Your search keyword '"Alcaro, M. C."' showing total 26 results

1. Genetic variants associated with rheumatoid arthritis patients and serotypes in European populations

Author

Ruiz-Larrañaga, O., Uribarri, M., Alcaro, M. C., Escorza-Treviño, S., Del Amo, J., Iriondo, M., Manzano, C., Migliorini, P., Lóránd, V., and Andone Estonba

Subjects

Adult, Male, Aged, Arthritis, Rheumatoid, Female, Humans, Middle Aged, Serogroup, Genetic Predisposition to Disease, Polymorphism, Single Nucleotide, Arthritis, Single Nucleotide, Rheumatoid, Polymorphism

Abstract

To replicate the association of rheumatoid arthritis (RA) susceptibility loci in an independent European sample and to assess their specificity with anti-citrullinated protein antibodies (ACPA) status.A selection of 64 SNP previously associated with RA have been typed in a cohort of 267 RA patients (169 ACPA-positive and 98 ACPA-negative) and 152 controls from the Rheumatology Units of the University Hospital of Pisa (Italy) and the University of Pécs Medical Center (Hungary). Regression analyses were performed first considering overall RA patients and secondly, taking both serotype subgroups as different disease entities. The results have been adjusted for age, gender and origin of individuals.The well-known CD2, REL, TNFAIP3, IRF5, PTPRC, and CCR6 have been confirmed as RA disease associated loci together with recently discovered BACH2, RASGRP1, and IKZF3 loci, taking all RA patients as a unique phenotype. Results from both serological subgroups separately reflect the specificity of these susceptibility loci and show additional ACPA-positive specific associations for variants at IL6R, IL2RA, BLK, DDX6, IL6, and TLE3 genes.The results from GAPAID project are consistent with previously established RA disease associations for CD2, PTPRC, REL, CCR6, TNFAIP3, IRF5, BLK, IL2RA, and DDX6 loci. In addition, IL6R, BACH2, RASGRP1, TLE3, and IKZF3 are replicated for the first time in an independent European population and IL6 appears to be a suggestive new RA associated locus. The stratified analysis based on ACPA status provides further support for distinct genetic aetiologies of RA subsets, which might have therapeutic implications.

Published

2015

2. The 'Chemical Reverse Approach to identify autoantibodies in Systemic Lupus Erithematosus patients

Author

Fantini, P., Alcaro, M. C., Paolini, I., Fabrizio Barbetti, Valoriani, D., Papini, A. M., Lolli, F., Rovero, P., Pratesi, F., and Migliorini, P.

Published

2010

3. Modified peptides as diagnostic tools for autoimmune diseases: A chemical reverse approach

Author

Paolini, I., Francesca Nuti, Alcaro, M. C., Pratesi, F., Migliorini, P., Lolli, F., Chelli, M., Rovero, P., and Papini, A. M.

Published

2007

4. GALACTOSYLATED PEPTIDES, THEIR PREPARATION AND USE IN AUTOIMMUNE DISEASES DIAGNOSIS'

Author

Alcaro, M. C., Chelli, M., Lolli, F., Migliorini, Paola, Paolini, I., Papini, A. M., and Rovero, P.

Published

2007

5. Conformationally driven rational design of glycopeptides as synthetic probes for the detection of autoantibodies, biomarkers of multiple sclerosis

Author

Carotenuto A., Alcaro M. C., Bonaccini C., Barbetti F., Lolli F., Tramontano A., Novellino E., Papini A. M., and Rovero P.

Published

2006

6. On-resin head-to-tail cyclization of cyclotetrapeptides: optimization of crucial parameters

Author

Alcaro M. C., Sabatino G., Uziel J., Chelli M., Ginanneschi M., Rovero P., and Papini A. M.

Published

2004

7. An Efficient Microwave-Assisted Synthesis of DKP Libraries

Author

Alcaro M. C., Campiglia P., Grieco P., Novellino E., M. Chelli, and Papini A. M.

Published

2003

8. Assessment of new 6-Cl-HOBt based coupling reagents for peptide synthesis. Part 1: Coupling efficiency study

Author

Sabatino G., Mulinacci B., Alcaro M. C., Chelli M., Rovero P., and Papini A. M.

