白血病细胞的粘附结构及其Src家族激酶的调控。

IF 3.3 3区 生物学 Q3 CELL BIOLOGY
Cell Adhesion & Migration Pub Date : 2018-05-04 Epub Date: 2017-08-18 DOI:10.1080/19336918.2017.1344796
Pavla Röselová, Adam Obr, Aleš Holoubek, Dana Grebeňová, Kateřina Kuželová
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引用次数: 6

摘要

白血病原细胞与骨髓细胞外基质的相互作用通常导致白血病细胞免受化疗的保护,并在随后复发的基础上持续存在残余疾病。粘附信号通路在贴壁细胞和成熟造血细胞中已被广泛研究,但在正常或恶性造血干细胞和祖细胞中的粘附结构和信号通路却很少被探索。我们使用干涉反射显微镜、免疫荧光、贴壁细胞分数测量、实时微阻抗测量和活细胞成像分析白血病细胞与纤维连接蛋白(FN)的相互作用。我们发现白血病细胞形成非常动态的黏附结构,类似于早期的局灶黏附。与粘附细胞相反,Src家族激酶(SFK)属于局灶粘附动力学的重要调节因子,我们观察到SFK抑制剂达沙替尼对白血病细胞与FN结合的影响很小。SFK参与粘附结构调节的相对微弱可能与白血病细胞缺乏细胞骨架机械张力有关。另一方面,活跃的Lyn激酶被发现特异性地定位于白血病细胞的粘附结构,并且较不牢固的细胞粘附FN通常与较高的Lyn活性相关(这在用抑制剂SKI-1处理细胞后也出乎意料地发生)。因此,Lyn可能对白血病细胞中整合素相关复合物到其他过程的信号传导很重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Adhesion structures in leukemia cells and their regulation by Src family kinases.

Adhesion structures in leukemia cells and their regulation by Src family kinases.

Adhesion structures in leukemia cells and their regulation by Src family kinases.

Adhesion structures in leukemia cells and their regulation by Src family kinases.

Interaction of leukemia blasts with the bone marrow extracellular matrix often results in protection of leukemia cells from chemotherapy and in persistence of the residual disease which is on the basis of subsequent relapses. The adhesion signaling pathways have been extensively studied in adherent cells as well as in mature haematopoietic cells, but the adhesion structures and signaling in haematopoietic stem and progenitor cells, either normal or malignant, are much less explored. We analyzed the interaction of leukemia cells with fibronectin (FN) using interference reflection microscopy, immunofluorescence, measurement of adherent cell fraction, real-time microimpedance measurement and live cell imaging. We found that leukemia cells form very dynamic adhesion structures similar to early stages of focal adhesions. In contrast to adherent cells, where Src family kinases (SFK) belong to important regulators of focal adhesion dynamics, we observed only minor effects of SFK inhibitor dasatinib on leukemia cell binding to FN. The relatively weak involvement of SFK in adhesion structure regulation might be associated with the lack of cytoskeletal mechanical tension in leukemia cells. On the other hand, active Lyn kinase was found to specifically localize to leukemia cell adhesion structures and a less firm cell attachment to FN was often associated with higher Lyn activity (this unexpectedly occurred also after cell treatment with the inhibitor SKI-1). Lyn thus may be important for signaling from integrin-associated complexes to other processes in leukemia cells.

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来源期刊
CiteScore
6.40
自引率
0.00%
发文量
7
审稿时长
53 weeks
期刊介绍: Cell Adhesion & Migration is a multi-disciplinary, peer reviewed open access journal that focuses on the biological or pathological implications of cell-cell and cell-microenvironment interactions. The main focus of this journal is fundamental science. The journal strives to serve a broad readership by regularly publishing review articles covering specific disciplines within the field, and by publishing focused issues that provide an overview on specific topics of interest within the field. Cell Adhesion & Migration publishes relevant and timely original research, as well as authoritative overviews, commentaries, and perspectives, providing context for the work presented in Cell Adhesion & Migration and for key results published elsewhere. Original research papers may cover all topics important in the field of cell-cell and cell-matrix interactions. Cell Adhesion & Migration also publishes articles related to cell biomechanics, biomaterial, and development of related imaging technologies.
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