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人骨髓来源祖细胞成骨分化过程中量子点偶联整合素的膜动力学改变

Altered membrane dynamics of quantum dot-conjugated integrins during osteogenic differentiation of human bone marrow derived progenitor cells.

作者信息

Chen Hongfeng, Titushkin Igor, Stroscio Michael, Cho Michael

机构信息

Department of Bioengineering, University of Illinois, Chicago, Illinois 60607, USA.

出版信息

Biophys J. 2007 Feb 15;92(4):1399-408. doi: 10.1529/biophysj.106.094896. Epub 2006 Nov 17.

Abstract

Functionalized quantum dots offer several advantages for tracking the motion of individual molecules on the cell surface, including selective binding, precise optical identification of cell surface molecules, and detailed examination of the molecular motion without photobleaching. We have used quantum dots conjugated with integrin antibodies and performed studies to quantitatively demonstrate changes in the integrin dynamics during osteogenic differentiation of human bone marrow derived progenitor cells (BMPCs). Consistent with the unusually strong BMPC adhesion previously observed, integrins on the surface of undifferentiated BMPC were found in clusters and the lateral diffusion was slow (e.g., approximately 10(-11) cm2/s). At times as early as those after a 3-day incubation in the osteogenic differentiation media, the integrin diffusion coefficients increased by an order of magnitude, and the integrin dynamics became indistinguishable from that measured on the surface of terminally differentiated human osteoblasts. Furthermore, microfilaments in BMPCs consisted of atypically thick bundles of stress fibers that were responsible for restricting the integrin lateral mobility. Studies using laser optical tweezers showed that, unlike fully differentiated osteoblasts, the BMPC cytoskeleton is weakly associated with its cell membrane. Based on these findings, it appears likely that the altered integrin dynamics is correlated with BMPC differentiation and that the integrin lateral mobility is restricted by direct links to microfilaments.

摘要

功能化量子点在追踪单个分子在细胞表面的运动方面具有多种优势,包括选择性结合、对细胞表面分子进行精确的光学识别,以及在不发生光漂白的情况下对分子运动进行详细检测。我们使用了与整合素抗体偶联的量子点,并进行了研究以定量证明人骨髓来源祖细胞(BMPC)成骨分化过程中整合素动力学的变化。与先前观察到的BMPC异常强的黏附力一致,未分化的BMPC表面的整合素呈簇状分布,侧向扩散缓慢(例如,约为10^(-11) cm2/s)。早在成骨分化培养基中培养3天后,整合素扩散系数就增加了一个数量级,并且整合素动力学变得与在终末分化的人成骨细胞表面测得的动力学无法区分。此外,BMPC中的微丝由异常粗大的应力纤维束组成,这些应力纤维束负责限制整合素的侧向移动性。使用激光光镊进行的研究表明,与完全分化的成骨细胞不同,BMPC细胞骨架与其细胞膜的关联较弱。基于这些发现,整合素动力学的改变似乎与BMPC分化相关,并且整合素的侧向移动性受到与微丝直接连接的限制。

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