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不仅仅是一个标志物:人类造血干/祖细胞上的CD34与CD44共同主导血管选择素结合。

Not just a marker: CD34 on human hematopoietic stem/progenitor cells dominates vascular selectin binding along with CD44.

作者信息

AbuSamra Dina B, Aleisa Fajr A, Al-Amoodi Asma S, Jalal Ahmed Heba M, Chin Chee Jia, Abuelela Ayman F, Bergam Ptissam, Sougrat Rachid, Merzaban Jasmeen S

机构信息

Cell Migration and Signaling Laboratory, Division of Biological and Environmental Sciences and Engineering, and.

Imaging and Characterization Core Facility, King Abdullah University of Science and Technology, Thuwal, Saudi Arabia.

出版信息

Blood Adv. 2017 Dec 26;1(27):2799-2816. doi: 10.1182/bloodadvances.2017004317.

Abstract

CD34 is routinely used to identify and isolate human hematopoietic stem/progenitor cells (HSPCs) for use clinically in bone marrow transplantation, but its function on these cells remains elusive. Glycoprotein ligands on HSPCs help guide their migration to specialized microvascular beds in the bone marrow that express vascular selectins (E- and P-selectin). Here, we show that HSPC-enriched fractions from human hematopoietic tissue expressing CD34 (CD34) bound selectins, whereas those lacking CD34 (CD34) did not. An unbiased proteomics screen identified potential glycoprotein ligands on CD34 cells revealing CD34 itself as a major vascular selectin ligand. Biochemical and CD34 knockdown analyses highlight a key role for CD34 in the first prerequisite step of cell migration, suggesting that it is not just a marker on these cells. Our results also entice future potential strategies to investigate the glycoforms of CD34 that discriminate normal HSPCs from leukemic cells and to manipulate CD34 HSPC-enriched bone marrow or cord blood populations as a source of stem cells for clinical use.

摘要

CD34通常用于识别和分离人类造血干/祖细胞(HSPCs),以便在骨髓移植中临床应用,但其在这些细胞上的功能仍不清楚。HSPCs上的糖蛋白配体有助于引导它们迁移到骨髓中表达血管选择素(E-选择素和P-选择素)的特殊微血管床。在这里,我们表明,来自表达CD34的人类造血组织的富含HSPC的部分(CD34)与选择素结合,而缺乏CD34的部分(CD34)则不结合。一项无偏向性蛋白质组学筛选确定了CD34细胞上潜在的糖蛋白配体,揭示CD34本身是主要的血管选择素配体。生化分析和CD34敲低分析突出了CD34在细胞迁移的第一个先决步骤中的关键作用,表明它不仅仅是这些细胞上的一个标志物。我们的结果还引发了未来潜在的策略,以研究区分正常HSPCs与白血病细胞的CD34糖型,并操纵富含CD34 HSPC的骨髓或脐带血群体作为临床使用的干细胞来源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d349/5745127/1f36e28dd402/advances004317absf1.jpg

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