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43 results on '"Cole, Amy L."'

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

Author

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

Subjects
Cervix Uteri, Vagina, Hela Cells, Animals, Macaca nemestrina, Humans, HIV-1, Simian Acquired Immunodeficiency Syndrome, Peptides, Antiviral Agents, Colposcopy, Administration, Intravaginal, Dose-Response Relationship, Drug, Time Factors, Female, Simian immunodeficiency virus, HeLa Cells, Simian Immunodeficiency Virus, Administration, Intravaginal, Dose-Response Relationship, Drug, General Science & Technology
Abstract

BackgroundRC-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.Methodology/principal findingsRC-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.Conclusions/significanceFormulated 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

19. Correction: Non-Cationic Proteins Are Associated with HIV Neutralizing Activity in Genital Secretions of Female Sex Workers

Author

Birse, Kenzie D. M., primary, Cole, Amy L., additional, Hirbod, Taha, additional, McKinnon, Lyle, additional, Ball, Terry B., additional, Westmacott, Garrett R., additional, Kimani, Joshua, additional, Plummer, Frank, additional, Cole, Alexander M., additional, Burgener, Adam, additional, and Broliden, Kristina, additional

Published
2015
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21. HIV-Enhancing and HIV-Inhibiting Properties of Cationic Peptides and Proteins.

Author

Cole, Alexander M. and Cole, Amy L.

Subjects
*PEPTIDES, *HIV, *PROTEINS, *HTLV, *NATURAL immunity
Abstract

Cationic antimicrobial peptides and proteins have historically been ascribed roles in innate immunity that infer killing of microbial and viral pathogens and protection of the host. In the context of sexually transmitted HIV-1, we take an unconventional approach that questions this paradigm. It is becoming increasingly apparent that many of the cationic polypeptides present in the human genital or anorectal mucosa, or human semen, are capable of enhancing HIV-1 infection, often in addition to other reported roles as viral inhibitors. We explore how the in vivo environment may select for or against the HIV-enhancing aspects of these cationic polypeptides by focusing on biological relevance. We stress that the distinction between enhancing and inhibiting HIV-1 infection is not mutually exclusive to specific classes of cationic polypeptides. Understanding how virally enhancing peptides and proteins act to promote sexual transmission of HIV-1 would be important for the design of topical microbicides, mucosal vaccines, and other preventative measures. [ABSTRACT FROM AUTHOR]

Published
2017
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22. HIV-1 Enhancing Effect of Prostatic Acid Phosphatase Peptides Is Reduced in Human Seminal Plasma

Author

Martellini, Julie A., Cole, Amy L., Svoboda, Pavel, Stuchlik, Olga, Chen, Li-Mei, Chai, Karl X., Gangrade, Bhushan K., Sørensen, Ole E, Pohl, Jan, Cole, Alexander M., Martellini, Julie A., Cole, Amy L., Svoboda, Pavel, Stuchlik, Olga, Chen, Li-Mei, Chai, Karl X., Gangrade, Bhushan K., Sørensen, Ole E, Pohl, Jan, and Cole, Alexander M.

Abstract

We recently reported that HIV-1 infection can be inhibited by innate antimicrobial components of human seminal plasma (SP). Conversely, naturally occurring peptidic fragments from the SP-derived prostatic acid phosphatase ( PAP) have been reported to form amyloid fibrils called "SEVI'' and enhance HIV-1 infection in vitro. In order to understand the biological consequence of this proviral effect, we extended these studies in the presence of human SP. PAP-derived peptides were agitated to form SEVI and incubated in the presence or absence of SP. While PAP-derived peptides and SEVI alone were proviral, the presence of 1% SP ablated their proviral activity in several different anti-HIV-1 assays. The anti-HIV-1 activity of SP was concentration dependent and was reduced following filtration. Supraphysiological concentrations of PAP peptides and SEVI incubated with diluted SP were degraded within hours, with SP exhibiting proteolytic activity at dilutions as high as 1:200. Sub-physiological concentrations of two prominent proteases of SP, prostate-specific antigen (PSA) and matriptase, could degrade physiological and supraphysiological concentrations of PAP peptides and SEVI. While human SP is a complex biological fluid, containing both antiviral and proviral factors, our results suggest that PAP peptides and SEVI may be subject to naturally occurring proteolytic components capable of reducing their proviral activity.

