity, medicine, Animals, Humans, Receptors, Neurotensin, Potency, Amino Acid Sequence, Phosphatidylinositol, Neurotensin receptor, Receptor, Molecular Biology, Neurotensin, digestive, oral, and skin physiology, Stereoisomerism, Cell Biology, Rats, Dissociation constant, chemistry, Protein Binding

Abstract

Recently, the rat neurotensin receptor and the two human neurotensin receptor clones (differing by one amino acid residue) have been isolated. We present results with 33 newly synthesized neurotensin analogs. We have evaluated their binding potency at the three neurotensin receptor clones by determining equilibrium dissociation constants and coupling to phosphatidylinositol turnover. Our work focused on position 8 and 9 substitutions as well as position 11 of the neurotensin hexamer NT8-13. The results presented include: 1) the development of a compound that is species selective, with a binding potency at the rat receptor that is 20-fold more potent than at the human receptor; 2) the development of a pair of stereoselective compounds with the L-isomer exhibiting 190-700-fold more potency than the D-isomer; and 3) the development of an agonist that has a Kd of 0.3 and 0.2 nM at the human and rat neurotensin receptor, respectively, ranking it as among the most potent tested. Also, we present the first evidence that 1) the effect of pi electrons at position 11 (L-Tyr) are important for binding to the neurotensin receptor, and 2) the length of the side chain on position 9 (L-Arg) changes binding potency.

Published

1995

43. Chemical synthesis and biological evaluation of 1d-1,2,4,5-InsP4 and its 3-fluorinated counterpart 1d-3-F-1,2,4,5-InsP4 — potent 1d-1,4,5-InsP3-like calcium mobilizing analogues

Author

Abdul H. Fauq, Stefan R. Nahorski, Robert A. Wilcox, and Alan P. Kozikowski

Subjects

Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, chemistry.chemical_element, Calcium, Biochemistry, Chemical synthesis, Combinatorial chemistry, chemistry, Drug Discovery, Molecular Medicine, Molecular Biology, Biological evaluation

Abstract

Syntheses of optically pure 1 d -3-F-2,4,5-InsP3, 1 d -3-F-1,2,4,5-InsP4, and 1 d -1,2,4,5-InsP4 are reported starting from l -quebrachitol. The latter two compounds are shown to be nearly equipotent to 1 d -1,4,5-InsP3 in both binding and calcium release experiments.

Published

1995

44. Chemical modification of ring c of himbacine: Discovery of a pharmacophoric element for M2-selectivity

Author

Alan P. Kozikowski, Patricia J. Aagaard, Michael McKinney, Abdul H. Fauq, and Michael Malaska

Subjects

chemistry.chemical_classification, biology, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Chemical modification, chemistry.chemical_element, Ring (chemistry), biology.organism_classification, Biochemistry, Oxygen, Galbulimima, chemistry.chemical_compound, Himbacine, Drug Discovery, Molecular Medicine, Molecule, Selectivity, Molecular Biology, Tricyclic

Abstract

Removal of the carbonyl oxygen of himbacine furnishes a molecule which binds with 20-fold and 4-fold lower affinity at the M2 and M1 receptor sites, respectively. Thus, the carbonyl oxygen constitutes an important pharmacophoric element responsible for some of the M2 selectivity of himbacine. Other modifications of the C-ring of the tricyclic portion of himbacine were examined and tested for potency at M1 and M2 sites, and the data confirm that M2 selectivity is optimal with a closed heterocyclic ring and with the presence of a proximal carbonyl oxygen.

