Your search keyword '"Robert I. Lehrer"' showing total 290 results

1. A novel method for oral delivery of apolipoprotein mimetic peptides synthesized from all L-amino acids

Author

Mohamad Navab, Piotr Ruchala, Alan J. Waring, Robert I. Lehrer, Susan Hama, Greg Hough, Mayakonda N. Palgunachari, G.M. Anantharamaiah, and Alan M. Fogelman

Subjects

atherosclerosis, apolipoprotein A-I, apolipoprotein A-I mimetic peptides, lipoproteins, HDL, Biochemistry, QD415-436

Abstract

Administered subcutaneously, D-4F or L-4F are equally efficacious, but only D-4F is orally efficacious because of digestion of L-4F by gut proteases. Orally administering niclosamide (a chlorinated salicylanilide used as a molluscicide, antihelminthic, and lampricide) in temporal proximity to oral L-4F (but not niclosamide alone) in apoE null mice resulted in significant improvement (P < 0.001) in the HDL-inflammatory index (HII), which measures the ability of HDL to inhibit LDL-induced monocyte chemotactic activity in endothelial cell cultures. Oral administration of L-[113-122]apoJ with niclosamide also resulted in significant improvement (P < 0.001) in HII. Oral administration of niclosamide and L-4F together with pravastatin to female apoE null mice at 9.5 months of age for six months significantly reduced aortic sinus lesion area (P = 0.02), en face lesion area (P = 0.033), and macrophage lesion area (P = 0.02) compared with pretreatment, indicating lesion regression. In contrast, lesions were significantly larger in mice receiving only niclosamide and pravastatin or L-4F and pravastatin (P < 0.001). In vitro niclosamide and L-4F tightly associated rendering the peptide resistant to trypsin digestion. Niclosamide itself did not inhibit trypsin activity. The combination of niclosamide with apolipoprotein mimetic peptides appears to be a promising method for oral delivery of these peptides.—Navab, M. P., Ruchala, A. J. Waring, R. I. Lehrer, S. Hama, G. Hough, M. N. Palgunachari, G. M. Anantharamaiah, and A. M. Fogelman. A novel method for oral delivery of apolipoprotein mimetic peptides synthesized from all L-amino acids. J. Lipid Res. 2009. 50: 1538–1547.

Published

2009

2. Anti-inflammatory apoA-I-mimetic peptides bind oxidized lipids with much higher affinity than human apoA-I

Author

Brian J. Van Lenten, Alan C. Wagner, Chun-Ling Jung, Piotr Ruchala, Alan J. Waring, Robert I. Lehrer, Andrew D. Watson, Susan Hama, Mohamad Navab, G.M. Anantharamaiah, and Alan M. Fogelman

Subjects

atherosclerosis, apolipoprotein A-I, lipoproteins, oxidized phospholipids, Biochemistry, QD415-436

Abstract

4F is an anti-inflammatory, apolipoprotein A-I (apoA-I)-mimetic peptide that is active in vivo at nanomolar concentrations in the presence of a large molar excess of apoA-I. Physiologic concentrations (∼35 μM) of human apoA-I did not inhibit the production of LDL-induced monocyte chemotactic activity by human aortic endothelial cell cultures, but adding nanomolar concentrations of 4F in the presence of ∼35 μM apoA-I significantly reduced this inflammatory response. We analyzed lipid binding by surface plasmon resonance. The anti-inflammatory 4F peptide bound oxidized lipids with much higher affinity than did apoA-I. Initially, we examined the binding of PAPC (1-palmitoyl-2-arachidonoyl-sn-glycero-3-phosphatidylcholine) and observed that its oxidized products bound 4F with an affinity that was ∼4–6 orders of magnitude higher than that of apoA-I. This high binding affinity was confirmed in studies with defined lipids and phospholipids. 3F-2 and 3F14 are also amphipathic α-helical octadecapeptides, but 3F-2 inhibits atherosclerosis in mice and 3F14 does not. Like 4F, 3F-2 also bound oxidized phospholipids with very high affinity, whereas 3F14 resembled apoA-I. The extraordinary ability of 4F to bind pro-inflammatory oxidized lipids probably accounts for its remarkable anti-inflammatory properties.

Published

2008

3. The formulated microbicide RC-101 was safe and antivirally active following intravaginal application in pigtailed macaques.

Author

Alexander M Cole, Dorothy L Patton, Lisa C Rohan, Amy L Cole, Yvonne Cosgrove-Sweeney, Nicole A Rogers, Deena Ratner, Alexandra B Sassi, Carol Lackman-Smith, Patrick Tarwater, Bharat Ramratnam, Piotr Ruchala, Robert I Lehrer, Alan J Waring, and Phalguni Gupta

Subjects

Medicine, Science

Abstract

RC-101 is a congener of the antiretroviral peptide retrocyclin, which we and others have reported is active against clinical HIV-1 isolates from all major clades, does not hemagglutinate, and is non-toxic and non-inflammatory in cervicovaginal cell culture. Herein, film-formulated RC-101 was assessed for its antiviral activity in vitro, safety in vivo, retention in the cervix and vagina, and ability to remain active against HIV-1 and SHIV after intravaginal application in macaques.RC-101 was formulated as a quick-dissolving film (2000 µg/film), retained complete activity in vitro as compared to unformulated peptide, and was applied intravaginally in six pigtailed macaques daily for four days. At one and four days following the final application, the presence of RC-101 was assessed in peripheral blood, cervicovaginal lavage, cytobrushed cervicovaginal cells, and biopsied cervical and vaginal tissues by quantitative western blots. One day following the last film application, cervical biopsies from RC-101-exposed and placebo-controlled macaques were collected and were subjected to challenge with RT-SHIV in an ex vivo organ culture model. RC-101 peptide was detected primarily in the cytobrush and biopsied cervical and vaginal tissues, with little to no peptide detected in lavage samples, suggesting that the peptide was associated with the cervicovaginal epithelia. RC-101 remained in the tissues and cytobrush samples up to four days post-application, yet was not detected in any sera or plasma samples. RC-101, extracted from cytobrushes obtained one day post-application, remained active against HIV-1 BaL. Importantly, cervical biopsies from RC-101-treated animals reduced RT-SHIV replication in ex vivo organ culture as compared to placebo-treated animals.Formulated RC-101 was stable in vivo and was retained in the mucosa. The presence of antivirally active RC-101 after five days in vivo suggests that RC-101 would be an important molecule to develop further as a topical microbicide to prevent HIV-1 transmission.

Published

2010

4. Oxpholipin 11D: an anti-inflammatory peptide that binds cholesterol and oxidized phospholipids.

Author

Piotr Ruchala, Mohamad Navab, Chun-Ling Jung, Susan Hama-Levy, Ewa D Micewicz, Hai Luong, Jonathan E Reyles, Shantanu Sharma, Alan J Waring, Alan M Fogelman, and Robert I Lehrer

Subjects

Medicine, Science

Abstract

Many gram-positive bacteria produce pore-forming exotoxins that contain a highly conserved, 12-residue domain (ECTGLAWEWWRT) that binds cholesterol. This domain is usually flanked N-terminally by arginine and C-terminally by valine. We used this 14-residue sequence as a template to create a small library of peptides that bind cholesterol and other lipids.Several of these peptides manifested anti-inflammatory properties in a predictive in vitro monocyte chemotactic assay, and some also diminished the pro-inflammatory effects of low-density lipoprotein in apoE-deficient mice. The most potent analog, Oxpholipin-11D (OxP-11D), contained D-amino acids exclusively and was identical to the 14-residue design template except that diphenylalanine replaced cysteine-3. In surface plasmon resonance binding studies, OxP-11D bound oxidized (phospho)lipids and sterols in much the same manner as D-4F, a widely studied cardioprotective apoA-I-mimetic peptide with anti-inflammatory properties. In contrast to D-4F, which adopts a stable alpha-helical structure in solution, the OxP-11D structure was flexible and contained multiple turn-like features.Given the substantial evidence that oxidized phospholipids are pro-inflammatory in vivo, OxP-11D and other Oxpholipins may have therapeutic potential.

Published

2010

5. θ-Defensins: Cyclic Peptides with Endless Potential: FIGURE 1

Author

Michael E. Selsted, Robert I. Lehrer, and Alexander M. Cole

Subjects

chemistry.chemical_classification, Innate immune system, integumentary system, Pseudogene, fungi, Minireviews, Peptide, Cell Biology, Biology, medicine.disease_cause, Peptides, Cyclic, Biochemistry, Virology, Cyclic peptide, Defensins, chemistry, RNA splicing, Influenza A virus, medicine, Humans, Peptide Biosynthesis, Molecular Biology, Biogenesis

Abstract

θ-Defensins, the only cyclic peptides of animal origin, have been isolated from the leukocytes of rhesus macaques and baboons. Their biogenesis is unusual because each peptide is an 18-residue chimera formed by the head-to-tail splicing of nonapeptides derived from two separate precursors. θ-Defensins have multiple arginines and a ladder-like tridisulfide array spanning their two antiparallel β-strands. Human θ-defensin genes contain a premature stop codon that prevents effective translation of the needed precursors; consequently, these peptides are not present in human leukocytes. Synthetic θ-defensins with sequences that correspond to those encoded within the human pseudogenes are called retrocyclins. Retrocyclin-1 inhibits the cellular entry of HIV-1, HSV, and influenza A virus. The rhesus θ-defensin RTD-1 protects mice from an experimental severe acute respiratory syndrome coronavirus infection, and retrocyclin-1 protects mice from infection by Bacillus anthracis spores. The small size, unique structure, and multiple host defense activities of θ-defensins make them intriguing potential therapeutic agents.

Published

2012

6. Hapivirins and Diprovirins: Novel θ-Defensin Analogs with Potent Activity against Influenza A Virus

Author

Kevan L. Hartshorn, Robert I. Lehrer, Erika C. Crouch, Ewa D. Micewicz, Hai Luong, Tesfaldet Tecle, Mona Doss, Piotr Ruchala, Alex Hartshorn, Donald L. Gantz, and Anamika Verma

Subjects

Neutrophils, Immunology, Molecular Sequence Data, Peptide, Chemistry Techniques, Synthetic, Biology, medicine.disease_cause, Antiviral Agents, Article, Monocytes, Cell Line, Defensins, Structure-Activity Relationship, Dogs, Microscopy, Electron, Transmission, In vivo, Influenza A virus, medicine, Immunology and Allergy, Structure–activity relationship, Animals, Humans, Amino Acid Sequence, Defensin, Peptide sequence, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Tumor Necrosis Factor-alpha, Virology, Cyclic peptide, chemistry, PEGylation, Peptides

Abstract

θ-Defensins are cyclic octadecapeptides found in nonhuman primates whose broad antiviral spectrum includes HIV-1, HSV-1, severe acute respiratory syndrome coronavirus, and influenza A virus (IAV). We previously reported that synthetic θ-defensins called retrocyclins can neutralize and aggregate various strains of IAV and increase IAV uptake by neutrophils. This study describes two families of peptides, hapivirins and diprovirins, whose design was inspired by retrocyclins. The goal was to develop smaller partially cyclic peptides that retain the antiviral activity of retrocyclins, while being easier to synthesize. The novel peptides also allowed for systemic substitution of key residues to evaluate the role of charge or hydrophobicity on antiviral activity. Seventy-two hapivirin or diprovirin peptides are described in this work, including several whose anti-IAV activity equals or exceeds that of normal α- or θ-defensins. Some of these also had strong antibacterial and antifungal activity. These new peptides were active against H3N2 and H1N1 strains of IAV. Structural features imparting strong antiviral activity were identified through iterative cycles of synthesis and testing. Our findings show the importance of hydrophobic residues for antiviral activity and show that pegylation, which often increases a peptide’s serum t1/2 in vivo, can increase the antiviral activity of DpVs. The new peptides acted at an early phase of viral infection, and, when combined with pulmonary surfactant protein D, their antiviral effects were additive. The peptides strongly increased neutrophil and macrophage uptake of IAV, while inhibiting monocyte cytokine generation. Development of modified θ-defensin analogs provides an approach for creating novel antiviral agents for IAV infections.