Published
2011

35. Role for Sterol Regulatory Element-Binding Protein in Activation of Endothelial Cells by Phospholipid Oxidation Products

Author

Yeh, Michael, primary, Cole, Amy L., additional, Choi, Jenny, additional, Liu, Yi, additional, Tulchinsky, Dmitry, additional, Qiao, Jian-Hua, additional, Fishbein, Michael C., additional, Dooley, Alek N., additional, Hovnanian, Talin, additional, Mouilleseaux, Kevin, additional, Vora, Devendra K., additional, Yang, Wen-Pin, additional, Gargalovic, Peter, additional, Kirchgessner, Todd, additional, Shyy, John Y.-J., additional, and Berliner, Judith A., additional

Published
2004
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39. Depression in Anderson-Fabry Disease: The Need for Greater Awareness.

Author

Cole, Amy L.

Subjects
*MENTAL depression, *LYSOSOMAL storage diseases, *LIFE change events, *QUALITY of life, *AWARENESS
Abstract

The article examines depression in patients with Anderson-Fabry Disease (AFD), a rare X-linked lysosomal storage disorder (LSD) resulting from deficient activity of α-galactosidase A (α-gal A) . The author says that depression in AFD patients develops because of the stress they experience as a result of a delay in the diagnosis and because of body function impairment. She notes the importance of early and proper treatment of the depression to improve the overall treatment outcome.

Published
2007

40. Characterization of the Retrocyclin Analogue RC-101 as a Preventative of Staphylococcus aureusNasal Colonization

Author

Lamers, Ryan P., Eade, Colleen R., Waring, Alan J., Cole, Amy L., and Cole, Alexander M.

Abstract

ABSTRACTNasal colonization of Staphylococcus aureusis a risk factor for pathogenic autoinfection, particularly in postoperative patients and the immunocompromised. As such, standardized preoperative nasal decolonization of S. aureushas become a major consideration for the prevention of nosocomial infection. However, only a few treatment options for nasal decolonization are currently available, with resistance to these approaches already a concern. Here we have identified the macrocyclic θ-defensin analogue RC-101 as a promising anti-S. aureusagent for nasal decolonization. RC-101 exhibits bactericidal effects against S. aureuswith the use of in vitroepithelium-free systems, while also preventing the pathogen's proliferation and attachment in an ex vivohuman nasal epithelial cell adhesion model and an organotypic model of human airway epithelia. Peptide concentrations as low as 2.5 μM elicited significant reductions in S. aureusgrowth in epithelium-free systems, with 10 μM concentrations being completely bactericidal for all strains tested, including USA300. In ex vivonasal colonization models, RC-101 significantly reduced adherence, survival, and proliferation of S. aureuson human nasal epithelia. Reductions in S. aureusviability were evident in these assays, with as little as 1 μg of peptide per tissue, while 10 μg of RC-101 completely prevented adhesion of all strains tested. Furthermore, RC-101 did not exhibit cellular toxicity to human nasal epithelia at concentrations up to 200 μM, nor did it induce a proinflammatory response in these cells. Collectively, the findings of this study identify RC-101 as a potential preventative of S. aureusnasal colonization.

Published
2011
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42. Evaluation of the Pig-Tailed Macaque (Macaca nemestrina) as a Model of Human Staphylococcus aureusNasal Carriage

Author

Cole, Amy L., Cosgrove Sweeney, Yvonne, Lasseter, Amanda G., Gray, Justin M., Beavis, Ashley C., Chong, Christine F., Hajheidari, Safarali V., Beyene, Alex, Patton, Dorothy L., and Cole, Alexander M.