Published

1995

45. Efficacy of Glycoconjugated Dinitroanilines against Cryptosporidium parvum

Author

Murad Ali Khan, Nina McNair, Abdul H. Fauq, and Jan R. Mead

Subjects

Cryptosporidium parvum, chemistry.chemical_classification, Aniline Compounds, biology, Glycoconjugate, biology.organism_classification, Microbiology, Virology, Cell Line, Apicomplexa, Structure-Activity Relationship, Antiprotozoal Agent, Dogs, chemistry, Animals, Parasite hosting, Protozoa, Amebicides, Protozoal disease, Glycoconjugates

Published

2003

46. Hydrolysis of low concentrations of the acetylthiocholine analogs acetyl(homo)thiocholine and acetyl(nor)thiocholine by acetylcholinesterase may be limited by selective gating at the enzyme peripheral site

Author

Jeffrey T. Auletta, Abdul H. Fauq, Terrone L. Rosenberry, Ghulam M. Maharvi, Juanita F. Wood, and Veena Beri

Subjects

Stereochemistry, Acylation, Toxicology, GPI-Linked Proteins, Article, Substrate Specificity, chemistry.chemical_compound, Catalytic Domain, Catalytic triad, Humans, Enzyme kinetics, biology, Hydrolysis, Active site, Substrate (chemistry), General Medicine, Acetylcholinesterase, Recombinant Proteins, Kinetics, Thiocholine, chemistry, Acetylthiocholine, biology.protein, Cholinesterase Inhibitors

Abstract

Hydrolysis of acetylcholine by acetylcholinesterase (AChE) is extremely rapid, with a second-order hydrolysis rate constant k(E) (often denoted k(cat)/K(M)) that approaches 10(8) M(-1) s(-1). AChE contains a deep active site gorge with two sites of ligand binding, an acylation site (or A-site) containing the catalytic triad at the base of the gorge and a peripheral site (or P-site) near the gorge entrance. The P-site is known to contribute to catalytic efficiency with acetylthiocholine (AcSCh) by transiently trapping the substrate in a low affinity complex on its way to the A-site, where a short-lived acyl enzyme intermediate is produced. Here we ask whether the P-site does more than simply trap the substrate but in fact selectively gates entry to the A-site to provide specificity for AcSCh (and acetylcholine) relative to the close structural analogs acetyl(homo)thiocholine (Ac-hSCh, which adds one additional methylene group to thiocholine) and acetyl(nor)thiocholine (Ac-nSCh, which deletes one methylene group from thiocholine). We synthesized Ac-hSCh and Ac-nSCh and overcame technical difficulties associated with instability of the northiocholine hydrolysis product. We then compared the catalytic parameters of these substrates with AChE to those of AcSCh. Values of k(E) for Ac-hSCh and Ac-nSCh were about 2% of that for AcSCh. The k(E) for AcSCh is close to the theoretical diffusion-controlled limit for the substrate association rate constant, but kE values for Ac-hSCh or Ac-nSCh are too low to be limited by diffusion control. However, analyses of kinetic solvent isotope effects and inhibition patterns for P-site inhibitors indicate that these two analogs also do not equilibrate with the A-site prior to the initial acylation step of catalysis. We propose that kE for these substrates is partially rate-limited by a gating step that involves the movement of bound substrate from the P-site to the A-site.

Published

2012

47. Transient pharmacologic lowering of Aβ production prior to deposition results in sustained reduction of amyloid plaque pathology

Author

Pritam Das, Ghulam M. Maharvi, Kevin M. Felsenstein, Paramita Chakrabarty, Abdul H. Fauq, Lisa M. Minter, Barbara A. Osborne, Todd E. Golde, Thomas Kukar, and Christophe Verbeeck

Subjects

medicine.medical_specialty, Pathology, Aging, Neurology, Clinical Neurology, Mice, Transgenic, Plaque, Amyloid, Therapeutics, Pharmacology, lcsh:Geriatrics, lcsh:RC346-429, 03 medical and health sciences, Amyloid beta-Protein Precursor, Mice, Cellular and Molecular Neuroscience, 0302 clinical medicine, Alzheimer Disease, medicine, Dementia, Animals, Humans, Molecular Biology, lcsh:Neurology. Diseases of the nervous system, 030304 developmental biology, Aβ, 0303 health sciences, Amyloid beta-Peptides, biology, business.industry, Brain, medicine.disease, Aβ deposition, Molecular medicine, 3. Good health, Discontinuation, Disease Models, Animal, lcsh:RC952-954.6, biology.protein, γ-secretase inhibition, Neurology (clinical), Alzheimer's disease, Amyloid Precursor Protein Secretases, business, Preclinical stage, APP, Amyloid precursor protein secretase, Alzheimer’s disease, 030217 neurology & neurosurgery, Research Article

