Team:HKUST-Hong Kong/Expectation

From 2012.igem.org

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           <p>Through assembly of the target binding  module, anti-tumor drug synthesis module and regulatory module, we would to introduce our genetically engineered <i>Bacillus subtilis</i>, B. hercules, as an anti-colon-tumor agent to provide direct tumoricidal effect during cancer therapy. It is applied as<u> oral medicine</u> which retains viability through digestive tract and executes anti-tumor activity when and only when it is  binding to colon cancer cell. </p>
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<p>Driven by pVeg constitutive promoter,  RPMrel, the colon-tumor specific peptide will be displayed on the cell wall of  B. hercules under the facilitation of LytC cell wall displaying system before it is orally intake. When B. Hercules is taken orally by patient, it is expected to reach colon after <strong>8 hours</strong> without retaining or colonizing in gastrointestinal tract. However, once it reaches colon, it will be held up around colon tumor cells and colonize around them, waiting for signal to produce anti-tumor molecule, BMP2 to the local environment. <br />
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           <p>Through assembly of the target binding  module, anti-tumor drug synthesis module and regulatory module, we would like to introduce our genetically engineered <i>Bacillus subtilis</i>, B. hercules, as an anti-colon-tumor agent to provide direct tumoricidal effect during cancer therapy. It is applied as an oral medicine which retains viability through gastrointestinal tract and executes anti-tumor activity when and only when it binds to colon cancer cell. </p>
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   Since the expression of BMP2 is controlled by xylose inducible promoter and no xylose is present in colon, xylose is taken orally or injected from anus to induce the  production of BMP2 when B. Hercules has successfully localized around colon tumor. The locally concentrated BMP2 is expected to suppress colon tumor grow and trigger the apoptosis of tumor while the low level BMP2 in colon introduces as little adverse effect as possible to normal colon tissues. <br />
+
<p>Driven by pVeg constitutive promoter,  RPMrel, the colon-tumor specific peptide will be displayed on the cell wall of  B. hercules under the facilitation of LytC cell wall displaying system before it is orally taken. When B. Hercules is taken orally by the patient, it is expected to reach colon in <strong>8 hours</strong> without retaining or colonizing in gastrointestinal tract. However, once it reaches colon, it will attach to colon tumor cells and colonize around them, waiting for signals to trigger the production and release of anti-tumor molecule, BMP2 to the local environment. <br />
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   When  BMP2 is intensively produced under the inducing from xylose, controlling by the same promoter, the expression of toxin ydcE will overwhelm the protection threshold from antitoxin ydcD. The overexpression of toxin with BMP2 production is to cause the suicide of B. hurcules and prevent any adverse effect from BMP overdose.</p>
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   Since the expression of BMP2 is controlled by xylose inducible promoter and no xylose is present in colon, xylose is taken orally or injected from anus to induce the  production of BMP2 when B. Hercules has successfully localized around colon tumor. The locally concentrated BMP2 is expected to suppress colon tumor growth and trigger the apoptosis of tumor while the low level BMP2 in non-tumor colon area introduces as little adverse effect as possible to normal colon tissues. <br />
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   Driven by the same promoter that regulates BMP2, autotoxin-encoding gene ydcE is simutaneously expressed and will gradually overwhelm the protection machinery by antitoxin ydcD. The overexpression of the autotoxin with BMP2 production will eventually cause the apoptosis of B. hurcules and prevent any adverse effect from BMP overdose.</p>
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Revision as of 17:46, 24 September 2012

Team:HKUST-Hong Kong - 2012.igem.org

EXPECTATION

Through assembly of the target binding module, anti-tumor drug synthesis module and regulatory module, we would like to introduce our genetically engineered Bacillus subtilis, B. hercules, as an anti-colon-tumor agent to provide direct tumoricidal effect during cancer therapy. It is applied as an oral medicine which retains viability through gastrointestinal tract and executes anti-tumor activity when and only when it binds to colon cancer cell.

Driven by pVeg constitutive promoter, RPMrel, the colon-tumor specific peptide will be displayed on the cell wall of B. hercules under the facilitation of LytC cell wall displaying system before it is orally taken. When B. Hercules is taken orally by the patient, it is expected to reach colon in 8 hours without retaining or colonizing in gastrointestinal tract. However, once it reaches colon, it will attach to colon tumor cells and colonize around them, waiting for signals to trigger the production and release of anti-tumor molecule, BMP2 to the local environment.
Since the expression of BMP2 is controlled by xylose inducible promoter and no xylose is present in colon, xylose is taken orally or injected from anus to induce the production of BMP2 when B. Hercules has successfully localized around colon tumor. The locally concentrated BMP2 is expected to suppress colon tumor growth and trigger the apoptosis of tumor while the low level BMP2 in non-tumor colon area introduces as little adverse effect as possible to normal colon tissues.
Driven by the same promoter that regulates BMP2, autotoxin-encoding gene ydcE is simutaneously expressed and will gradually overwhelm the protection machinery by antitoxin ydcD. The overexpression of the autotoxin with BMP2 production will eventually cause the apoptosis of B. hurcules and prevent any adverse effect from BMP overdose.