Your search keyword '"Uotani, Yuuki"' showing total 2 results

1. Recognition of the base pair-mimic nucleosides by DNA polymerases.

Author

Nakano S, Uotani Y, Sato Y, Oka H, Uenishi K, Fujii M, and Sugimoto N

Subjects

Adenosine chemistry, Base Pairing, Cytosine chemistry, DNA biosynthesis, DNA Polymerase I metabolism, Templates, Genetic, Adenosine analogs & derivatives, Cytosine analogs & derivatives, DNA chemistry, DNA-Directed DNA Polymerase metabolism, Phenylurea Compounds chemistry

Abstract

We previously reported that the deoxyadenosine derivative tethering the phenyl group at the N6 position of deoxyadenosine, A(phe) stacked efficiently with the adjacent nucleotide bases at a DNA duplex terminus and in the middle of a DNA duplex. In contrast with the observations for A(phe), this study revealed that the phenyl group of the deoxycytidine derivative, C(phe) located outside the helix and allowed the base pair formation with guanine in a DNA duplex, although its phenyl group could stack with the adjacent DNA bases as efficient as A(phe). Klenow fragment of DNA polymerase I and T7 DNA polymerase selectively incorporated dTTP and dGTP opposite A(phe) and C(phe) in the template DNA, respectively, implying that the conformation of A(phe) differs between in the DNA polymerase and in solution.

Published

2006

2. Site-selective RNA cleavage by DNA bearing a base pair-mimic nucleoside.

Author

Nakano S, Uotani Y, Uenishi K, Fujii M, and Sugimoto N

Subjects

Adenosine chemistry, Base Pairing, Base Sequence, Biomimetic Materials chemistry, Biomimetic Materials metabolism, DNA metabolism, Deoxyadenosines metabolism, Nucleic Acid Heteroduplexes chemistry, Nucleic Acid Heteroduplexes metabolism, Phenylurea Compounds chemical synthesis, RNA metabolism, Substrate Specificity, Adenosine analogs & derivatives, DNA chemistry, Deoxyadenosines chemistry, Phenylurea Compounds chemistry, RNA chemistry

Abstract

We have synthesized the deoxyadenosine derivative tethering a phenyl group (X), which mimics the Watson-Crick A/T base pair. The RNA/DNA hybrid duplexes containing X in the middle of the DNA sequence showed a similar thermal stability regardless of the ribonucleotide species (A, G, C, or U) opposite to X, probably because of the phenyl group stacking inside of the duplex accompanied by the opposite ribonucleotide base flipped in an extrahelical position. The RNA strand hybridized with the DNA strand bearing X was cleaved on the 3'-side of the ribonucleotide opposite to X in the presence of MgCl2, and the RNA sequence to be cleaved was not restricted. The site-specific RNA hydrolysis suggests that the DNA strand bearing X has the advantage of the site-selective base flipping in the target sequence and the development of a "universal deoxyribozyme" to exclusively cleave a target RNA sequence.

Published

2005