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논문 기본 정보

자료유형
학술저널
저자정보
Sawyer, Eric M. (Department of Biology, Davidson College) Barta, Cody (Department of Biology, Missouri Western State University) Clemente, Romina (Department of Biology, Davidson College) Conn, Michel (Department of Biology, Missouri Western State University) Davis, Clif (Department of Biology, Missouri Western State University) Doyle, Catherine (Department of Biology, Davidson College) Gearing, Mary (Department of Biology, Davidson College) Ho-Shing, Olivia (Department of Biology, Davidson College) Mooney, Alyndria (Department of Biology, Davidson College) Morton, Jerrad (Department of Biology, Missouri Western State University) Punjabi, Shamita (Department of Biology, Davidson College) Schnoor, Ashley (Department of Computer Science, Math and Physics, Missouri Western State University) Sun, Siya (Department of Computer Science, Math and Physics, Missouri Western State University) Suresh, Shashank (Department of Mathematics, Davidson College) Szczepanik, Bryce (Department of Biology, Missouri Western State University) Taylor, D. Leland (Department of Biology, Davidson College) Temmink, Annie (Department of Mathematics, Davidson College) Vernon, William (Department of Biology, Missouri Western State University) Campbell, A. Malcolm (Department of Biology, Davidson College) Heyer, Laurie J. (Depa) Poet, Jeffrey L. Eckdahl, Todd T.
저널정보
한국생물정보시스템생물학회 Interdisciplinary Bio Central Interdisciplinary Bio Central 제4권 제3호
발행연도
2012.1
수록면
101 - 1,012 (912page)

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Introduction: We investigated frameshift suppressor tRNAs previously reported to use five-base anticodon-codon interactions in order to provide a collection of frameshift suppressor tRNAs to the synthetic biology community and to develop modular frameshift suppressor logic devices for use in synthetic biology applications. Results and Discussion: We adapted eleven previously described frameshift suppressor tRNAs to the BioBrick cloning format, and built three genetic logic circuits to detect frameshift suppression. The three circuits employed three different mechanisms: direct frameshift suppression of reporter gene mutations, frameshift suppression leading to positive feedback via quorum sensing, and enzymatic amplification of frameshift suppression signals. In the course of testing frameshift suppressor logic, we uncovered unexpected behavior in the frameshift suppressor tRNAs. The results led us to posit a four-base binding hypothesis for the frameshift suppressor tRNA interactions with mRNA as an alternative to the published five-base binding model. Conclusion and Prospects: The published five-base anticodon/codon rule explained only 17 of the 58 frameshift suppression experiments we conducted. Our deduced four-base binding rule successfully explained 56 out of our 58 frameshift suppression results. In the process of applying biological knowledge about frameshift suppressor tRNAs to the engineering application of frameshift suppressor logic, we discovered new biological knowledge. This knowledge leads to a redesign of the original engineering application and encourages new ones. Our study reinforces the concept that synthetic biology is often a winding path from science to engineering and back again; scientific investigations spark engineering applications, the implementation of which suggests new scientific investigations.

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