Published

2012

7. α-Defensins in human innate immunity

Author

Robert I. Lehrer and Wuyuan Lu

Subjects

Innate immune system, integumentary system, fungi, Immunology, Binding properties, Antimicrobial peptides, respiratory system, Biology, bacterial infections and mycoses, digestive system, Protein structure, medicine.anatomical_structure, Evolutionary biology, Paneth cell, medicine, Immunology and Allergy, α defensin, Mostly bad, Function (biology)

Abstract

Defensins are small, multifunctional cationic peptides. They typically contain six conserved cysteines whose three intramolecular disulfides stabilize a largely β-sheet structure. This review of human α-defensins begins by describing their evolution, including their likely relationship to the Big Defensins of invertebrates, and their kinship to the β-defensin peptides of many if not all vertebrates, and the θ-defensins found in certain non-human primates. We provide a short history of the search for leukocyte-derived microbicidal molecules, emphasizing the roles played by luck (good), preconceived notions (mostly bad), and proper timing (essential). The antimicrobial, antiviral, antitoxic, and binding properties of human α-defensins are summarized. The structural features of α-defensins are described extensively and their functional contributions are assessed. The properties of HD6, an enigmatic Paneth cell α-defensin, are contrasted with those of the four myeloid α-defensins (HNP1-4) and of HD5, the other α-defensin of human Paneth cells. The review ends with a decalogue that may assist researchers or students interested in α-defensins and related aspects of neutrophil function.

Published

2011

8. Simplified θ-Defensins: Search for New Antivirals

Author

Alan J. Waring, Robert I. Lehrer, Piotr Ruchala, Ewa D. Micewicz, Hai Luong, Betsy C. Herold, Colleen Carpenter, Alexander M. Cole, Amy L. Cole, Chun Ling Jung, and Sylvia Cho

Subjects

chemistry.chemical_classification, Innate immune system, Pharmacology toxicology, Bioengineering, Peptide, Computational biology, Biology, Biochemistry, Combinatorial chemistry, Nonhuman primate, Analytical Chemistry, Topical microbicides, chemistry, Active compound, Drug Discovery, Molecular Medicine, Clearance, Enzymatic degradation

Abstract

Peptides of the innate immune system provide intriguing templates for designing novel antiviral molecules. θ-defensins are nonhuman primate peptides with broad-spectrum antiviral activities. The activity of these compounds is mediated through interference with viral fusion, and this activity is based upon key structural features. However, two major limitations to their clinical use hampered their development as potential antivirals, namely difficult multi-step synthesis for their production with low final yield of desired product (~5%), and unfavorable pharmacokinetics (rapid enzymatic degradation and/or renal clearance). Recently we designed and screened two sub-libraries of new peptide-based entry inhibitors mimicking the structure of humanized θ-defensins, designated as Hapivirins (HpVs) and Diprovirins (DpVs). Although the new peptides are smaller (13-residues) and structurally more simple than retrocyclins, several retained their ability to protect cells from infection by HIV-1 and HSV-2. The most active compound, DpV16, was chosen for a second round of modifications based on (1) its potent antiviral activity (2) its ease of synthesis, and (3) the low cost of production. Subsequently, we created a library of a second generation DpV-analogues with enhanced properties. Collectively, our findings to date suggest that simplified θ-defensins are suitable candidates for further modifications to obtain analogues with clinically favorable pharmacokinetics that may be produced in large quantities using a standard chemical approach. Considering their small size, they could be used either topically (topical microbicides) and/or for systemic applications (entry inhibitors).

Published

2011

9. Defensins enable macrophages to inhibit the intracellular proliferation of Listeria monocytogenes

Author

Stephanie Seveau, Eusondia Arnett, Wuyuan Lu, Robert I. Lehrer, and Pratikhya Pratikhya

Subjects

Innate immune system, Intracellular parasite, Immunology, Antimicrobial peptides, Perforation (oil well), Listeriolysin O, Biology, medicine.disease_cause, Microbiology, Listeria monocytogenes, Virology, medicine, Macrophage, Phagosome

Abstract

Summary Listeria monocytogenes is a facultative intracellular pathogen that infects a large diversity of host cells, including macrophages. To avoid the phagosome microbicidal environment, L. monocytogenes secretes a pore-forming toxin (listeriolysin O, LLO) that releases the bacterium into the cytoplasm. We hypothesized that the α-defensins (HNPs) and/or humanized θ-defensin (RC-1) peptides produced by human and non-human primate neutrophils, respectively, cooperate with macrophages to control L. monocytogenes infection. Our results establish that HNP-1 and RC-1 enable macrophages to control L. monocytogenes intracellular growth by inhibiting phagosomal escape, as a consequence, bacteria remain trapped in a LAMP-1-positive phagosome. Importantly, HNP-1 interaction with macrophages and RC-1 interaction with bacteria are required to prevent macrophage infection. In accordance with these results, RC-1 is a more potent anti-listerial peptide than HNP-1 and HNP-1 is acquired by macrophages and trafficked to the phagocytosed bacteria. Finally, HNP-1 and RC-1 antimicrobial activity is complemented by their ability to prevent LLO function through two mechanisms, blocking LLO-dependent perforation of macrophage membranes and the release of LLO from the bacteria. In conclusion, at the site of infection the cooperation between antimicrobial peptides, such as HNP-1, and macrophages likely plays a critical role in the innate immune defence against L. monocytogenes.

Published

2011

10. Trp-26 Imparts Functional Versatility to Human α-Defensin HNP1

Author

Marzena Pazgier, Weiyue Lu, Wuyuan Lu, Robert I. Lehrer, Erik de Leeuw, Gang Wei, Weirong Yuan, Jing Li, Mohsen Rajabi, Grace Jung, and Guozhang Zou

Subjects

Staphylococcus aureus, alpha-Defensins, Bacterial Toxins, Antimicrobial peptides, Mutation, Missense, Peptide, HIV Envelope Protein gp120, Biology, Biochemistry, Alpha defensin, Structure-Activity Relationship, Protein structure, Humans, Protein Structure, Quaternary, Molecular Biology, Defensin, chemistry.chemical_classification, Alanine, Antigens, Bacterial, Tryptophan, Wild type, Cell Biology, Immunity, Innate, Amino acid, chemistry, Protein Structure and Folding, Protein Multimerization, Hydrophobic and Hydrophilic Interactions

Abstract

We performed a comprehensive alanine scan of human alpha-defensin HNP1 and tested the ability of the resulting analogs to kill Staphylococcus aureus, inhibit anthrax lethal factor, and bind human immunodeficiency virus-1 gp120. By far, the most deleterious mutation for all of these functions was W26A. The activities lost by W26A-HNP1 were restored progressively by replacing W26 with non-coded, straight-chain aliphatic amino acids of increasing chain length. The hydrophobicity of residue 26 also correlated with the ability of the analogs to bind immobilized wild type HNP1 and to undergo further self-association. Thus, the hydrophobicity of residue 26 is not only a key determinant of the direct interactions of HNP1 with target molecules, but it also governs the ability of this peptide to form dimers and more complex quaternary structures at micromolar concentrations. Although all defensin peptides are cationic, their amphipathicity is at least as important as their positive charge in enabling them to participate in innate host defense.

Published

2010

11. De novosequencing of two new cyclicθ-defensins from baboon (Papio hamadryas) leukocytes by matrix-assisted laser desorption/ionization mass spectrometry

Author

Christin Stegemann, Robert I. Lehrer, Ralf Hoffmann, V. N. Kokryakov, Elena V. Tsvetkova, and G. M. Aleshina

Subjects

Gel electrophoresis, Chromatography, biology, Chemistry, Organic Chemistry, medicine.disease_cause, Mass spectrometry, biology.organism_classification, Theta defensin, Analytical Chemistry, Matrix-assisted laser desorption/ionization, chemistry.chemical_compound, medicine, Derivatization, Escherichia coli, Hamadryas baboon, Spectroscopy, Papio hamadryas

Abstract

Two cyclic theta-defensin peptides were isolated from leukocytes of the hamadryas baboon, Papio hamadryas, and purified to homogeneity by gel electrophoresis and reversed-phase high-performance liquid chromatography. Both peptides had high in vitro activity against Escherichia coli, Listeria monocytogenes, methicillin-resistant Staphylococcus aureus (MRSA) and Candida albicans. Here, we report their de novo sequencing by matrix-assisted laser desorption/ionization tandem time-of-flight mass spectrometry (MALDI-TOF/TOF-MS). This was accomplished by combining conventional enzymatic digestion with N-terminal derivatization by 2-sulfobenzoic acid cyclic anhydride (SACA) or 4-sulfophenylisothiocyanate (SPITC) to facilitate the interpretation of fragment ion spectra. In addition to the two cyclic theta-defensins (PhTDs) we also sequenced a novel Papio hamadryas alpha-defensin, PhD-4, which showed high sequence homology to rhesus alpha-defensin RMAD-1 and human alpha-defensin HNP-1.

Published

2010

12. Human α-Defensins Inhibit Hemolysis Mediated by Cholesterol-Dependent Cytolysins

Author

Robert I. Lehrer, Piotr Ruchala, Alan J. Waring, Ewa D. Micewicz, Kenneth A. Bradley, Grace Jung, Eugene J. Gillespie, Wuyuan Lu, Adam J. Ratner, Richard F. Rest, and Wei Wang

Subjects

Serum, alpha-Defensins, Bacterial Toxins, Molecular Sequence Data, Immunology, Enzyme-Linked Immunosorbent Assay, Clostridium difficile toxin B, Biology, Hemolysis, Microbiology, Hemolysin Proteins, Bacterial Proteins, medicine, Animals, Humans, Pseudomonas exotoxin, Amino Acid Sequence, Defensin, Heat-Shock Proteins, Diphtheria toxin, Membrane Glycoproteins, Pneumolysin, Listeriolysin O, Hydrogen-Ion Concentration, medicine.disease, Molecular Pathogenesis, Cholesterol, Infectious Diseases, Biochemistry, Streptolysins, Electrophoresis, Polyacrylamide Gel, Parasitology, Rabbits, Cytolysin

Abstract

Many pathogenic gram-positive bacteria release exotoxins that belong to the family of cholesterol-dependent cytolysins. Here, we report that human α-defensins HNP-1 to HNP-3 acted in a concentration-dependent manner to protect human red blood cells from the lytic effects of three of these exotoxins: anthrolysin O (ALO), listeriolysin O, and pneumolysin. HD-5 was very effective against listeriolysin O but less effective against the other toxins. Human α-defensins HNP-4 and HD-6 and human β-defensin-1, -2, and -3 lacked protective ability. HNP-1 required intact disulfide bonds to prevent toxin-mediated hemolysis. A fully linearized analog, in which all six cysteines were replaced by aminobutyric acid (Abu) residues, showed greatly reduced binding and protection. A partially unfolded HNP-1 analog, in which only cysteines 9 and 29 were replaced by Abu residues, showed intact ALO binding but was 10-fold less potent in preventing hemolysis. Surface plasmon resonance assays revealed that HNP-1 to HNP-3 bound all three toxins at multiple sites and also that solution-phase HNP molecules could bind immobilized HNP molecules. Defensin concentrations that inhibited hemolysis by ALO and listeriolysin did not prevent these toxins from binding either to red blood cells or to cholesterol. Others have shown that HNP-1 to HNP-3 inhibit lethal toxin ofBacillus anthracis, toxin B ofClostridium difficile, diphtheria toxin, and exotoxin A ofPseudomonas aeruginosa; however, this is the first time these defensins have been shown to inhibit pore-forming toxins. An “ABCDE mechanism” that can account for the ability of HNP-1 to HNP-3 to inhibit so many different exotoxins is proposed.

Published

2009

13. Interactions of α-, β-, and θ-Defensins with Influenza A Virus and Surfactant Protein D

Author

Alan J. Waring, Piotr Ruchala, Kevan L. Hartshorn, Mona Doss, Robert I. Lehrer, Erika C. Crouch, Grace Jung, Tesfaldet Tecle, Mitchell R. White, and Donald L. Gantz

Subjects

Retrocyclin, Pulmonary surfactant, Human neutrophil, Immunology, Influenza A virus, medicine, Immunology and Allergy, Surfactant protein D, Surface plasmon resonance, Biology, medicine.disease_cause, Virology, Microbiology

Abstract

We have reported that the α-defensins human neutrophil peptides (HNP)-1 and HNP-2 neutralize and aggregate influenza A virus (IAV) and promote uptake of IAV by neutrophils. These α-defensins were also shown to bind to surfactant protein (SP)-D and reduce its antiviral activity. In this study, we examined retrocyclin (RC)1 and RC2, humanized versions of the antiviral θ-defensins found in the leukocytes of certain nonhuman primates. RC1 was just as effective as HNP-1–3 in neutralizing IAV, and RC2 and RC101 (an analog of RC1) were more effective. In contrast, human β-defensins (HBDs) showed less neutralizing activity. Human defensins 5 and 6 (mainly produced by intestinal Paneth cells) had viral neutralizing activity similar to HNP-1–3. Like HNP-1–3, RCs induced viral aggregation and promoted the uptake of IAV by neutrophils. We used surface plasmon resonance to evaluate binding of defensins to SP-D. HBDs, HD6, and HNP-4 bound minimally to SP-D. HNP-1–3 and RCs bound SP-D with high affinity; however, unlike HNP-1 and HNP-2, RCs did not inhibit SP-D antiviral activity. HBDs also did not inhibit antiviral activity of SP-D. Given their strong neutralizing activity and compatibility with SP-D, RCs may provide attractive prototypes for designing therapeutics that can prevent or treat respiratory infections caused by IAV.

