IGEM:Harvard/2006/DNA nanostructures: Difference between revisions
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==Working Team Members== | ==Working Team Members== | ||
*[[User:TChan|Tiffany Chan]] ([[User_talk:TChan|talk]]) | *[[User:TChan|Tiffany Chan]] ([[User_talk:TChan|talk]], [[Special:Contributions&target=TChan|edits]]) | ||
*[[User:Kfifer|Katherine Fifer]] ([[User_talk:Kfifer|talk]]) | *[[User:Kfifer|Katherine Fifer]] ([[User_talk:Kfifer|talk]], [[Special:Contributions&target=Kfifer|edits]]) | ||
*[[User:Vlau|Valerie Lau]] ([[User_talk:Vlau|talk]]) | *[[User:Vlau|Valerie Lau]] ([[User_talk:Vlau|talk]], [[Special:Contributions&target=Vlau|edits]]) | ||
*[[User:Matthewmeisel|Matthew Meisel]] ([[User_talk:Matthewmeisel|talk]]) | *[[User:Matthewmeisel|Matthew Meisel]] ([[User_talk:Matthewmeisel|talk]], [[Special:Contributions&target=Matthewmeisel|edits]]) |
Revision as of 12:26, 11 July 2006
Project Overview
- Our goal is to to design and implement molecular containers, which can be dynamically opened and closed by an external stimulus.
- The containers will be implemented as DNA nanostructures, which afford a significant degree of positional control and chemical versatility.
- As an initial proof-of-concept, we plan to use our DNA containers to demonstrate controllable activation ("delivery") of anti-thrombin aptamers.
- We expect that molecular containers could have several interesting scientific and clinical applications, such as
- Drug and gene delivery
- Bio-marker scavenging (early detection of biomarkers)
- Directed evolution (compartmentalized selections)
- Using multiplexing for combinatorial chemical synthesis
- Capture and stabilization of multiprotein complexes
- Protein folding (chaperones)
- Cell sorting
Working Team Members
- Tiffany Chan (talk, edits)
- Katherine Fifer (talk, edits)
- Valerie Lau (talk, edits)
- Matthew Meisel (talk, edits)