Your search keyword '"Amy S Espeseth"' showing total 78 results

51. Compounds That Bind APP and Inhibit Aβ Processing in Vitro Suggest a Novel Approach to Alzheimer Disease Therapeutics

Author

Elizabeth Chen Dodson, Janet Lineberger, Adam J. Simon, Ming-Tain Lai, Mohinder K. Sardana, Beth Pietrak, Katherine Tugusheva, Berta Strulovici, Amy S. Espeseth, Xiao-Ping Shi, Guoxin Wu, Qian Huang, Renzo Bazzo, Ming-Chih Crouthamel, Eric A. Price, Abigail Wolfe, Yue-Ming Li, Daria J. Hazuda, Marc Ferrer, Jones Kristen L G, Paul Zuck, Craig A. Coburn, and Min Xu

Subjects

Peptide, Bioinformatics, Biochemistry, Amyloid beta-Protein Precursor, Alzheimer Disease, Endopeptidases, mental disorders, medicine, Amyloid precursor protein, Aspartic Acid Endopeptidases, Humans, Protease Inhibitors, Molecular Biology, chemistry.chemical_classification, Amyloid beta-Peptides, Binding Sites, Dose-Response Relationship, Drug, biology, P3 peptide, Cell Biology, medicine.disease, In vitro, Cell biology, Enzyme, Mechanism of action, chemistry, biology.protein, Amyloid Precursor Protein Secretases, medicine.symptom, Alzheimer's disease, Protein Processing, Post-Translational, Amyloid precursor protein secretase, HeLa Cells

Abstract

Extracellular deposits of aggregated amyloid-beta (Abeta) peptides are a hallmark of Alzheimer disease; thus, inhibition of Abeta production and/or aggregation is an appealing strategy to thwart the onset and progression of this disease. The release of Abeta requires processing of the amyloid precursor protein (APP) by both beta- and gamma-secretase. Using an assay that incorporates full-length recombinant APP as a substrate for beta-secretase (BACE), we have identified a series of compounds that inhibit APP processing, but do not affect the cleavage of peptide substrates by BACE1. These molecules also inhibit the processing of APP and Abeta by BACE2 and selectively inhibit the production of Abeta(42) species by gamma-secretase in assays using CTF99. The compounds bind directly to APP, likely within the Abeta domain, and therefore, unlike previously described inhibitors of the secretase enzymes, their mechanism of action is mediated through APP. These studies demonstrate that APP binding agents can affect its processing through multiple pathways, providing proof of concept for novel strategies aimed at selectively modulating Abeta production.

Published

2005

52. Discovery of Isonicotinamide Derived β-Secretase Inhibitors: In Vivo Reduction of β-Amyloid

Author

Sethu Sankaranarayanan, Samuel L. Graham, Matthew G. Stanton, Adam J. Simon, Amy S. Espeseth, Alison R. Gregro, Ming-Chih Crouthamel, Guoxin Wu, Xiao-Ping Shi, Shaun R. Stauffer, Qian Huang, Eric A. Price, Joseph P. Vacca, Lixia Jin, Philippe G. Nantermet, Dennis Colussi, Joan D. Ellis, Harold G. Selnick, Beth Pietrak, Min Xu, Melissa A. Steinbeiser, and Ming-Tain Lai

Subjects

Isostere, Biological Availability, Blood–brain barrier, Mice, Structure-Activity Relationship, chemistry.chemical_compound, In vivo, Drug Discovery, Amyloid precursor protein, medicine, Animals, Structure–activity relationship, Isonicotinamide, Amyloid beta-Peptides, Dose-Response Relationship, Drug, biology, Brain, Amides, Peptide Fragments, Rats, medicine.anatomical_structure, chemistry, Biochemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases, Isonicotinic Acids, Amyloid precursor protein secretase

Abstract

beta-Secretase inhibition offers an exciting opportunity for therapeutic intervention in the progression of Alzheimer's disease. A series of isonicotinamides derived from traditional aspartyl protease transition state isostere inhibitors has been optimized to yield low nanomolar inhibitors with sufficient penetration across the blood-brain barrier to demonstrate beta-amyloid lowering in a murine model.

Published

2007

53. Selective HDAC inhibition for the disruption of latent HIV-1 infection

Author

Yan Ling Zhang, Kara S. Keedy, Amy S. Espeseth, Florence F. Wagner, Edward Holson, David M. Margolis, Kirston Barton, Jennifer Gale, and Nancie M. Archin

Subjects

CD4-Positive T-Lymphocytes, Viral Diseases, Histone Deacetylase 2, lcsh:Medicine, HIV Infections, Histone Deacetylase 1, Immunodeficiency Viruses, Virus latency, Molecular Cell Biology, Medicine and Health Sciences, RNA, Small Interfering, Promoter Regions, Genetic, lcsh:Science, Cell Line, Transformed, Regulation of gene expression, 0303 health sciences, Gene knockdown, Multidisciplinary, Histone deacetylase 2, Chromosome Biology, 030302 biochemistry & molecular biology, Histone Modification, Chromatin, 3. Good health, Cell biology, Virus Latency, Infectious Diseases, Medical Microbiology, Viral Pathogens, Host-Pathogen Interactions, Epigenetics, Signal transduction, Research Article, Signal Transduction, Anti-HIV Agents, DNA transcription, Biology, Microbiology, Histone Deacetylases, 03 medical and health sciences, medicine, Genetics, Humans, Microbial Pathogens, 030304 developmental biology, Biology and life sciences, lcsh:R, HIV, Cell Biology, HDAC3, medicine.disease, Molecular biology, HDAC1, Histone Deacetylase Inhibitors, Gene Expression Regulation, HIV-1, lcsh:Q, Histone deacetylase, Gene expression, Gene Deletion

Abstract

Selective histone deacetylase (HDAC) inhibitors have emerged as a potential anti-latency therapy for persistent human immunodeficiency virus type 1 (HIV-1) infection. We utilized a combination of small molecule inhibitors and short hairpin (sh)RNA-mediated gene knockdown strategies to delineate the key HDAC(s) to be targeted for selective induction of latent HIV-1 expression. Individual depletion of HDAC3 significantly induced expression from the HIV-1 promoter in the 2D10 latency cell line model. However, depletion of HDAC1 or −2 alone or in combination did not significantly induce HIV-1 expression. Co-depletion of HDAC2 and −3 resulted in a significant increase in expression from the HIV-1 promoter. Furthermore, concurrent knockdown of HDAC1, −2, and −3 resulted in a significant increase in expression from the HIV-1 promoter. Using small molecule HDAC inhibitors of differing selectivity to ablate the residual HDAC activity that remained after (sh)RNA depletion, the effect of depletion of HDAC3 was further enhanced. Enzymatic inhibition of HDAC3 with the selective small-molecule inhibitor BRD3308 activated HIV-1 transcription in the 2D10 cell line. Furthermore, ex vivo exposure to BRD3308 induced outgrowth of HIV-1 from resting CD4+ T cells isolated from antiretroviral-treated, aviremic HIV+ patients. Taken together these findings suggest that HDAC3 is an essential target to disrupt HIV-1 latency, and inhibition of HDAC2 may also contribute to the effort to purge and eradicate latent HIV-1 infection.

