Team:Oxford/why do we need microcompartments
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- | <h1>Why do we need | + | <h1>Why do we need microcompartments?</h1> |
BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES | BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES BIOREMEDIATION INTRODUCTION PLUS QUOTES | ||
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- | <h1black> | + | <h1black>Increasing the reaction rate</h1black> |
<img src="https://static.igem.org/mediawiki/2014/4/4d/Oxford_plus-sign-clip-art.png" style="float:right;position:relative; width:2%;" /> | <img src="https://static.igem.org/mediawiki/2014/4/4d/Oxford_plus-sign-clip-art.png" style="float:right;position:relative; width:2%;" /> | ||
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- | <h1white> | + | <h1white>Increasing the reaction rate</h1white> |
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- | <h1> | + | <h1>Increased concentration of metabolic enzymes</h1> |
Proteins can be targeted into microcompartments via an 18-amino acid leader sequence that forms a well-defined helical structure (Lawrence AD, 2014). We added this leader sequence to dcmA in both E. coli and P. putida. The resulting accumulation of dcmA in the microcompartments leads to an increased local concentration of the metabolic enzyme. This allows more rapid degradation of DCM, which can diffuse freely through the plasma membrane and into microcompartments. | Proteins can be targeted into microcompartments via an 18-amino acid leader sequence that forms a well-defined helical structure (Lawrence AD, 2014). We added this leader sequence to dcmA in both E. coli and P. putida. The resulting accumulation of dcmA in the microcompartments leads to an increased local concentration of the metabolic enzyme. This allows more rapid degradation of DCM, which can diffuse freely through the plasma membrane and into microcompartments. | ||
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- | <h1> | + | <h1>Preventing interference with cell metabolism</h1> |
Additionally, the products of DCM degradation are only produced within the confines of the microcompartment. This prevents HCl and formaldehyde from interfering with other metabolic processes in the cell. | Additionally, the products of DCM degradation are only produced within the confines of the microcompartment. This prevents HCl and formaldehyde from interfering with other metabolic processes in the cell. | ||
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- | <h1white> | + | <h1white>Microcompartment/rate of collision models</h1white> |
<img src="https://static.igem.org/mediawiki/2014/4/4d/Oxford_plus-sign-clip-art.png" style="float:right;position:relative; width:2%;" /> | <img src="https://static.igem.org/mediawiki/2014/4/4d/Oxford_plus-sign-clip-art.png" style="float:right;position:relative; width:2%;" /> | ||
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- | <h1white> | + | <h1white>Microcompartment/rate of collision models</h1white> |
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- | <h1black> | + | <h1black>Reduce accumulation of toxic intermediates</h1black> |
<img src="https://static.igem.org/mediawiki/2014/4/4d/Oxford_plus-sign-clip-art.png" style="float:right;position:relative; width:2%;" /> | <img src="https://static.igem.org/mediawiki/2014/4/4d/Oxford_plus-sign-clip-art.png" style="float:right;position:relative; width:2%;" /> | ||
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- | <h1white> | + | <h1white>Reducing accumulation of toxic intermediates</h1white> |
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Revision as of 08:28, 21 September 2014
#list li { list-style-image: url("https://static.igem.org/mediawiki/2014/6/6f/OxigemTick.png"); } }