Abstract

The efficiency of a series of well-known coupling reagents (TBTU, HATU, and PyBOP) and of new in situ activating reagents (TCTU, HCTU, and DMTMM) was compared by synthesizing the 65-74 fragment of the Acyl Carrier Protein (H-Val-Gln-Ala-Ala-Ile-Asp-Tyr-Ile-Asn-Gly-NH2), contg. a difficult sequence', as a test peptide, in a multiple peptide synthesizer. The longer sequence rMOG(35-55) was also synthesized. It was clear that the aminium salts are more efficient than the phosphonium salt (PyBOP) and that the new 6Cl-HOBt based reagents (HCTU and particularly TCTU) are very efficient, while DMTMM appeared to be not suitable for SPPS.

Published

2003

9. Solid-phase approach to the synthesis of cyclen scaffolds from cyclotetrapeptides

Author

Alcaro M. C., Orfei M., Chelli M., Ginanneschi M., and Papini A. M.

Abstract

Cyclen derivs., as coordinating ligands, have recovered considerable interest for the development of diagnostic and therapeutic drugs, mimicking the binding site of metalloproteins. We demonstrate that the on-resin redn. of head-to-tail cyclotetrapeptides, anchored to a solid support by the side-chain of a trifunctional amino acid, is an efficient synthetic strategy. The proposed approach leads to the cyclen scaffold still bound to the resin, ready for further decorations.

Published

2003

10. New Constrained Amino Acids for the Study of the Role of the Basic Residues in Bradykinin Antagonists

Author

Alcaro, M. C., Anichini, Beatrice, Terzani, Tullio, Nuti, Francesca, Chelli, Mario, Machetti, Fabrizio, Quaratara, Laura, Maggi, C. A. MAGGI, Brandi, Alberto, and Papini, Anna Maria

Published

2002

11. THU0093 Deiminated Histone 4 from Neutrophil Extracellular Traps is a Novel Autontigen in Rheumatoid Arthritis

Author

Migliorini, P., primary, Pratesi, F., additional, Dioni, I., additional, Alcaro, M. C., additional, Paolini, I., additional, Panza, F., additional, and Rovero, P., additional

Published

2013

12. Carbonic Anhydrase Inhibitors:  The First On-Resin Screening of a 4-Sulfamoylphenylthiourea Library

Author

Innocenti, A., Casini, A., Alcaro, M. C., Papini, A. M., Scozzafava, A., and Supuran, C. T.

Abstract

Sulfonamide carbonic anhydrase (CA) inhibitors are widely employed in the diagnosis and treatment of diverse diseases such as glaucoma and different neuromuscular disorders. Moreover, an emerging area is represented by their use in the prevention and treatment of tumors. In this paper we propose an optimized synthesis of on-resin CA inhibitor libraries to be used for a high-throughput biological screening. A library of 4-sulfamoylphenylthioureas, previously described to be attractive candidates as novel antiglaucoma drugs, has been synthesized by a solid-phase approach, avoiding the formation of thiohydantoin side products. The on-resin screening assay has been developed for the inhibition tests of different CA isozymes with the on-resin supported sulfonamides, allowing the direct identification of the biologically active lead compounds. These results allow the development of new designed libraries in the solid phase of sulfonamide CA inhibitors characterized by a set of prefixed parameters to be used as possible drug candidates.

Published

2004

13. A chemical reverse approach for autoimmune diseases diagnosis

Author

Alcaro, M. C., Paolini, I., Fantini, P., Fabrizio Barbetti, Chelli, M., Migliorini, P., Lolli, F., Rovero, P., and Papini, A. M.

14. Influence of MTHFR C677T polymorphism on methotrexate monotherapy discontinuation in rheumatoid arthritis patients: Results: from the GAPAID European project

Author

Uribarri, M., Ruiz-Larrañaga, O., Arteta, D., Hernández, L., Alcaro, M. C., Martínez, A., Escorza-Treviño, S., Andone Estonba, Migliorini, P., Czirják, L., and Del Amo, J.