Published

2014

54. Pentameric complex of viral glycoprotein H is the primary target for potent neutralization by a human cytomegalovirus vaccine

Author

Ningyan Zhang, Eberhard Durr, Zhiqiang An, Adam C. Finnefrock, Weixu Meng, John W. Shiver, Lin Xia, Tong-Ming Fu, Xi He, Danilo R. Casimiro, Daniel C. Freed, Zhao Huang, Fengsheng Li, Dai Wang, Amy S. Espeseth, Qi Tang, and Aimin Tang

Subjects

Human cytomegalovirus, medicine.drug_class, viruses, Cytomegalovirus, Antibodies, Viral, Monoclonal antibody, Virus, Cytomegalovirus Vaccines, Viral Envelope Proteins, Viral entry, medicine, Animals, Humans, chemistry.chemical_classification, Membrane Glycoproteins, Multidisciplinary, biology, Antibodies, Monoclonal, Antiviral antibody, medicine.disease, Antibodies, Neutralizing, Complementarity Determining Regions, Virology, PNAS Plus, chemistry, Multiprotein Complexes, Cytomegalovirus Infections, biology.protein, Female, Immunoglobulin Light Chains, Rabbits, Antibody, Cytomegalovirus vaccine, Immunoglobulin Heavy Chains, Glycoprotein, medicine.drug

Abstract

Human cytomegalovirus (HCMV) can cause serious morbidity/mortality in transplant patients, and congenital HCMV infection can lead to birth defects. Developing an effective HCMV vaccine is a high medical priority. One of the challenges to the efforts has been our limited understanding of the viral antigens important for protective antibodies. Receptor-mediated viral entry to endothelial/epithelial cells requires a glycoprotein H (gH) complex comprising five viral proteins (gH, gL, UL128, UL130, and UL131). This gH complex is notably missing from HCMV laboratory strains as well as HCMV vaccines previously evaluated in the clinic. To support a unique vaccine concept based on the pentameric gH complex, we established a panel of 45 monoclonal antibodies (mAbs) from a rabbit immunized with an experimental vaccine virus in which the expression of the pentameric gH complex was restored. Over one-half (25 of 45) of the mAbs have neutralizing activity. Interestingly, affinity for an antibody to bind virions was not correlated with its ability to neutralize the virus. Genetic analysis of the 45 mAbs based on their heavy- and light-chain sequences identified at least 26 B-cell linage groups characterized by distinct binding or neutralizing properties. Moreover, neutralizing antibodies possessed longer complementarity-determining region 3 for both heavy and light chains than those with no neutralizing activity. Importantly, potent neutralizing mAbs reacted to the pentameric gH complex but not to gB. Thus, the pentameric gH complex is the primary target for antiviral antibodies by vaccination.

Published

2013

55. siRNA screening of a targeted library of DNA repair factors in HIV infection reveals a role for base excision repair in HIV integration

Author

Qian Huang, Richard Fishel, Min Xu, Honglin Zhou, Daria J. Hazuda, Amy S. Espeseth, and Kristine E. Yoder

Subjects

Small interfering RNA, DNA, Complementary, DNA Repair, DNA repair, Virus Integration, Genetic Vectors, HIV integration, lcsh:Medicine, HIV Infections, Biology, Microbiology, Gene Knockout Techniques, Mice, 03 medical and health sciences, Transduction (genetics), Molecular cell biology, RNA interference, Immunodeficiency Viruses, Transduction, Genetic, Virology, Animals, Humans, RNA, Small Interfering, lcsh:Science, 3' Untranslated Regions, Gene Library, 030304 developmental biology, Cell Nucleus, 0303 health sciences, Gene knockdown, Multidisciplinary, 030302 biochemistry & molecular biology, lcsh:R, HIV, Reproducibility of Results, Genomics, Reverse Transcription, Base excision repair, Reverse transcriptase, 3. Good health, Host-Pathogen Interaction, DNA Repair Enzymes, lcsh:Q, Gene expression, Research Article, HeLa Cells

Abstract

Host DNA repair enzymes have long been assumed to play a role in HIV replication, and many different DNA repair factors have been associated with HIV. In order to identify DNA repair pathways required for HIV infection, we conducted a targeted siRNA screen using 232 siRNA pools for genes associated with DNA repair. Mapping the genes targeted by effective siRNA pools to well-defined DNA repair pathways revealed that many of the siRNAs targeting enzymes associated with the short patch base excision repair (BER) pathway reduced HIV infection. For six siRNA pools targeting BER enzymes, the negative effect of mRNA knockdown was rescued by expression of the corresponding cDNA, validating the importance of the gene in HIV replication. Additionally, mouse embryo fibroblasts (MEFs) lacking expression of specific BER enzymes had decreased transduction by HIV-based retroviral vectors. Examining the role BER enzymes play in HIV infection suggests a role for the BER pathway in HIV integration.

