首页> 外文期刊>Biomaterials Science >Endothelial cell adhesion and blood response to hemocompatible peptide 1 (HCP-1), REDV, and RGD peptide sequences with free N-terminal amino groups immobilized on a biomedical expanded polytetrafluorethylene surface
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Endothelial cell adhesion and blood response to hemocompatible peptide 1 (HCP-1), REDV, and RGD peptide sequences with free N-terminal amino groups immobilized on a biomedical expanded polytetrafluorethylene surface

机译:内皮细胞粘附和血液反应对血液相容性肽1(HCP-1),REDV和RGD肽序列,其具有固定在生物医学膨胀的聚四氟乙烯表面上的游离N-末端氨基

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摘要

Blood compatibility generally requires two contradictory characteristics: reduced protein/platelet adhesion and excellent endothelium-related cell affinity. To understand the effect of cell adhesion peptides on blood compatibility, the peptides REDV, RGD, and hemocompatible peptide-1 (HCP-1) were immobilized on an expanded polytetrafluorethylene (ePTFE) surface and evaluated in vitro, in situ, and in vivo. Since the terminal amino groups of functional peptides often have an important effect, a cysteine residue was added to the C terminal and used for immobilization to keep the terminal amino groups free. Maleimide groups were added to carboxylic groups of highly hydrophilic and biologically inert (bioinert) polymer chains grafted onto ePTFE and coupled with cysteine residues. In vitro tests revealed that free N-terminal HCP-1 and RGD-immobilized surfaces improved the adhesion and spread of human umbilical vein endothelial cells (HUVECs), while, unexpectedly, a free N-terminal adjacent to REDV suppressed cell affinity. In situ evaluation with a porcine closed-circuit system for 2 h showed that no platelets adhered to the modified ePTFE sutures due to the bioinert graft chain containing phosphorylcholine groups. Simultaneously, leukocyte-related and endothelium-related cells were observed on RGD-immobilized ePTFE sutures because RGD was recognized by broad types of cells. These cells were not observed on the HCP-1- and REDV-immobilized ePTFE sutures, which may be due to insufficient exposure time. HCP-1-modified ePTFE graft implantation in a porcine femorofemoral (FF) bypass model for 10 days showed that the thrombus layer was clearly mitigated by HCP-1 immobilization. This study suggests that the HCP-1-immobilized ePTFE surface has potential for long-term application by mitigating thrombus and supporting endothelial cell adhesion.
机译:血液相容性通常需要两个矛盾特征:降低蛋白质/血小板粘附和优异的内皮相关细胞亲和力。为了了解细胞粘附肽对血液相容性的影响,将肽REDV,RGD和血液相容性肽-1(HCP-1)固定在膨胀的聚四氟乙烯(EPTFE)表面上,并在体外评估,原位和体内。由于功能性肽的末端氨基通常具有重要作用,因此将半胱氨酸残基加入到C末端并用于固定以保持末端氨基不含氨基。将马来酰亚胺基团加入到高度亲水和生物惰性(Bioinert)聚合物链中嫁接到EPTFE上并与半胱氨酸残基偶联的羧基。体外试验显示,自由N-末端HCP-1和RGD-固定的表面改善了人脐静脉内皮细胞(HUVEC)的粘附和扩散,而意外地,邻近REDV抑制细胞亲和力的自由N-末端。用猪闭电路系统的原位评估为2小时,表明,由于含有磷胆碱基的生物素接枝链,没有粘附到改性EPTFE缝合线的血小板。同时,在RGD固定的EPTFE缝合线上观察到与白细胞相关和内皮相关的细胞,因为RGD被广泛的细胞识别。在HCP-1-和RedV-固定的EPTFE缝合线上未观察到这些细胞,其可能是由于暴露时间不足。 HCP-1改性EPTFE猪股骨型(FF)旁路模型中的移植物注入10天显示,通过HCP-1固定化清楚地减轻血栓层。本研究表明,通过减轻血栓和支持内皮细胞粘附,HCP-1固定化的EPTFE表面具有长期施用。

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  • 来源
    《Biomaterials Science》 |2021年第3期|共10页
  • 作者单位

    Natl Cerebral &

    Cardiovasc Ctr Res Inst Dept Biomed Engn 6-1 Kishibe Shimmachi Suita Osaka 5648565 Japan;

    Natl Cerebral &

    Cardiovasc Ctr Res Inst Dept Biomed Engn 6-1 Kishibe Shimmachi Suita Osaka 5648565 Japan;

    Natl Cerebral &

    Cardiovasc Ctr Res Inst Dept Biomed Engn 6-1 Kishibe Shimmachi Suita Osaka 5648565 Japan;

    Natl Cerebral &

    Cardiovasc Ctr Res Inst Dept Biomed Engn 6-1 Kishibe Shimmachi Suita Osaka 5648565 Japan;

    Natl Cerebral &

    Cardiovasc Ctr Res Inst Dept Biomed Engn 6-1 Kishibe Shimmachi Suita Osaka 5648565 Japan;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
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