Literature DB >> 22494890

Engineered phage-based therapeutic materials inhibit Chlamydia trachomatis intracellular infection.

Shanta Raj Bhattarai1, So Young Yoo, Seung-Wuk Lee, Deborah Dean.   

Abstract

Developing materials that are effective against sexually transmitted pathogens such as Chlamydia trachomatis (Ct) and HIV-1 is challenging both in terms of material selection and improving bio-membrane and cellular permeability at desired mucosal sites. Here, we engineered the prokaryotic bacterial virus (M13 phage) carrying two functional peptides, integrin binding peptide (RGD) and a segment of the polymorphic membrane protein D (PmpD) from Ct, as a phage-based material that can ameliorate Ct infection. Ct is a globally prevalent human pathogen for which there are no effective vaccines or microbicides. We show that engineered phage stably express both RGD motifs and Ct peptides and traffic intracellularly and into the lumen of the inclusion in which the organism resides within the host cell. Engineered phage were able to significantly reduce Ct infection in both HeLa and primary endocervical cells compared with Ct infection alone. Polyclonal antibodies raised against PmpD and co-incubated with constructs prior to infection did not alter the course of infection, indicating that PmpD is responsible for the observed decrease in Ct infection. Our results suggest that phage-based design approaches to vector delivery that overcome mucosal cellular barriers may be effective in preventing Ct and other sexually transmitted pathogens.
Copyright © 2012 Elsevier Ltd. All rights reserved.

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Year:  2012        PMID: 22494890      PMCID: PMC3341514          DOI: 10.1016/j.biomaterials.2012.03.054

Source DB:  PubMed          Journal:  Biomaterials        ISSN: 0142-9612            Impact factor:   12.479


  58 in total

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Authors:  Deborah D Crane; John H Carlson; Elizabeth R Fischer; Patrik Bavoil; Ru-ching Hsia; Chun Tan; Cho-chou Kuo; Harlan D Caldwell
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  14 in total

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Review 3.  Antibiotic resistance in prevalent bacterial and protozoan sexually transmitted infections.

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Review 4.  Chemical modulation of M13 bacteriophage and its functional opportunities for nanomedicine.

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5.  A cancer-favoring oncolytic vaccinia virus shows enhanced suppression of stem-cell like colon cancer.

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6.  Identification of proteins differentially expressed by Chlamydia trachomatis treated with chlamydiaphage capsid protein VP1 during intracellular growth.

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7.  Bioinspired M-13 bacteriophage-based photonic nose for differential cell recognition.

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Review 10.  Immunocontraception: Filamentous Bacteriophage as a Platform for Vaccine Development.

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