Published

2011

56. SAR of tertiary carbinamine derived BACE1 inhibitors: role of aspartate ligand amine pKa in enzyme inhibition

Author

Phung L. Ngo, Harold G. Selnick, Xiao Ping Shi, Dennis Colussi, Beth Pietrak, Sanjeev Munshi, Ming Tain Lai, Min Xu, Georgia B. McGaughey, James C. Barrow, Lawrence Kuo, Philippe G. Nantermet, Adam J. Simon, Mary Beth Young, Daria J. Hazuda, Stacey R. Lindsley, Hemaka A. Rajapakse, Ming-Chih Crouthamel, Amy S. Espeseth, Katherine Tugusheva, Samuel L. Graham, M. Katharine Holloway, Qian Huang, and Joseph P. Vacca

Subjects

Models, Molecular, Stereochemistry, Clinical Biochemistry, Cell, Pharmaceutical Science, Biochemistry, Catalysis, Structure-Activity Relationship, Drug Discovery, medicine, Potency, Aspartic Acid Endopeptidases, Humans, Amines, Enzyme Inhibitors, Molecular Biology, chemistry.chemical_classification, Aspartic Acid, biology, Organic Chemistry, Ligand (biochemistry), Enzyme assay, Enzyme, medicine.anatomical_structure, chemistry, biology.protein, Molecular Medicine, Amine gas treating, Amyloid Precursor Protein Secretases, Cell culture assays

Abstract

The optimization of tertiary carbinamine derived inhibitors of BACE1 from its discovery as an unstable lead to low nanomolar cell active compounds is described. Five-membered heterocycles are reported as stable and potency enhancing linkers. In the course of this work, we have discovered a clear trend where the activity of inhibitors at a given assay pH is dependent on pKa of the amino group that interacts directly with the catalytic aspartates. The potency of compounds as inhibitors of Αβ production in a cell culture assay correlated much better with BACE1 enzyme potency measured at pH 7.5 than at pH 4.5.

Published

2010

57. Host cell factors in HIV replication: meta-analysis of genome-wide studies

Author

Jason D Fernandes, Sourav Bandyopadhyay, Sumit K. Chanda, Tracy L. Diamond, Trey Ideker, Renate König, Gerard Cagney, Honglin Zhou, Nirav Malani, Frederic D. Bushman, Iván D'Orso, Daria J. Hazuda, Stephen P. Goff, John A. T. Young, Nevan J. Krogan, Amy S. Espeseth, Alan D. Frankel, and Rall, Glenn F

Subjects

lcsh:Immunologic diseases. Allergy, Immunology, Review, Biology, Virus Replication, Genome, DNA-binding protein, Microbiology, 03 medical and health sciences, Databases, Virology, Replication (statistics), Genetics, Humans, Cluster Analysis, 2.1 Biological and endogenous factors, Aetiology, Databases, Protein, Molecular Biology, Gene, lcsh:QH301-705.5, 030304 developmental biology, 0303 health sciences, Internet, Genome, Human, Protein, 030302 biochemistry & molecular biology, Human Genome, HIV, Infectious Diseases/HIV Infection and AIDS, Human genetics, 3. Good health, Infectious Diseases, Viral replication, lcsh:Biology (General), Medical Microbiology, Host-Pathogen Interactions, HIV/AIDS, Parasitology, Human genome, lcsh:RC581-607, Infection, Genetic screen, Protein Binding, Human, Biotechnology

Abstract

We have analyzed host cell genes linked to HIV replication that were identified in nine genome-wide studies, including three independent siRNA screens. Overlaps among the siRNA screens were very modest (

Published

2009

58. Expression of latent human immunodeficiency type 1 is induced by novel and selective histone deacetylase inhibitors

Author

David M. Margolis, Daria J. Hazuda, Herbert Dang, Kara S. Keedy, Nancie M. Archin, and Amy S. Espeseth

Subjects

CD4-Positive T-Lymphocytes, Immunology, Drug Evaluation, Preclinical, Histone Deacetylase 1, Biology, Virus Replication, Article, Chromatin remodeling, Jurkat Cells, Humans, Immunology and Allergy, Enzyme Inhibitors, Psychological repression, Cells, Cultured, HIV Long Terminal Repeat, Genetics, Chromatin, HDAC1, Virus Latency, Cell biology, Histone Deacetylase Inhibitors, Infectious Diseases, Histone, Acetylation, HIV-1, biology.protein, Histone deacetylase, HeLa Cells

Abstract

A family of histone deacetylases (HDACs) mediates chromatin remodeling, and repression of gene expression. Deacetylation of histones within the HIV-1 long terminal repeat (LTR) by HDACs plays a key role in the maintenance of latency, whereas acetylation of histones about the LTR is linked to proviral expression and escape of HIV from latency. Global HDAC inhibition may adversely affect host gene expression, leading to cellular toxicities. Potent inhibitors selective for HDACs that maintain LTR repression could be ideal antilatency therapeutics.We investigated the ability of selective HDAC inhibitors to de-repress the HIV-1 LTR in both a cell line model of latency and in resting CD4 T cells isolated from patients who were aviremic on antiretroviral therapy (ART).We found that inhibition of class I HDACs increased acetylation of histones at the LTR, but that LTR chromatin was unaffected by class II HDAC inhibitors. In a latently infected cell line, inhibitors selective for class I HDACs were more efficient activators of the LTR than inhibitors that target class II HDACs. Class I HDAC inhibitors were strikingly efficient inducers of virus outgrowth from resting CD4 T cells of aviremic patients, whereas HIV was rarely recovered from patient's cells exposed to class II HDAC inhibitors.Further development of selective HDAC inhibitors as part of a clinical strategy to target persistent HIV infection is warranted.

Published

2009

59. High-throughput screening by RNA interference: control of two distinct types of variance

Author

Adam J. Simon, William J. Ray, David J. Stone, Marc Ferrer, Amy S. Espeseth, Shane Marine, and John Majercak

Subjects

High-throughput screening, Negative control, Guidelines as Topic, Biology, Machine learning, computer.software_genre, RNA interference, False positive paradox, Animals, Humans, RNA, Small Interfering, Control (linguistics), Molecular Biology, Genetics, Observer Variation, Analysis of Variance, business.industry, Cell Biology, Variance (accounting), Research Design, RNA Interference, Artificial intelligence, business, Observer variation, computer, Developmental Biology

Abstract

The availability of genome-wide RNAi libraries has enabled researchers to rapidly assess the functions of thousands of genes; however the fact that these screens are run in living biological systems add complications above and beyond that normally seen in high-throughput screening (HTS). Specifically, error due to variance in both measurement and biology are large in such screens, leading to the conclusion that the majority of "hits" are expected to be false positives. Here, we outline basic guidelines for screen development that will help the researcher to control these forms of variance. By running a large number of positive and negative control genes, error of measurement can be accurately estimated and false negatives reduced. Likewise, by using a complex readout for the screen, which is not easily mimicked by other biological pathways and phenomena, false positives, can be minimized. By controlling variance in these ways, the researcher can maximize the utility of genome-wide RNAi screening.

