A large-scale targeted proteomics assay resource based on an in vitro human proteome

Masaki Matsumoto; Fumiko Matsuzaki; Kiyotaka Oshikawa; Naoki Goshima; Masatoshi Mori; Yoshifumi Kawamura; Koji Ogawa; Eriko Fukuda; Hirokazu Nakatsumi; Tohru Natsume; Kazuhiko Fukui; Katsuhisa Horimoto; Takeshi Nagashima; Ryo Funayama; Keiko Nakayama; Keiichi I. Nakayama

doi:10.1038/nmeth.4116

A large-scale targeted proteomics assay resource based on an in vitro human proteome

Masaki Matsumoto, Fumiko Matsuzaki, Kiyotaka Oshikawa, Naoki Goshima, Masatoshi Mori, Yoshifumi Kawamura, Koji Ogawa, Eriko Fukuda, Hirokazu Nakatsumi, Tohru Natsume, Kazuhiko Fukui, Katsuhisa Horimoto, Takeshi Nagashima, Ryo Funayama, Keiko Nakayama, Keiichi I. Nakayama

MED - United Centers for Advanced Research and Translational Medicine (ART)

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

70 Citations (Scopus)

Abstract

Targeted proteomics approaches are of value for deep and accurate quantification of protein abundance. Extending such methods to quantify large numbers of proteins requires the construction of predefined targeted assays. We developed a targeted proteomics platform-in vitro proteome-assisted multiple reaction monitoring (MRM) for protein absolute quantification (iMPAQT)-by using >18,000 human recombinant proteins, thus enabling protein absolute quantification on a genome-wide scale. Our platform comprises experimentally confirmed MRM assays of mass tag (mTRAQ)-labeled peptides to allow for rapid and straightforward measurement of the absolute abundance of predefined sets of proteins by mass spectrometry. We applied iMPAQT to delineate the quantitative metabolic landscape of normal and transformed human fibroblasts. Oncogenic transformation gave rise to relatively small but global changes in metabolic pathways resulting in aerobic glycolysis (Warburg effect) and increased rates of macromolecule synthesis. iMPAQT should facilitate quantitative biology studies based on protein abundance measurements.

Original language	English
Pages (from-to)	251-258
Number of pages	8
Journal	Nature Methods
Volume	14
Issue number	3
DOIs	https://doi.org/10.1038/nmeth.4116
Publication status	Published - 2017 Feb 28

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Matsumoto, M., Matsuzaki, F., Oshikawa, K., Goshima, N., Mori, M., Kawamura, Y., Ogawa, K., Fukuda, E., Nakatsumi, H., Natsume, T., Fukui, K., Horimoto, K., Nagashima, T., Funayama, R., Nakayama, K., & Nakayama, K. I. (2017). A large-scale targeted proteomics assay resource based on an in vitro human proteome. Nature Methods, 14(3), 251-258. https://doi.org/10.1038/nmeth.4116

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abstract = "Targeted proteomics approaches are of value for deep and accurate quantification of protein abundance. Extending such methods to quantify large numbers of proteins requires the construction of predefined targeted assays. We developed a targeted proteomics platform-in vitro proteome-assisted multiple reaction monitoring (MRM) for protein absolute quantification (iMPAQT)-by using >18,000 human recombinant proteins, thus enabling protein absolute quantification on a genome-wide scale. Our platform comprises experimentally confirmed MRM assays of mass tag (mTRAQ)-labeled peptides to allow for rapid and straightforward measurement of the absolute abundance of predefined sets of proteins by mass spectrometry. We applied iMPAQT to delineate the quantitative metabolic landscape of normal and transformed human fibroblasts. Oncogenic transformation gave rise to relatively small but global changes in metabolic pathways resulting in aerobic glycolysis (Warburg effect) and increased rates of macromolecule synthesis. iMPAQT should facilitate quantitative biology studies based on protein abundance measurements.",

author = "Masaki Matsumoto and Fumiko Matsuzaki and Kiyotaka Oshikawa and Naoki Goshima and Masatoshi Mori and Yoshifumi Kawamura and Koji Ogawa and Eriko Fukuda and Hirokazu Nakatsumi and Tohru Natsume and Kazuhiko Fukui and Katsuhisa Horimoto and Takeshi Nagashima and Ryo Funayama and Keiko Nakayama and Nakayama, {Keiichi I.}",

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Matsumoto, M, Matsuzaki, F, Oshikawa, K, Goshima, N, Mori, M, Kawamura, Y, Ogawa, K, Fukuda, E, Nakatsumi, H, Natsume, T, Fukui, K, Horimoto, K, Nagashima, T, Funayama, R , Nakayama, K & Nakayama, KI 2017, 'A large-scale targeted proteomics assay resource based on an in vitro human proteome', Nature Methods, vol. 14, no. 3, pp. 251-258. https://doi.org/10.1038/nmeth.4116

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AU - Fukui, Kazuhiko

AU - Horimoto, Katsuhisa

AU - Nagashima, Takeshi

AU - Funayama, Ryo

AU - Nakayama, Keiko

AU - Nakayama, Keiichi I.

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A large-scale targeted proteomics assay resource based on an in vitro human proteome

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