Published

2009

14. Defensins

Author

Tomas Ganz, Michael E. Selsted, and Robert I. Lehrer

Subjects

Models, Molecular, Blood Bactericidal Activity, alpha-Defensins, Neutrophils, Protein Conformation, Molecular Sequence Data, Blood Proteins, Hematology, General Medicine, Defensins, Sequence Homology, Nucleic Acid, Animals, Humans, Amino Acid Sequence

Abstract

Defensins are a family of small, variably cationic proteins which are highly abundant in the granules of mammalian phagocytes. Three defensins, HNP-1, 2, and 3, comprise 30-50% of total protein in azurophil granules of human neutrophils. Some defensins are broadly antimicrobial, antiviral and cytotoxic, while others are chemotactic, opsonic, or may modulate hormonal responses. The defensin molecule typically consists of 29-34 amino acids with a conserved pattern of disulfide linkage among its 6 cysteines. The three-dimensional fold of defensins forms a highly amphiphilic molecule. Microbicidal and cytotoxic properties of defensins are most likely a consequence of their ability to insert into biological membranes and to generate pores. Defensins are synthesized by phagocytes or their precursors as a 94-95 amino acid charge-neutralized preprodefensin, an arrangement which may avoid cytotoxic injury to the phagocyte. Although defensins were recognized only recently, the existence of homologs in certain invertebrates suggests that they are ancestral components of the host defense system.

Published

2009

15. Anti-inflammatory apoA-I-mimetic peptides bind oxidized lipids with much higher affinity than human apoA-I

Author

Andrew D. Watson, Brian J. Van Lenten, Alan J. Waring, Alan C. Wagner, Mohamad Navab, Robert I. Lehrer, Piotr Ruchala, Susan Hama, Gattadahalli M. Anantharamaiah, Alan M. Fogelman, and Chun-Ling Jung

Subjects

Apolipoprotein B, Molecular Sequence Data, Peptide, QD415-436, Plasma protein binding, Biochemistry, Lipid peroxidation, chemistry.chemical_compound, Endocrinology, In vivo, medicine, Humans, Amino Acid Sequence, Surface plasmon resonance, Peptide sequence, Cells, Cultured, Phospholipids, chemistry.chemical_classification, Apolipoprotein A-I, biology, Monocyte, Anti-Inflammatory Agents, Non-Steroidal, Molecular Mimicry, Cell Biology, lipoproteins, medicine.anatomical_structure, chemistry, biology.protein, oxidized phospholipids, lipids (amino acids, peptides, and proteins), Lipid Peroxidation, atherosclerosis, Inflammation Mediators, Peptides, Research Article, Protein Binding

Abstract

4F is an anti-inflammatory, apolipoprotein A-I (apoA-I)-mimetic peptide that is active in vivo at nanomolar concentrations in the presence of a large molar excess of apoA-I. Physiologic concentrations ( approximately 35 microM) of human apoA-I did not inhibit the production of LDL-induced monocyte chemotactic activity by human aortic endothelial cell cultures, but adding nanomolar concentrations of 4F in the presence of approximately 35 microM apoA-I significantly reduced this inflammatory response. We analyzed lipid binding by surface plasmon resonance. The anti-inflammatory 4F peptide bound oxidized lipids with much higher affinity than did apoA-I. Initially, we examined the binding of PAPC (1-palmitoyl-2-arachidonoyl-sn-glycero-3-phosphatidylcholine) and observed that its oxidized products bound 4F with an affinity that was approximately 4-6 orders of magnitude higher than that of apoA-I. This high binding affinity was confirmed in studies with defined lipids and phospholipids. 3F-2 and 3F(14) are also amphipathic alpha-helical octadecapeptides, but 3F-2 inhibits atherosclerosis in mice and 3F(14) does not. Like 4F, 3F-2 also bound oxidized phospholipids with very high affinity, whereas 3F(14) resembled apoA-I. The extraordinary ability of 4F to bind pro-inflammatory oxidized lipids probably accounts for its remarkable anti-inflammatory properties.

Published

2008

16. Induction of group A Streptococcus virulence by a human antimicrobial peptide

Author

Ioannis Gryllos, Hachung Chung, Robert Iii. Bolcome, Hien J. Tran-Winkler, Michael R. Wessels, Wuyuan Lu, Ming-Fang Cheng, and Robert I. Lehrer

Subjects

Bacterial capsule, Streptococcus pyogenes, medicine.medical_treatment, Molecular Sequence Data, Virulence, Biology, medicine.disease_cause, Microbiology, Cathelicidin, Bacterial Proteins, Phagocytosis, Cathelicidins, Streptococcal Infections, Operon, Leukocytes, medicine, Humans, Bacterial Capsules, Cells, Cultured, Regulation of gene expression, Multidisciplinary, Protease, Streptococcus, Gene Expression Regulation, Bacterial, Biological Sciences, Antimicrobial, Disease Susceptibility, Protein Kinases, Antimicrobial Cationic Peptides

Abstract

Group A streptococci ( Streptococcus pyogenes or GAS) freshly isolated from individuals with streptococcal sore throat or invasive (“flesh-eating”) infection often grow as mucoid colonies on primary culture but lose this colony appearance after laboratory passage. The mucoid phenotype is due to abundant production of the hyaluronic acid capsular polysaccharide, a key virulence determinant associated with severe GAS infections. These observations suggest that signal(s) from the human host trigger increased production of capsule and perhaps other virulence factors during infection. Here we show that subinhibitory concentrations of the human antimicrobial cathelicidin peptide LL-37 stimulate expression of the GAS capsule synthesis operon ( hasABC ). Up-regulation is mediated by the CsrRS 2-component regulatory system: it requires a functional CsrS sensor protein and can be antagonized by increased extracellular Mg 2+ , the other identified environmental signal for CsrS. Up-regulation was also evident for other CsrRS-regulated virulence genes, including the IL-8 protease PrtS/ScpC and the integrin-like/IgG protease Mac/IdeS, findings that suggest a coordinated GAS virulence response elicited by this antimicrobial immune effector peptide. LL-37 signaling through CsrRS led to a marked increase in GAS resistance to opsonophagocytic killing by human leukocytes, an in vitro measure of enhanced GAS virulence, consistent with increased expression of the antiphagocytic capsular polysaccharide and Mac/IdeS. We propose that the human cathelicidin LL-37 has the paradoxical effect of stimulating CsrRS-regulated virulence gene expression, thereby enhancing GAS pathogenicity during infection. The ability of GAS to sense and respond to LL-37 may explain, at least in part, the unique susceptibility of the human species to streptococcal infection.

Published

2008

17. Correlation between simulated physicochemical properties and hemolycity of protegrin-like antimicrobial peptides: Predicting experimental toxicity

Author

Alan J. Waring, Himanshu Khandelia, Benjamin S. Schuster, Robert I. Lehrer, Yiannis N. Kaznessis, and Allison A. Langham

Subjects

Models, Molecular, Quantitative structure–activity relationship, Erythrocytes, Chemical Phenomena, Physiology, Molecular Sequence Data, Antimicrobial peptides, Quantitative Structure-Activity Relationship, Peptide, Cervix Uteri, Hemolysis, Biochemistry, Article, Inhibitory Concentration 50, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Endocrinology, Predictive Value of Tests, Humans, Computer Simulation, Amino Acid Sequence, Cytotoxicity, Antibacterial agent, chemistry.chemical_classification, Dose-Response Relationship, Drug, Chemistry, Physical, Temperature, Epithelial Cells, Antimicrobial, chemistry, Toxicity, Protegrin, Female, Antimicrobial Cationic Peptides

Abstract

The therapeutic, antibiotic potential of antimicrobial peptides can be prohibitively diminished because of the cytotoxicity and hemolytic profiles they exhibit. Quantifying and predicting antimicrobial peptide toxicity against host cells is thus an important goal of AMP related research. In this work, we present quantitative structure activity relationships for toxicity of protegrin-like antimicrobial peptides against human cells (epithelial and red blood cells) based on physicochemical properties, such as interaction energies and radius of gyration, calculated from molecular dynamics simulations of the peptides in aqueous solvent. The hypothesis is that physicochemical properties of peptides, as manifest by their structure and interactions in a solvent and as captured by atomistic simulations, are responsible for their toxicity against human cells. Protegrins are beta-hairpin peptides with high activity against a wide variety of microbial species, but in their native state are toxic to human cells. Sixty peptides with experimentally determined toxicities were used to develop the models. We test the resulting relationships to determine their ability to predict the toxicity of several protegrin-like peptides. The developed QSARs provide insight into the mechanism of cytotoxic action of antimicrobial peptides. In a subsequent blind test, the QSAR correctly ranked four of five protegrin analogues newly synthesized and tested for toxicity.

Published

2008

18. Effects of Guanidinium–Phosphate Hydrogen Bonding on the Membrane-Bound Structure and Activity of an Arginine-Rich Membrane Peptide from Solid-State NMR Spectroscopy

Author

Ming Tang, Alan J. Waring, Robert I. Lehrer, and Mei Hong

Subjects

chemistry.chemical_classification, Magnetic Resonance Spectroscopy, Molecular Structure, Hydrogen bond, Lipid Bilayers, Analytical chemistry, Hydrogen Bonding, Peptide, General Chemistry, Nuclear magnetic resonance spectroscopy, Arginine, Catalysis, Phosphates, chemistry.chemical_compound, Crystallography, Membrane, chemistry, Membrane protein, Peptides, Lipid bilayer, POPC, Peptide sequence, Guanidine

Abstract

Arginineand lysine-rich cationic peptides and protein domains are found in a wide range of membrane-active proteins such as antimicrobial peptides, cell-penetrating peptides, and voltage-sensing domains of potassium channels. Yet the three-dimensional structures these proteins adopt to enable translocation of the charged residues into the low dielectric milieu of the hydrophobic part of the lipid membrane, despite the free-energy barrier, remain poorly understood. An increasing number of molecular dynamics simulations and experimental studies have suggested the importance of Arg interactions with lipids in membrane protein function. Magic-angle spinning (MAS) solid-state NMR (SSNMR) spectroscopy can provide direct experimental insights into these intriguing questions of energetics and structure. We have recently reported SSNMR distance-constrained guanidinium–phosphate (Gdn–PO4 ) complex formation between the Arg residues of a b-hairpin antimicrobial peptide, PG-1, and the lipid phosphate groups. The existence of these complexes suggests that the Arg residues are neutralized by the phosphate groups to enable transmembrane insertion of the peptide. We hypothesized that the peptide-associated phosphate headgroups transferred to the hydrophobic part of the membrane are responsible for the toroidal pore defects. Such Gdn–PO4 complexes should be stabilized by N H···O=P hydrogen bonds and electrostatic attractions. Herein we test the importance of Gdn–PO4 hydrogen bonding to the structure and activity of PG-1 by dimethylating each guanidinium group, thus reducing the number of N H hydrogen-bond donors (Figure 1). We show that this dimethylation of the Arg groups significantly alters the membrane insertion and activity of PG-1. Figure 2 shows oriented P NMR spectra of palmitoyloleoylphosphatidylcholine/palmitoyloleoylphosphatidylglycerol (POPC/POPG) membranes containing 0–4% of the mutant (Arg-PG-1). Without the peptide, the membranes uniaxially aligned on glass plates and exhibited the expected single peak at approximately 30 ppm without other intensities in the anisotropic chemical shift range. Residual powder intensities indicative of misalignment and a small 0 ppm isotropic peak indicative of toroidal pores are observed with increasing concentrations of Arg-PG-1. Line-shape simulations indicate that the isotropic component in the 4% Arg-PG-1 sample is 20% of the total intensity, much less than the 39% caused by PG-1; thus, dimethylation of the Arg residues reduces membrane disruption. Corroborating the P NMR data are the minimal effective concentrations (MECs) of Arg-PG-1 and PG-1 against Figure 1. a) Structure of dimethylated Arg residue and its bidentate complex with phosphate ions. b) Arg-PG-1 amino acid sequence.