Published

2007

60. Discovery of oxadiazoyl tertiary carbinamine inhibitors of beta-secretase (BACE-1)

Author

Stacey R. Lindsley, Georgia B. McGaughey, Xiao-Ping Shi, Lawrence Kuo, Katherine Tugusheva, Hemaka A. Rajapakse, Min Xu, Adam J. Simon, Sanjeev Munshi, Ming-Tain Lai, Samuel L. Graham, Mary Beth Young, Dennis Colussi, Qian Huang, Joseph P. Vacca, Harold G. Selnick, Beth Pietrak, Daria J. Hazuda, Amy S. Espeseth, Ming-Chih Crouthamel, and Philippe G. Nantermet

Subjects

chemistry.chemical_classification, Models, Molecular, Oxadiazoles, Aniline Compounds, Molecular model, biology, medicine.drug_class, Isostere, Chemistry, Stereochemistry, Carboxamide, Crystallography, X-Ray, Enzyme, Enzyme inhibitor, Drug Discovery, Hydrolase, medicine, biology.protein, Amyloid precursor protein, Molecular Medicine, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase

Abstract

We describe the discovery and optimization of tertiary carbinamine derived inhibitors of the enzyme beta-secretase (BACE-1). These novel non-transition-state-derived ligands incorporate a single primary amine to interact with the catalytic aspartates of the target enzyme. Optimization of this series provided inhibitors with intrinsic and functional potency comparable to evolved transition state isostere derived inhibitors of BACE-1.

Published

2006

61. LRRTM3 promotes processing of amyloid-precursor protein by BACE1 and is a positional candidate gene for late-onset Alzheimer's disease

Author

Min Xu, Kenneth S. Koblan, Steven R. Bartz, Krista Getty, Jason Kahana, Beth Pietrak, Daria J. Hazuda, William J. Ray, Erica Stec, Adam Gates, Xiao-Ping Shi, David J. Stone, Amy S. Espeseth, Dennis Colussi, Thomas W. Rosahl, Adam J. Simon, Qian Huang, Shane Marine, Mark S. Shearman, Marc Ferrer, Alan B. Sachs, Berta Strulovici, Carrie Wolffe, John Majercak, Paul J. Shughrue, Julja Burchard, Dirk Beher, Guy R. Seabrook, and Lei Ma

Subjects

Small interfering RNA, Nerve Tissue Proteins, Receptors, Cell Surface, Leucine-Rich Repeat Proteins, Amyloid beta-Protein Precursor, Mice, Alzheimer Disease, mental disorders, medicine, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Secretion, RNA, Small Interfering, Receptor, Cells, Cultured, Neurons, Multidisciplinary, Amyloid beta-Peptides, biology, Chromosomes, Human, Pair 10, Dentate gyrus, Membrane Proteins, Nuclear Proteins, Proteins, Biological Sciences, medicine.disease, Molecular biology, Transmembrane protein, Peptide Fragments, Enzyme Activation, biology.protein, Alzheimer's disease, Amyloid Precursor Protein Secretases, Carrier Proteins, Amyloid precursor protein secretase

Abstract

Rare familial forms of Alzheimer's disease (AD) are thought to be caused by elevated proteolytic production of the Aβ42 peptide from the β-amyloid-precursor protein (APP). Although the pathogenesis of the more common late-onset AD (LOAD) is not understood, BACE1, the protease that cleaves APP to generate the N terminus of Aβ42, is more active in patients with LOAD, suggesting that increased amyloid production processing might also contribute to the sporadic disease. Using high-throughput siRNA screening technology, we assessed 15,200 genes for their role in Aβ42 secretion and identified leucine-rich repeat transmembrane 3 ( LRRTM3 ) as a neuronal gene that promotes APP processing by BACE1. siRNAs targeting LRRTM3 inhibit the secretion of Aβ40, Aβ42, and sAPPβ, the N-terminal APP fragment produced by BACE1 cleavage, from cultured cells and primary neurons by up to 60%, whereas overexpression increases Aβ secretion. LRRTM3 is expressed nearly exclusively in the nervous system, including regions affected during AD, such as the dentate gyrus. Furthermore, LRRTM3 maps to a region of chromosome 10 linked to both LOAD and elevated plasma Aβ42, and is structurally similar to a family of neuronal receptors that includes the NOGO receptor, an inhibitor of neuronal regeneration and APP processing. Thus, LRRTM3 is a functional and positional candidate gene for AD, and, given its receptor-like structure and restricted expression, a potential therapeutic target.

Published

2006

62. Macrocyclic inhibitors of beta-secretase: functional activity in an animal model

Author

Timothy J. Allison, Beth Pietrak, Craig A. Coburn, Eric A. Price, Janet Lineberger, Samuel L. Graham, M. Katharine Holloway, Michelle Crouthamel, Adam J. Simon, Daria J. Hazuda, Guoxin Wu, Qian Huang, Joseph P. Vacca, Lixia Jin, Amy S. Espeseth, Sethu Sankaranarayanan, Sanjeev Munshi, Joan D. Ellis, and Shawn J. Stachel

Subjects

Macrocyclic Compounds, Stereochemistry, Molecular Conformation, Phthalic Acids, Stereoisomerism, Chemical synthesis, Mice, Structure-Activity Relationship, In vivo, Drug Discovery, Amyloid precursor protein, Structure–activity relationship, Animals, Protease Inhibitors, Tissue Distribution, chemistry.chemical_classification, Amyloid beta-Peptides, biology, Chemistry, Brain, Biological activity, Amides, Enzyme, Biochemistry, Enzyme inhibitor, Blood-Brain Barrier, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases

Abstract

A macrocyclic inhibitor of beta-secretase was designed by covalently cross-linking the P1 and P3 side chains of an isophthalamide-based inhibitor. Macrocyclization resulted in significantly improved potency and physical properties when compared to the initial lead structures. More importantly, these macrocyclic inhibitors also displayed in vivo amyloid lowering when dosed in a murine model.

