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淋巴细胞功能相关抗原-1的I结构域介导聚苯乙烯颗粒在流动状态下于细胞间黏附分子-1上滚动。

I-domain of lymphocyte function-associated antigen-1 mediates rolling of polystyrene particles on ICAM-1 under flow.

作者信息

Eniola A Omolola, Krasik Ellen F, Smith Lee A, Song Gang, Hammer Daniel A

机构信息

Department of Chemical and Biomolecular Engineering, Institute for Medicine and Engineering, University of Pennsylvania, 3320 Smith Walk, Philadelphia, PA 19104, USA.

出版信息

Biophys J. 2005 Nov;89(5):3577-88. doi: 10.1529/biophysj.104.057729. Epub 2005 Aug 12.

Abstract

In their active state, beta(2)-integrins, such as LFA-1, mediate the firm arrest of leukocytes by binding intercellular adhesion molecules (ICAMs) expressed on endothelium. Although the primary function of LFA-1 is assumed to be the ability to mediate firm adhesion, recent work has shown that LFA-1 can contribute to cell tethering and rolling under hydrodynamic flow, a role previously largely attributed to the selectins. The inserted (I) domain of LFA-1 has recently been crystallized in the wild-type (wt) and locked-open conformations and has been shown to, respectively, support rolling and firm adhesion under flow when expressed in alpha(L)beta(2) heterodimers or as isolated domains on cells. Here, we report results from cell-free adhesion assays where wt I-domain-coated polystyrene particles were allowed to interact with ICAM-1-coated surfaces in shear flow. We show that wt I-domain can independently mediate the capture of particles from flow and support their rolling on ICAM-1 surfaces in a manner similar to how carbohydrate-selectin interactions mediate rolling. Adhesion is specific and blocked by appropriate antibodies. We also show that the rolling velocity of I-domain-coated particles depends on the wall shear stress in flow chamber, I-domain site density on microsphere surfaces, and ICAM-1 site density on substrate surfaces. Furthermore, we show that rolling is less sensitive to wall shear stress and ICAM-1 substrate density at high density of I-domain on the microsphere surface. Computer simulations using adhesive dynamics can recreate bead rolling dynamics and show that the mechanochemical properties of ICAM-1-I-domain interactions are similar to those of carbohydrate-selectin interactions. Understanding the biophysics of adhesion mediated by the I-domain of LFA-1 can elucidate the complex roles this integrin plays in leukocyte adhesion in inflammation.

摘要

在其激活状态下,β₂整合素(如淋巴细胞功能相关抗原-1,LFA-1)通过结合内皮细胞上表达的细胞间黏附分子(ICAMs)介导白细胞的牢固黏附。尽管LFA-1的主要功能被认为是介导牢固黏附的能力,但最近的研究表明,LFA-1在流体动力学流动下可促进细胞的 tethering 和滚动,这一作用以前主要归因于选择素。LFA-1的插入(I)结构域最近已结晶为野生型(wt)和锁定开放构象,并且当在α(L)β₂异二聚体中表达或作为细胞上的分离结构域时,分别显示在流动下支持滚动和牢固黏附。在这里,我们报告了无细胞黏附试验的结果,其中wt I结构域包被的聚苯乙烯颗粒在剪切流中与ICAM-1包被的表面相互作用。我们表明,wt I结构域可以独立介导颗粒从流动中的捕获,并以类似于碳水化合物-选择素相互作用介导滚动的方式支持它们在ICAM-1表面上的滚动。黏附是特异性的,并被适当的抗体阻断。我们还表明,I结构域包被的颗粒的滚动速度取决于流动室中的壁面剪应力、微球表面上I结构域位点密度以及底物表面上ICAM-1位点密度。此外,我们表明,在微球表面上I结构域高密度时,滚动对壁面剪应力和ICAM-1底物密度不太敏感。使用黏附动力学的计算机模拟可以重现珠子滚动动力学,并表明ICAM-1-I结构域相互作用的机械化学性质与碳水化合物-选择素相互作用的相似。了解由LFA-1的I结构域介导的黏附生物物理学可以阐明这种整合素在炎症中白细胞黏附中所起的复杂作用。

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