论文信息 - De novo design of antimicrobial polymers, foldamers, and small molecules: from discovery to practical applications.

De novo design of antimicrobial polymers, foldamers, and small molecules: from discovery to practical applications.

Antimicrobial peptides (AMPs) provide protection against a variety of pathogenic bacteria and are, therefore, an important part of the innate immune system. Over the past decade, there has been considerable interest in developing AMPs as intravenously administered antibiotics. However, despite extensive efforts in the pharmaceutical and biotechnology industry, it has proven difficult to achieve this goal. While researchers have solved some relatively simple problems such as susceptibility to proteolysis, more severe problems have included the expense of the materials, toxicity, poor efficacy, and limited tissue distribution. In this Account, we describe our efforts to design and synthesize "foldamers"-- short sequence-specific oligomers based on arylamide and beta-amino acid backbones, which fold into well-defined secondary structures-- that could act as antimicrobial agents. We reasoned that small "foldamers" would be less expensive to produce than peptides, and might have better tissue distribution. It should be easier to fine-tune the structures and activities of these molecules to minimize toxicity. Because the activities of many AMPs depends primarily on their overall physicochemical properties rather than the fine details of their precise amino acid sequences, we have designed and synthesized very small "coarse-grained" molecules, which are far simpler than naturally produced AMPs. The molecular design of these foldamers epitomizes the positively charged amphiphilic structures believed to be responsible for the activity of AMPs. The designed oligomers show greater activity than the parent peptides. They have also provided leads for novel small molecule therapeutics that show excellent potency in animal models for multidrug resistant bacterial infections. In addition, such molecules can serve as relatively simple experimental systems for investigations aimed at understanding the mechanism of action for this class of antimicrobial agents. The foldamers' specificity for bacterial membranes relative to mammalian membranes appears to arise from differences in membrane composition and physical properties between these cell types. Furthermore, because experimental coarse-graining provided such outstanding results, we developed computational coarse-grained models to enable molecular dynamic simulations of these molecules with phospholipid membranes. These simulations allow investigation of larger systems for longer times than conventional molecular dynamics simulations, allowing us to investigate how physiologically relevant surface concentrations of AMP mimics affect the bilayer structure and properties. Finally, we apply the principles discovered through this work to the design of inexpensive antimicrobial polymers and materials.

[1] W. DeGrado,et al. De novo design and in vivo activity of conformationally restrained antimicrobial arylamide foldamers , 2009, Proceedings of the National Academy of Sciences.

[2] W. DeGrado,et al. The role of hydrophobicity in the antimicrobial and hemolytic activities of polymethacrylate derivatives. , 2009, Chemistry.

[3] G. J. Gabriel,et al. Comparison of facially amphiphilic versus segregated monomers in the design of antibacterial copolymers. , 2009, Chemistry.

[4] Gregory N Tew,et al. De novo designed synthetic mimics of antimicrobial peptides. , 2008, Current opinion in biotechnology.

[5] J. Nowick. Exploring beta-sheet structure and interactions with chemical model systems. , 2008, Accounts of chemical research.

[6] Y. Shai,et al. Antimicrobial lipopolypeptides composed of palmitoyl Di- and tricationic peptides: in vitro and in vivo activities, self-assembly to nanostructures, and a plausible mode of action. , 2008, Biochemistry.

[7] G. Tew,et al. Antimicrobial polymers prepared by ROMP with unprecedented selectivity: a molecular construction kit approach. , 2008, Journal of the American Chemical Society.

[8] W Seth Horne,et al. Foldamers with heterogeneous backbones. , 2008, Accounts of chemical research.

[9] S. Gellman,et al. Dual mechanism of bacterial lethality for a cationic sequence-random copolymer that mimics host-defense antimicrobial peptides. , 2008, Journal of molecular biology.

[10] M. Struelens,et al. The bacterial envelope as a target for novel anti-MRSA antibiotics. , 2008, Trends in pharmacological sciences.

[11] A. Ramamoorthy,et al. Using Fluorous Amino Acids to Modulate the Biological Activity of an Antimicrobial Peptide , 2008, Chembiochem : a European journal of chemical biology.

