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经功能修饰的治疗细胞:聚合物接枝的分子特性对体内循环、清除、免疫原性和抗原保护的影响。

Therapeutic cells via functional modification: influence of molecular properties of polymer grafts on in vivo circulation, clearance, immunogenicity, and antigen protection.

机构信息

Centre for Blood Research, University of British Columbia , Vancouver, BC, Canada, V6T 1Z3.

出版信息

Biomacromolecules. 2013 Jun 10;14(6):2052-62. doi: 10.1021/bm4003943. Epub 2013 May 28.

Abstract

Modulation of cell surface properties via functional modification is of great interest in cell-based therapies, drug delivery, and in transfusion. We study the in vivo circulation, immuogenicity, and mechanism of clearance of hyperbranched polyglycerol (HPG)-modified red blood cells (RBCs) as a function of molecular properties of HPGs. The circulation half-life of modified cells can be modulated by controlling the polymer graft concentration on RBCs; low graft concentrations (0.25 and 0.5 mM) showed normal circulation as that of control RBCs. Molecular weight of HPG did not affect the circulation of modified RBCs. HPG grafting on RBCs reduced CD47 self-protein accessibility in a graft concentration-dependent fashion. HPG-grafted RBCs are not immunogenic, as is evident from their similar circulation profile upon repeated administration in mice and monitoring over 100 days. Histological examination of the spleen, liver, and kidneys of the mice injected with modified RBCs revealed distinct differences, such as elevated iron deposits and an increase in the number of CD45 expressing cells at high graft concentration of HPGs (1.5 mM); no changes were seen at low graft concentration. The absence of iron deposits in the white pulp region of the spleen and its presence in the red pulp region indicates that the clearance of functional RBCs occurs in the venous sinuses mechanical filtering system, similar to the clearance of unmodified senescent RBCs. HPG modification at grafting concentrations that yield long circulation in mice produced camouflage of a large number of minor blood group antigens on human RBCs, demonstrating its utility in chronic transfusion. The normal circulation, nonimmunogenic nature, and the potential to modulate the circulation time of modified cells without toxicity make this HPG-based cell surface modification approach attractive for drug delivery and other cell-based therapies.

摘要

通过功能修饰来调节细胞表面特性在基于细胞的治疗、药物输送和输血中具有重要意义。我们研究了超支化聚甘油(HPG)修饰的红细胞(RBC)的体内循环、免疫原性和清除机制,作为 HPG 分子特性的函数。通过控制 RBC 上聚合物接枝浓度可以调节修饰细胞的循环半衰期;低接枝浓度(0.25 和 0.5mM)表现出与对照 RBC 相同的正常循环。HPG 的分子量不影响修饰 RBC 的循环。HPG 接枝到 RBC 上以接枝浓度依赖的方式降低 CD47 自身蛋白的可及性。HPG 接枝的 RBC 没有免疫原性,这从它们在小鼠中重复给药后的相似循环曲线和 100 天以上的监测中可以明显看出。用修饰的 RBC 注射的小鼠的脾、肝和肾的组织学检查显示出明显的差异,例如在高接枝浓度的 HPG(1.5mM)时升高的铁沉积和表达 CD45 的细胞数量增加;在低接枝浓度时没有变化。脾白髓区没有铁沉积,而红髓区有铁沉积,这表明功能性 RBC 的清除发生在静脉窦机械过滤系统中,类似于未修饰的衰老 RBC 的清除。在产生小鼠长循环的接枝浓度下进行 HPG 修饰,对人 RBC 上的大量次要血型抗原进行伪装,证明其在慢性输血中的实用性。正常循环、非免疫原性和在没有毒性的情况下调节修饰细胞循环时间的潜力,使这种基于 HPG 的细胞表面修饰方法在药物输送和其他基于细胞的治疗中具有吸引力。

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