Abstract

Background Alzheimer’s disease (AD) is the leading cause of dementia among the elderly. Disease modifying therapies targeting Aβ that are in development have been proposed to be more effective if treatment was initiated prior to significant accumulation of Aβ in the brain, but optimal timing of treatment initiation has not been clearly established in the clinic. We compared the efficacy of transient pharmacologic reduction of brain Aβ with a γ-secretase inhibitor (GSI ) for 1–3 months (M) treatment windows in APP Tg2576 mice and subsequent aging of the mice to either 15M or 18M. Results These data show that reducing Aβ production in a 2-3M windows both initiated and discontinued before detectable Aβ deposition has the most significant impact on Aβ loads up to 11M after treatment discontinuation. In contrast, initiation of treatment for 3M windows from 7-10M or 12-15M shows progressively decreasing efficacy. Conclusions These data have major implications for clinical testing of therapeutics aimed at lowering Aβ production, indicating that; i) these therapies may have little efficacy unless tested as prophylactics or in the earliest preclinical stage of AD where there is no or minimal Aβ accumulation and ii) lowering Aβ production transiently during a critical pre-deposition window potentially provides long-lasting efficacy after discontinuation of the treatment.

Published

2012

48. Synthesis of a DOTA(Gd3+)-conjugate of proton-pump inhibitor pantoprazole for gastric wall imaging studies

Author

Adil E. Bharucha, Ghulam M. Maharvi, and Abdul H. Fauq

Subjects

MRI contrast agent, Gadolinium, Clinical Biochemistry, Pharmaceutical Science, chemistry.chemical_element, Lumen (anatomy), Contrast Media, Biochemistry, Article, 2-Pyridinylmethylsulfinylbenzimidazoles, chemistry.chemical_compound, Heterocyclic Compounds, 1-Ring, Nuclear magnetic resonance, Coordination Complexes, Drug Discovery, medicine, DOTA, Humans, Molecular Biology, Pantoprazole, Adenosine Triphosphatases, medicine.diagnostic_test, Chemistry, Organic Chemistry, Stomach, Temperature, Magnetic resonance imaging, Proton Pump Inhibitors, Magnetic Resonance Imaging, Proton pump, Radiography, Molecular Medicine, medicine.drug, Conjugate

Abstract

Magnetic resonance imaging (MRI) is used to evaluate gastrointestinal (GI) structure and functions in humans. Despite filling the viscus lumen with a contrast agent, visualization of the viscus wall is limited. To overcome this limitation, we de novo synthesized a conjugate that covalently combines a Gd-based MRI contrast agent, encaged with a chelating agent (DOTA), with pantoprazole, which is a widely used proton pump inhibitor that binds to proton pumps in the stomach and colon. The DOTA linkage was installed at a mechanism-based strategic location in the pantoprazole molecule to minimize a possible negative effect of the structural modification on the drug. It is anticipated that by defining the wall of the stomach and colon, this compound will facilitate functional MRI of the GI tract in humans.

