Team:NJU NJUT China/project

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Revision as of 16:31, 25 August 2013

 

Poject Introduction

basic information

    Most of the bacteria and archaea acquire virus resistance by integrating short viral nucleotide acid fragments into the clusters of regularly interspaced short palindromic repeats (CRISPRs). And CRISPR-based defense system can also protects them against the invading DNA and/or RNA elements. It is believed that the integrated CRISPR sequences have the ability to form a genetic memory which prevents the host from being infected. The CRISPRs and Cas (CRISPR-associated) interact and form this prokaryotic adaptive immune system.

;  A CRISPR array consists of the palindromic repeating sequences of typically 30bp that are interspaced by similar-sized acquired spacer sequences. The CRISPR loci are generally flanked bu an AT-rich leader sequence which contains promoter and the binding sites for regulatory proteins.

There three highly diverse CRISPR/Ca types exist, and major structural and functional differences are displayed in their mode of generating resistance against the invading DNA and/or RNA elements.

We focus on the type I-E CRISPR/Cas system from the model bacterium Escberichia coli k12 w3110 whose CRISPR loci has been identified so that we can download the essential sequence from NCBI(http://www.ncbi.nlm.nih.gov/nuccore/85674274?report=graph).

The mechanism of all CRISPR/Cas systems is divided into three stages: adaption, expression, and interference. At the adaption stage, the host cell acquires the resistance by integration of a new spacer sequence into a CRISPR loci. During the expression stage, cas genes are transcribed and translated. At the same time, CRISPRs are transcribed into pre-crRNAs (precursor CRISPR RNAs), and a Cas6 homolog in

Type I cleave it subsequently.

At the interference stage, the complex formed by the Cas proteins and the maturecrRNA cleave the complementary invading nucleic acids.


Project ...

This is IGEM_TEST 参考文献


 

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