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肌动球蛋白马达热激活的成像

Imaging of thermal activation of actomyosin motors.

作者信息

Kato H, Nishizaka T, Iga T, Kinosita K, Ishiwata S

机构信息

Central Research Laboratory, Hitachi Ltd., Hatoyama, Saitama 350-0395, Japan.

出版信息

Proc Natl Acad Sci U S A. 1999 Aug 17;96(17):9602-6. doi: 10.1073/pnas.96.17.9602.

Abstract

We have developed temperature-pulse microscopy in which the temperature of a microscopic sample is raised reversibly in a square-wave fashion with rise and fall times of several ms, and locally in a region of approximately 10 micrometers in diameter with a temperature gradient up to 2 degrees C/micrometers. Temperature distribution was imaged pixel by pixel by image processing of the fluorescence intensity of rhodamine phalloidin attached to (single) actin filaments. With short pulses, actomyosin motors could be activated above physiological temperatures (higher than 60 degrees C at the peak) before thermally induced protein damage began to occur. When a sliding actin filament was heated to 40-45 degrees C, the sliding velocity reached 30 micrometers/s at 25 mM KCl and 50 micrometers/s at 50 mM KCl, the highest velocities reported for skeletal myosin in usual in vitro assay systems. Both the sliding velocity and force increased by an order of magnitude when heated from 18 degrees C to 40-45 degrees C. Temperature-pulse microscopy is expected to be useful for studies of biomolecules and cells requiring temporal and/or spatial thermal modulation.

摘要

我们开发了温度脉冲显微镜技术,在该技术中,微观样品的温度以方波形式可逆升高,上升和下降时间为几毫秒,且在直径约10微米的区域内局部升高,温度梯度高达2摄氏度/微米。通过对附着在(单根)肌动蛋白丝上的罗丹明鬼笔环肽荧光强度进行图像处理,逐像素成像温度分布。使用短脉冲时,在热诱导蛋白质损伤开始发生之前,肌动球蛋白马达可在高于生理温度(峰值时高于60摄氏度)的情况下被激活。当滑动的肌动蛋白丝加热到40 - 45摄氏度时,在25 mM KCl条件下滑动速度达到30微米/秒,在50 mM KCl条件下达到50微米/秒,这是常规体外检测系统中骨骼肌肌球蛋白报道的最高速度。当从18摄氏度加热到40 - 45摄氏度时,滑动速度和力都增加了一个数量级。温度脉冲显微镜技术有望用于需要时间和/或空间热调制的生物分子和细胞研究。

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Imaging of thermal activation of actomyosin motors.肌动球蛋白马达热激活的成像
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