Published

2006

63. BACE-1 inhibition by a series of psi[CH2NH] reduced amide isosteres

Author

Janet Lineberger, Thomas G. Steele, Diane M Rush, Ming-Tain Lai, Samuel L. Graham, M. Katharine Holloway, Qian Huang, Joseph P. Vacca, Adam J. Simon, Craig A. Coburn, Beth Pietrak, Daria J. Hazuda, Amy S. Espeseth, Lixia Jin, Sanjeev Munshi, Kristen G. Jones, Jillian DiMuzio, and Shawn J. Stachel

Subjects

Stereochemistry, Isostere, Clinical Biochemistry, Pharmaceutical Science, Peptide, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Structure-Activity Relationship, Amide, Drug Discovery, Hydrolase, Endopeptidases, Amyloid precursor protein, Peptide bond, Protease Inhibitors, Molecular Biology, chemistry.chemical_classification, Immunoassay, Binding Sites, biology, Chemistry, Organic Chemistry, Amides, Enzyme inhibitor, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases, Peptides

Abstract

A series of beta-site amyloid precursor protein cleaving enzyme (BACE-1) inhibitors containing a psi(CH2NH) reduced amide bond were synthesized. Incorporation of this reduced amide isostere as a non-cleavable peptide surrogate afforded inhibitors possessing low nanomolar potencies in both an enzymatic and cell-based assay.

Published

2006

64. Novel mutations introduced at the beta-site of amyloid beta protein precursor enhance the production of amyloid beta peptide by BACE1 in vitro and in cells

Author

James E. Bruce, Min Xu, Daria J. Hazuda, Jason Kahana, Abigail Wolfe, Mei Jy Tang, Guo Xin Wu, Beth Pietrak, Ming-Chih Crouthamel, Robert Bruce Register, Ming Tain Lai, Ronald A. Miller, Katherine Tugusheva, Amy S. Espeseth, Lin Chen, Adam Lucka, Sethu Sankaranarayanan, Qian Huang, Eric A. Price, Janet Lineberger, Yueming Li, Victor M. Garsky, Elizabeth Chen-Dodson, Binghua Hu, Xiao Ping Shi, Mohinder K. Sardana, Adam J. Simon, and Jillian DiMuzio

Subjects

Amyloid beta, Molecular Sequence Data, In Vitro Techniques, Transfection, Gene Expression Regulation, Enzymologic, Substrate Specificity, Amyloid beta-Protein Precursor, Mice, Alzheimer Disease, mental disorders, Endopeptidases, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Point Mutation, Protein precursor, Amyloid beta-Peptides, biology, Chemistry, General Neuroscience, P3 peptide, Antibodies, Monoclonal, General Medicine, Fibroblasts, Molecular biology, In vitro, Peptide Fragments, Biochemistry of Alzheimer's disease, Enzyme Activation, Psychiatry and Mental health, Clinical Psychology, Disease Models, Animal, Alpha secretase, biology.protein, Geriatrics and Gerontology, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase

Abstract

Abnormal production and accumulation of amyloid-beta peptide (Abeta) plays a major role in the pathogenesis of Alzheimer's disease (AD). beta-secretase (BACE1) is responsible for the cleavage at thebeta-site in amyloid beta protein precursor (AbetaPP/APP) to generate the N-terminus of Abeta. Here we report the stepwise identification and characterization of a novel APP-beta-site mutant, "NFEV" (APP_NFEV) in vitro and in cells. In vitro, the APP_NFEV exhibits 100-fold enhanced cleavage rate relative to the "wild-type" substrate (APPwt) and 10-fold increase relative to the Swedish-type mutation variant (APPsw). In cells, it was preferably cleaved among 24 APP beta-site mutations tested. More importantly, the APP_NFEV mutant failed to generate any detectable Abeta peptides in BACE1-KO mouse fibroblast cells. The production of Abeta peptides was restored by co-transfecting human BACE1, demonstrating that BACE1 is the only enzyme responsible for the processing of APP_NFEV in these cells. Analysis of APP_NFEV cleavage products secreted in the media revealed that in cells BACE1 cleaves APP_NFEV at the position between NF and EV, identical to that observed in vitro. A BACE inhibitor blocked the processing of the APP_NFEV beta-site in vitro and in cells. Our data indicates that the "NFEV" mutant is not only an enhanced substrate for BACE1 in vitro, but also a specific substrate for BACE1 in cells.

Published

2005

65. Biochemical and cell-based assays for characterization of BACE-1 inhibitors

Author

Katherine Tugusheva, Thomas G. Steele, Daria J. Hazuda, Ming-Chih Crouthamel, Samuel L. Graham, Joseph P. Vacca, Janet Lineberger, Min Xu, Amy S. Espeseth, Jillian DiMuzio, Shawn J. Stachel, Ming-Tain Lai, Beth Pietrak, Craig A. Coburn, Adam J. Simon, and Xiao-Ping Shi

Subjects

Biophysics, Cathepsin D, Transfection, Biochemistry, Sensitivity and Specificity, Cell Line, Amyloid beta-Protein Precursor, Endopeptidases, Amyloid precursor protein, Aspartic Acid Endopeptidases, Humans, Protease Inhibitors, Senile plaques, Molecular Biology, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Sulfonamides, biology, Chemistry, Cellular Assay, Assay, Cell Biology, Molecular biology, Enzyme, biology.protein, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase, Oligopeptides

Abstract

The deposition of beta-amyloid peptides (A beta42 and A beta40) in neuritic plaques is one of the hallmarks of Alzheimer's disease (AD). A beta peptides are derived from sequential cleavage of amyloid precursor protein (APP) by beta- and gamma-secretases. BACE-1 has been shown to be the major beta-secretase and is a primary therapeutic target for AD. In this article, two novel assays for the characterization of BACE-1 inhibitors are reported. The first is a sensitive 96-well HPLC biochemical assay that uses a unique substrate containing an optimized peptide cleavage sequence, NFEV, spanning from the P2-P2' positions This substrate was processed by BACE-1 approximately 10 times more efficiently than was the widely used substrate containing the Swedish (NLDA) sequence. As a result, the concentration of the enzyme required for the assay can be as low as 100 pM, permitting the evaluation of inhibitors with subnanomolar potency. The assay has also been applied to related aspartyl proteases such as cathepsin D (Cat D) and BACE-2. The second assay is a homogeneous electrochemiluminescence assay for the evaluation of BACE-1 inhibition in cultured cells that assesses the level of secreted amyloid EV40_NF from HEK293T cells stably transfected with APP containing the novel NFEV sequence. To illustrate the use of these assays, the properties of a potent, cell-active BACE-1 inhibitor are described.

