Direct observation of catch bonds involving cell-adhesion molecules

被引:0
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作者
Bryan T. Marshall
Mian Long
James W. Piper
Tadayuki Yago
Rodger P. McEver
Cheng Zhu
机构
[1] Woodruff School of Mechanical Engineering,Coulter School of Biomedical Engineering
[2] Georgia Institute of Technology,Cardiovascular Biology Research Program, Oklahoma Medical Research Foundation
[3] Georgia Institute of Technology,Department of Biochemistry and Molecular Biology and Oklahoma Center for Medical Glycobiology
[4] University of Oklahoma Health Sciences Center,National Microgravity Laboratory, Institute of Mechanics
[5] University of Oklahoma Health Sciences Center,undefined
[6] Chinese Academy of Sciences,undefined
[7] Immucor,undefined
[8] Inc.,undefined
来源
Nature | 2003年 / 423卷
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摘要
Bonds between adhesion molecules are often mechanically stressed. A striking example is the tensile force applied to selectin–ligand bonds, which mediate the tethering and rolling of flowing leukocytes on vascular surfaces1,2,3. It has been suggested that force could either shorten bond lifetimes, because work done by the force could lower the energy barrier between the bound and free states4 (‘slip’), or prolong bond lifetimes by deforming the molecules such that they lock more tightly5,6 (‘catch’). Whereas slip bonds have been widely observed7,8,9,10,11,12,13,14, catch bonds have not been demonstrated experimentally. Here, using atomic force microscopy and flow-chamber experiments, we show that increasing force first prolonged and then shortened the lifetimes of P-selectin complexes with P-selectin glycoprotein ligand-1, revealing both catch and slip bond behaviour. Transitions between catch and slip bonds might explain why leukocyte rolling on selectins first increases and then decreases as wall shear stress increases9,15,16. This dual response to force provides a mechanism for regulating cell adhesion under conditions of variable mechanical stress.
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页码:190 / 193
页数:3
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