Published

2008

19. Retrocyclin RC-101 overcomes cationic mutations on the heptad repeat 2 region of HIV-1 gp41

Author

Christopher A. Fuhrman, Alan J. Waring, Stephen M. Dutz, Andrew Warren, Shantanu Sharma, Alexander M. Cole, Robert I. Lehrer, and Amy L. Cole

Subjects

Genetics, In silico, Mutant, Cell Biology, Plasma protein binding, Biology, Gp41, Biochemistry, Virology, Heptad repeat, Protein structure, Molecular Biology, Peptide sequence, Defensin

Abstract

Retrocyclin RC-101, a theta-defensin with lectin-like properties, potently inhibits infection by many HIV-1 subtypes by binding to the heptad repeat 2 (HR2) region of glycoprotein 41 (gp41) and preventing six-helix bundle formation. In the present study, we used in silico computational exploration to identify residues of HR2 that interacted with RC-101, and then analyzed the HIV-1 sequence database at Los Alamos National Laboratory (New Mexico, USA) for residue variations in the heptad repeat 1 (HR1) and HR2 segments that could plausibly impart in vivo resistance. Docking RC-101 to gp41 peptides in silico confirmed its strong preference for HR2 over HR1, and implicated residues crucial for its ability to bind HR2. We mutagenized these residues in pseudotyped HIV-1 JR.FL reporter viruses, and subjected them to single-round replication assays in the presence of 1.25-10 microg x mL(-1) RC-101. Apart from one mutant that was partially resistant to RC-101, the other pseudotyped viruses with single-site cationic mutations in HR2 manifested absent or impaired infectivity or retained wild-type susceptibility to RC-101. Overall, these data suggest that most mutations capable of rendering HIV-1 resistant to RC-101 will also exert deleterious effects on the ability of HIV-1 to initiate infections - an interesting and novel property for a potential topical microbicide.

Published

2007

20. Paradoxical Effects of Two Theta-Defensins on HIV Type 1 Infection

Author

Alan J. Waring, Otto O. Yang, Sina Tabibian, Robert Chiu, Wei Wang, Irvin S. Y. Chen, Junying Zheng, Qiuwei Wang, Jun Song, Yiming Xie, Shen Pang, and Robert I. Lehrer

Subjects

CD4-Positive T-Lymphocytes, Immunology, HIV Infections, Peptide, Gene delivery, Kidney, Virus, Theta defensin, Defensins, Virology, Humans, Defensin, Peptide sequence, Cell Line, Transformed, chemistry.chemical_classification, biology, Epithelial Cells, biology.organism_classification, Infectious Diseases, chemistry, Cell culture, Lentivirus, HIV-1, Neuroglia, HeLa Cells

Abstract

Retrocyclin-1 (RC-100) is a cyclic octadecapeptide whose primary structure is based on the sequence of an expressed human theta-defensin pseudogene. RC-111 has the same amino acid sequence as RC-100 and is also cyclic, but its residues are placed in reverse order along the peptide's backbone. We quantified the effects of RC-100 and RC-111 on HIV-1 infection using HIV clones that expressed green fluorescent protein. Whereas 0.2 microg/ml of RC-100 inhibited infection of CD4-positive cells by approximately 80%, its retro-analogue significantly enhanced infection of the cells. RC-100 and RC-111 also demonstrate their effects in HIV infection of CD4-negative cells. Whereas 40 ng/ml of RC-111 significantly enhanced infection of CD4-negative cells by HIV-1, RC-100 demonstrated significant inhibition of HIV infection with a concentration of approximately 10 microg/ml. RC-111ox, an acyclic variant of RC-111 with a beta-hairpin structure, also enhanced HIV-1 infection, but did so less effectively than cyclic RC-111. The divergent actions of RC-100 and RC-111 show that topology and polarity of theta-defensin peptides can determine their effect on HIV infection. The ability of RC-111 to enhance HIV-1 infection might prove useful in developing peptides that can enhance gene delivery by HIV-based lentiviral vectors.

Published

2007

21. Human α- and β-Defensins Block Multiple Steps in Herpes Simplex Virus Infection

Author

Robert I. Lehrer, Betsy C. Herold, Wei Wang, Benjamin T. Galen, Wuyuan Lu, Marla J. Keller, Yan Ouyang, and Ehsan Hazrati

Subjects

Herpes simplex virus infection, alpha-Defensins, beta-Defensins, Immunology, Peptide, Plasma protein binding, HSL and HSV, Biology, Mice, chemistry.chemical_compound, Viral Envelope Proteins, Animals, Humans, Immunology and Allergy, Receptor, Cells, Cultured, chemistry.chemical_classification, Hsv infection, Heparin, Epithelial Cells, Herpes Simplex, Heparan sulfate, Surface Plasmon Resonance, Virology, Molecular biology, Microbicides for sexually transmitted diseases, Disease Models, Animal, chemistry, Protein Binding

Abstract

This study examined the ability of nine human defensins (HD) to protect against herpes simplex virus infection. Noncytotoxic concentrations of all six α-defensins (HNP1–4, HD5, and HD6) and human β-defensin (hBD) 3 inhibited HSV infection. Two other β-defensins, hBD1 and 2, lacked this protective activity. Synchronized assays revealed that HNP-4, HD6, and hBD3 acted primarily by preventing binding and entry, whereas HNP1–3 and HD5 also inhibited postentry events. Even when added several hours after entry, substantial reduction in viral gene expression ensued. Human cervical epithelial cells incubated with HNP-1 or HD5 accumulated the peptides intracellularly. Surface plasmon resonance studies revealed that HNPs 1, 2, 3, and HD5 bound HSV glycoprotein B (gB) with high affinity, but showed minimal binding to heparan sulfate, the receptor for attachment. In contrast, HNP-4 and HD6 bound heparan sulfate, but not gB. HBD3 bound both gB and heparan sulfate, but hBD1 and hBD2 bound neither. Admixture of HD5 with hydroxyethylcellulose significantly protected mice from a viral challenge lethal to controls receiving an inactive peptide or hydroxyethylcellulose alone. These findings demonstrate that HDs act at multiple steps in the HSV life cycle and support the development of defensins or defensin-like peptides as microbicides.

Published

2006

22. Retrocyclins Kill Bacilli and Germinating Spores of Bacillus anthracis and Inactivate Anthrax Lethal Toxin

Author

Grace Jung, Robert I. Lehrer, Chandrika Mulakala, Yiannis N. Kaznessis, Hai Luong, Kenneth A. Bradley, Alan J. Waring, Wuyuan Lu, Duy Stephen L. Pham, Wei Wang, and Sabrina C. Ward

Subjects

Models, Molecular, Spores, Bacilli, Arginine, Bacterial Toxins, Molecular Sequence Data, Colony Count, Microbial, Peptide, Microbial Sensitivity Tests, Biochemistry, Protein Structure, Secondary, Article, Microbiology, Anthrax, Defensins, Mice, Antigen, In vivo, Animals, Amino Acid Sequence, Molecular Biology, chemistry.chemical_classification, Antigens, Bacterial, biology, fungi, Cell Biology, Surface Plasmon Resonance, biology.organism_classification, In vitro, Bacillus anthracis, Kinetics, Enzyme, chemistry, Macrophages, Peritoneal

Abstract

Theta-defensins are cyclic octadecapeptides encoded by the modified alpha-defensin genes of certain nonhuman primates. The recent demonstration that human alpha-defensins could prevent deleterious effects of anthrax lethal toxin in vitro and in vivo led us to examine the effects of theta-defensins on Bacillus anthracis (Sterne). We tested rhesus theta-defensins 1-3, retrocyclins 1-3, and several analogues of RC-1. Low concentrations of theta-defensins not only killed vegetative cells of B. anthracis (Sterne) and rendered their germinating spores nonviable, they also inactivated the enzymatic activity of anthrax lethal factor and protected murine RAW-264.7 cells from lethal toxin, a mixture of lethal factor and protective antigen. Structure-function studies indicated that the cyclic backbone, intramolecular tri-disulfide ladder, and arginine residues of theta-defensins contributed substantially to these protective effects. Surface plasmon resonance studies showed that retrocyclins bound the lethal factor rapidly and with high affinity. Retrocyclin-mediated inhibition of the enzymatic activity of lethal factor increased substantially if the enzyme and peptide were preincubated before substrate was added. The temporal discrepancy between the rapidity of binding and the slowly progressive extent of lethal factor inhibition suggest that post-binding events, perhaps in situ oligomerization, contribute to the antitoxic properties of retrocyclins. Overall, these findings suggest that theta-defensins provide molecular templates that could be used to create novel agents effective against B. anthracis and its toxins.

Published

2006

23. Insertion selectivity of antimicrobial peptide protegrin-1 into lipid monolayers: Effect of head group electrostatics and tail group packing

Author

Robert I. Lehrer, Alan J. Waring, Duy Stephen L. Pham, Yuji Ishitsuka, and Ka Yee C. Lee

Subjects

Surface Properties, Static Electricity, Phospholipid, Biophysics, POPG, POPE, POPC, Biochemistry, Cell membrane, Lipid A, chemistry.chemical_compound, Anti-Infective Agents, Monolayer, Membrane fluidity, medicine, Selectivity, Langmuir monolayer, Phosphatidylethanolamine, Fluorescence microscopy, Proteins, Cell Biology, Lipids, Protegrin-1, Peptide–membrane interaction, Membrane, medicine.anatomical_structure, Spectrometry, Fluorescence, chemistry, Ganglioside, DPPE, Model cell membrane, DPPC, Dihydrocholesterol, Antimicrobial peptide, Disordering, DPPG, Antimicrobial Cationic Peptides

Abstract

The ability to selectively target the harmful microbial membrane over that of the host cell is one of the most important characteristics of the antimicrobial peptides (AMPs). This selectivity strongly depends on the chemical and structural properties of the lipids that make up the cell membrane. A systematic study of the initial membrane selectivity of protegrin-1 (PG-1), a β-sheet AMP, was performed using Langmuir monolayers. Constant pressure insertion assay was used to quantify the amount of PG-1 insertion and fluorescence microscopy was employed to observe the effect of PG-1 on lipid ordering. Charge and packing properties of the monolayer were altered by using lipids with different head groups, substituting saturated with unsaturated lipid tail group(s) and incorporating spacer molecules. PG-1 inserted most readily into anionic films composed of phosphatidylglycerol (PG) and lipid A, consistent with its high selectivity for microbial membranes. It also discriminated between zwitteranionic phospholipids, inserting more readily into phosphatidylcholine (PC) monolayers than those composed of phosphatidylethanolamine, potentially explaining why PG-1 is hemolytic for PC-rich human erythrocytes and not for the PE-rich erythrocytes of ruminants. Increased packing density of the monolayer by increased surface pressure, increased tail group saturation or incorporation of dihydrocholesterol diminishes the insertion of PG-1. Fluorescence microscopy shows that lipid packing is disordered upon PG-1 insertion. However, the presence of PG-1 can still affect lipid morphology even with no observed PG-1 insertion. These results show the important role that lipid composition of the cell membrane plays in the activity of AMPs.

Published

2006

24. α-Defensins from blood leukocytes of the monkey Papio hamadryas

Author

O. V. Shamova, Robert I. Lehrer, V. N. Kokryakov, G. M. Aleshina, E. V. Tsvetkova, and L. E. Leonova

Subjects

Staphylococcus aureus, alpha-Defensins, Molecular Sequence Data, Antimicrobial peptides, Biophysics, In Vitro Techniques, medicine.disease_cause, digestive system, Biochemistry, Biochemistry, Genetics and Molecular Biology (miscellaneous), Microbiology, Species Specificity, Candida albicans, Escherichia coli, Leukocytes, medicine, Animals, Humans, Amino Acid Sequence, Defensin, Hamadryas baboon, Chromatography, High Pressure Liquid, Phylogeny, Papio hamadryas, Sequence Homology, Amino Acid, integumentary system, biology, Edman degradation, fungi, General Medicine, respiratory system, bacterial infections and mycoses, biology.organism_classification, Listeria monocytogenes, Macaca mulatta, Rhesus macaque, Geriatrics and Gerontology

Abstract

Three antimicrobial peptides named PHD1-3 (Papio hamadryas defensin) have been isolated from hamadryas baboon blood leukocytes using preparative electrophoresis and reverse-phase HPLC. The primary structures of these peptides have been determined by automated Edman degradation and mass-spectrometry. The results suggest that the peptides belong to the alpha-defensin family. Structural homology analysis reveals that among alpha-defensins from other animal species, PHD3 is the most closely related to RMAD5 (rhesus macaque alpha-defensin) (90% homology) from rhesus macaque leukocytes and also highly similar to human alpha-defensin HD5 (60% homology), which is produced by intestinal Paneth cells. The homology of PHD3 with human neutrophil alpha-defensin HNP1 (human natural peptide) was 30%. The primary structures of PHD1 and PHD2 are most similar to RED1 (rhesus enteral defensin), one of six enteral alpha-defensins of rhesus monkeys. PHD1-3 have been shown to be active against the Gram-positive bacteria Listeria monocytogenes and Staphylococcus aureus, the Gram-negative bacterium Escherichia coli, and the fungus Candida albicans, similarly to the human HNP1 defensin.

