Construction of integrated gene logic-chip

Takeya Masubuchi; Masayuki Endo; Ryo Iizuka; Ayaka Iguchi; Dong Hyun Yoon; Tetsushi Sekiguchi; Hao Qi; Ryosuke Iinuma; Yuya Miyazono; Shuichi Shoji; Takashi Funatsu; Hiroshi Sugiyama; Yoshie Harada; Takuya Ueda; Hisashi Tadakuma

doi:10.1038/s41565-018-0202-3

Construction of integrated gene logic-chip

Takeya Masubuchi, Masayuki Endo, Ryo Iizuka, Ayaka Iguchi, Dong Hyun Yoon, Tetsushi Sekiguchi, Hao Qi, Ryosuke Iinuma, Yuya Miyazono, Shuichi Shoji, Takashi Funatsu, Hiroshi Sugiyama, Yoshie Harada, Takuya Ueda^*, Hisashi Tadakuma

^*Corresponding author for this work

Research output: Contribution to journal › Letter › peer-review

28 Citations (Scopus)

Abstract

In synthetic biology, the control of gene expression requires a multistep processing of biological signals. The key steps are sensing the environment, computing information and outputting products¹. To achieve such functions, the laborious, combinational networking of enzymes and substrate-genes is required, and to resolve problems, sophisticated design automation tools have been introduced². However, the complexity of genetic circuits remains low because it is difficult to completely avoid crosstalk between the circuits. Here, we have made an orthogonal self-contained device by integrating an actuator and sensors onto a DNA origami-based nanochip that contains an enzyme, T7 RNA polymerase (RNAP) and multiple target-gene substrates. This gene nanochip orthogonally transcribes its own genes, and the nano-layout ability of DNA origami allows us to rationally design gene expression levels by controlling the intermolecular distances between the enzyme and the target genes. We further integrated reprogrammable logic gates so that the nanochip responds to water-in-oil droplets and computes their small RNA (miRNA) profiles, which demonstrates that the nanochip can function as a gene logic-chip. Our approach to component integration on a nanochip may provide a basis for large-scale, integrated genetic circuits.

Original language	English
Pages (from-to)	933-940
Number of pages	8
Journal	Nature Nanotechnology
Volume	13
Issue number	10
DOIs	https://doi.org/10.1038/s41565-018-0202-3
Publication status	Published - 2018 Oct 1

ASJC Scopus subject areas

Bioengineering
Atomic and Molecular Physics, and Optics
Biomedical Engineering
Materials Science(all)
Condensed Matter Physics
Electrical and Electronic Engineering

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10.1038/s41565-018-0202-3

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@article{a43cfa250cf34264af143eda9b30d222,

title = "Construction of integrated gene logic-chip",

abstract = "In synthetic biology, the control of gene expression requires a multistep processing of biological signals. The key steps are sensing the environment, computing information and outputting products1. To achieve such functions, the laborious, combinational networking of enzymes and substrate-genes is required, and to resolve problems, sophisticated design automation tools have been introduced2. However, the complexity of genetic circuits remains low because it is difficult to completely avoid crosstalk between the circuits. Here, we have made an orthogonal self-contained device by integrating an actuator and sensors onto a DNA origami-based nanochip that contains an enzyme, T7 RNA polymerase (RNAP) and multiple target-gene substrates. This gene nanochip orthogonally transcribes its own genes, and the nano-layout ability of DNA origami allows us to rationally design gene expression levels by controlling the intermolecular distances between the enzyme and the target genes. We further integrated reprogrammable logic gates so that the nanochip responds to water-in-oil droplets and computes their small RNA (miRNA) profiles, which demonstrates that the nanochip can function as a gene logic-chip. Our approach to component integration on a nanochip may provide a basis for large-scale, integrated genetic circuits.",

author = "Takeya Masubuchi and Masayuki Endo and Ryo Iizuka and Ayaka Iguchi and Yoon, {Dong Hyun} and Tetsushi Sekiguchi and Hao Qi and Ryosuke Iinuma and Yuya Miyazono and Shuichi Shoji and Takashi Funatsu and Hiroshi Sugiyama and Yoshie Harada and Takuya Ueda and Hisashi Tadakuma",

note = "Funding Information: The authors thank RIBM for AFM imaging, T. Sakurai, H. Okada and K. Nakamura (The University of Tokyo) for help with construction of the microfluidics system, and Y. Tomari and members of the Tomari Laboratory for providing comments on the miRNA studies and on this manuscript. The authors also thank Y. Hatano (Osaka University) and M. Hagiya (The University of Tokyo) for their comments on logic circuits, and I. Kawamata (Tohoku University) for comments on the kinetically based simulation of logic circuit. This work was partially supported by Grants-in-Aid for Scientific Research on Innovative Areas ({\textquoteleft}Molecular Robotics{\textquoteright} to H.T. and M.E., nos. 15H00798 and 24104002; {\textquoteleft}Non-coding RNA Neo-taxonomy{\textquoteright} to H.T., no. 26113007), a Grant-in-Aid for Young Scientists (A), a Grant-in-Aid for Scientific Research (B) and a Grant-in-Aid for Challenging Exploratory Research (to H.T., nos. 24687018, 16KT0068 and 15K14485), Grants-in-Aid for Scientific Research (S) (to Y.H., no. 26220602) and (A) (to S.S., no. 16H02349), Grants-in-Aid for Young Scientists (B) (to R.I., no. 15K18668) from the Japan Ministry of Education, Culture, Sports, Science and Technology, Research Fellowships for Young Scientists (to T.M., no. 15J08491), Core-to-Core Program, A, Advanced Research Networks (Phototheranostics) (to R.I.) from the Japan Society for the Promotion of Science, CREST (to Y.H., no. JPMJCR1333), the Centre of Innovation (COI) Program (to T.F.) from the Japan Science and Technology Agency, the Cooperative Research Program of the Institute for Protein Research, Osaka University (CRa-18-01, to H.T and M.E.), the Asahi Glass Foundation, Futaba Electronics Memorial Foundation, and Hamaguchi Foundation for the Advancement of Biochemistry (to H.T.), and Futaba Electronics Memorial Foundation Scholarship (to T.M.). Publisher Copyright: {\textcopyright} 2018, The Author(s).",

