Team:Chiba/Project

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==Our project==
==Our project==
[[Image:Image time manager chiba.jpg|frame|right|'''Fig.''' Our system]]
[[Image:Image time manager chiba.jpg|frame|right|'''Fig.''' Our system]]
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あるスレッショルド超えるまでの時間を遅くして、発現を遅らせる。
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常に一定の割合で蓄積されるとき、あるスレッショルド超えるまでの時間を遅くする
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遅くする方法には、蓄積するときの割合を変える。
 +
スレッショルド自体を変える
 +
この二つが挙げられる。

Revision as of 04:40, 26 October 2008

Chiba-U.gif

Home The Team The Project Parts Submitted to the Registry Reference Notebook Acknowledgements


Contents

Abstract

Fig.1 Project desgin
"Team : Chiba - E.coli time manager"

  We control the timing of gene expression by using multiple signaling devices.To this end,we utilize molecules associated with Quorum sensing, a phenomenon that allows bacteria to communicate with each other.Our project uses two classes of bacteria: senders and receivers. Senders produce signaling molecules, and Receivers are activated only after a particular concentration of this molecule is reached.Although different quorum sensing species have slightly different signaling molecules, these molecules are not completely specific to their hosts and cross-species reactivity is observed [http://www3.interscience.wiley.com/journal/119124142/abstract (1)],[http://partsregistry.org/Part:BBa_F2620:Specificity (2)]. Communication using non-endogenous molecules is less sensitive, and requires a higher signal concentration to take effect.This results in slower activation of receivers.

Introduction

Fig.2 Team logo








Our project

Fig. Our system

常に一定の割合で蓄積されるとき、あるスレッショルド超えるまでの時間を遅くする

遅くする方法には、蓄積するときの割合を変える。

スレッショルド自体を変える

この二つが挙げられる。







System design

Our project uses two classes of bacteria: senders and receivers.Senders produce signaling molecules, and receivers are activated only after a particular concentration of this molecule is reached.The communication using non-endogenous molecules is less sensitive,and it requires higher signal concentration to take effect.This results in slower activation of receivers.

About Quorum Sensing

Fig.3 Constructed circuit of Quorum sensing(Vibrio fischeri model).

  Quorum sensing is a cell-to-cell signaling action of bacteria. They detect the cell density of the same species and coordinate the expression behavior of their cells. Species of Gram-Negative signaling transfer molecules (so-called autoinducer) is a series of acyl homoserine lactone (AHL). The signals are synthesized from S-adenosylmethionine(SAM) by a synthase protein(LuxI-type proteins) and once they have reached a threshold concentration,they bound to a transcriptional regulatory protein(LuxR-type proteins) to induce expression of target genes.

More about Quorum Sensing

  • [http://parts.mit.edu/registry/index.php/Featured_Parts:Cell-Cell-Signaling Cell-Cell-Signaling]
  • [http://www.che.caltech.edu/groups/fha/quorum.html About Quorum sensing]

Controlling the time of a cell-to-cell signaling action

Communication using non-endogenous molecules is less sensitive, and requires a higher signal concentration to take effect.This results in slower activation of receivers.

Sender

Fig.4 AHL varieties

 English:Each species has their own LuxI-type proteins,which synthesize their specific autoinducers,AHLs.AHLs produced by different LuxI-type proteins differ only in the length of the acyl-chain moiety and substitution at position C-3.Vibrio fischeri has LuxI,which synthesize 3OC6HSL.Pseudomonas aeruginosa has RhlI and LasI,which synthesize C4HSL、C6HSL,respectively.LuxR,which is original for Vibrio fischeri,is activated by its cognate autoinducer,3OC6HSL.However,LuxR is also activated by non-endogenous molecules,C4HSL,C6HSL,and 3OC12HSL.Activation by non-endogenous molecules requires a higher signal concentration[http://partsregistry.org/Part:BBa_F2620:Specificity (2)].This results in slower activation of receivers,when AHL concentration is increasing.

日本語:異なる生物はそれぞれに異なるLuxIタイプのタンパク質を持ち、アシル鎖の長さ、あるいはC-3位の置換基が異なる種類のAHLを合成する。Vibrio fischeriはLuxIにより3OC6HSLを、Pseudomonas aeruginosaはRhlIにより、C4HSL、C6HSLを、LasIにより3OC12HSLを合成する(Fig.4).AHLを受け取り応答するLuxRタンパク質はVibrio fischeri由来であり、低濃度の3OC6HSLに対して(~5nM)、応答する。しかし、他種生物由来のAHLに対しても応答することが知られており、より高い濃度のAHLが必要となる[http://partsregistry.org/Part:BBa_F2620:Specificity (2)].AHLがゆっくり溜まっていく時、LuxRは3OC6HSLに対して最も早く応答し、他のAHLに対してはそれよりも遅く応答する。

(冨永)

Sender experiments detail

Receiver

English:

日本語:AHLを合成するSenderだけではなく、AHLを受け取る側のReceiverを変えれば、その応答時間を変えることができる。そこで私たちは、以下のいくつかの方法を考えた。

  1. 一種類のSender(AHL<--LuxI)に対して、由来生物の異なるレシーバタンパク質でそれを受信する.
  2. レシーバータンパク質であるLuxRに変異を入れることで、AHLに対する応答感度を上下させること.
  3. レシーバーのコピーナンバーを変える.
  4. AiiAによるAHL分解を同時に起こすことで、AHL供給速度を遅くする.

(福冨、小林)


  • Quorum-Sensing Cross-talk
Table.1 LuxR family gene Data modified from Fekete et.al. Anal Bioanal Chem (2007)

English:

日本語:

  • LuxR/Plux mutants show
  1. a greater response to 3OC6HSL[http://authors.library.caltech.edu/5553/ (3)]
  2. a increase in sensitivity to 3OC12HSL[http://mic.sgmjournals.org/cgi/content/abstract/151/11/3589 (4)].


Receiver experiments detail

AiiA

  • AHL reporter with aiiA
Express LuxR and aiiA constantly. AiiA degrades AHL as signaling molecule. Express GFP when the AHL concentration exceed the capacity of aiiA.
This enables the delay of the activation time of receiver.


AiiA experiments detail

Demo Experiments

実験内容とdataかるく

Demo experiments detail

Conclusion

けつろん

Future Work

references

  1. [http://www3.interscience.wiley.com/journal/119124142/abstract M.K Winson et al.:Construction and analysis of luxCDABE-based plasmid sensors for investigating N-acyl homoserine lactone-mediated quorum sensing.FEMS Microbiology Letters 163 (1998) 185-192]
  2. [http://partsregistry.org/Part:BBa_F2620:Specificity BBa_F2620:Specificity]
  3. [http://authors.library.caltech.edu/5553/ C. H. Collins.et al.:Directed evolution of Vibrio fischeri LuxR for increased sensitivity to a broad spectrum of acyl-homoserine lactones.Mol.Microbiol.2005.55(3).712–723]
  4. [http://mic.sgmjournals.org/cgi/content/abstract/151/11/3589 B. Koch. et al.:The LuxR receptor: the sites of interaction with quorum-sensing signals and inhibitors.Microbiology 151 (2005),3589-3602]
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