[12] Alisa Opar. Bad bugs need more drugs , 2007, Nature Reviews Drug Discovery.

[13] S. Gellman,et al. Mimicry of antimicrobial host-defense peptides by random copolymers. , 2007, Journal of the American Chemical Society.

[14] Scott J. Shandler,et al. Foldamers as versatile frameworks for the design and evolution of function. , 2007, Nature chemical biology.

[15] G. Wong,et al. Synthetic antimicrobial oligomers induce a composition-dependent topological transition in membranes. , 2007, Journal of the American Chemical Society.

[16] D. Cardo,et al. Estimating Health Care-Associated Infections and Deaths in U.S. Hospitals, 2002 , 2007, Public health reports.

[17] S. Gellman,et al. Interplay among Folding, Sequence, and Lipophilicity in the Antibacterial and Hemolytic Activities of α/β-Peptides , 2007 .

[18] Y. Shai,et al. Host defense peptides and lipopeptides: modes of action and potential candidates for the treatment of bacterial and fungal infections. , 2006, Current protein & peptide science.

[19] S. Gellman,et al. Role of membrane lipids in the mechanism of bacterial species selective toxicity by two α/β-antimicrobial peptides , 2006 .

[20] J. Lehn,et al. Formation of RACK- and grid-type metallosupramolecular architectures and generation of molecular motion by reversible uncoiling of helical ligand strands. , 2006, Chemistry.

[21] Michelle D. Brazas,et al. Contribution of the PhoP-PhoQ and PmrA-PmrB Two-Component Regulatory Systems to Mg2+-Induced Gene Regulation in Pseudomonas aeruginosa , 2006, Journal of bacteriology.

[22] S. Fournel,et al. Mimicking helical antibacterial peptides with nonpeptidic folding oligomers. , 2006, Chemistry & biology.

[23] R. J. Doerksen,et al. Biomimetic facially amphiphilic antibacterial oligomers with conformationally stiff backbones. , 2006, Chemistry & biology.

[24] Michael L Klein,et al. Probing Membrane Insertion Activity of Antimicrobial Polymers via Coarse-grain Molecular Dynamics. , 2006, Journal of chemical theory and computation.

[25] M. Klein,et al. Controlling the shape and flexibility of arylamides: a combined ab initio, ab initio molecular dynamics, and classical molecular dynamics study. , 2006, The journal of physical chemistry. B.

[26] G. Tew,et al. Membrane activity of biomimetic facially amphiphilic antibiotics. , 2006, The journal of physical chemistry. B.

[27] Graham Bell,et al. Experimental evolution of resistance to an antimicrobial peptide , 2006, Proceedings of the Royal Society B: Biological Sciences.

[28] M. Klein,et al. Characterization of nonbiological antimicrobial polymers in aqueous solution and at water-lipid interfaces from all-atom molecular dynamics. , 2006, Journal of the American Chemical Society.

[29] A. Buckling,et al. Microbiology: RAMP resistance , 2005, Nature.

[30] Rachel E. Klevit,et al. Recognition of Antimicrobial Peptides by a Bacterial Sensor Kinase , 2005, Cell.

[31] S. Gellman,et al. Use of parallel synthesis to probe structure-activity relationships among 12-helical beta-peptides: evidence of a limit on antimicrobial activity. , 2005, Journal of the American Chemical Society.

[32] G. Tew,et al. Simple oligomers as antimicrobial peptide mimics , 2005, Journal of Industrial Microbiology and Biotechnology.

[33] Robert E W Hancock,et al. Rational Design of α-Helical Antimicrobial Peptides with Enhanced Activities and Specificity/Therapeutic Index* , 2005, Journal of Biological Chemistry.

[34] R. J. Doerksen,et al. Synthesis of urea oligomers and their antibacterial activity. , 2005, Chemical communications.

[35] W. DeGrado,et al. Amphiphilic polymethacrylate derivatives as antimicrobial agents. , 2005, Journal of the American Chemical Society.