Published

2005

66. Structure-based design of potent and selective cell-permeable inhibitors of human beta-secretase (BACE-1)

Author

Ming-Tain Lai, Kristen G. Jones, Janet Lineberger, Xiao-Ping Shi, Adam J. Simon, Alison R. Gregro, Joseph P. Vacca, Beth Pietrak, Min Xu, Craig A. Coburn, Hemaka A. Rajapakse, M. Katharine Holloway, Lawrence Kuo, Elizabeth F. Loutzenhiser, Thomas G. Steele, Amy S. Espeseth, Katherine Tugusheva, Sanjeev Munshi, Shawn J. Stachel, Ming-Chih Crouthamel, and Elizabeth Chen-Dodson

Subjects

Models, Molecular, Cell Membrane Permeability, medicine.drug_class, Cell, Carboxamide, Crystallography, X-Ray, Chemical synthesis, Cell Line, Structure-Activity Relationship, Drug Discovery, medicine, Amyloid precursor protein, Ethylamines, Aspartic Acid Endopeptidases, Humans, IC50, chemistry.chemical_classification, Sulfonamides, Binding Sites, biology, In vitro, Enzyme, medicine.anatomical_structure, Biochemistry, chemistry, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases

Abstract

We describe the development of cell-permeable β-secretase inhibitors that demonstratively inhibit the production of the secreted amino terminal fragment of an artificial amyloid precursor protein in cell culture. In addition to potent inhibition in a cell-based assay (IC50 < 100 nM), these inhibitors display impressive selectivity against other biologically relevant aspartyl proteases.

Published

2004

67. Diketo acid inhibitor mechanism and HIV-1 integrase: implications for metal binding in the active site of phosphotransferase enzymes

Author

Steve Young, Jay A. Grobler, Kara A. Stillmock, Joseph P. Vacca, Jeffrey Y. Melamed, Daria J. Hazuda, Peter J. Felock, Melissa S. Egbertson, Abigail Wolfe, John S. Wai, Amy S. Espeseth, Marc V. Witmer, Michele Bourgeois, and Binghua Hu

Subjects

Enzyme complex, Stereochemistry, Anti-HIV Agents, Context (language use), HIV Integrase, Ligands, Binding, Competitive, Styrenes, Phosphotransferase, chemistry.chemical_compound, Moiety, Humans, Magnesium, HIV Integrase Inhibitors, HIV Long Terminal Repeat, chemistry.chemical_classification, Manganese, Multidisciplinary, biology, Molecular Structure, Chemistry, Phosphotransferases, Active site, Biological Sciences, Integrase, Enzyme, Biochemistry, Models, Chemical, biology.protein, HIV-1, Streptavidin, DNA

Abstract

The process of integrating the reverse-transcribed HIV-1 DNA into the host chromosomal DNA is catalyzed by the virally encoded enzyme integrase (IN). Integration requires two metal-dependent reactions, 3′ end processing and strand transfer. Compounds that contain a diketo acid moiety have been shown to selectively inhibit the strand transfer reaction of IN in vitro and in infected cells and are effective as inhibitors of HIV-1 replication. To characterize the molecular basis of inhibition, we used functional assays and binding assays to evaluate a series of structurally related analogs. These studies focused on investigating the role of the conserved carboxylate and metal binding. We demonstrate that an acidic moiety such as a carboxylate or isosteric heterocycle is not required for binding to the enzyme complex but is essential for inhibition and confers distinct metal-dependent properties on the inhibitor. Binding requires divalent metal and resistance is metal dependent with active site mutants displaying resistance only when the enzymes are evaluated in the context of Mg 2+ . The mechanism of action of these inhibitors is therefore likely a consequence of the interaction between the acid moiety and metal ion(s) in the IN active site, resulting in a functional sequestration of the critical metal cofactor(s). These studies thus have implications for modeling active site inhibitors of IN, designing and evaluating analogs with improved efficacy, and identifying inhibitors of other metal-dependent phosphotransferases.

Published

2002

68. HIV-1 integrase inhibitors that compete with the target DNA substrate define a unique strand transfer conformation for integrase

Author

Steve Young, Melissa S. Egbertson, Peter J. Felock, Neville J. Anthony, James L. Cole, Marc V. Witmer, Amy S. Espeseth, Terence G. Hamill, Jay A. Grobler, Abigail Wolfe, Daria J. Hazuda, and Jeffrey Y. Melamed

Subjects

HIV Integrase, Epitope, Catalysis, Acetoacetates, Substrate Specificity, chemistry.chemical_compound, Epitopes, Pyrroles, HIV Integrase Inhibitors, Binding site, DNA Primers, Multidisciplinary, biology, Base Sequence, Drug discovery, Biological Sciences, Molecular biology, Long terminal repeat, Integrase, Scintillation proximity assay, Biochemistry, Viral replication, chemistry, DNA, Viral, biology.protein, HIV-1, DNA

Abstract

Diketo acids such as L-731,988 are potent inhibitors of HIV-1 integrase that inhibit integration and viral replication in cells. These compounds exhibit the unique ability to inhibit the strand transfer activity of integrase in the absence of an effect on 3′ end processing. To understand the reasons for this distinct inhibitory profile, we developed a scintillation proximity assay that permits analysis of radiolabeled inhibitor binding and integrase function. High-affinity binding of L-731,988 is shown to require the assembly of a specific complex on the HIV-1 long terminal repeat. The interaction of L-731,988 with the complex and the efficacy of L-731,988 in strand transfer can be abrogated by the interaction with target substrates, suggesting competition between the inhibitor and the target DNA. The L-731,988 binding site and that of the target substrate are thus distinct from that of the donor substrate and are defined by a conformation of integrase that is only adopted after assembly with the viral end. These results elucidate the basis for diketo acid inhibition of strand transfer and have implications for integrase-directed HIV-1 drug discovery efforts.

Published

2000

69. Inhibitors of strand transfer that prevent integration and inhibit HIV-1 replication in cells

Author

Lori J. Gabryelski, Peter J. Felock, Daria J. Hazuda, Carol Blau, Jay A. Grobler, Abigail Wolfe, Michael D. Miller, Marc V. Witmer, William A. Schleif, Amy S. Espeseth, and Kara A. Stillmock

Subjects

Transcription, Genetic, Anti-HIV Agents, T-Lymphocytes, Virus Integration, Integrase inhibitor, HIV Integrase, Virus Replication, Catalysis, Raltegravir Potassium, Acetoacetates, medicine, Tumor Cells, Cultured, Humans, Pyrroles, HIV Integrase Inhibitors, HIV Long Terminal Repeat, chemistry.chemical_classification, Multidisciplinary, biology, Drug Resistance, Microbial, Raltegravir, Virology, Coculture Techniques, Recombinant Proteins, Integrase, Enzyme, Viral replication, chemistry, Biochemistry, Enzyme inhibitor, DNA, Viral, Mutation, biology.protein, HIV-1, DNA, Circular, medicine.drug

Abstract

Integrase is essential for human immunodeficiency virus–type 1 (HIV-1) replication; however, potent inhibition of the isolated enzyme in biochemical assays has not readily translated into antiviral activity in a manner consistent with inhibition of integration. In this report, we describe diketo acid inhibitors of HIV-1 integrase that manifest antiviral activity as a consequence of their effect on integration. The antiviral activity of these compounds is due exclusively to inhibition of one of the two catalytic functions of integrase, strand transfer.