year = "2018",

month = oct,

day = "1",

doi = "10.1038/s41565-018-0202-3",

language = "English",

volume = "13",

pages = "933--940",

journal = "Nature Nanotechnology",

issn = "1748-3387",

publisher = "Nature Publishing Group",

number = "10",

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T1 - Construction of integrated gene logic-chip

AU - Masubuchi, Takeya

AU - Endo, Masayuki

AU - Iizuka, Ryo

AU - Iguchi, Ayaka

AU - Yoon, Dong Hyun

AU - Sekiguchi, Tetsushi

AU - Qi, Hao

AU - Iinuma, Ryosuke

AU - Miyazono, Yuya

AU - Shoji, Shuichi

AU - Funatsu, Takashi

AU - Sugiyama, Hiroshi

AU - Harada, Yoshie

AU - Ueda, Takuya

AU - Tadakuma, Hisashi

N1 - Funding Information: The authors thank RIBM for AFM imaging, T. Sakurai, H. Okada and K. Nakamura (The University of Tokyo) for help with construction of the microfluidics system, and Y. Tomari and members of the Tomari Laboratory for providing comments on the miRNA studies and on this manuscript. The authors also thank Y. Hatano (Osaka University) and M. Hagiya (The University of Tokyo) for their comments on logic circuits, and I. Kawamata (Tohoku University) for comments on the kinetically based simulation of logic circuit. This work was partially supported by Grants-in-Aid for Scientific Research on Innovative Areas (‘Molecular Robotics’ to H.T. and M.E., nos. 15H00798 and 24104002; ‘Non-coding RNA Neo-taxonomy’ to H.T., no. 26113007), a Grant-in-Aid for Young Scientists (A), a Grant-in-Aid for Scientific Research (B) and a Grant-in-Aid for Challenging Exploratory Research (to H.T., nos. 24687018, 16KT0068 and 15K14485), Grants-in-Aid for Scientific Research (S) (to Y.H., no. 26220602) and (A) (to S.S., no. 16H02349), Grants-in-Aid for Young Scientists (B) (to R.I., no. 15K18668) from the Japan Ministry of Education, Culture, Sports, Science and Technology, Research Fellowships for Young Scientists (to T.M., no. 15J08491), Core-to-Core Program, A, Advanced Research Networks (Phototheranostics) (to R.I.) from the Japan Society for the Promotion of Science, CREST (to Y.H., no. JPMJCR1333), the Centre of Innovation (COI) Program (to T.F.) from the Japan Science and Technology Agency, the Cooperative Research Program of the Institute for Protein Research, Osaka University (CRa-18-01, to H.T and M.E.), the Asahi Glass Foundation, Futaba Electronics Memorial Foundation, and Hamaguchi Foundation for the Advancement of Biochemistry (to H.T.), and Futaba Electronics Memorial Foundation Scholarship (to T.M.). Publisher Copyright: © 2018, The Author(s).

PY - 2018/10/1

Y1 - 2018/10/1

N2 - In synthetic biology, the control of gene expression requires a multistep processing of biological signals. The key steps are sensing the environment, computing information and outputting products1. To achieve such functions, the laborious, combinational networking of enzymes and substrate-genes is required, and to resolve problems, sophisticated design automation tools have been introduced2. However, the complexity of genetic circuits remains low because it is difficult to completely avoid crosstalk between the circuits. Here, we have made an orthogonal self-contained device by integrating an actuator and sensors onto a DNA origami-based nanochip that contains an enzyme, T7 RNA polymerase (RNAP) and multiple target-gene substrates. This gene nanochip orthogonally transcribes its own genes, and the nano-layout ability of DNA origami allows us to rationally design gene expression levels by controlling the intermolecular distances between the enzyme and the target genes. We further integrated reprogrammable logic gates so that the nanochip responds to water-in-oil droplets and computes their small RNA (miRNA) profiles, which demonstrates that the nanochip can function as a gene logic-chip. Our approach to component integration on a nanochip may provide a basis for large-scale, integrated genetic circuits.

AB - In synthetic biology, the control of gene expression requires a multistep processing of biological signals. The key steps are sensing the environment, computing information and outputting products1. To achieve such functions, the laborious, combinational networking of enzymes and substrate-genes is required, and to resolve problems, sophisticated design automation tools have been introduced2. However, the complexity of genetic circuits remains low because it is difficult to completely avoid crosstalk between the circuits. Here, we have made an orthogonal self-contained device by integrating an actuator and sensors onto a DNA origami-based nanochip that contains an enzyme, T7 RNA polymerase (RNAP) and multiple target-gene substrates. This gene nanochip orthogonally transcribes its own genes, and the nano-layout ability of DNA origami allows us to rationally design gene expression levels by controlling the intermolecular distances between the enzyme and the target genes. We further integrated reprogrammable logic gates so that the nanochip responds to water-in-oil droplets and computes their small RNA (miRNA) profiles, which demonstrates that the nanochip can function as a gene logic-chip. Our approach to component integration on a nanochip may provide a basis for large-scale, integrated genetic circuits.

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VL - 13

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JO - Nature Nanotechnology

JF - Nature Nanotechnology

IS - 10

ER -

Construction of integrated gene logic-chip

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