[36] D. Seebach,et al. Exploring the Antibacterial and Hemolytic Activity of Shorter‐ and Longer‐Chain β‐, α,β‐, and γ‐Peptides, and of β‐Peptides from β2‐3‐Aza‐ and β3‐2‐Methylidene‐amino Acids Bearing Proteinogenic Side Chains – A Survey , 2005 .

[37] K. Brogden. Antimicrobial peptides: pore formers or metabolic inhibitors in bacteria? , 2005, Nature Reviews Microbiology.

[38] R. Hodges,et al. Structure-Activity Relationships of Diastereomeric Lysine Ring Size Analogs of the Antimicrobial Peptide Gramicidin S , 2005, Journal of Biological Chemistry.

[39] S. Gellman,et al. Bacterial species selective toxicity of two isomeric α/β-peptides: Role of membrane lipids , 2005 .

[40] G. Tew,et al. Tuning the hemolytic and antibacterial activities of amphiphilic polynorbornene derivatives. , 2004, Journal of the American Chemical Society.

[41] R. J. Doerksen,et al. Controlling the conformation of arylamides: computational studies of intramolecular hydrogen bonds between amides and ethers or thioethers. , 2004, Chemistry.

[42] Carlos F. Lopez,et al. Transmembrane peptide-induced lipid sorting and mechanism of Lalpha-to-inverted phase transition using coarse-grain molecular dynamics. , 2004, Biophysical journal.

[43] G. Tew,et al. Nonhemolytic abiogenic polymers as antimicrobial peptide mimics , 2004 .

[44] Niv Papo,et al. In Vitro Activity and Potency of an Intravenously Injected Antimicrobial Peptide and Its dl Amino Acid Analog in Mice Infected with Bacteria , 2004, Antimicrobial Agents and Chemotherapy.

[45] D. Seebach,et al. The World of β‐ and γ‐Peptides Comprised of Homologated Proteinogenic Amino Acids and Other Components , 2004 .

[46] S. Gellman,et al. Antimicrobial 14-Helical β-Peptides: Potent Bilayer Disrupting Agents† , 2004 .

[47] Robert E. W. Hancock,et al. Can innate immunity be enhanced to treat microbial infections? , 2004, Nature Reviews Microbiology.

[48] S. Gellman,et al. Unexpected Relationships between Structure and Function in α,β-Peptides: Antimicrobial Foldamers with Heterogeneous Backbones , 2004 .

[49] I. Huc. Aromatic Oligoamide Foldamers , 2004 .

[50] R. J. Doerksen,et al. Nontoxic membrane-active antimicrobial arylamide oligomers. , 2004, Angewandte Chemie.

[51] Jean-Marie Lehn,et al. Contraction/extension molecular motion by protonation/deprotonation induced structural switching of pyridine derived oligoamides. , 2003, Chemical communications.

[52] A. Barron,et al. Helical peptoid mimics of magainin-2 amide. , 2003, Journal of the American Chemical Society.

[53] Justin L. MacCallum,et al. Molecular dynamics simulations of pentapeptides at interfaces: Salt bridge and cation-π interactions , 2003 .

[54] M. Másson,et al. Soft antibacterial agents. , 2003, Current medicinal chemistry.

[55] E. Kenawy,et al. Biologically Active Polymers, 6 , 2003 .

[56] R. J. Doerksen,et al. De novo design of biomimetic antimicrobial polymers , 2002, Proceedings of the National Academy of Sciences of the United States of America.

[57] R. Haag,et al. Dendritic polymers in biomedical applications: from potential to clinical use in diagnostics and therapy. , 2002, Angewandte Chemie.

[58] Y. Shai. From innate immunity to de-novo designed antimicrobial peptides. , 2002, Current pharmaceutical design.

[59] M. Zasloff. Antimicrobial peptides of multicellular organisms , 2002, Nature.

[60] Matthew J. Mio,et al. A field guide to foldamers. , 2001, Chemical reviews.

[61] T. Nakano,et al. Synthetic helical polymers: conformation and function. , 2001, Chemical reviews.

[62] W. DeGrado,et al. beta-Peptides: from structure to function. , 2001, Chemical reviews.

[63] Y. Shai,et al. From “carpet” mechanism to de-novo designed diastereomeric cell-selective antimicrobial peptides , 2001, Peptides.

