Difference between revisions of "Team:Nottingham/Project"

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        <h2>Description</h2>
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        CDI (C. difficile introduction, what the disease is, current treatments, antibiotic resistance)
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        Phage and phage therapy
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        Project description
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                        Antibiotics serve a critical role in remedying bacterial infections, however a major disadvantage to their use is the non-specificity of broad spectrum antibiotics that drastically kills off beneficial bacteria reducing the diversity of the gut flora. The use of antibiotics allows opportunistic pathogens like <i>Clostridium difficile</i> to take advantage of the dysbiosis caused. </p><p>
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A consequence of antibiotic misuse and the capability of bacteria to readily adapt to versatile conditions, has allowed antibiotic resistance in bacteria to become a major dilemma. Each year in the United States alone 2 million people are subject to infection from antibiotic resistant bacteria. Phage therapy is an alternative to antibiotics. The goal of our project was to engineer a bacteriophage which will infect C. difficile and express genetic constructs designed to suppress toxin production. We will pursue two strategies to achieve this; asRNA and dCAS-9, both of which will target the toxin genes tcdB and tcdA. Ultimately, we aim to produce a phage therapy which will reduce toxigenicity of resident strains of C. difficile without significantly affecting the native gastrointestinal microbiota.</p>
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<h2>Project description</h2>
 
<h2>Project description</h2>
 
<h3>What is ClostridiumdTOX?</h3>
 
<h3>What is ClostridiumdTOX?</h3>
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                         <a href="#dCas9" class="ui button">More information</a>
 
                         <a href="#dCas9" class="ui button">More information</a>
 
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<h2>Abstract</h2>
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                        Antibiotics serve a critical role in remedying bacterial infections, however a major disadvantage to their use is the non-specificity of broad spectrum antibiotics that drastically kills off beneficial bacteria reducing the diversity of the gut flora. The use of antibiotics allows opportunistic pathogens like <i>Clostridium difficile</i> to take advantage of the dysbiosis caused. </p><p>
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A consequence of antibiotic misuse and the capability of bacteria to readily adapt to versatile conditions, has allowed antibiotic resistance in bacteria to become a major dilemma. Each year in the United States alone 2 million people are subject to infection from antibiotic resistant bacteria. Phage therapy is an alternative to antibiotics. The goal of our project was to engineer a bacteriophage which will infect C. difficile and express genetic constructs designed to suppress toxin production. We will pursue two strategies to achieve this; asRNA and dCAS-9, both of which will target the toxin genes tcdB and tcdA. Ultimately, we aim to produce a phage therapy which will reduce toxigenicity of resident strains of C. difficile without significantly affecting the native gastrointestinal microbiota.</p>
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Revision as of 19:27, 16 October 2018

Clostridium dTox Project Human Practices Public Engagement Lab Modelling Collaborations Achievements Team Attributions