Published

2006

25. HIV-1 Adapts to a Retrocyclin with Cationic Amino Acid Substitutions That Reduce Fusion Efficiency of gp41

Author

Otto O. Yang, Alan J. Waring, Amy L. Cole, Robert I. Lehrer, Alexander M. Cole, and Andrew Warren

Subjects

Anti-HIV Agents, viruses, Molecular Sequence Data, Immunology, Adaptation, Biological, Down-Regulation, Peptide, Virus Replication, Gp41, medicine.disease_cause, Membrane Fusion, Cell Line, Defensins, Viral entry, Drug Resistance, Viral, medicine, Humans, Immunology and Allergy, Amino Acid Sequence, chemistry.chemical_classification, Mutation, biology, biology.organism_classification, Virology, HIV Envelope Protein gp41, Cell biology, Amino acid, Heptad repeat, Amino Acid Substitution, chemistry, HIV-1, Glycoprotein, Viral Fusion Proteins, Bacteria

Abstract

Retrocyclin (RC)-101 is a cationic θ-defensin that inhibits HIV-1 entry. Passaging HIV-1BAL under selective pressure by this cyclic minidefensin resulted in only a 5- to 10-fold decrease in viral susceptibility to RC-101. Emergent viral isolates had three amino acid substitutions in their envelope glycoprotein. One was in a CD4-binding region of gp120, and the others were in the heptad repeat (HR) domains of gp41 (HR1 and HR2). Each mutation replaced an electroneutral or electronegative residue with one that was positively charged. These mutations were evaluated either alone or in combination in a single-round viral entry assay. Although the mutation in gp120 did not affect viral entry, the mutation in HR1 of gp41 conferred relative resistance to RC-101. Interestingly, the envelope with the HR2 mutation was less efficient and became codependent on the presence of RC-101 for entry. The adaptive response of HIV-1 to this cationic host defense peptide resembles the responses of bacteria that modulate their surface or membrane charge to evade analogous host defense peptides. These findings also suggest that interactions between θ-defensins and gp41 may contribute to the ability of these cyclic minidefensins to prevent HIV-1 entry into target cells.

Published

2006

26. Secretory Lipophilins: A Tale of Two Species

Author

Robert I. Lehrer, Chen Xian Ha, Ben J. Glasgow, Tung Nguyen, and Chengquan Zhao

Subjects

Bodily Secretions, Subfamily, Proteolipids, Protein subunit, Cystine, Peptide, Biology, Secretoglobins, General Biochemistry, Genetics and Molecular Biology, Prostatein, chemistry.chemical_compound, Mammaglobin, History and Philosophy of Science, Animals, Humans, Uteroglobin, PTEN, Gene, Chromatography, High Pressure Liquid, Phylogeny, Genetics, chemistry.chemical_classification, Sequence Homology, Amino Acid, General Neuroscience, Mammaglobin B, Biochemistry, chemistry, Tears, biology.protein, Myelin Proteins

Abstract

Secretory lipophilins are “lipid-loving” proteins that are major constituents of several mammalian secretions, including the prostatic fluid of rats and the tears of humans and rabbits. These proteins form covalent heterodimers that are stabilized by three intramolecular cystine disulfide bonds. The heterodimers, some of which are glycosylated, may undergo additional noncovalent assembly to form tetramers. The peptide components found in secretory lipophilins are from two subfamilies: lipophilins A/B and lipophilin C. The C subfamily members described in this report are three rabbit and one human lipophilin, plus human mammaglobin and the C3 subunit of rat prostatein. Human A/B and C lipophilins are expressed by many tissues and are especially prominent in endocrine-responsive organs. The gene for human lipophilin B resides at chromosome 10q22–23. This region harbors the PTEN/MMAC1 gene and is believed to contain additional tumor suppressor genes. Although the functions of secretory lipophilins are imperfectly understood, their abundance in glandular secretions and in hormone-responsive tissues suggests that they deserve considerably more attention than they have received to date.

Published

2006

27. Carbohydrate-binding molecules inhibit viral fusion and entry by crosslinking membrane glycoproteins

Author

Myoung-Soon Cho, Yongming Xie, Kamran Melikov, Alan J. Waring, Robert I. Lehrer, Hélène Delanoë-Ayari, Joseph A. Loo, Leonid V. Chernomordik, Andrew Y. Chen, Eugenia Leikina, and Wei Wang

Subjects

Sindbis virus, Erythrocytes, Immunology, Hemagglutinins, Viral, Hemagglutinin (influenza), Virus Replication, Membrane Fusion, Virus, Defensins, Anti-Infective Agents, Orthomyxoviridae Infections, Viral Envelope Proteins, Cell Line, Tumor, Humans, Immunology and Allergy, Membrane Glycoproteins, Innate immune system, biology, Lectin, Lipid bilayer fusion, Orthomyxoviridae, biology.organism_classification, Molecular biology, Immunity, Innate, Cell biology, Membrane glycoproteins, Cell culture, biology.protein, Carbohydrate Metabolism, Viral Fusion Proteins

Abstract

Defensins are peptides that protect the host against microorganisms. Here we show that the theta-defensin retrocyclin 2 (RC2) inhibited influenza virus infection by blocking membrane fusion mediated by the viral hemagglutinin. RC2 was effective even after hemagglutinin attained a fusogenic conformation or had induced membrane hemifusion. RC2, a multivalent lectin, prevented hemagglutinin-mediated fusion by erecting a network of crosslinked and immobilized surface glycoproteins. RC2 also inhibited fusion mediated by Sindbis virus and baculovirus. Human beta-defensin 3 and mannan-binding lectin also blocked viral fusion by creating a protective barricade of immobilized surface proteins. This general mechanism might explain the broad-spectrum antiviral activity of many multivalent lectins of the innate immune system.

Published

2005

28. Antibacterial Activity and Specificity of the Six Human α-Defensins

Author

Wuyuan Lu, Robert I. Lehrer, Bryan Ericksen, and Zhibin Wu

Subjects

Pharmacology, Analytical Procedures, alpha-Defensins, biology, Colony Count, Microbial, Bacillus cereus, Microbial Sensitivity Tests, Gram-Positive Bacteria, Antimicrobial, biology.organism_classification, medicine.disease_cause, Enterobacter aerogenes, Anti-Bacterial Agents, Microbiology, Infectious Diseases, Species Specificity, Cereus, Staphylococcus aureus, Gram-Negative Bacteria, medicine, Humans, Pharmacology (medical), Escherichia coli, Bacteria, Antibacterial agent

Abstract

We developed a kinetic, 96-well turbidimetric procedure that is capable of testing the antimicrobial properties of six human α-defensins concurrently on a single microplate. The defensins were prepared by solid-phase peptide synthesis and tested against gram-positive bacteria ( Staphylococcus aureus and Bacillus cereus ) and gram-negative bacteria ( Enterobacter aerogenes and Escherichia coli ). Analysis of the growth curves provided virtual lethal doses (vLDs) equivalent to conventional 50% lethal doses (LD 50 s), LD 90 s, LD 99 s, and LD 99.9 s obtained from colony counts. On the basis of their respective vLD 90 s and vLD 99 s, the relative potencies of human myeloid α-defensins against S. aureus were HNP2 > HNP1 > HNP3 > HNP4. In contrast, their relative potencies against E. coli and E. aerogenes were HNP4 > HNP2 > HNP1 = HNP3. HD5 was as effective as HNP2 against S. aureus and as effective as HNP4 against the gram-negative bacteria in our panel. HD6 showed little or no activity against any of the bacteria in our panel, including B. cereus , which was highly susceptible to the other five α-defensins. The assay described provides a quantitative, precise, and economical way to study the antimicrobial activities of host-defense peptides. Its use has clarified the relative potencies of human α-defensins and raised intriguing questions about the in vivo function(s) of HD6.

Published

2005

29. Solid-State NMR Investigation of the Selective Disruption of Lipid Membranes by Protegrin-1

Author

Alan J. Waring, Robert I. Lehrer, Mei Hong, Rajeswari Mani, and Jarrod J. Buffy

Subjects

Anions, Swine, Lipid Bilayers, Analytical chemistry, Biochemistry, chemistry.chemical_compound, Phase (matter), Animals, Lamellar structure, Lipid bilayer phase behavior, Lipid bilayer, Nuclear Magnetic Resonance, Biomolecular, Phosphatidylglycerol, Carbon Isotopes, Phosphorus Isotopes, Proteins, Lipid bilayer fusion, Phosphatidylglycerols, Biological membrane, Deuterium, Cholesterol, Membrane, chemistry, Phosphatidylcholines, Biophysics, Thermodynamics, Protons, Hydrophobic and Hydrophilic Interactions, Antimicrobial Cationic Peptides

Abstract

The interaction of a beta-hairpin antimicrobial peptide, protegrin-1 (PG-1), with various lipid membranes is investigated by (31)P, (2)H, and (13)C solid-state NMR. Mixed lipid bilayers containing anionic lipids and cholesterol are used to mimic the bacterial and mammalian cell membranes, respectively. (31)P and (2)H spectra of macroscopically oriented samples show that PG-1 induces the formation of an isotropic phase in anionic bilayers containing phosphatidylglycerol. Two-dimensional (31)P exchange experiments indicate that these isotropic lipids are significantly separate from the residual oriented lamellar bilayers, ruling out toroidal pores as the cause for the isotropic signal. (1)H spin diffusion experiments show that PG-1 is not exclusively bound to the isotropic phase but is also present in the residual oriented lamellar bilayers. This dynamic and morphological heterogeneity of the anionic membranes induced by PG-1 is supported by the fact that (13)C T(2) relaxation times measured under cross polarization and direct polarization conditions differ significantly. In contrast to the anionic membrane, the zwitterionic phosphatidylcholine (PC) membrane does not form an isotropic phase in the presence of PG-1 but shows significant orientational disorder. The addition of cholesterol to the PC bilayer significantly reduces this orientational disorder. The (13)C T(2) relaxation times of the PC lipids in the presence of both cholesterol and PG-1 suggest that the peptide may decrease the dynamic heterogeneity of the cholesterol-containing membrane. The observed selective interaction of PG-1 with different lipid membranes is consistent with its biological function and may be caused by its strong cationic and amphipathic structure.

Published

2004

30. Interaction of Antimicrobial Peptides with Lipopolysaccharides

Author

Lin Yang, Thomas M. Weiss, Alan J. Waring, Huey W. Huang, Robert I. Lehrer, and Lai Ding

Subjects

chemistry.chemical_classification, Circular dichroism, Antimicrobial peptides, Magainin, Peptide, Biochemistry, Melittin, chemistry.chemical_compound, chemistry, Protegrin, lipids (amino acids, peptides, and proteins), Lipid bilayer, Bacterial outer membrane

Abstract

We study the interaction of antimicrobial peptides with lipopolysaccharide (LPS) bilayers to understand how antimicrobial peptides interact with the LPS monolayer on the outer membrane of Gram-negative bacteria. LPS in water spontaneously forms a multilamellar structure composed of symmetric bilayers. We performed X-ray lamellar diffraction and wide-angle in-plane scattering to study the physical characteristics of LPS multilayers. The multilayer alignment of LPS is comparable to phospholipids. Thus, it is suitable for the application of oriented circular dichroism (OCD) to study the state of peptides in LPS bilayers. At high hydration levels, the chain melting temperature in multilamella detected by X-ray diffraction is the same as that of LPS aqueous dispersions, as measured by calorimetry. LPS has a strong CD, but with a careful subtraction of the lipid background, the OCD of peptides in LPS is measurable. The method was tested successfully with melittin. It was then applied to two representative antimicrobial peptides, magainin and protegrin. At peptide concentrations comparable to the physiological conditions, both peptides penetrate transmembrane in LPS bilayers. The results imply that antimicrobial peptides readily penetrate the LPS monolayer of the outer membrane.