Published

2000

70. The Base Excision Repair Pathway Is Required for Efficient Lentivirus Integration

Author

Robert W. Sobol, R. Stephen Lloyd, Daria J. Hazuda, Maria Teresa Russo, Xiao-hong Wang, Kristine E. Yoder, Qingming Fang, Amy S. Espeseth, and Richard Fishel

Subjects

DNA, Complementary, Time Factors, DNA Repair, Cell Survival, DNA damage, DNA repair, Virus Integration, HIV integration, Active Transport, Cell Nucleus, NEIL1, lcsh:Medicine, HIV Infections, Biology, Microbiology, Cell Line, Mice, 03 medical and health sciences, Molecular cell biology, Virology, Host chromosome, Animals, Humans, lcsh:Science, 030304 developmental biology, Cell Nucleus, 0303 health sciences, Multidisciplinary, lcsh:R, Lentivirus, 030302 biochemistry & molecular biology, DNA, Reverse Transcription, Base excision repair, Molecular biology, 3. Good health, Host-Pathogen Interaction, Nucleic acids, DNA glycosylase, DNA, Viral, Lentivirus Infections, lcsh:Q, Gene Deletion, Research Article, DNA Damage, Signal Transduction

Abstract

An siRNA screen has identified several proteins throughout the base excision repair (BER) pathway of oxidative DNA damage as important for efficient HIV infection. The proteins identified included early repair factors such as the base damage recognition glycosylases OGG1 and MYH and the late repair factor POLß, implicating the entire BER pathway. Murine cells with deletions of the genes Ogg1, Myh, Neil1 and Polß recapitulate the defect of HIV infection in the absence of BER. Defective infection in the absence of BER proteins was also seen with the lentivirus FIV, but not the gammaretrovirus MMLV. BER proteins do not affect HIV infection through its accessory genes nor the central polypurine tract. HIV reverse transcription and nuclear entry appear unaffected by the absence of BER proteins. However, HIV integration to the host chromosome is reduced in the absence of BER proteins. Pre-integration complexes from BER deficient cell lines show reduced integration activity in vitro. Integration activity is restored by addition of recombinant BER protein POLß. Lentiviral infection and integration efficiency appears to depend on the presence of BER proteins.

Published

2011

71. Activity profile-based siRNA screen to explore the functional genomics of Alzheimer's disease

Author

Xiao-Ping Shi, Ken S. Koblan, Thomas W. Rosahl, Adam J. Simon, Dirk Beher, Berta Strulovici, Min Xu, Eric Minch, Ira Hoffman, Shane Marine, Daria J. Hazuda, Mark S. Shearman, Stacey Szymanski, John Majercak, David J. Stone, Marc Ferrer, Ansu Bagchi, Amy S. Espeseth, Peter Chase, William J. Ray, Adam Gates, Erica Stec, and Steven R. Bartz

Subjects

Small interfering RNA, RNA interference, HEK 293 cells, Biological activity, Human genome, Transfection, Biology, Functional genomics, Gene, Molecular biology, General Biochemistry, Genetics and Molecular Biology, Biotechnology, Cell biology

Abstract

Multiparametric assays generate biological activity profiles that provide valuable insight into complex disease models. The use of multiple assay measurements in RNA interference (RNAi) high-throughput screening (HTS) provides biological signatures produced by knocking down individual genes. This strategy has been applied to a genome-wide high-throughput small interfering RNA (siRNA) screen measuring proteolysis of β-amyloid precursor protein (APP) into amyloid β peptides, a critical step in the pathogenesis of Alzheimer’s disease. The assay measures amounts of secreted Aβ40, Aβ42, sAPPα, and sAPPβ from HEK 293 cells stably expressing an optimized APP construct following siRNA transfection. The effect of each siRNA on the four different APP products was simultaneously measured in order to identify human genes that regulate the amyloidogenic processing of APP. Genes with BACE-like and γ-secretase-like activity profiles were identified for further biological characterization.

Published

2007

72. Cover Picture: Design and Synthesis of 2,3,5-Substituted Imidazolidin-4-one Inhibitors of BACE-1 (ChemMedChem 7/2007)

Author

Sanjeev Munshi, Samuel L. Graham, Phung L. Ngo, Qian Huang, Joseph P. Vacca, Dennis Colussi, Katherine Tugusheva, Georgia B. McGaughey, Amy S. Espeseth, Ming-Tain Lai, Kenneth E. Rittle, Steven M. Pitzenberger, Adam J. Simon, James C. Barrow, and Harold G. Selnick

Subjects

Pharmacology, Chemistry, Stereochemistry, Organic Chemistry, Drug Discovery, β secretase, Molecular Medicine, Cover (algebra), General Pharmacology, Toxicology and Pharmaceutics, Biochemistry, Combinatorial chemistry

Published

2007

73. P4-418 Inhibition of APP processing by substrate-binding compounds: a novel approach to amyloid lowering

Author

Elizabeth Chen Dodson, Kate Tugusheva, Guoxin Wu, Qian Huang, Ming-Tain Lai, Lin Chen, Beth Pietrak, Ming-Chih Crouthamel, Janet Lineberger, Daria J. Hazuda, Yue-Ming Li, Abigail Wolfe, Kristen G. Jones, Min Xu, Marc Ferrer, Craig A. Coburn, Amy S. Espeseth, Xiao-Ping Shi, Eric A. Price, Adam J. Simon, and Paul Zuck

Subjects

Aging, Amyloid, Chemistry, General Neuroscience, Biophysics, Substrate (chemistry), Neurology (clinical), Geriatrics and Gerontology, Developmental Biology

Published

2004

74. P2-066 A genetically engineered mouse model with an enhanced beta-secretase substrate exhibits increased amyloid generation

