A chemical genomics approach for understanding chemical communication

2017 Fiscal Year Annual Research Report

• Project Area: Frontier research of chemical communications
• Project/Area Number: 17H06411
• Research Institution: Institute of Physical and Chemical Research
• Principal Investigator: BOONE CHARLES 国立研究開発法人理化学研究所, 環境資源科学研究センター, チームリーダー (70601342)
• Co-Investigator(Kenkyū-buntansha): 八代田 陽子 国立研究開発法人理化学研究所, その他, 研究員 (60360658)
• Project Period (FY): 2017-06-30 – 2022-03-31
• Keywords: chemical genomics / yeast / chemical communication

Outline of Annual Research Achievements

We developed a high-throughput chemical genomics platform based on a diagnostic set of ~300 viable yeast gene deletion mutants, spanning all major biological processes, within a drug-sensitized genetic background. We also developed a highly multiplexed barcode sequencing protocol, allowing us to decipher rich chemical-genetic profiles on a large-scale. We generated profiles for ~10,000 compounds from the RIKEN Natural Product Depository (NPDepo) and other large compound collections, and, through the profile matching strategy we predicted the cellular targets at the biological process level. From FY2017, we expanded this chemical genomics platform to enable the prediction of precise essential gene targets. To do so, we developed a collection of barcoded conditional, temperature-sensitive alleles of essential genes (TS library) for chemical genomic profiling. In a complementary approach, we deleted a single copy of each essential gene in a diploid yeast (HET library) to enable drug-induced haploinsufficiency profiling (HIP). On the other hand, we started to screen drug-resistant mutants and we so far obtained ~20 mutants for several compounds. We are first approaching detailed target-compound validation by orthogonal genetic approaches. Drug-resistant mutants often identify the precise cellular target. For example, we selected spontaneous drug-resistant mutants to a RIKEN NPDepo compound. In total, we isolated drug-resistant mutants for the compound, one of which showed a nsSNP alteration in the FAS1 gene. HIP validation also suggested the compound targeted to Fas1.

Current Status of Research Progress

2: Research has progressed on the whole more than it was originally planned.

Reason

We already screened bioactive compounds from NPDepo using HET/TS library and obtained several drug resistant mutants as we planned.

Strategy for Future Research Activity

We will continuously do the following project; 1) computational analysis for screening of the HET/TS libraries; 2) identification of mutations of the drug resistant mutants. We are also planning other screening using the MoBY-ORF library and the SUP library. Furthermore, we will validate interactions between ligands and their targets using biochemical assays, for example, for a RIKEN NPDepo compound and Fas1.

Research Products

• [Int'l Joint Research] トロント大学/マギル大学/ブリティッシュコロンビア大学(カナダ)
  • Country Name: CANADA
  • Counterpart Institution: トロント大学/マギル大学/ブリティッシュコロンビア大学
• [Int'l Joint Research] ミネソタ大学(米国)
  • Country Name: U.S.A.
  • Counterpart Institution: ミネソタ大学
• [Int'l Joint Research] the National Center for Drug Screening(中国)
  • Country Name: CHINA
  • Counterpart Institution: the National Center for Drug Screening
• [Journal Article] MOSAIC: a chemical-genetic interaction data repository and web resource for exploring chemical modes of action (2018)
  • Author(s): Nelson J, Simpkins SW, Safizadeh H, Li SC, Piotrowski JS, Hirano H, Yashiroda Y, Osada H, Yoshida M, Boone C, Myers CL.
  • Journal Title: Bioinformatics Volume: 34 Pages: 1251-1252
  • DOI: 10.1093/bioinformatics/btx732
  • Peer Reviewed / Int'l Joint Research
• [Journal Article] Functional annotation of chemical libraries across diverse biological processes (2017)
  • Author(s): Piotrowski JS, et al.
  • Journal Title: Nature Chemical Biology Volume: 13 Pages: 982-993
  • DOI: 10.1038/nchembio.2436
  • Peer Reviewed / Int'l Joint Research
• [Presentation] Mapping Chemical-Genetic Interactions to Link Bioactive Compounds to Cellular Targets (2018)
  • Author(s): Charles Boone
  • Organizer: 新学術領域研究「化学コミュニケーションのフロンティア」第２回公開シンポジウム
  • Invited
• [Presentation] Mapping Genetic Networks on a Global Scale (2017)
  • Author(s): Charles Boone
  • Organizer: From Genetic Networks to a Cellular Wiring Diagram
  • Int'l Joint Research / Invited
• [Presentation] Target Identification Using an Integrated Chemical Genetic Approach (2017)
  • Author(s): Sheena Li, Charles Boone
  • Organizer: the CIFAR meeting
  • Int'l Joint Research
• [Presentation] 窒素代謝を変えるコミュニケーション- 脂肪酸をつかった分裂酵母の種の生存戦略 - (2017)
  • Author(s): 八代田陽子
  • Organizer: 第69回日本生物工学会 シンポジウム「微生物の「声」が聴きたくて… 単細胞生物のコミュニケーションスキル」
  • Invited
• [Presentation] 脂肪酸化合物を介した酵母細胞間のコミュニケーション (2017)
  • Author(s): 八代田陽子
  • Organizer: 第54回植物化学シンポジウム「ファイトバイオーム：植物化学物質による生物間コミュニケーションへの誘い」
  • Invited
• [Presentation] アミノ酸取り込みを調節する酵母細胞間相互作用 (2017)
  • Author(s): 八代田陽子
  • Organizer: 2017年度生命科学系学会合同年次大会 ワークショップ「ライフイベントを紡ぐ栄養環境への適応機構」
  • Invited
• [Book] 第10章 酵母ケミカルゲノミクスを用いた化合物作用機序解明のための大規模高速解析法（「酵母菌・麹菌・乳酸菌の産業応用展開」） (2018)
  • Author(s): 八代田陽子、吉田稔
  • Total Pages: 264
  • Publisher: シーエムシー出版
  • ISBN: 978-4-7813-1317-7
• [Remarks] 化合物の標的機能を決定するツールを開発－酵母の化学遺伝学アプローチで化合物の標的予測／同定が迅速に－
  • URL: http://www.riken.jp/pr/press/2017/20170725_1/