Published

2003

31. Supported lipid bilayers lifted from the substrate by layer-by-layer polyion cushions on self-assembled monolayers

Author

Chen Ma, Robert I. Lehrer, Alan J. Waring, M.P. Srinivasan, Pieter Stroeve, and Marjorie L. Longo

Subjects

Layer by layer, Analytical chemistry, Self-assembled monolayer, Surfaces and Interfaces, General Medicine, Polystyrene sulfonate, chemistry.chemical_compound, Colloid and Surface Chemistry, Membrane, chemistry, Chemical engineering, Monolayer, lipids (amino acids, peptides, and proteins), Physical and Theoretical Chemistry, Surface plasmon resonance, Lipid bilayer, POPC, Biotechnology

Abstract

The formation of lipid bilayers, lifted from the solid substrate by layer-by-layer polyion cushions, on self-assembled monolayers (SAMs) on gold was investigated by surface plasmon resonance (SPR) and fluorescence recovery after photobleaching (FRAP). The polyions poly(diallyldimethylammonium chloride) (PDDA) and polystyrene sulfonate (PSS) sodium salt were used for the layer-by-layer polyion macromolecular assembly. The cushion was formed by electrostatic interaction of PDDA/PSS/PDDA layers with a negatively charged surface of an SAM of 11-mercaptoundecanoic acid (MUA) on gold. The lipid bilayer membranes were deposited by vesicle fusion with different compositions of SOPS (an anionic lipid, 1-stearoyl-2-oleoyl-phosphatidylserine) and POPC (a zwitterionic lipid, 1-palmitoyl-2-oleoylphosphatidylcholine). In the case of pure SOPS and for lipid mixtures with a POPC composition up to 25%, single bilayers were deposited. FRAP experiments showed that single bilayers supported on PDDA/PSS/PDDA/MUA were mobile at room temperature, with lateral coefficients of approximately (1.2–2.1)×10 −9 cm 2 /s. The kinetics of the addition of the ion-channel-forming peptide protegrin-1 to the supported bilayers was detected by SPR. A two-step interaction was observed, similar to the association behavior of protegrin-1 with bilayers supported on PDDA/MUA. The results are similar to that of supported lipid bilayers without a layer-by-layer cushion. The model membrane system in this work is a potential biosensor for mimicking the natural activities of biomolecules and is a possible tool to investigate the fundamental properties of biomembranes.

Published

2003

32. Plicatamide, an Antimicrobial Octapeptide from Styela plicata Hemocytes

Author

Alan J. Waring, Robert I. Lehrer, Jennifer Sands, Rustam Azimov, Steven W. Taylor, Lorenzo P. Menzel, J. Andy Tincu, and Teresa Hong

Subjects

Hemocytes, Lipid Bilayers, Cervix Uteri, medicine.disease_cause, Hemolysis, Biochemistry, Cell Line, Microbiology, Oxygen Consumption, medicine, Animals, Humans, Amino Acid Sequence, Urochordata, Molecular Biology, biology, Cell Membrane, Wild type, Cell Biology, medicine.disease, biology.organism_classification, Antimicrobial, Kinetics, Mesosome, Styela plicata, Staphylococcus aureus, Potassium, Female, Efflux, Oligopeptides, Bacteria

Abstract

Plicatamide (Phe-Phe-His-Leu-His-Phe-His-dc Delta DOPA), where dc Delta DOPA represents decarboxy-(E)-alpha,beta-dehydro-3,4-dihydroxyphenylalanine, is a potently antimicrobial octapeptide from the blood cells of the solitary tunicate, Styela plicata. Wild type and methicillin-resistant Staphylococcus aureus (MRSA) responded to plicatamide exposure with a massive potassium efflux that began within seconds. Soon thereafter, treated bacteria largely ceased consuming oxygen, and most became nonviable. Native plicatamide also formed cation-selective channels in model lipid bilayers composed of bacterial lipids. Methicillin-resistant S. aureus treated with plicatamide for 5 min contained prominent mesosomes as well as multiple, small dome-shaped surface protrusions that suggested the involvement of osmotic forces in its antimicrobial effects. To ascertain the contribution of the C-terminal dc Delta DOPA residue to antimicrobial activity, we synthesized several analogues of plicatamide that lacked it. One of these peptides, PL-101 (Phe-Phe-His-Leu-His-Phe-His-Tyr-amide), closely resembled native plicatamide in its antimicrobial activity and its ability to induce potassium efflux. Plicatamide was potently hemolytic for human red blood cells but did not lyse ovine erythrocytes. The small size, rapid action, and potent anti-staphylococcal activity of plicatamide and PL-101 make them intriguing subjects for future antimicrobial peptide design.

Published

2003

33. Activity of Novispirin G-10, a novel antimicrobial peptide against Chlamydia trachomatis and vaginosis-associated bacteria

Author

Bushra Yasin, Robert I. Lehrer, Elizabeth A. Wagar, and Mabel Pang

Subjects

Clinical Biochemistry, Antimicrobial peptides, ved/biology.organism_classification_rank.species, Prevotella, Chlamydia trachomatis, Microbial Sensitivity Tests, Biology, medicine.disease_cause, Prevotella bivia, Protein Structure, Secondary, Cell Line, Pathology and Forensic Medicine, Microbiology, Colony-Forming Units Assay, Bacteroidaceae Infections, medicine, Humans, Gardnerella vaginalis, Serotyping, Molecular Biology, Antibacterial agent, Mobiluncus, Vaginal flora, ved/biology, Vaginosis, Bacterial, Chlamydia Infections, medicine.disease, Virology, Anti-Bacterial Agents, Mobiluncus curtisii, Female, Bacterial vaginosis, Peptides, Antimicrobial Cationic Peptides

Abstract

We tested the activity of Novispirin G-10, a novel antimicrobial alpha-helical octadecapeptide structurally related to cathelicidins and other innate immunity peptides, against Chlamydia trachomatis serovars L2, D, and E and three organisms associated with bacterial vaginosis (BV). The peptide's activity against C. trachomatis was measured in 48-h shell vial assays with McCoy cell targets. Exposure to 100 micro g/ml of Novispirin G-10 reduced the infectivity of serovars D and E by 99.4-100% and serovar L2 by 91.7-99.1%. At the same concentration of 100 micro g/ml, Novispirin G-10 rapidly killed >99% of Mobiluncus curtisii, Gardnerella vaginalis, and Prevotella bivia, in standard colony-forming unit (CFU) assays. Given its simple structure and relative lack of cytotoxic and hemolytic activity, Novispirin G-10 may be a useful component of microbicide preparations designed to prevent chlamydial infection and/or remediate the abnormal vaginal flora associated with BV.

Published

2003

34. Phospholipid bilayers on a polyion-alkylthiol layer pair: microprobe imaging, electrochemical properties and peptide association

Author

Robert I. Lehrer, Alan J. Waring, Marjorie L. Longo, Liqin Zhang, Ruxandra Vidu, and Pieter Stroeve

Subjects

Materials science, Membrane permeability, Mechanical Engineering, Vesicle, Analytical chemistry, Condensed Matter Physics, Membrane, Adsorption, Chemical engineering, Mechanics of Materials, General Materials Science, Self-assembly, Surface plasmon resonance, Cyclic voltammetry, Lipid bilayer

Abstract

Atomic force microscopy (AFM) images of successive layers and peptide insertion in supported mobile phospholipid bilayers on polyion/alkylthiol layer pairs are reported. The morphology of each layer observed in a step-by-step adsorption process is correlated with electrochemical (cyclic voltammetry (CV)) and surface plasmon spectroscopy (SPR) results. The insulating properties of long-chain and short-chain alkylthiol layers are associated with a continuous layer and domain formation, respectively. The multilayer surface morphology is quantitatively characterized using roughness measurements for a large set of data involving root-mean-square roughness (RMS). Since the AFM observation with atomic and molecular resolution requires very flat and wide terraces to monitor the adsorption process, it is very important that initial surface morphology and roughness is known. Peptide association with the lipid membrane was studied by high resolution AFM in liquid, where pore formation was demonstrated for protegrin transmembrane insertion. The association of peptides with supported lipid bilayer of various compositions is discussed in terms of mobility and membrane permeability to charge transfer through the formation of pores.

Published

2002

35. Examination of Chlamydia trachomatis Infection in Environments Mimicking Normal and Abnormal Vaginal pH

Author

Bushra Yasin, Robert I. Lehrer, Elizabeth A. Wagar, and Mabel Pang

Subjects

Male, Microbiology (medical), Serial dilution, medicine.drug_class, Antibiotics, Chlamydia trachomatis, Microbial Sensitivity Tests, Dermatology, Biology, medicine.disease_cause, Cell Line, Microbiology, Semen, medicine, Humans, Chlamydiaceae, Vaginitis, Public Health, Environmental and Occupational Health, Proteins, Chlamydia Infections, Hydrogen-Ion Concentration, medicine.disease, biology.organism_classification, In vitro, Anti-Bacterial Agents, Infectious Diseases, Chlamydiales, Vagina, Female, Bacteria, Antimicrobial Cationic Peptides

Abstract

Background It has long been assumed that a healthy acidic vaginal environment inhibits infection by Chlamydia trachomatis. The research objectives were to evaluate the effect of pH on C trachomatis infection by two in vitro methods, to assess pH effect at different serial dilutions of C trachomatis elementary bodies (EBs), and to examine protection by an antibiotic peptide, protegrin (PG-1), over a pH range. Goals The goals of this study were to test the hypothesis that acidic pH inhibits C trachomatis infection and to determine the ability of PG-1 to provide protection at acidic and neutral pH. Study design The effect of pH on C trachomatis was examined using two pH-adjusted preincubation shell vial assays. C trachomatis EBs (serovars L2, D, and E) were exposed to pH-adjusted media, with and without PG-1, and infection was assessed by inclusion forming unit (IFU) formation in McCoy cell monolayers. Results Acidic pH in preincubation media markedly decreased IFUs by both in vitro methods. Serial dilution experiments showed a 3- to 10-fold reduction in IFUs for C trachomatis (L2 and E) at pH 5.0, compared with those at pH 7.5. C trachomatis (D) showed a 17- to 23-fold reduction in IFUs (serial dilutions 1:1-1:4). PG-1 protected McCoy cell monolayers from infection by C trachomatis after exposure to varied pH environments. Conclusion Acidic pH exposure significantly reduced C trachomatis infection in vitro. Our results support the hypothesis that a healthy acidic vaginal environment protects women from C trachomatis infection. In addition, antibiotic peptides may provide protection as topical microbicides, regardless of vaginal pH.

Published

2002

36. Solid-State NMR Investigations of Peptide−Lipid Interaction and Orientation of a β-Sheet Antimicrobial Peptide, Protegrin

Author

Mei Hong, Alan J. Waring, Robert I. Lehrer, Satoru Yamaguchi, and Teresa Hong

Subjects

Chemistry, Bilayer, Molecular Sequence Data, technology, industry, and agriculture, Proteins, Lipid bilayer fusion, Lipid bilayer mechanics, Model lipid bilayer, Biochemistry, Anti-Bacterial Agents, chemistry.chemical_compound, Crystallography, Lamellar phase, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, lipids (amino acids, peptides, and proteins), Amino Acid Sequence, Lipid bilayer phase behavior, Peptides, Lipid bilayer, Nuclear Magnetic Resonance, Biomolecular, POPC, Phospholipids, Antimicrobial Cationic Peptides

Abstract

Protegrin-1 (PG-1) is a broad-spectrum beta-sheet antimicrobial peptide found in porcine leukocytes. The mechanism of action and the orientation of PG-1 in lipid bilayers are here investigated using (2)H, (31)P, (13)C, and (15)N solid-state NMR spectroscopy. (2)H spectra of mechanically aligned and chain-perdeuterated 1-palmitoyl-2-oleoyl-sn-glycero-3-phosphatidylcholine (POPC) bilayers indicate that PG-1 at high concentrations destroys the orientational order of the aligned lamellar bilayer. The conformation of the lipid headgroups in the unoriented region is significantly altered, as seen from the (31)P spectra of POPC and the (2)H spectra of headgroup-deuterated 1,2-dipalmitoyl-sn-glycero-3-phosphatidylcholine. These observations indicate that PG-1 disrupts microbial membranes by breaking the extended bilayer into smaller disks, where a significant fraction of lipids is located in the edges of the disks with a distribution of orientations. These edges allow the lipid bilayer to bend back on itself as in toroidal pores. Interestingly, this loss of bilayer orientation occurs only in long-chain lipids such as POPC and not in shorter chain lipids such as 1,2-dilauroyl-sn-glycero-3-phosphatidylcholine (DLPC). To understand the mode of binding of PG-1 to the lipid bilayer, we determined the orientation of PG-1 in DLPC bilayers. The (13)CO and (15)N chemical shifts of Val-16 labeled PG-1 indicate that the beta-strand axis is tilted by 55 degrees +/- 5 degrees from the bilayer normal while the normal of the beta-sheet plane is 48 degrees +/- 5 degrees from the bilayer normal. This orientation favors interaction of the hydrophobic backbone of the peptide with the hydrophobic core of the bilayer and positions the cationic Arg side chains to interact with the anionic phosphate groups. This is the first time that the orientation of a disulfide-stabilized beta-sheet membrane peptide has been determined by solid-state NMR.

