Literature DB >> 17685517

Efforts toward expansion of the genetic alphabet: structure and replication of unnatural base pairs.

Shigeo Matsuda1, Jeremiah D Fillo, Allison A Henry, Priyamrada Rai, Steven J Wilkens, Tammy J Dwyer, Bernhard H Geierstanger, David E Wemmer, Peter G Schultz, Glen Spraggon, Floyd E Romesberg.   

Abstract

Expansion of the genetic alphabet has been a long-time goal of chemical biology. A third DNA base pair that is stable and replicable would have a great number of practical applications and would also lay the foundation for a semisynthetic organism. We have reported that DNA base pairs formed between deoxyribonucleotides with large aromatic, predominantly hydrophobic nucleobase analogues, such as propynylisocarbostyril (dPICS), are stable and efficiently synthesized by DNA polymerases. However, once incorporated into the primer, these analogues inhibit continued primer elongation. More recently, we have found that DNA base pairs formed between nucleobase analogues that have minimal aromatic surface area in addition to little or no hydrogen-bonding potential, such as 3-fluorobenzene (d3FB), are synthesized and extended by DNA polymerases with greatly increased efficiency. Here we show that the rate of synthesis and extension of the self-pair formed between two d3FB analogues is sufficient for in vitro DNA replication. To better understand the origins of efficient replication, we examined the structure of DNA duplexes containing either the d3FB or dPICS self-pairs. We find that the large aromatic rings of dPICS pair in an intercalative manner within duplex DNA, while the d3FB nucleobases interact in an edge-on manner, much closer in structure to natural base pairs. We also synthesized duplexes containing the 5-methyl-substituted derivatives of d3FB (d5Me3FB) paired opposite d3FB or the unsubstituted analogue (dBEN). In all, the data suggest that the structure, electrostatics, and dynamics can all contribute to the extension of unnatural primer termini. The results also help explain the replication properties of many previously examined unnatural base pairs and should help design unnatural base pairs that are better replicated.

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Year:  2007        PMID: 17685517      PMCID: PMC2536688          DOI: 10.1021/ja072276d

Source DB:  PubMed          Journal:  J Am Chem Soc        ISSN: 0002-7863            Impact factor:   15.419


  40 in total

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Review 3.  Beyond A, C, G and T: augmenting nature's alphabet.

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4.  An unnatural hydrophobic base pair with shape complementarity between pyrrole-2-carbaldehyde and 9-methylimidazo[(4,5)-b]pyridine.

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5.  3DNA: a software package for the analysis, rebuilding and visualization of three-dimensional nucleic acid structures.

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6.  Integrity of duplex structures without hydrogen bonding: DNA with pyrene paired at abasic sites.

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7.  A stable DNA duplex containing a non-hydrogen-bonding and non-shape-complementary base couple: interstrand stacking as the stability determining factor.

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8.  DNA with hydrophobic base substitutes: a stable, zipperlike recognition motif based on interstrand-stacking interactions.

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9.  A specific partner for abasic damage in DNA.

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10.  Facile polymerization of dNTPs bearing unnatural base analogues by DNA polymerase alpha and Klenow fragment (DNA polymerase I).

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  25 in total

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3.  Polymerase amplification, cloning, and gene expression of benzo-homologous "yDNA" base pairs.

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Review 5.  New insights into Hoogsteen base pairs in DNA duplexes from a structure-based survey.

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6.  Site-specific labeling of DNA and RNA using an efficiently replicated and transcribed class of unnatural base pairs.

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7.  Structural insights into DNA replication without hydrogen bonds.

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Review 8.  The expanding world of DNA and RNA.

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9.  Discovery, characterization, and optimization of an unnatural base pair for expansion of the genetic alphabet.

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10.  The effects of unnatural base pairs and mispairs on DNA duplex stability and solvation.

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