Rational design of an orthogonal pair of bimolecular rnase p ribozymes through heterologous assembly of their modular domains

Yuri Nozawa; Megumi Hagihara; Md Sohanur Rahman; Shigeyoshi Matsumura; Yoshiya Ikawa

doi:10.3390/biology8030065

Rational design of an orthogonal pair of bimolecular rnase p ribozymes through heterologous assembly of their modular domains

Yuri Nozawa, Megumi Hagihara, Md Sohanur Rahman, Shigeyoshi Matsumura, Yoshiya Ikawa^*

^*この論文の責任著者

化学科

研究成果: ジャーナルへの寄稿 › 学術論文 › 査読

4 被引用数 (Scopus)

抄録

The modular structural domains of multidomain RNA enzymes can often be dissected into separate domain RNAs and their noncovalent assembly can often reconstitute active enzymes. These properties are important to understand their basic characteristics and are useful for their application to RNA-based nanostructures. Bimolecular forms of bacterial RNase P ribozymes consisting of S-domain and C-domain RNAs are attractive as platforms for catalytic RNA nanostructures, but their S-domain/C-domain assembly was not optimized for this purpose. Through analysis and engineering of bimolecular forms of the two bacterial RNase P ribozymes, we constructed a chimeric ribozyme with improved catalytic ability and S-domain/C-domain assembly and developed a pair of bimolecular RNase P ribozymes the assembly of which was considerably orthogonal to each other.

本文言語	英語
論文番号	65
ジャーナル	Biology
巻	8
号	3
DOI	https://doi.org/10.3390/biology8030065
出版ステータス	出版済み - 2019/09

ASJC Scopus 主題領域

生化学、遺伝学、分子生物学一般
免疫学および微生物学一般
農業および生物科学一般

文献へのアクセス

10.3390/biology8030065

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引用スタイル

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author = "Yuri Nozawa and Megumi Hagihara and Rahman, {Md Sohanur} and Shigeyoshi Matsumura and Yoshiya Ikawa",

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AU - Rahman, Md Sohanur

AU - Matsumura, Shigeyoshi

AU - Ikawa, Yoshiya

PY - 2019/9

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N2 - The modular structural domains of multidomain RNA enzymes can often be dissected into separate domain RNAs and their noncovalent assembly can often reconstitute active enzymes. These properties are important to understand their basic characteristics and are useful for their application to RNA-based nanostructures. Bimolecular forms of bacterial RNase P ribozymes consisting of S-domain and C-domain RNAs are attractive as platforms for catalytic RNA nanostructures, but their S-domain/C-domain assembly was not optimized for this purpose. Through analysis and engineering of bimolecular forms of the two bacterial RNase P ribozymes, we constructed a chimeric ribozyme with improved catalytic ability and S-domain/C-domain assembly and developed a pair of bimolecular RNase P ribozymes the assembly of which was considerably orthogonal to each other.

AB - The modular structural domains of multidomain RNA enzymes can often be dissected into separate domain RNAs and their noncovalent assembly can often reconstitute active enzymes. These properties are important to understand their basic characteristics and are useful for their application to RNA-based nanostructures. Bimolecular forms of bacterial RNase P ribozymes consisting of S-domain and C-domain RNAs are attractive as platforms for catalytic RNA nanostructures, but their S-domain/C-domain assembly was not optimized for this purpose. Through analysis and engineering of bimolecular forms of the two bacterial RNase P ribozymes, we constructed a chimeric ribozyme with improved catalytic ability and S-domain/C-domain assembly and developed a pair of bimolecular RNase P ribozymes the assembly of which was considerably orthogonal to each other.

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