Subjects

Male, Heterozygote, Time Factors, Aged, Antirheumatic Agents, Arthritis, Rheumatoid, Chi-Square Distribution, Female, Homozygote, Humans, Hungary, Italy, Kaplan-Meier Estimate, Longitudinal Studies, Methotrexate, Methylenetetrahydrofolate Reductase (NADPH2), Middle Aged, Odds Ratio, Pharmacogenetics, Phenotype, Retrospective Studies, Risk Factors, Treatment Outcome, Polymorphism, Genetic, Genetic, Rheumatoid, Polymorphism, Arthritis

Abstract

Methotrexate (MTX) is the most widely prescribed drug for rheumatoid arthritis (RA) patients, but 45% of them discontinue therapy within two years, either due to inefficacy or toxicity. Several authors have reported contradictory results related to C677T polymorphism in the MTHFR gene and response to MTX in RA. The purpose of this study was to further explore this genotype-response association in a European RA population.This retrospective longitudinal study included a total of 269 RA patients from Italy and Hungary, of whom 73.2% had available data on MTX treatment (197 patients). C677T polymorphism (rs1801133) was genotyped by quantitative PCR using TaqMan assays. Genotype association analysis and Kaplan-Meier method were used for statistical comparisons between patients continuing and patients who abandoned MTX treatment.A total of 85 out of the 197 RA patients (43%) abandoned MTX treatment by the time of analysis. No significant genotype-MTX discontinuation association was found for the overall population, either at the end of the study (p=0.375), or during the follow-up (p=0.324). When the analysis was restricted to the 68 patients on MTX monotherapy, a borderline association (OR 3.15, 95% CI 0.93-10.67, p=0.057) was noted with the recessive genetic model. In agreement with that, a Kaplan-Meier analysis showed a significantly shorter time-to-discontinuation of MTX monotherapy for homozygous carriers of the T-allele (p=0.042).These results demonstrate that the C677T polymorphism in the MTHFR gene is involved in MTX monotherapy discontinuation in a multicentre European patient cohort, confirming previous results.

15. An efficient microwave-assisted solid phase synthesis of gramicidin A for studies in bilayer-lipid membrane

Author

Rizzolo, F., Sabatino, G., Paolini, I., Alcaro, M. C., Moncelli, M. R., Guidelli, R., Mario Chelli, Papini, A. M., and Rovero, P.

16. Feline immunodeficiency virus plasma load reduction by a retroinverso octapeptide reproducing the Trp-rich motif of the transmembrane glycoprotein

Author

Giannecchini, S., Alcaro, M. C., Isola, P., Sichi, O., Pistello, M., Anna Maria Papini, Rovero, P., and Bendinelli, M.

Subjects

Pharmacology, Amino Acid Motifs, Molecular Sequence Data, Drug Evaluation, Preclinical, Tryptophan, Transmembrane glycoprotein, Immunodeficiency Virus, Feline, Viral Load, Antiviral Agents, FIV, Infectious Diseases, Feline immunodeficiency virus, Cell Line, Tumor, Feline Acquired Immunodeficiency Syndrome, Chronic Disease, Cats, Animals, Pharmacology (medical), Female, Amino Acid Sequence, Oligopeptides

Abstract

The Trp-rich motif (TrpM) of the transmembrane glycoprotein (TM) of lentiviruses is an attractive domain on which to design new potential cell entry peptide inhibitors. We recently demonstrated that an octapeptide reproducing the TrpM of feline immunodeficiency virus (FIV), designated C8, broadly inhibited this virus in vitro and that the retroinverso analogue of this peptide (riC8) was almost as inhibitory and exhibited features suggestive of a much increased stability. Here, we demonstrated that riC8 is indeed highly stable, maintaining its concentration unchanged for at least 24 h in cat serum in vitro. Furthermore, once inoculated into cats, riC8 produced no major acute toxic effects and exhibited satisfactory pharmacokinetic properties. Finally, we report the results of a short-term monotherapy experiment in chronically FIV-infected cats showing that riC8 is well tolerated and also has substantial antiviral activity in vivo. In particular, the mean viral load of riC8-treated animals declined progressively with increasing time of treatment, whereas that of control animals given C8 or solvent alone did not. These results provide the first evidence that clinically useful inhibition of virus replication with a small peptide derived from a functional domain of the TM of a lentivirus can be achieved in vivo.

17. Conformationally driven rational design of glycopeptides as synthetic probes for the detection of autoantibodes, biomarkers of multiple sclerosis

Author

Carotenuto, A., Alcaro, M. C., Bonaccini, C., Fabrizio Barbetti, Lolli, F., Chelli, M., Tramontano, A., Novellino, E., Papini, A. M., and Rovero, P.

