Effect of molecular weight of tyramine-modified hyaluronan on polarization state of THP-1 and peripheral blood mononuclear cells-derived macrophages

IF 5.5 2区 医学 Q2 MATERIALS SCIENCE, BIOMATERIALS Materials Science & Engineering C-Materials for Biological Applications Pub Date : 2024-12-29 DOI:10.1016/j.bioadv.2024.214166
Jacek K. Wychowaniec , Ezgi Irem Bektas , Andrea J. Vernengo , Marcia Muerner , Marielle Airoldi , Paul Sean Tipay , Jiranuwat Sapudom , Jeremy Teo , David Eglin , Matteo D'Este
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Abstract

The immunomodulatory properties of hyaluronan and its derivatives are key to their use in medicine and tissue engineering. In this work we evaluated the capability of soluble tyramine-modified hyaluronan (THA) synthesized from hyaluronan of two molecular weights (low Mw = 280 kDa and high Mw = 1640 kDa) for polarization of THP-1 and peripheral blood mononuclear cells (PBMCs)-derived macrophages (MΦs). We demonstrate the polarization effects of the supplemented THA by flow cytometry and bead-based multiplex immunoassay for the THP-1 derived MΦs and by semi-automated image analysis from confocal microscopy, immunofluorescent staining utilizing CD68 and CD206 surface markers, RT-qPCR gene expression analysis, as well as using the enzyme-linked immunosorbent assay (ELISA) for PBMCs-derived MΦs. Our data indicate that supplementation with LMW THA drives changes in THP-1 derived MΦs towards a pro-inflammatory M1-like phenotype, whereas supplementation with the HMW THA leads to a more mixed profile with some features of both M1 and M2 phenotypes, suggesting either a heterogeneous population or a transitional state. For cells directly sourced from human patients, PMBCs-derived MΦs, results exhibit a higher degree of variability, pointing out a differential regulation of factors including IL-10 and CD206 between the two cell sources. While human primary cells add to the clinical relevance, donor diversity introduces wider variability in the dataset, preventing drawing strong conclusions. Nevertheless, the MΦs profiles observed in THP-1 derived cells for treatments with LMW and HMW THA are generally consistent with what might be expected for the treatment with non-modified hyaluronans of respective molecular weights, confirming the known association holds true for the chemically tyramine-modified hyaluronan. We stipulate that these responses will provide basis for more accurate in vivo representation and translational immunomodulatory guidance for the use of THA-based biomaterials to a wider biomaterials and tissue engineering communities.

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酪胺修饰透明质酸分子量对THP-1和外周血单核细胞源性巨噬细胞极化状态的影响。
透明质酸及其衍生物的免疫调节特性是其在医学和组织工程中应用的关键。在这项工作中,我们评估了由两种分子量的透明质酸(低Mw = 280 kDa和高Mw = 1640 kDa)合成的可溶性酪胺修饰透明质酸(THA)对THP-1和外周血单核细胞(PBMCs)来源的巨噬细胞极化的能力(MΦs)。我们通过流式细胞术和基于微球的多重免疫分析法对THP-1衍生物MΦs、共聚焦显微镜的半自动图像分析、利用CD68和CD206表面标记物的免疫荧光染色、RT-qPCR基因表达分析以及酶联免疫吸附法(ELISA)对pbmcs衍生物MΦs证明了补充THA的极化效应。我们的数据表明,补充LMW THA会导致THP-1衍生的MΦs向着促炎性M1样表型变化,而补充HMW THA会导致更混合的特征,具有M1和M2表型的一些特征,这表明要么是异质群体,要么是过渡状态。对于直接来源于人类患者的细胞,pmbc衍生的MΦs,结果显示出更高程度的可变性,指出两种细胞来源之间IL-10和CD206等因子的差异调节。虽然人类原代细胞增加了临床相关性,但供体多样性在数据集中引入了更大的可变性,从而无法得出强有力的结论。然而,在THP-1衍生细胞中观察到的MΦs谱图与LMW和HMW THA处理的结果大致一致,这证实了已知的关联对于化学酪胺修饰的透明质酸是正确的。我们认为这些反应将为更准确的体内表征和翻译免疫调节指导提供基础,为更广泛的生物材料和组织工程领域使用基于tha的生物材料提供指导。
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来源期刊
CiteScore
17.80
自引率
0.00%
发文量
501
审稿时长
27 days
期刊介绍: Biomaterials Advances, previously known as Materials Science and Engineering: C-Materials for Biological Applications (P-ISSN: 0928-4931, E-ISSN: 1873-0191). Includes topics at the interface of the biomedical sciences and materials engineering. These topics include: • Bioinspired and biomimetic materials for medical applications • Materials of biological origin for medical applications • Materials for "active" medical applications • Self-assembling and self-healing materials for medical applications • "Smart" (i.e., stimulus-response) materials for medical applications • Ceramic, metallic, polymeric, and composite materials for medical applications • Materials for in vivo sensing • Materials for in vivo imaging • Materials for delivery of pharmacologic agents and vaccines • Novel approaches for characterizing and modeling materials for medical applications Manuscripts on biological topics without a materials science component, or manuscripts on materials science without biological applications, will not be considered for publication in Materials Science and Engineering C. New submissions are first assessed for language, scope and originality (plagiarism check) and can be desk rejected before review if they need English language improvements, are out of scope or present excessive duplication with published sources. Biomaterials Advances sits within Elsevier''s biomaterials science portfolio alongside Biomaterials, Materials Today Bio and Biomaterials and Biosystems. As part of the broader Materials Today family, Biomaterials Advances offers authors rigorous peer review, rapid decisions, and high visibility. We look forward to receiving your submissions!
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