Difference between revisions of "Part:BBa K1351043"
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== Background == | == Background == | ||
− | '''The sdp-System of B. subtilis''' consists of two operons: The ''sdpABC'' operon, coding for the production and secretion of the cannibalism toxin SDP and the ''sdpRI'' operon responsible for the regulation and production of the immunity protein SdpI (Fig. 1). | + | '''The sdp-System of B. subtilis''' consists of three two operons: The ''sdpABC'' operon, coding for the production and secretion of the cannibalism toxin SDP and the ''sdpRI'' operon responsible for the regulation and production of the immunity protein SdpI (Fig. 1). |
[[File:LMU14 suicide background Fig.1.png|thumb|800px|center|Fig. 1. Gene organization for the sdpABC sdpRI operons. The hairpin symbolizes thetranscriptional terminators. [1]]] | [[File:LMU14 suicide background Fig.1.png|thumb|800px|center|Fig. 1. Gene organization for the sdpABC sdpRI operons. The hairpin symbolizes thetranscriptional terminators. [1]]] |
Revision as of 00:11, 28 October 2014
Canibalism toxin SDP of B. subtilis
Background
The sdp-System of B. subtilis consists of three two operons: The sdpABC operon, coding for the production and secretion of the cannibalism toxin SDP and the sdpRI operon responsible for the regulation and production of the immunity protein SdpI (Fig. 1).
In vegetative cells, both operons are repressed by the unstable AbrB regulator. However, during early stages of sporulation AbrB itself is repressed by the master regulator of sporulation Spo0A, making sdpABC and sdpRI accessible for RNA polymerase. [1]
The sdpABC Operon – Production and Secretion of the Cannibalism Toxin SDP
The production of the Cannibalism Toxin SDP is a multi-step process. The sdpC sequence encodes the Pro-SdpC1-203,,which is translated by the ribosome.It is a precursor peptide which needs to be processed by a signal peptidases and the two membrane proteins SdpA and SdpB to become functional. This active form of SDP is a 42-amino-acid antimicrobial peptide (AMP) containing a disulfide bond between two cysteine residues located at the N-terminus.(Fig. 2). [2]]
SDP has been shown to be a very effective AMP against a variety of Gram-positive bacteria in the Phylum of the Firmicutes (Fig. 3). It rapidly collapses the proton motive force (PMF), thus inducing autolysis. [3]
Sources
[1] Gonzalez-Pastor, J. E. (2011). "Cannibalism: a social behavior in sporulating Bacillus subtilis." FEMS Microbiol Rev 35(3): 415-424.
[2] Perez Morales, T. G., et al. (2013). "Production of the cannibalism toxin SDP is a multistep process that requires SdpA and SdpB." J Bacteriol 195(14): 3244-3251.
[3] Lamsa, A., et al. (2012). "The Bacillus subtilis cannibalism toxin SDP collapses the proton motive force and induces autolysis." Mol Microbiol 84(3): 486-500.
Design
Production of the toxin SDP and the immunity protein SdpI
By the activation of the QS-dependent promoter PQS, BaKillus produces the Cannibalism Toxin SDP (Fig. 1A). For evaluation purposes we cloned the sdpABC operon under the control of inducable xylose promoter Pxyl (Fig. 1B) into a ∆sdpAB and a ∆sdpC mutant strain of B. subtilis W168. The construct was then tested by spot-on-lawn assays on B. subtilis W168 and B. subtilis W168 ∆sdpI mutant lawns.
Results
SdpC is a functional BioBrick and Spot-on-lawn assays shown that an overproduction under a xylose promoter leads to killing of Streptococcus pneumoniae.
Sequence and Features
- 10COMPATIBLE WITH RFC[10]
- 12COMPATIBLE WITH RFC[12]
- 21COMPATIBLE WITH RFC[21]
- 23COMPATIBLE WITH RFC[23]
- 25INCOMPATIBLE WITH RFC[25]Illegal AgeI site found at 759
- 1000INCOMPATIBLE WITH RFC[1000]Illegal BsaI.rc site found at 746