18. Assessment of 6Cl-HOBt-based coupling reagents in solid-phase cyclopeptide synthesis

Author

Giuseppina Sabatino, Alcaro, M. C., Pozo-Carrero, M. C., Chelli, M., Rovero, P., and Papini, A. M.

19. New generation of families of antigenic probes for detection of multiple sclerosis biomarkers

Author

Alcaro, M. C., Nuti, F., Bonechi, G., Fabrizio Barbetti, Carotenuto, A., Bonaccini, C., Gratteri, P., Tramontano, A., Lolli, F., Chelli, M., Novellino, E., Rovero, P., Papini, A. M., M. C., Alcaro, F., Nuti, G., Bonechi, F., Barbetti, Carotenuto, Alfonso, C., Bonaccini, P., Gratteri, A., Tramontano, F., Lolli, M., Chelli, Novellino, Ettore, P., Rovero, and A. M., Papini

Subjects

Multiple Sclerosis

20. Identification of cytoskeletal proteins monoclonal antibodies recognized by CSF114(Glc), the synthetic probe of Multiple Sclerosis

Author

Shashank, S. P., Lambardi, D., Alcaro, M. C., Fernandez, F. R., Peroni, E., Rovero, P., Mario Chelli, Lolli, F., and Papini, A. M.

21. Evaluation of new immunological targets in neuromyelitis optica

Author

Jerome de Seze, Collongues, N., Paolini, I., Chanson, J. B., Alcaro, M. C., Blanc, F., Lolli, F., Fleury, M., Rudolf, G., Rovero, P., Trifilieff, E., and Papini, A. M.

22. Identification of the minimal epitope(s) mimicked by the synthetic glucopeptide CSF114(Glc)

Author

Nuti, F., Alcaro, M. C., Paolini, I., Peroni, E., Ciolli, F., Mario Chelli, Lolli, F., Rovero, P., and Papini, A. M.

23. Designed Glycopeptides with Different β-Turn Types as Synthetic Probes for the Detection of Autoantibodies as Biomarkers of Multiple Sclerosis

Author

Anna Maria Papini, Maria C. Alcaro, E. Peroni, Francesca Nuti, Alfonso Carotenuto, Paolo Rovero, Ettore Novellino, Maria Rosaria Saviello, Carotenuto, Alfonso, Alcaro, M. C., Saviello, M. R., Peroni, E., Nuti, F., Papini, A. M., Novellino, Ettore, and Rovero, P.

Subjects

Multiple Sclerosis, Chemistry, Antibody Affinity, Glycopeptides, Autoantibody, Context (language use), medicine.disease_cause, Protein Structure, Secondary, Epitope, Glycopeptide, Autoimmunity, Antigen-Antibody Reactions, Structure-Activity Relationship, Blood serum, Antigen, Biochemistry, Drug Design, Molecular Probes, Drug Discovery, medicine, Humans, Molecular Medicine, Biomarker (medicine), Biomarkers, Autoantibodies

Abstract

Circulating autoantibodies have been recognized as disease biomarkers of autoimmune diseases. We have previously disclosed a synthetic glycopeptide that is able to detect specific autoantibodies in sera of patients who are affected by multiple sclerosis (MS). This glycopeptide is characterized by a type I' beta-turn around the minimal epitope Asn(Glc) that allows an efficient exposure of this moiety to antibody interactions in the context of a solid-phase immunoenzymatic assay. With the aim of optimizing the glycopeptide-antibody interactions, we analyze a series of new glycopeptides based on different turn structures. Our results confirm the role of conformation in the recognition and binding of synthetic antigenic probes to MS autoantibodies. Glycopeptide 2, which is characterized by a type I beta-turn around the minimal epitope Asn(Glc), shows the highest antibody affinity (IC50 = 11.8 nM), and thus it appears to be a promising tool for the detection of specific autoantibodies as MS biomarker in patients' sera.

