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2018 Fiscal Year Final Research Report

Genome-wide screen-based identification of non-selective hypertonicity-induced cation channel

Research Project

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Project/Area Number 17K15086
Research Category

Grant-in-Aid for Young Scientists (B)

Allocation TypeMulti-year Fund
Research Field Functional biochemistry
Research InstitutionThe University of Tokyo

Principal Investigator

Watanabe Kengo  東京大学, 大学院薬学系研究科(薬学部), 特任助教 (20781727)

Research Collaborator MORISHITA Kazuhiro  
Project Period (FY) 2017-04-01 – 2019-03-31
Keywords高浸透圧ストレス / HICC / ゲノムワイドsiRNAスクリーニング / ASK3
Outline of Final Research Achievements

Similar to slugs poured salt on, cells shrink when the concentration of extracellular solution becomes higher than that of intracellular solution, which is called as hyperosmotic stress. If this goes on, cells die; therefore, cells recover their volume to survive. To achieve cell volume recovery, cells firstly have to recognize the state under hyperosmotic stress. It is said that the protein passing ions, called HICC, is the cellular sensor for hyperosmotic stress; however, the molecular identity of HICC remains unclear. In this study, the scientist investigated about 20,000 proteins coded on the human genome one by one to identify the components of HICC. Although he could not surely identify it during this period, he successfully obtained the candidate protein and important knowledge establishing a foothold to further researches.

Free Research Field

生化学・分子生物学・細胞生物学

Academic Significance and Societal Importance of the Research Achievements

液体と接している細胞は常に浸透圧ストレスに晒されるリスクがあり,浸透圧ストレスに適切に応答する仕組みは細胞が生存する上で必須の基本的なシステムの1つである.さらに細胞はこのシステムを浸透圧ストレスに対抗する時だけでなく,分裂や移動する時など体積を変化させる細胞機能時にも利用すると言われている.つまり,このシステムの異常が高血圧やがん,炎症などの疾患に関わっている可能性がある.本研究はシステムを始動させるセンサー部分に着目したものであり,本成果を足掛かりにシステムの全貌解明に向けてさらに研究を発展させることで,様々な疾患に対する創薬基盤・治療戦略の開発に資することが期待される.

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Published: 2020-03-30  

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