Abstract

ABSTRACTStaphylococcus aureusnasal carriage is a common condition affecting both healthy and immunocompromised populations and provides a reservoir for dissemination of potentially infectious strains by casual contact. The factors regulating the onset and duration of nasal S. aureuscolonization are mostly unknown, and a human-relevant animal model is needed. Here, we screened 17 pig-tailed macaques (Macaca nemestrina) for S. aureuscarriage, and 14 of 17 animals tested positive in the nose at one or both screening sessions (8 weeks apart), while the other 3 animals were negative in the nose but positive in the pharynx at least once. As in humans, S. aureuscolonization was densest in the nose, and treatment of the nostrils with mupirocin ointment effectively cleared the nostrils and 6 extranasal body sites. Experimental nasal S. aureuscolonization was established with 104CFU/nostril, and both autologous and nonautologous strains survived over 40 days without any apparent adverse effects. A human nasal S. aureusisolate (strain D579, sequence type 398) was carried in 4 of 6 animals for over 3 weeks. Nostrils that did eradicate experimentally applied S. aureusexhibited neutrophilic innate immunity marked by elevated nasal interleukin-1β (IL-1β), IL-8, and monocyte chemotactic protein 1 levels and a 10-fold decreased IL-1 receptor antagonist/IL-1β ratio within 7 days postinoculation, analogous to the human condition. Taken together, pig-tailed macaques represent a physiological model of human S. aureusnasal carriage that may be utilized for testing natural colonization and decolonization mechanisms as well as novel classes of anti-S. aureustherapeutics.

Published
2018
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43. HIV-Enhancing Factors Are Secreted by Reproductive Epithelia upon Inoculation with Bacterial Vaginosis-Associated Bacteria.

Author

Eade CR, Diaz C, Chen S, Cole AL, and Cole AM

Subjects
Actinobacteria, Acute-Phase Proteins analysis, Acute-Phase Proteins metabolism, Cell Line, Cervix Uteri cytology, Cyclophilin A analysis, Cyclophilin A metabolism, Elafin analysis, Elafin metabolism, Female, HIV-1 pathogenicity, Humans, Immunity, Innate, Lipocalin-2, Lipocalins analysis, Lipocalins metabolism, Mucous Membrane cytology, Mucous Membrane immunology, Mucous Membrane microbiology, Proteins analysis, Proteins metabolism, Proto-Oncogene Proteins analysis, Proto-Oncogene Proteins metabolism, Up-Regulation, WAP Four-Disulfide Core Domain Protein 2, Disease Susceptibility immunology, Disease Susceptibility microbiology, Disease Susceptibility virology, HIV Infections microbiology, HIV Infections virology, Host-Pathogen Interactions immunology, Host-Pathogen Interactions physiology, Vaginosis, Bacterial immunology, Vaginosis, Bacterial microbiology, Vaginosis, Bacterial virology
Abstract

Bacterial vaginosis is a common reproductive infection in which commensal vaginal lactobacilli are displaced by a mixed population of pathogenic bacteria. Bacterial vaginosis increases susceptibility to HIV, and it has been suggested that host innate immune responses to pathogenic bacteria contribute to enhanced infection, yet the cellular mechanisms mediating the increased HIV susceptibility remain uncharacterized. We evaluated the HIV-enhancing effects of bacterial vaginosis by inoculating endocervical epithelia with Atopobium vaginae, a bacterial vaginosis-associated bacteria, and assaying secreted factors for HIV-enhancing activity. When epithelia and A. vaginae were cocultured, we observed increased HIV-enhancing activity mediated by secreted low molecular weight factors. From this complex mixture we identified several upregulated host proteins, which functioned in combination to enhance HIV infection. These studies suggest that the host immune response to bacterial vaginosis-associated bacteria results in the release of HIV-enhancing factors. The combined activity of bacterial vaginosis-induced proteins likely mediates HIV enhancement.

Published
2015
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