Published

2008

24. An N-glucosylated peptide detecting disease-specific autoantibodies, biomarkers of multiple sclerosis

Author

Alfonso Carotenuto, Barbara Mulinacci, Maria C. Alcaro, Laura Lovato, Maria de la Cruz Pozo-Carrero, Ettore Novellino, Elisa Peroni, Giuseppina Sabatino, Anna Maria Papini, Giovanna Borsellino, Luca Battistini, Bruno Bonetti, Paolo Rovero, Benedetta Mazzanti, Marta Pazzagli, Francesca Nuti, Mario Chelli, Francesco Lolli, Anna Maria D'Ursi, Lolli, F, Mulinacci, B, Carotenuto, Alfonso, Bonetti, B, Sabatino, G, Mazzanti, B, D'URSI A., M, Novellino, E, Pazzagli, M, Lovato, L, ALCARO M., C, Peroni, E, POZO CARRERO M., C, Nuti, F, Battistini, L, Borsellino, G, Chelli, M, Rovero, P, and Papini, A. M.

Subjects

synthetic antigen, Adult, Magnetic Resonance Spectroscopy, Multiple Sclerosis, Synthetic antigen, Enzyme-Linked Immunosorbent Assay, macromolecular substances, aberrant glycosylation, prognostic probe, β-hairpin, Myelin, Antigen, medicine, Humans, Autoantibodies, Immunoassay, Multidisciplinary, medicine.diagnostic_test, business.industry, Multiple sclerosis, Glycopeptides, Autoantibody, Biological Sciences, Middle Aged, medicine.disease, Immunohistochemistry, Oligodendrocyte, carbohydrates (lipids), medicine.anatomical_structure, Immunology, beta-hairpin, MYELIN OLIGODENDROCYTE GLYCOPROTEIN, BASIC-PROTEIN, NEUROLOGICAL DISEASES, ANTIBODY, PATHOGENESIS, LESIONS, MOG, HETEROGENEITY, DEMYELINATION, REACTIVITY, business, Biomarkers

Abstract

Multiple sclerosis (MS) is a complex disease that seems to depend on several pathophysiological processes. Because of its varied clinical presentation, natural history, and response to therapeutic interventions, MS can be considered to be a group of diseases that have not been yet characterized, thus resulting in difficult evaluation of prognosis. In the last few years, the role of autoAbs in MS has been reevaluated, and, therefore, their identification as specific biomarkers became a relevant target. In this paper, we demonstrate that an aberrant N -glucosylation is a fundamental determinant of autoAb recognition in MS. Thus, we developed CSF114(Glc), an antigenic probe accurately measuring IgM autoAbs in the sera of a patient population, as disease biomarker. The relevance of CSF114(Glc) is demonstrated by its clinical application and correlation with disease activity and prognosis. In fact, CSF114(Glc), a structure-based designed glycopeptide, is able to recognize, by ELISA, the presence of specific IgM autoAbs in the sera of a MS patient population but not in blood donors and other autoimmune conditions. AutoAbs specific for CSF114(Glc) isolated from MS patients recognized myelin and oligodendrocyte antigens by immunohistochemistry but not other nonrelevant tissues. We demonstrate that CSF114(Glc) is a reliable, specific probe in a longitudinal study of untreated MS patients. Development of IgG/IgM anti-CSF114(Glc) Abs paralleled clinical activity and brain lesions positive to MRI. Therefore, a CSF114(Glc)-based immunoassay on sera may have important prognostic value in monitoring MS disease progression guiding optimal therapeutic treatment.

Published

2005

25. Designed glucopeptides mimetics of myelin protein epitopes as synthetic probes for the detection of autoantibodies, biomarkers of multiple sclerosis

Author

Ettore Novellino, Francesca Barbetti, Shashank Pandey, Sara Di Marino, Elisa Peroni, Anna Maria Papini, Mario Scrima, Anna Maria D'Ursi, Ilaria Paolini, Alfonso Carotenuto, Paolo Rovero, Maria C. Alcaro, Pandey, S., Alcaro, M. C., Scrima, M., Peroni, E., Paolini, I., Di Marino, S., Barbetti, F., Carotenuto, Alfonso, Novellino, Ettore, Papini, A. M., D'Ursi, A. M., and Rovero, P.

