Team:USTC-China/project/motion

From 2014.igem.org

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           <h4 id="dgrab">DgrA/B</h4>
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           <h4 id="dgrab"><i>DgrA/B</i></h4>
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           <p>The concentration of c-di-GMP is varying, and for our experiment we will promote its expression to inhibit rotation of flagella. It will bind to DgrA and DgrB. The resulting complex will have two routes to go: one is the [c-di-GMP&amp;DgrA] complex which will inhibit FliL, a protein bound to the membrane playing a key role in rotation of flagella. And the other route is that the DgrB will directly affect the rotation of the flagella.</p>
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           <p>The concentration of <i>c-di-GMP</i> is varying, and for our experiment we will promote its expression to inhibit rotation of flagella. It will bind to <i>DgrA</i> and <i>DgrB</i>. The resulting complex will have two routes to go: one is the [<i>c-di-GMP&amp</i>;<i>DgrA</i>] complex which will inhibit <i>FliL</i>, a protein bound to the membrane playing a key role in rotation of flagella. And the other route is that the <i>DgrB</i> will directly affect the rotation of the flagella.</p>
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           <h4 id="hf">HfiA/HfsJ</h4>
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           <h4 id="hf"><i>HfiA/HfsJ</i></h4>
           <p>Ref: A Cell Cycle and Nutritional Checkpoint Controlling Bacterial Surface Adhesion</p>
           <p>Ref: A Cell Cycle and Nutritional Checkpoint Controlling Bacterial Surface Adhesion</p>
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           <p>In this paper, author describes a novel regulatory mechanism by which the C.c. bacterium integrates cell cycle and nutritional signals to control development of an adhesive envelop structure known as holdfast.</p>
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           <p>In this paper, author describes a novel regulatory mechanism by which the <i>C.c.</i> bacterium integrates cell cycle and nutritional signals to control development of an adhesive envelop structure known as holdfast.</p>
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           <p>They discovered a novel inhibitor of holdfast development. HfiA, that is regulated downstream of lovK-lovR. They also discovered a bio-synthesis related gene named HfsJ. And the suppressing mutations in HfsJ attenuate the HfsJ-HfiA interaction.</p>
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           <p>They discovered a novel inhibitor of holdfast development. HfiA, that is regulated downstream of lovK-lovR. They also discovered a bio-synthesis related gene named <i>HfsJ</i>. And the suppressing mutations in HfsJ attenuate the <i>HfsJ-HfiA</i> interaction.</p>
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           <p>These results support a model in which HfiA inhibits holdfast development via direct interaction with an enzyme required for holdfast biosynthesis</p>
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           <p>These results support a model in which <i>HfiA</i> inhibits holdfast development via direct interaction with an enzyme required for holdfast biosynthesis</p>
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           <p>In conclusion, author says: We demonstrate that the predicted glycosyltransferase, HfsJ, is a required component of the holdfast development machinery and that residues at the C-terminus of HsfJ mediate a direct interaction with HfiA, leading to a post-translational inhibition of HfsJ.</p>
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           <p>In conclusion, author says: We demonstrate that the predicted glycosyltransferase, <i>HfsJ</i>, is a required component of the holdfast development machinery and that residues at the C-terminus of <i>HsfJ</i> mediate a direct interaction with <i>HfiA</i>, leading to a post-translational inhibition of <i>HfsJ</i>.</p>
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Revision as of 12:35, 17 October 2014

Our Project

DgrA/B

The concentration of c-di-GMP is varying, and for our experiment we will promote its expression to inhibit rotation of flagella. It will bind to DgrA and DgrB. The resulting complex will have two routes to go: one is the [c-di-GMP&amp;DgrA] complex which will inhibit FliL, a protein bound to the membrane playing a key role in rotation of flagella. And the other route is that the DgrB will directly affect the rotation of the flagella.

HfiA/HfsJ

Ref: A Cell Cycle and Nutritional Checkpoint Controlling Bacterial Surface Adhesion

In this paper, author describes a novel regulatory mechanism by which the C.c. bacterium integrates cell cycle and nutritional signals to control development of an adhesive envelop structure known as holdfast.

They discovered a novel inhibitor of holdfast development. HfiA, that is regulated downstream of lovK-lovR. They also discovered a bio-synthesis related gene named HfsJ. And the suppressing mutations in HfsJ attenuate the HfsJ-HfiA interaction.

These results support a model in which HfiA inhibits holdfast development via direct interaction with an enzyme required for holdfast biosynthesis

In conclusion, author says: We demonstrate that the predicted glycosyltransferase, HfsJ, is a required component of the holdfast development machinery and that residues at the C-terminus of HsfJ mediate a direct interaction with HfiA, leading to a post-translational inhibition of HfsJ.

Lots of thanks to our sponsors, who help us to achieve what we have today

© 2014 USTC-iGEM Design. Distributed under BY-SA 3.0

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