Team:BYU Provo/Team OxyR/The Beginning

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Team BYU Provo

BYU Provo
 

Contents

5 January 2011

Colon Cancer Detection Questions

Can isopeptags be used to detect a cancer biomarker and then create a response inside the cell? If not, what other transmembrane proteins can?

Heat Production

[http://openwetware.org/images/f/fd/Cold_Switch_Mechanism.jpg Diagram of proposed mechanism]

What's a good "cold switch" - a riboswitch that would stop transcription at a specific temperature?

Does the UCP1 create enough heat, fast enough, to make a difference?

Does activation of UCP1 harmfully inhibit ATP production? Or can we overproduce ATP to compensate?

CO Detection

Can E. coli be altered to survive in CO long enough to detect it?

7 January 2011

Heat Production

We discovered that the yeast heating project was originally done by an iGEM team from Valencia. If we continue with it, our original contribution would be linking it to a riboswitch, and optimizing the heating mechanism. Addison also suggested optimizing it in E. coli because they grow in denser colonies (it has already been shown not to be lethal in E. coli, but we aren't sure if it produces heat).

Furthermore, there is a better chance of E. coli heating its environment more efficiently as the UCP-1 protein would be expressed on its membrane as opposed to the mitochondrial membrane.

Pamphlet printing is cheap, and Rob volunteered to work on the graphic design.

Colon Cancer Detection

We've found that cancer cells produce more reactive oxygen species than normal cells. E. Coli already has detection systems for ROS so we could couple those detection systems with some sort of report to detect the ROS. Such as GFP for fluorescence, or banana aroma for a little added flavor.


The carbon monoxide project ...


10 January 2011

We discovered that the CO detection project was already done by an iGEM team last year.

Brainstorming:

  • Sound-sensitive bacteria using TRP channels or MSCL channel
  • Engineer Lactobascillus to add vitamins to yogurt
  • ROS sensor in E. coli to detect cancer (and/or heat sensitivity)
  • Thermogenesis in E. coli


12 January 2011

Continued Brainstorming

  • Caffeine synthesis (Starbacts :)
  • Creating a psychrophile (cold-loving) E. coli (E. skimocoli :) using phychrophilic proteins, chaperonins and UCP1
  • Pathogenic plasmid-sharing bacteria (shares lactase-encoding plasmid with other flora in gut)
  • Fabric (long bacteria that interlace ... create polymer within cell then allow to die ... when cell dies, long polymers are already interlaced)
  • Paper (decompose plant matter and create pulp that can be made into paper)
  • Sound detection (TRP proteins, MSCL + MSCS proteins in bacteria)
  • Organic nanowires
  • Electron sharing between species
  • Cell migration

We settled on Cancer detection, when all was said and done...

Colon Cancer Detection Mechanism Proposals for Continued Research

The idea is to detect various inputs and create unique reporters or levels of reporters according to inputs. To detect colon cancer we would focus on two or more of the following:

  • Unique metabolic products (Fermentation - lactic acids)
  • Reactive Oxygen Species (ROS)
  • Heat Detection (Riboswitch)
  • Collagen cutting enzymes (detect the byproducts)

Unique parts will include: ROS sensor (fine-tune those existing in nature), Riboswitch sensitive to specific temperature, and multi-input switch (creating our own).

[http://partsregistry.org/wiki/index.php?title=Part:BBa_K228258 Sample AND switch]

Pamphlet Design

Trifold Pamphlet:

  • Who we are
  • What is iGEM
  • Our Goals within iGEM
  • What we need
  • How you can help


14 January 2011

Wrote pamphlet text. See Papers section.

19 January 2011

Proofread pamphlet text and plan to take pictures on Friday. Friday afternoon, Addison and his friend will work on the layout.


Started research in earnest for colon cancer biomarkers that will be useful in our project.


[http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B6WN2-4NRMDCT-3&_user=456938&_coverDate=12%2F31%2F2007&_rdoc=1&_fmt=high&_orig=search&_origin=search&_sort=d&_docanchor=&view=c&_searchStrId=1613028817&_rerunOrigin=google&_acct=C000021830&_version=1&_urlVersion=0&_userid=456938&md5=6434a6e2cbf35e44e5540c2b1799759c&searchtype=a ROS are decreased in cancerous cells]

[http://www.ncbi.nlm.nih.gov/pubmed/1331990 ROS are increased in CRC]

ROS-sensing transcriptional regulators already in E. Coli are OxyR, SoxR, and FNR. These could potentially be used to detect different concentrations of ROS.