Published

2002

37. Immunolocalization of clavanins in Styela clava hemocytes

Author

Lorenzo P. Menzel, In Hee Lee, Robert I. Lehrer, and Birgitta Sjostrand

Subjects

Hemocytes, Phagocytosis, Blotting, Western, Molecular Sequence Data, Immunology, Antimicrobial peptides, Population, Styela clava, Biology, Microbiology, Methyl Green, Animals, Microscopy, Phase-Contrast, Trichrome stain, Amino Acid Sequence, Urochordata, Coloring Agents, education, education.field_of_study, Innate immune system, Sequence Homology, Amino Acid, Blood Proteins, biology.organism_classification, Immunohistochemistry, Microscopy, Electron, Cytoplasm, Polyclonal antibodies, biology.protein, Eosine Yellowish-(YS), Electrophoresis, Polyacrylamide Gel, Azo Compounds, Developmental Biology

Abstract

Antimicrobial peptides play an important role in innate host defenses against infection. Clavanins are histidine-rich, amidated, 23-residue alpha-helical antimicrobial peptides that were isolated from a mixed population of Styela clava hemocytes. To learn which types of hemocytes contained clavanins, we raised a polyclonal antibody that recognized five different clavanins, and used it to localize these peptides by light and electron microscopy. Clavanins were present in the cytoplasmic granules and/or cytoplasm of five different types of granulocytes and they also occurred throughout the cytoplasm of macrophages. The orange G component of Mallory's trichrome stain had a high affinity for clavanins, and for the cytoplasmic granules of S. clava's hemocytes. Semiquantitative analysis of acid urea-PAGE gels suggested that clavanins and styelins comprised between 10 and 20% of the total cellular protein of eosinophilic granulocytes. Orange G and the century-old trichrome stain may provide simple screening tools for identifying cells that contain large amounts of antimicrobial peptides in mixed hemocyte populations.

Published

2002

38. Potassium release, a useful tool for studying antimicrobial peptides

Author

Tung Nguyen, Dmitri S Orlov, and Robert I. Lehrer

Subjects

Microbiology (medical), Bacteria, Dose-Response Relationship, Drug, biology, Potassium, Antimicrobial peptides, Proteins, chemistry.chemical_element, Blood Proteins, biology.organism_classification, Microbiology, Anti-Bacterial Agents, Cathelicidins, Membrane integrity, Biochemistry, chemistry, Regression Analysis, Peptides, Electrodes, Molecular Biology, Antimicrobial Cationic Peptides

Abstract

We used an ion-selective electrode to measure potassium release from bacteria treated with antimicrobial peptides. This broadly applicable and simple technique for assessing membrane integrity deserves greater use.

Published

2002

39. Retrocyclin: A primate peptide that protects cells from infection by T- and M-tropic strains of HIV-1

Author

Chengquan Zhao, Alexander M. Cole, Alan J. Waring, Jerome A. Zack, Robert I. Lehrer, Teresa Hong, Tung Nguyen, Greg Bristol, Lee Ming Boo, and Otto O. Yang

Subjects

Boron Compounds, CD4-Positive T-Lymphocytes, DNA, Complementary, Time Factors, Molecular Sequence Data, Bone Marrow Cells, Enzyme-Linked Immunosorbent Assay, Peptide, Biology, Models, Biological, Polymerase Chain Reaction, Theta defensin, law.invention, Defensins, chemistry.chemical_compound, law, Fluorescence microscope, Animals, Humans, Polymerase chain reaction, chemistry.chemical_classification, Microscopy, Confocal, Multidisciplinary, Base Sequence, Dose-Response Relationship, Drug, Sequence Homology, Amino Acid, Reverse Transcriptase Polymerase Chain Reaction, Oligonucleotide, Circular Dichroism, Proteins, Oligonucleotides, Antisense, Biological Sciences, Macaca mulatta, Virology, In vitro, Amino acid, chemistry, DNA, Viral, HIV-1, Salts, Peptides, DNA

Abstract

Human bone marrow expresses a pseudogene that encodes an antimicrobial peptide homologous to rhesus monkey circular minidefensins (θ-defensins). We prepared the putative ancestral human peptide by solid-phase synthesis and named it “retrocyclin.” Retrocyclin did not cause direct inactivation of HIV-1, and its modest antibacterial properties resembled those of its rhesus homologs. Nevertheless, retrocyclin had a remarkable ability to inhibit proviral DNA formation and to protect immortalized and primary human CD4+lymphocytes fromin vitroinfection bybothT-tropic and M-tropic strains of HIV-1. Confocal fluorescent microscopy studies performed with BODIPY-FL-labeled RC-101, a close analog of retrocyclin, showed that the peptide formed patch-like aggregates on the surface of CD4+cells. These findings suggest that retrocyclin interferes with an early stage of HIV-1 infection and that retrocyclin-like agents might be useful topical agents to prevent sexually acquired HIV-1 infections.

Published

2002

40. SMAP-29 has two LPS-binding sites and a central hinge

Author

William R. Kearney, Huiyuan Wu, Brian F. Tack, Alan J. Waring, Andrew D. Robertson, Wei Wang, Monali V. Sawai, Mark A. Sherman, Robert I. Lehrer, Teresa Hong, and Lee Ming Boo

Subjects

chemistry.chemical_classification, biology, Stereochemistry, Cooperative binding, Cooperativity, Peptide, biology.organism_classification, Biochemistry, Micelle, Cathelicidins, chemistry, Limulus, lipids (amino acids, peptides, and proteins), Binding site, Peptide sequence

Abstract

The CD spectra of SMAP-29, an antimicrobial peptide from sheep, showed disordered structure in aqueous buffers, and significant helicity in membrane-like environments, including SDS micelles, lipopolysaccharide (LPS) dispersions, and trifluoroethanol buffer systems. A structure determined by NMR in 40% perdeuterated trifluoroethanol indicated that residues 8-17 were helical, residues 18-19 formed a hinge, and residues 20-28 formed an ordered, hydrophobic segment. SMAP-29 was flexible in 40% trifluoroethanol, forming two sets of conformers that differed in the relative orientation of the N-terminal domain. We used a chromogenic Limulus assay to determine the EC50 of the peptide (the concentration that bound 50% of the added LPS). Studies with full-length and truncated SMAP-29 molecules revealed that each end of the holopeptide contained an LPS-binding domain. The higher affinity LPS-binding domain was situated in the flexible N-terminal portion. LPS binding to full-length SMAP-29 showed positive cooperativity, so the EC50 of the peptide (2.6 microm) was considerably lower than that of the individual LPS-binding domains. LPS-binding studies with a mixture of truncated peptides revealed that this cooperativity was primarily intramolecular (i.e. involving the N- and C-terminal LPS-binding sites of the same peptide molecule). CAP-18[106 -142], an antimicrobial cathelicidin peptide of rabbits, resembled SMAP-29 in that it contained N- and C-terminal LPS-binding domains, had an EC50 of 2.5 microm, and bound LPS with positive cooperativity. We conclude that the presence of multiple binding sites that function cooperatively allow peptides such as SMAP-29 and CAP-18 to bind LPS with high affinity.

Published

2002

41. Defensins of vertebrate animals

Author

Tomas Ganz and Robert I. Lehrer

Subjects

Genetics, Subfamily, integumentary system, fungi, Immunology, Vertebrate Animals, hemic and immune systems, respiratory system, Biology, bacterial infections and mycoses, Immunity, Innate, Defensins, Mice, Immune system, Microbial resistance, Immunity, Vertebrates, Animals, Immunology and Allergy, Defensin

Abstract

During the past year, novel β-defensins of mice and men have been identified, together with a novel defensin subfamily (the circular or ‘θ’ minidefensins) in primates. Insight into the evolution of defensins has been obtained from structural studies, and several mechanisms related to microbial resistance to defensins have been delineated. There is now convincing evidence that defensins augment adaptive immune responses.

Published

2002

42. Electrochemical and Surface Properties of Solid-Supported, Mobile Phospholipid Bilayers on a Polyion/Alkylthiol Layer Pair Used for Detection of Antimicrobial Peptide Insertion

Author

Alan J. Waring, and Marjorie L. Longo, Robert I. Lehrer, Liqin Zhang, Ruxandra Vidu, and Pieter Stroeve

Subjects

chemistry.chemical_classification, Bilayer, Analytical chemistry, Phospholipid, Peptide, Surfaces and Interfaces, Condensed Matter Physics, Electrochemistry, chemistry.chemical_compound, Membrane, chemistry, Chemical engineering, General Materials Science, Surface plasmon resonance, Cyclic voltammetry, Layer (electronics), Spectroscopy

Abstract

Successive layer properties and peptide insertion in an assembly of supported mobile phospholipid bilayers on polyion/alkylthiol layer pairs were investigated in a combined optical, electrochemical, and surface topography study using surface plasmon resonance (SPR), cyclic voltammetry (CV), and atomic force microscopy (AFM). The use of a long-chain alkylthiol in this assembly was too insulating, and thus, a short-chain alkylthiol was used to probe membrane electrochemical properties. Using AFM, we found that the insulating properties of long-chain and short-chain alkylthiol layers are associated with a continuous layer and domain formation, respectively. Increased insulating properties of the supported bilayers were observed when mixtures of negatively charged and zwitterionic/neutral lipids were used. By attempting to obtain high-resolution images and make depressions in the surface using AFM, we found that this bilayer was more mobile than a bilayer composed completely of negatively charged lipid. A por...

Published

2002

43. Cathelicidins: a family of endogenous antimicrobial peptides

Author

Tomas Ganz and Robert I. Lehrer

Subjects

Neutrophils, Molecular Sequence Data, Antimicrobial peptides, Peptide, Endogeny, Biology, Biological effect, Cytoplasmic granules, Mice, Anti-Infective Agents, Cathelicidins, Gene expression, Animals, Humans, Amino Acid Sequence, chemistry.chemical_classification, Proteins, Blood Proteins, Hematology, Antimicrobial, Chemotaxis, Leukocyte, Biochemistry, chemistry, Multigene Family, Immunology, Peptides, Antimicrobial Cationic Peptides

Abstract

The cytoplasmic granules of mammalian neutrophils contain several antimicrobial peptides. Some, like defensins, are fully processed before storage, whereas others are stored as precursors that require additional processing. Cathelicidins are bipartite molecules with an N-terminal cathelin domain and an antimicrobial C-terminal domain. Humans apparently have only one cathelicidin gene. Its product, hCAP-18, is present in the secondary (specific) granules of neutrophils, and its C-terminal antimicrobial peptide, LL-37, is liberated by proteinase 3 coincident with degranulation and secretion. Many nonmyeloid tissues also express hCAP-18, including epididymis, spermatids, keratinocytes, epithelial cells, and various lymphocytes. LL-37 stimulates chemotaxis, acting via the formyl peptide-like receptor-1. The structurally diverse cathelicidin-derived antimicrobial peptides of animals provide interesting models for pharmaceutical development. PR-39, a proline-rich porcine cathelicidin, has shown efficacy in limiting myocardial damage after experimental ischemia in rodent models. Porcine protegrins are in stage III clinical trials to prevent oral mucositis caused by radiation or chemo-therapy.

Published

2002

44. Is there a single porcine protegrin gene?

Author

Robert I. Lehrer

Subjects

chemistry.chemical_compound, chemistry, Protegrin, Animals, Cell Biology, Biology, Molecular Biology, Biochemistry, Molecular biology, Gene, Antimicrobial Cationic Peptides

Published

2014

45. Defensins and Cathelicidins: Antimicrobial Peptide Effectors of Mammalian Innate Immunity

Author

Tomas Ganz and Robert I. Lehrer

Subjects

NADPH oxidase, Innate immune system, Effector, medicine.medical_treatment, Antimicrobial peptides, Biology, Antimicrobial, Cathelicidin, Microbiology, Cathelicidins, Beta defensin, Biochemistry, biology.protein, medicine

Abstract

This chapter centers on antimicrobial peptides, effector molecules that generally act by disrupting microbial membranes. When human neutrophils ingest Salmonella enterica serovar Typhimurium in the presence of radioactive iodide, defensins are the most abundant radioiodinated polypeptides in phagocytic vacuoles. Since iodination is produced by the neutrophil’s myeloperoxidase-hydrogen peroxide system, iodinated defensins provide evidence that the neutrophil’s oxidative and nonoxidative systems operate concurrently within the phagosome. Presumably, adverse consequences from the lack of neutrophil defensins in these species are mitigated by the presence of other antimicrobial effector mechanisms, such as NADPH oxidase, inducible nitric oxide synthase, cathelicidins, serprocidins, and other antimicrobial polypeptides. The only known human cathelicidin has been designated hCAP18 or FALL39/LL-37 by the three groups that described its cDNA, gene and peptide forms. Unlike defensins, which are stored in their mature form in the granules of neutrophils, hCAP18/LL-37 is stored as a 16-kDa (140-aminoacid) proform. Individual peptides differ in their antimicrobial spectrum, and early evidence suggests that they sometimes act synergistically with each other or with larger antimicrobial polypeptides. At sites that are more distant from the infected or inflamed locus, lower concentrations of defensins may act as signaling molecules, similarly to chemokines.