Published

2012

49. Synthesis and Biological Activity of the D-3-Deoxy-3-fluoro and D-3-Chloro-3-deoxy Analogs of Phosphatidylinositol

Author

Werner Tückmantel, Alan P. Kozikowski, Abdul H. Fauq, Alfred Gallegos, and Garth Powis

Subjects

Phosphoramidite, chemistry.chemical_compound, Chemistry, Cyclitol, Stereochemistry, Organic Chemistry, Moiety, Biological activity, Inositol, Phosphatidylinositol, Phosphatidic acid, Selectivity

Abstract

The naturally occurring inositol derivative, L-quebrachitol (1), serves as starting material for the synthesis of D-3-deoxy-3-fluoro- and D-3-chloro-3-deoxy-myo-inositol (4, 28). Their transformation into the title compounds 22 and 40 (abbreviated as FPI and CPI, respectively) is accomplished by benzylation of all hydroxyl groups but OH-1 to which the phosphatidic acid side chain is subsequently attached using the phosphoramidite protocol, and hydrogenolytic deprotection. Compounds 4 and 28, as reported earlier, exhibit moderate and high selectivity, respectively, in the growth inhibition of υ-sis transformed vs wild type murine NIH 3T3 cells if myo-inositol is agent but are inactive in the presence of physiological inositol levels. On the other hand, FPI possesses a nearly 2 orders of magnitude higher activity but no selectivity both in the absence or presence of myo-inositol. CPI is inactive as is the simplified analogue 24 of FPI in which the phosphatidic acid moiety has been replaced by an octadecyl group

Published

1994

50. Cellular pharmacology ofd-3-azido-3-deoxy-myo-inositol, an inhibitor of phosphatidylinositol signaling having antiproliferative activity

Author

Garth Powis, G. Brunn, Alan P. Kozikowski, Sek C. Chow, Abdul H. Fauq, and Alfred Gallegos

Subjects

Cancer Research, Inositol Phosphates, Transferases (Other Substituted Phosphate Groups), Biology, Toxicology, Michaelis–Menten kinetics, 3T3 cells, Mice, chemistry.chemical_compound, medicine, Animals, Pharmacology (medical), Inositol, Phosphatidylinositol, Phospholipids, Pharmacology, Cell growth, 3T3 Cells, CDP-Diacylglycerol-Inositol 3-Phosphatidyltransferase, In vitro, medicine.anatomical_structure, Oncology, chemistry, Biochemistry, Growth inhibition, Signal transduction, Lithium Chloride, Cell Division

Abstract

D-3-Azido-3-deoxy-myo-inositol (3AMI) is an inhibitor of the growth of v-sis-transformed NIH 3T3 cells but not of wild-type NIH 3T3 cells, whose effects may be mediated through the phosphatidylinositol-3'-kinase pathway. We studied some properties of the cellular pharmacology of 3AMI using high-specific-activity [3H]-3AMI. The uptake of [3H]-3AMI by wild-type NIH 3T3 and v-sis NIH 3T3 cells was similar. [3H]-3AMI was a substrate for phosphatidylinositol synthetase, with the maximal velocity (Vmax) being 1.0 nmol min-1 mg-1 and the Michaelis constant (Km) being 23 mM. Corresponding values obtained for [3H]-myo-inositol as a substrate were 5.5 nmol min-1 mg-1 and 3.2 mM. [3H]-3AMI was incorporated into the cellular inositol lipids of v-sis NIH 3T3 cells to a similar extent as that observed for [3H]-myo-inositol but was not incorporated into the inositol lipids of wild-type NIH 3T3 cells. The [3H]-3AMI incorporated by the v-sis NIH 3T3 cells was present in the phosphatidylinositol and phosphatidylinositol phosphate fractions but not in bisphosphorylated phosphatidylinositol. myo-Inositol antagonized the growth-inhibitory effects of 3AMI. The v-sis NIH 3T3 cells were found to be more sensitive than the wild-type NIH 3T3 cells to growth inhibition (without 3AMI) caused by the removal of myo-inositol from the medium. The results of the study suggest that 3AMI is an antimetabolite of myo-inositol. The relative sensitivity of v-sis NIH 3T3 and some other cells to 3AMI may be a reflection of increased myo-inositol requirements for the growth of these cells as compared with wild-type NIH 3T3 cells.

Published

1994