Biomarkers Unique to Colon Cancer

[http://en.wikipedia.org/wiki/Carcinoembryonic_antigen Carcinoembryonic antigen]

[http://cebp.aacrjournals.org/content/12/10/1095.full.pdf+html Detection of Glycoprotein 87 Using Monoclonal Antibody Adnab-9]

[http://cebp.aacrjournals.org/content/17/3/543.full.pdf+html Consistently Reported Candidate Biomarkers - Check last pages for lists of genes/proteins]

[http://www.aolnews.com/2010/03/22/scientists-find-first-ever-colon-cancer-biomarkers/ TFF3 and GDF15]


Goals for Next Few Weeks

Subjects to Study: Circuit design Directed evolution Mathematical modeling Colon cancer biology basics Other tools that will be useful.

Professors to give lectures: Dr. Clement Dr. Grose Dr. O'Neil Dr. Griffitts

21 January 2011

Assignments: Matt and Rob - ROS Transcription Factors

Addison and Chet - Riboswitches

Mark and Cameron (and Josh?) - Colon Cancer Specifics (Where are biomarkers released? Where and how does it develop, etc.)

Mackay and Julie - AND/OR Gate mechanisms [http://openwetware.org/images/9/95/AND_GateBYU.jpg AND Gate Mechanism]


GOAL: Detailed strategy and schedule within two weeks

24 January 2011

  • Can internal biomarkers be used by our E. coli if the cells die and are found in the stool?
  • What biomarkers are common to most colon cancers?
  • What are the stages of cancer development and how much do signals/biomarkers change through the stages?
  • ROS/ROM's ... do they reach the environment? What causes them? Are they a good signal?
  • Anatomy and pathophysiology of the cancer? What is a polyp? Where does it dump things out? Is a polyp made only of cancer, or is it made of mixed cells?


And Or Gate Switches

Various Gates-AND,OR,NAND,XOR,NOT Various promoters How to get best combined response from two inputs


Colon Cancer

Colon cancer begins as normal colonic epithelium which can develop into an adenomatous polyp which can further develop in to an invasive cancer polyp-abnormal growth of tissue projecting from a mucous membrane Polyps are an early warning for colon cancer. There are two types of colon cancer: 1.adenoma-pre malignant polyp 2.hyperplastic polyps-rarely forms a cancerous tumor

26 January 2011

Mathematical Modeling Example (UBC Example)

28 January 2011

Circuit Design Brainstorming

We spent the day coming up with various mechanisms to express a desired gene in the presence of ROS and heat. Once expressed properly, we would like our marker gene of choice to be expressed constitutively. Following are four proposed mechanisms. The mechanism we have decided to try is the fourth mechanism, which we have named the "SuperFlp Mechanism." Below is a diagram.

  1. Basic FLp Recombinase Mechanism: A DNA section that is transcribed normally in the presence of ROS, but there is nothing important downstream. When heated, the promoter inverts (5' to 3' as well as switching strands), leading to transcription in the opposite direction, which contains our desired marker.
  2. IRES Mechanism: The promoter on the strand is ROS activated, but the mRNA lacks a Shine Dalgarno sequence. The SD sequence will be inserted by a heat-activated internal ribosomal entry site (IRES) in the proper position to result in translation of the marker protein.
  3. Riboswitch Mechanism: The presence of ROS leads to translation of protein A. Protein A is required for translation of the desired mRNA coding for the marker. The mRNA starts with a heat-activated riboswitch flanked by LoxP sites and followed by the Cre protein. So, when activated by heat, the heat-sensitive riboswitch will be eliminated, allowing constituent translation. The Cre sequence is followed by a duplicate sequence for protein A.
  4. SuperFlp Mechanism: (Method of choice) An ROS transcription factor is followed by a riboswitch and a Flp recombinase. In the presence of both ROS and heat, the recombinase is expressed, flipping non-local promoter to the desired position. The big question is whether the Flp recombinase's work will be undone by time or the same Flp recombinase. If the recombination is permanent, the E. Coli will continue to express the desired marker even when no longer in the presence of ROS or heat.