Author

Richard Z. Chen, Michael J. Marino, Guoxin Wu, Elizabeth Chen, Lin Chen, Mohinder K. Sardana, Adam Lucka, Mei Tang, Xiao-Ping Shi, Sethu Sankaranarayanan, Adam J. Simon, Min Xu, Eric A. Price, Thomas F. Vogt, Daria J. Hazuda, and Amy S. Espeseth

Subjects

Aging, biology, Amyloid, Chemistry, General Neuroscience, Substrate (chemistry), Genetically Engineered Mouse, biology.protein, Biophysics, Neurology (clinical), Geriatrics and Gerontology, Beta (finance), Amyloid precursor protein secretase, Developmental Biology

Published

2004

75. Discovery and X-ray Crystallographic Analysis of a Spiropiperidine Iminohydantoin Inhibitor of β-Secretase.

Author

James C. Barrow, Shaun R. Stauffer, Kenneth E. Rittle, Phung L. Ngo, ZhiQiang Yang, Harold G. Selnick, Samuel L. Graham, Sanjeev Munshi, Georgia B. McGaughey, M. Katharine Holloway, Adam J. Simon, Eric A. Price, Sethu Sankaranarayanan, Dennis Colussi, Katherine Tugusheva, Ming-Tain Lai, Amy S. Espeseth, Min Xu, Qian Huang, and Abigail Wolfe

Published

2008

76. Retinoic acid receptor expression vector inhibits differentiation of F9 embryonal carcinoma cells

Author

Shawn P. Murphy, Amy S. Espeseth, and Elwood Linney

Subjects

Embryonal Carcinoma Stem Cells, Receptors, Retinoic Acid, Recombinant Fusion Proteins, Blotting, Western, Genetic Vectors, Retinoic acid, Gene Expression, Tretinoin, Retinoic acid receptor beta, Biology, Transfection, Cell Line, Retinoic acid-inducible orphan G protein-coupled receptor, chemistry.chemical_compound, Genetics, Humans, Cloning, Molecular, Cell Differentiation, Retinoic acid receptor gamma, Blotting, Northern, Retinoid X receptor gamma, Molecular biology, Retinoic acid receptor, Phenotype, P19 cell, chemistry, Retinoic acid receptor alpha, Neoplastic Stem Cells, Carrier Proteins, Developmental Biology

Abstract

Expression vectors have been constructed for a region of the human retinoic acid receptor-alpha (hRAR-alpha) and transferred into F9 embryonal carcinoma (EC) cells. When the vectors are overexpressed in F9 cells, clones can be selected for resistance to retinoic acid-induced differentiation. This effect is obtained even when the hRAR-alpha region is expressed as a beta-galactosidase fusion protein. Using the beta-galactosidase component of the fusion protein as a marker, overexpression of the fusion protein has been correlated with the retinoic acid-resistance effect. The clones resistant to retinoic acid no longer exhibit the normal retinoic acid induction of endo B cytokeratin, laminin B-1, and tissue plasminogen activator mRNAs observed with normal F9 cells. Retinoic acid induction of type IV alpha-1 collagen and Hox-1.3 RNAs is observed with these clones. When transfected with a thyroid receptor DNA-binding sequence (TRE)/thymidine kinase promoter/luciferase construct, the retinoic acid-resistant clones do not yield the same retinoic acid-induced level of luciferase obtained with F9 cells. It is hypothesized that the RAR vectors are interfering with endogenous RAR(s) in a dominant-negative manner to inhibit retinoic acid-induced differentiation of F9 EC cells.

Published

1989

77. Discovery of Isonicotinamide Derived -Secretase Inhibitors:  In Vivo Reduction of -Amyloid.

Author

Matthew G. Stanton, Shaun R. Stauffer, Alison R. Gregro, Melissa Steinbeiser, Philippe Nantermet, Sethu Sankaranarayanan, Eric A. Price, Guoxin Wu, Ming-Chih Crouthamel, Joan Ellis, Ming-Tain Lai, Amy S. Espeseth, Xiao-Ping Shi, Lixia Jin, Dennis Colussi, Beth Pietrak, Qian Huang, Min Xu, Adam J. Simon, and Samuel L. Graham

Published

2007

78. A phase 1, randomized, placebo-controlled study to evaluate the safety and immunogenicity of an mRNA-based RSV prefusion F protein vaccine in healthy younger and older adults

Author

Antonios O. Aliprantis, Christine A. Shaw, Paul Griffin, Nicholas Farinola, Radha A. Railkar, Xin Cao, Wen Liu, Jeffrey R. Sachs, Christine J. Swenson, Heather Lee, Kara S. Cox, Daniel S. Spellman, Colleen J. Winstead, Igor Smolenov, Eseng Lai, Tal Zaks, Amy S. Espeseth, and Lori Panther

Subjects

respiratory syncytial virus, rsv, vaccine, vaccine safety and immunogenicity, prefusion f, Immunologic diseases. Allergy, RC581-607, Therapeutics. Pharmacology, RM1-950

Abstract

Respiratory Syncytial Virus (RSV) causes lower respiratory tract infections that can be severe and sometimes fatal. The risk for severe RSV infection is highest in infants and older adults. A safe and effective RSV vaccine for older adults represents a serious unmet medical need due to higher morbidity and mortality in this age group. In this randomized, partially double-blind, placebo-controlled, phase 1 dose-escalation study, we evaluated the safety, tolerability and immunogenicity of an investigational messenger ribonucleic acid (mRNA) vaccine encoding the RSV fusion protein (F) stabilized in the prefusion conformation. The study was conducted in healthy younger adults (ages ≥18 and ≤49 years) and healthy older adults (ages ≥60 and ≤79 years). Participants received mRNA-1777 (V171) or placebo as a single intramuscular dose. For each dose level, three sentinel participants were administered open-label mRNA-1777 (V171). Seventy-two younger adults were randomized and administered 25, 100, or 200 µg mRNA-1777 (V171) or placebo, and 107 older adults were randomized and administered 25, 100, 200 or 300 µg mRNA-1777 (V171) or placebo. Primary objectives were safety and tolerability and secondary objectives included humoral and cell-mediated immunogenicity. All dose levels of mRNA-1777 (V171) were generally well tolerated and no serious adverse events related to the vaccine were reported. Immunization with mRNA-1777 (V171) elicited a humoral immune response as measured by increases in RSV neutralizing antibody titers, serum antibody titers to RSV prefusion F protein, D25 competing antibody titers to RSV prefusion F protein, and cell-mediated immune responses to RSV-F peptides.

Published

2021