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論文

Cross-scale analysis of temperature compensation in the cyanobacterial circadian clock system

古池 美彦*; Ouyang, D.*; 富永 大輝*; 松尾 龍人*; 向山 厚*; 川北 至信; 藤原 悟*; 秋山 修志*

Communications Physics (Internet), 5(1), p.75_1 - 75_12, 2022/04

 被引用回数:4 パーセンタイル:65.23(Physics, Multidisciplinary)

Circadian clock proteins often reveal temperature-compensatory responses that counteract temperature influences to keep their enzymatic activities constant over a physiological range of temperature. This temperature-compensating ability at the reaction level is likely crucial for circadian clock systems, to which the clock proteins are incorporated, to achieve the system-level temperature compensation of the oscillation frequency. Nevertheless, temperature compensation is yet a puzzling phenomenon, since side chains that make up the clock proteins fluctuate more frequently due to greater thermal energy at higher temperature. Here, we investigated temperature influences on the dynamics of KaiC, a temperature-compensated enzyme (ATPase) that hydrolyzes ATP into ADP in the cyanobacterial circadian clock system, using quasielastic neutron scattering. The frequency of picosecond to subnanosecond incoherent local motions in KaiC was accelerated by a factor of only 1.2 by increasing the temperature by 10$$^{circ}$$C. This temperature insensitivity of the local motions was not necessarily unique to KaiC, but confirmed also for a series of temperature-sensitive mutants of KaiC and proteins other than clock-related proteins. Rather, the dynamics associated with the temperature-compensatory nature of the reaction- and system-level was found in global diffusional motions, which was suggested to regulate the temperature dependence of ATPase activity and dephosphorylation process presumably through changes in the hexamer conformation of KaiC. The spatiotemporal scale at which cross-scale causality of the temperature sensitivity is established is finite, and extends down to picosecond to subnanosecond dynamics only in a very limited part of KaiC, not in its entire part.

論文

モジュールにもとづくゲノム機能予測; 3Dキーノート

由良 敬; 郷 通子*

蛋白質 核酸 酵素, 47(8), p.1090 - 1096, 2002/06

全ゲノム配列が判明している生物種は70種を越えている。生物の全ゲノム配列がわかったことへの感激は急速に減り、もう普通のことになってしまった。ゲノム配列を決定する技術はここ数年ほどで格段に進んだが、ゲノムの中の情報を抽出する方法はどの程度進歩したのであろうか。4種類の塩基の羅列から生命活動における意味を抽出することができるようになって、われわれは初めてゲノムを「解読」したことになる。この重要な問題へのひとつのアプローチを紹介する。

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