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Cell surface conjugation of sialyl Lewis X induces a rolling response for mesenchymal stem cells

机译:唾液酸化的路易斯X的细胞表面结合诱导间充质干细胞的滚动反应

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There has been significant interest in the clinical use of adult mesenchymal stem cells (MSCs), which are connective tissue progenitor cells. One of the greatest challenges in traditional stem cell therapy is to deliver a large quantity of viable stem cells with high engraftment efficiency. MSCs home at a low efficiency due to the lack of relevant adhesion molecules on their surface. We have engineered the surface of the MSCs with the sialyl Lewisx (SLeX) moiety, found on the surfaces of leukocytes representing the active site of the P-selectin glycoprotein ligand (PSGL-1) for inducing rolling response as the first step in the homing process which involves reversible, adhesive interactions between glycoprotein receptors on specific circulating cells and ligands expressed on the surface of the vascular endothelium. MSCs were covalently modified SLeX through biotin-streptavidin linkage and the rolling response of the modified MSCs were examined on P-selectin surface. Modified MSCs exhibited velocities of 2 mum/sec whereas the unmodified MSCs exhibited velocities of 65 mum/sec at a wall shear stress of 0.366 dynes/cm2 on P-selectin surface in a parallel plate flow chamber assay. Most importantly, the MSCs' native phenotype including its ability to proliferate and differentiate into multi-lineages was retained after the modification. This platform strategy demonstrates the potential to target MSCs to specific tissues within the body by conjugation of specific targeting ligands.
机译:成人间充质干细胞(MSCs)是结缔组织祖细胞的临床应用引起了人们的极大兴趣。传统干细胞疗法的最大挑战之一是以高植入效率递送大量活细胞。由于其表面上缺乏相关的粘附分子,因此MSC的归巢效率较低。我们用唾液酸化的Lewis x (SLeX)部分工程化了MSC的表面,该部分在代表P-选择蛋白糖蛋白配体(PSGL-1)活性位点的白细胞表面上被发现以诱导滚动作为归巢过程的第一步,它涉及特定循环细胞上糖蛋白受体与血管内皮表面表达的配体之间可逆的粘附相互作用。通过生物素-链霉亲和素键对MSC进行共价修饰的SLeX,并在P-选择蛋白表面上检测了修饰的MSC的滚动反应。在平行板流动室测定中,修饰的MSC在P-选择素表面的壁切应力为0.366达因/ cm 2 时的速度为2 mum / sec,而未修饰的MSC的速度为65 mm / sec。 。最重要的是,修饰后保留了MSC的天然表型,包括其增殖和分化成多谱系的能力。该平台策略证明了通过结合特异性靶向配体将MSC靶向体内特定组织的潜力。

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