[64] Juan R. Granja,et al. Antibacterial agents based on the cyclic d,l-α-peptide architecture , 2001, Nature.

[65] W. DeGrado,et al. De Novo Design, Synthesis, and Characterization of Antimicrobial β-Peptides , 2001 .

[66] R. C. Reeder,et al. A Coarse Grain Model for Phospholipid Simulations , 2001 .

[67] I. del Castillo,et al. Construction and Characterization of Mutations at Codon 751 of the Escherichia coli gyrB Gene That Confer Resistance to the Antimicrobial Peptide Microcin B17 and Alter the Activity of DNA Gyrase , 2001, Journal of bacteriology.

[68] S. Lovas,et al. The antibacterial peptide pyrrhocoricin inhibits the ATPase actions of DnaK and prevents chaperone-assisted protein folding. , 2001, Biochemistry.

[69] R. Weinstein. Controlling antimicrobial resistance in hospitals: infection control and use of antibiotics. , 2001, Emerging infectious diseases.

[70] T. Tashiro,et al. ANTIBACTERIAL AND BACTERIUM ADSORBING MACROMOLECULES , 2001 .

[71] J. Lehn,et al. Enforced helicity: efficient access to self-organized helical molecular strands by the imine route. , 2000, Chemistry.

[72] S. Gellman,et al. Antibiotics: Non-haemolytic β-amino-acid oligomers , 2000, Nature.

[73] H. G. Boman. Innate immunity and the normal microflora , 2000, Immunological reviews.

[74] J. Homo,et al. Encoded Helical Self‐Organization and Self‐Assembly into Helical Fibers of an Oligoheterocyclic Pyridine – Pyridazine Molecular Strand , 2000 .

[75] W. DeGrado,et al. De Novo Design of Antibacterial β-Peptides , 1999 .

[76] Jeffery G. Saven,et al. Cooperative Conformational Transitions in Phenylene Ethynylene Oligomers: Chain-Length Dependence , 1999 .

[77] Y. Shai,et al. Peptide-bilayer interactions: simulations of dermaseptin B, an antimicrobial peptide. , 1999, Biophysical chemistry.

[78] Samuel H. Gellman,et al. Foldamers: A Manifesto , 1998 .

[79] C. B. Park,et al. Mechanism of action of the antimicrobial peptide buforin II: buforin II kills microorganisms by penetrating the cell membrane and inhibiting cellular functions. , 1998, Biochemical and biophysical research communications.

[80] J S Moore,et al. Solvophobically driven folding of nonbiological oligomers. , 1997, Science.

[81] Y. Hamuro,et al. Oligoanthranilamides. Non-Peptide Subunits That Show Formation of Specific Secondary Structure , 1996 .

[82] Thomas Steiner,et al. C–H···O hydrogen bonding in crystals , 1996 .

[83] A B Smith,et al. The design and synthesis of 2,5-linked pyrrolinones. A potential non-peptide peptidomimetic scaffold. , 1996, Bioorganic & medicinal chemistry.

[84] Paj Peter Hilbers,et al. Simulating the Self-Assembly of Gemini (Dimeric) Surfactants , 1994, Science.

[85] S R Cherry,et al. An unnatural biopolymer. , 1993, Science.

[86] L Wang,et al. Peptoids: a modular approach to drug discovery. , 1992, Proceedings of the National Academy of Sciences of the United States of America.

[87] P. Dervan. Design of sequence-specific DNA-binding molecules. , 1986, Science.

[88] B. Finlay,et al. Friend or foe? Antimicrobial peptides trigger pathogen virulence. , 2006, Trends in molecular medicine.

[89] Alessandro Tossi,et al. Amphipathic, α‐helical antimicrobial peptides , 2000 .

[90] Y. Shai,et al. Mode of action of linear amphipathic α-helical antimicrobial peptides , 1998 .

[91] F. Devínsky,et al. Quantitative Relationships Between Structure, Aggregation Properties and Antimicrobial Activity of Quaternary Ammonium Bolaamphiphiles , 1995 .

[92] W. DeGrado. Design of peptides and proteins. , 1988, Advances in protein chemistry.