Subjects

Models, Molecular, Magnetic Resonance Spectroscopy, Multiple Sclerosis, Molecular Sequence Data, Homology (biology), Epitope, Epitopes, Myelin, Drug Discovery, medicine, Humans, Multiple sclerosi, Amino Acid Sequence, Conformation, Autoantibodies, Sequence Homology, Amino Acid, Chemistry, Multiple sclerosis, Molecular Mimicry, Glycopeptides, Autoantibody, Antibody titer, Biomarker, Nuclear magnetic resonance spectroscopy, NMR conformational analysi, medicine.disease, Molecular biology, medicine.anatomical_structure, Biochemistry, Molecular Medicine, Biomarker (medicine), glucopeptides, Myelin Proteins

Abstract

We previously reported that CSF114(Glc) detects diagnostic autoantibodies in multiple sclerosis sera. We report herein a bioinformatic analysis of myelin proteins and CSF114(Glc), which led to the identification of five sequences. These glucopeptides were synthesized and tested in enzymatic assays, showing a common minimal epitope. Starting from that, we designed an optimized sequence, SP077, showing a higher homology with both CSF114(Glc) and the five sequences selected using the bioinformatic approach. SP077 was synthesized and tested on 50 multiple sclerosis patients' sera, and was able to detect higher antibody titers as compared to CSF114(Glc). Finally, the conformational properties of SP077 were studied by NMR spectroscopy and structure calculations. Thus, the immunological activity of SP077 in the recognition of specific autoantibodies in multiple sclerosis patients' sera may be ascribed to both the optimized design of its epitopic region and the superior surface interacting properties of its C-terminal region.

Published

2012

26. Development of antiviral fusion inhibitors: short modified peptides derived from the transmembrane glycoprotein of feline immunodeficiency virus

Author

D'Ursi, Anna Maria, Giannecchini, S, Esposito, Cinzia, Alcaro, Mc, Sichi, O, Armenante, Mr, Carotenuto, A, Papini, Am, Bendinelli, M, RELATED ARTICLES, ROVERO P., Links, DEVELOPMENT OF ANTIVIRAL FUSION INHIBITORS SHORT MODIFIED PEPTIDES DERIVED FROM THE TRANSMEMBRANE GLYCOPROTEIN OF FELINE IMMUNODEFICIENCY VIRUS, D'URSI A., M, Giannecchini, S, Esposito, C, ALCARO M., C, Sichi, O, ARMENANTE M., R, Carotenuto, Alfonso, PAPINI A., M, Bendinelli, M, and Rovero, P.

Subjects

Models, Molecular, Feline immunodeficiency virus, Magnetic Resonance Spectroscopy, Molecular Conformation, Peptide, Microbial Sensitivity Tests, Immunodeficiency Virus, Feline, In Vitro Techniques, Biochemistry, Antiviral Agents, Membrane Fusion, Structure-Activity Relationship, In vivo, Structure–activity relationship, Animals, Molecular Biology, chemistry.chemical_classification, Membrane Glycoproteins, biology, Organic Chemistry, Lipid bilayer fusion, biology.organism_classification, In vitro, Peptide Fragments, Amino acid, Enzyme, chemistry, Amino Acid Substitution, Cats, Molecular Medicine

Abstract

Feline immunodeficiency virus (FIV) is a naturally occurring pathogen that causes an AIDS-like syndrome in domestic cats and is a valuable model system by which criteria for antiviral vaccines and drugs development can be tested. The cell-entry step of the lentivirus life cycle is regarded as a promising target for the development of new generation inhibitors. We have previously described potent in vitro anti-FIV activity associated with a synthetic octapeptide, termed C8 (Ac-Trp-Glu-Asp-Trp-Val-Gly-Trp-Ile-NH2), containing the Trp-rich motif of FIV transmembrane glycoprotein, which shares a common structural framework with the corresponding molecule of HIV and appears to play a similar role in cell entry. In this report, in an attempt to develop simpler potential fusion inhibitors to be tested in vivo, we describe further studies focused on synthetic peptide analogues of C8. Since C8 inhibitory activity is dependent upon the Trp motif, we systematically replaced these residues with bulky and/or aromatic natural and unnatural amino acids, in order to develop a rational structure-activity relationship. Furthermore, the amino acids located between the Trp residues, which are not crucial for inhibitory activity, were replaced by simple alkyl spacers of appropriate length. Design, NMR structural analysis, in vitro anti-FIV activity in lymphoid cell cultures, and serum stability of these new analogues are reported. The final results indicate that a simpler hexapeptide (Ac-Nal2-Ape-Nal2-Ape-Nal2-Ile-NH2; Nal2 = 3-naphthalen-2-yl-L-alanine, Ape = 5-aminopentanoic acid), almost entirely made up of unnatural amino acid residues, has markedly increased enzymatic stability, while maintaining strong antiviral potency in vitro.

Published

2006