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炎症环境适应型图案表面实现巨噬细胞的时空免疫调节。

Inflammatory environment-adaptive patterned surface for spatiotemporal immunomodulation of macrophages.

机构信息

MOE Key Laboratory of Macromolecular Synthesis and Functionalization, Department of Polymer Science and Engineering, Zhejiang University, Hangzhou 310027, China.

MOE Key Laboratory of Macromolecular Synthesis and Functionalization, Department of Polymer Science and Engineering, Zhejiang University, Hangzhou 310027, China.

出版信息

Acta Biomater. 2022 Nov;153:139-148. doi: 10.1016/j.actbio.2022.09.055. Epub 2022 Sep 24.

Abstract

Designing biomaterials with precise immunomodulation can help to decipher the dynamic interactions between macrophages and biomaterials to match the tissue healing process. Although some advanced stimuli-responsive immunomodulatory biomaterials were reported for cell dynamic modulation, while most triggers need external stimuli by manual intervention, there would be the inevitable errors and uncertainties. Thus, developing immunomodulatory biomaterials with adaptive abilities, which can recognize the inflammation signals, change their properties spatiotemporally under the microenvironment triggers, and provide feedback to realize macrophages modulation in different healing stages, has become a promising strategy. In this work, we developed an inflammation-adaptive Arg-Gly-Asp (RGD) -patterned surface for spatiotemporal immunomodulation of macrophage. We fabricated a methacrylated hyaluronic acid (MA-HA) hydrogel with thiol-functionalized RGD-patterned surface by employing photolithography technology. Then, thiol-functionalized RGD contained ROS-cleavable linker was filled the remaining sites and consequently, a dynamic surface with temporary homogeneous RGD was obtained. Under the overproduction of ROS by the inflammation-activated macrophages, the linker was cleaved, and the homogeneous RGD surface was transformed to the RGD patterned surface, which triggered elongation of macrophages and consequently the upregulated expressions of arginase-1, IL-10 and TNF-β1, indicating the polarization toward to anti-inflammatory phenotype. Developing inflammatory environment-adaptive surface for spatiotemporal modulation of macrophages polarization provides a precise and smart strategy for the healing-matched immunomodulation to facilitate healing outcomes. STATEMENT OF SIGNIFICANCE: Designing biomaterials with precise immunomodulation can help to decipher the dynamic interactions between macrophages and biomaterials to match tissue repair process. Some immunomodulatory biomaterials were reported for cell dynamic modulation, while most triggers need external manual intervention. Thus, we developed an immunomodulatory biomaterial with inflammation-adaptive patterned surface, which can recognize abnormal signals and change its properties spatiotemporally under the microenvironment triggers, and provide feedback to realize macrophages modulation in different stages. The dynamic surface can adapt to the changes of microenvironment and dynamically to match the cell behavior and tissue healing process on demand without external manual intervention. Additionally, the surface achieves the balance of macrophages with pro- and anti-inflammatory phenotypes in the tissue repair process.

摘要

设计具有精确免疫调节功能的生物材料有助于揭示巨噬细胞与生物材料之间的动态相互作用,以匹配组织愈合过程。虽然已经有一些先进的响应性免疫调节生物材料被报道用于细胞动态调节,而大多数触发因素需要手动干预的外部刺激,但这不可避免地会存在误差和不确定性。因此,开发具有自适应能力的免疫调节生物材料,使其能够识别炎症信号,在微环境触发下在空间和时间上改变其特性,并提供反馈以在不同的愈合阶段实现巨噬细胞的调节,已成为一种很有前途的策略。在这项工作中,我们开发了一种用于巨噬细胞时空免疫调节的炎症适应性 Arg-Gly-Asp(RGD)图案表面。我们通过光光刻技术制备了一种带有巯基功能化 RGD 图案表面的甲基丙烯酰化透明质酸(MA-HA)水凝胶。然后,填充了含有 ROS 可切割连接物的巯基功能化 RGD,从而获得了具有暂时均匀 RGD 的动态表面。在炎症激活的巨噬细胞过度产生 ROS 的情况下,连接物被切割,均匀的 RGD 表面转化为 RGD 图案表面,这触发了巨噬细胞的伸长,进而上调了精氨酸酶-1、IL-10 和 TNF-β1 的表达,表明向抗炎表型极化。开发用于巨噬细胞极化时空调节的炎症环境适应性表面为精确和智能的免疫调节提供了一种策略,以促进愈合效果。

意义

设计具有精确免疫调节功能的生物材料有助于揭示巨噬细胞与生物材料之间的动态相互作用,以匹配组织修复过程。一些免疫调节生物材料被报道用于细胞动态调节,而大多数触发因素需要外部手动干预。因此,我们开发了一种具有炎症适应性图案表面的免疫调节生物材料,它可以识别异常信号,并在微环境触发下在空间和时间上改变其特性,并提供反馈以在不同阶段实现巨噬细胞的调节。动态表面可以适应微环境的变化,并根据需要动态地匹配细胞行为和组织愈合过程,而无需外部手动干预。此外,该表面在组织修复过程中实现了促炎和抗炎表型巨噬细胞的平衡。

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