Published

2014

46. RL-37, an Alpha-Helical Antimicrobial Peptide of the Rhesus Monkey

Author

Cesar Espiritu, Wei Wang, Lee Ming Boo, Teresa Hong, Alan J. Waring, Dmitri S Orlov, Tung Nguyen, Robert I. Lehrer, and Chengquan Zhao

Subjects

Lipopolysaccharides, DNA, Complementary, medicine.medical_treatment, Molecular Sequence Data, Peptide, Microbial Sensitivity Tests, Biology, Protein Structure, Secondary, Cathelicidin, chemistry.chemical_compound, Cathelicidins, Aspartic acid, Escherichia coli, Staphylococcus epidermidis, medicine, Peptide synthesis, Animals, Pharmacology (medical), Amino Acid Sequence, Asparagine, Mechanisms of Action: Physiological Effects, Peptide sequence, Antibacterial agent, Pharmacology, chemistry.chemical_classification, Base Sequence, Sequence Homology, Amino Acid, Circular Dichroism, Proteins, Macaca mulatta, Peptide Fragments, Anti-Bacterial Agents, Protein Structure, Tertiary, Glutamine, Infectious Diseases, Biochemistry, chemistry, Liposomes, Antimicrobial Cationic Peptides

Abstract

Rhesus monkey bone marrow expresses a cathelicidin whose C-terminal domain comprises a 37-residue alpha-helical peptide (RL-37) that resembles human LL-37. Like its human counterpart, RL-37 rapidly permeabilized the membranes of Escherichia coli ML-35p and lysed liposomes that simulated bacterial membranes. When tested in media whose NaCl concentrations approximated those of extracellular fluids, RL-37 was considerably more active than LL-37 against staphylococci. Whereas human LL-37 contains five acidic residues and has a net charge of +6, rhesus RL-37 has only two acidic residues and a net charge of +8. Speculating that the multiple acidic residues of human LL-37 reduced its efficacy against staphylococci, we made a peptide (LL-37 pentamide) in which each aspartic acid of LL-37 was replaced by an asparagine and each glutamic acid was replaced by a glutamine. LL-37 pentamide's antistaphylococcal activity was substantially greater than that of LL-37. Thus, although the precursor of LL-37 is induced in human skin keratinocytes by injury or inflammation, its insufficiently cationic antimicrobial domain may contribute to the success of staphylococci in colonizing and infecting human skin.

Published

2001

47. Orientation and Dynamics of an Antimicrobial Peptide in the Lipid Bilayer by Solid-State NMR Spectroscopy

Author

Alan J. Waring, Robert I. Lehrer, Brian F. Tack, William R. Kearney, Mei Hong, Daniel Huster, and Satoru Yamaguchi

Subjects

Magnetic Resonance Spectroscopy, Rotation, Surface Properties, Lipid Bilayers, Biophysics, Peptide binding, Peptide, Diffusion, Lipid bilayer phase behavior, Lipid bilayer, Phospholipids, chemistry.chemical_classification, Binding Sites, Chemistry, Bilayer, Water, Membranes, Artificial, Nuclear magnetic resonance spectroscopy, Crystallography, Models, Chemical, Solid-state nuclear magnetic resonance, Helix, Thermodynamics, lipids (amino acids, peptides, and proteins), Research Article, Antimicrobial Cationic Peptides

Abstract

The orientation and dynamics of an 18-residue antimicrobial peptide, ovispirin, has been investigated using solid-state NMR spectroscopy. Ovispirin is a cathelicidin-like model peptide (NH(2)-KNLRRIIRKIIHIIKKYG-COOH) with potent, broad-spectrum bactericidal activity. (15)N NMR spectra of oriented ovispirin reconstituted into synthetic phospholipids show that the helical peptide is predominantly oriented in the plane of the lipid bilayer, except for a small portion of the helix, possibly at the C-terminus, which deviates from the surface orientation. This suggests differential insertion of the peptide backbone into the lipid bilayer. (15)N spectra of both oriented and unoriented peptides show a reduced (15)N chemical shift anisotropy at room temperature compared with that of rigid proteins, indicating that the peptide undergoes uniaxial rotational diffusion around the bilayer normal with correlation times shorter than 10(-4) s. This motion is frozen below the gel-to-liquid crystalline transition temperature of the lipids. Ovispirin interacts strongly with the lipid bilayer, as manifested by the significantly reduced (2)H quadrupolar splittings of perdeuterated palmitoyloleoylphosphatidylcholine acyl chains upon peptide binding. Therefore, ovispirin is a curved helix residing in the membrane-water interface that executes rapid uniaxial rotation. These structural and dynamic features are important for understanding the antimicrobial function of this peptide.

Published

2001

48. Dicynthaurin: an antimicrobial peptide from hemocytes of the solitary tunicate, Halocynthia aurantium

Author

Alan J. Waring, Robert I. Lehrer, Lorenzo P. Menzel, Mark A. Sherman, Jan Pohl, Chong Han Kim, Young Shin Lee, Chung Ryul Kim, Teresa Hong, Lee Ming Boo, and In Hee Lee

Subjects

Models, Molecular, Hemocytes, Molecular Sequence Data, Biophysics, Peptide, Microbial Sensitivity Tests, medicine.disease_cause, Biochemistry, Microbiology, Anti-Infective Agents, medicine, Animals, Amino Acid Sequence, Urochordata, Candida albicans, Molecular Biology, Escherichia coli, chemistry.chemical_classification, biology, Tissue Extracts, Chemistry, Circular Dichroism, Dipeptides, biology.organism_classification, Antimicrobial, Anti-Bacterial Agents, Tunicate, Molecular Weight, Staphylococcus aureus, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Peptides, Micrococcus luteus, Dimerization, Bacteria

Abstract

We isolated a novel antimicrobial peptide, dicynthaurin, from hemocytes of a tunicate, Halocynthia aurantium. The native peptide had a mass of approximately 6.2 kDa and was composed of two 30-residue monomers without sequence homology to any previously identified peptides (ILQKAVLDCLKAAGSSLSKAAITAIYNKIT). Most cynthaurin molecules were C-terminally amidated and were linked covalently by a single cystine disulfide bond. When performed in membrane-mimetic environments, circular dichroism studies of dicynthaurin revealed largely K-helical conformations. Dicynthaurin’s broad-spectrum activity encompassed Gram-positive (Micrococcus luteus, Staphylococcus aureus, Listeria monocytogenes) and Gram-negative bacteria (Escherichia coli, Pseudomonas aeruginosa), but not Candida albicans, a fungus. Although dicynthaurin was purified from a marine invertebrate, its antimicrobial activity was optimal at NaCl concentrations below 100 mM. This suggests that the antimicrobial actions of this molecule may take place intracellularly (e.g., within a phagosome) rather than extracellularly. fl 2001 Elsevier Science B.V. All rights reserved.

Published

2001

49. Analogs of the antimicrobial peptide trichogin having opposite membrane properties

Author

Huiyuan Wu, Marco Crisma, Richard M. Epand, Fernando Formaggio, Robert I. Lehrer, Claudio Toniolo, and Raquel F. Epand

Subjects

chemistry.chemical_classification, Liposome, Aqueous solution, Stereochemistry, Vesicle, Dimer, Lipid bilayer fusion, Peptide, Biochemistry, Amino acid, chemistry.chemical_compound, Membrane, chemistry, Organic chemistry

Abstract

Four analogs of the antimicrobial peptide trichogin GA IV were studied. Their sequences are as follows: GT, n-octanoyl-Aib-Gly-Leu-Aib-Gly-Gly-Leu-Aib-Gly-Ile-Leu-OMe; ST, n-octanoyl-Aib-Ser-Leu-Aib-Ser-Ser-Leu-Aib-Ser-Ile-Leu-OMe; BT, n-octanoyl-Aib-Ser(tBu)-Leu-Aib-Ser(tBu)-Ser(tBu)-Leu-Aib-Ser(tBu)-Ile-Leu-OMe; and DT, n-octanoyl-Aib-Ser(tBu)-Leu-Aib-Ser(tBu)-Ser(tBu)-Leu-Aib-Ser(tBu)-Ile-Leu-Aib-Ser(tBu)-Leu-Aib-Ser(tBu)-Ser(tBu)-Leu-Aib-Ser(tBu)-Ile-Leu-OMe. The trichogin GA IV differs from GT only in the nature of the C-terminal residue, being a 1,2 aminoalcohol (leucinol) in the case of the parent peptide. Compared with GT, ST has an increased amphiphilicity. In contrast, BT has little amphiphilicity being composed only of hydrophobic amino acids. DT is an octanoylated head-to-tail dimer of BT. We show that BT and DT lower the bilayer-to-hexagonal phase transition temperature (TH) of dipalmitoleoylphosphatidylethanolamine, indicating that the peptides promote negative curvature. These two peptides, composed of only hydrophobic amino acids, have their bulkier groups on one face of the helix, suggesting that they may penetrate membranes at an oblique angle. In contrast, GT and ST, like trichogin itself, increase TH, promoting positive curvature. These peptides have contrasting membrane lytic activities. Whereas DT and BT did not produce leakage of aqueous contents, GT and ST, like trichogin, did cause rapid leakage. The leakage activity with liposomes also correlates with the greater potency of GT and ST, compared with the hydrophobic analogs, in their hemolytic and bacteriostatic action. ST has greater lytic ability than GT in liposomal leakage as well as hemolysis. We also measured the rate of peptide-promoted lipid mixing as an indication of membrane fusion. BT produced lipid mixing only with large unilamellar vesicles enriched with dioleoylphosphatidylethanolamine; ST did not produce lipid mixing, as its apparent reduction of energy transfer proved to be artifactual. Quasi-elastic light scattering of large unilamellar vesicles was also carried out after adding ST and BT. Peptide BT, but not ST, was able to aggregate large unilamellar vesicles. Thus, one of the properties of BT that leads to the induction of lipid mixing is that it is able to aggregate vesicles, placing the bilayers in juxtaposition. Thus, the two pairs of peptides, BT and DT vs GT and ST, exhibit contrasting behaviour with respect to a number of membrane biophysical properties. This occurs despite the fact that the chemical structures of the peptides are rather similar. Such distinct behavior is also reflected in their hemolytic and bacteriostatic actions.

Published

2001

50. Styelin D, an Extensively Modified Antimicrobial Peptide from Ascidian Hemocytes

Author

Wolfgang H. Fischer, Steven W. Taylor, Minkyu Park, Robert I. Lehrer, and A. Grey Craig

Subjects

Cell Membrane Permeability, Hemocytes, Molecular Sequence Data, Lysine, Peptide, Styela clava, Biology, Biochemistry, Gas Chromatography-Mass Spectrometry, Escherichia coli, Animals, Cytotoxic T cell, Amino Acid Sequence, Urochordata, Molecular Biology, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Innate immune system, Tryptophan, Proteins, Cell Biology, biology.organism_classification, Antimicrobial, Peptide Fragments, Anti-Bacterial Agents, Dihydroxyphenylalanine, Amino acid, chemistry, Bacteria, Antimicrobial Cationic Peptides

Abstract

We isolated styelin D, a 32-residue, C-terminally amidated antimicrobial peptide, from the blood cells (hemocytes) of the solitary ascidian, Styela clava. Styelin D had remarkably extensive post-translational modifications, containing two novel amino acids, dihydroxyarginine and dihydroxylysine, and two distinctly unusual ones, 6-bromotryptophan and 3,4-dihydroxyphenylalanine. In addition, the peptide exhibited microheterogeneity because of differential mono- and dihydroxylation of several lysine residues. The primary sequence of one variant was: GW(*)LR(**)K(**)AAK(**)SVGK(**)FY(*)Y(*)K(**)HK(*)Y(*) Y(*)IK(*)AAWQIG KHAL-NH(2), where W(*) is 6-bromotryptophan, R(**) is dihydroxyarginine, Y(*) is 3,4-dihydroxyphenylalanine, K(*) is 5-hydroxylysine, and K(**) is dihydroxylysine. Styelin D exhibited activity against Gram-negative and Gram-positive bacteria, and this activity was retained in 200 mm NaCl. The role of the extensive modifications may be to preserve activity at low pH and/or high salinity because, under these conditions, the native peptide was considerably more active against the Gram-positive bacterial strains than its unmodified synthetic analogue. The peptide was also hemolytic and quite cytotoxic to eukaryotic cells. These broad ranging activities, combined with its relative abundance in ascidian hemocytes, suggest that styelin D plays a significant role in the innate immune mechanisms of S. clava.

Published

2000