Self-Assembled Injectable Peptide Hydrogels Capable of Triggering Antitumor Immune Response

IF 5.4 2区 化学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Ruirui Xing , Shukun Li , Ning Zhang , Guizhi Shen , Helmuth Möhwald , Xuehai Yan
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引用次数: 134

Abstract

Self-assembled peptide hydrogels are particularly appealing for drug delivery, tissue engineering, and antitumor therapy due to various advantageous features including excellent biocompatibility and biodegradability, defined molecular and higher organized structures, and easy availability. However, the poor mechanical and rheological properties of assembled peptide hydrogels cause difficulties in injection, thus limiting further applications. Herein, injectable peptide-based hydrogels with tunable mechanical and rheological properties were obtained by combination with a positively charged poly peptide (poly-l-lysine, PLL). Electrostatic coupling between PLL and a self-assembling dipeptide (Fmoc-FF) provides a smart switch to enable the fibrous hydrogels to be shear-thinning and self-healing, thus leading to the formation of supramolecular hydrogels with rheological properties suitable for injection. The latter can be flexibly adjusted by merely varying the concentration or the molecular weight of the polypeptide to satisfy a variety of requirements in biological applications. The hydrogels, consisting of helical nanofibers stabilized with disulfide bonds, are prepared and further injected for antitumor therapy. The results demonstrate that the helical fibrous hydrogel, without the addition of antigens, immune regulatory factors, and adjuvants, can activate T cell response and efficiently suppress tumor growth. Therefore, injectable hydrogels self-assembled by a combination of small peptides and biomacromolecules present a great potential for biomedical applications, especially for development of a new type of immuno-responsive materials toward antitumor therapy.

Abstract Image

能够触发抗肿瘤免疫反应的自组装注射肽水凝胶
自组装肽水凝胶因其优异的生物相容性和生物降解性、明确的分子结构和更高的组织结构以及易于获得等优点,在药物输送、组织工程和抗肿瘤治疗方面尤其具有吸引力。然而,组装肽水凝胶较差的机械和流变特性导致注射困难,从而限制了进一步的应用。通过与带正电荷的多肽(聚赖氨酸,PLL)结合,获得了具有可调力学和流变性能的可注射肽基水凝胶。PLL与自组装二肽(Fmoc-FF)之间的静电耦合提供了一个智能开关,使纤维水凝胶能够剪切变薄和自修复,从而形成具有适合注射的流变特性的超分子水凝胶。后者可以通过仅仅改变多肽的浓度或分子量来灵活调节,以满足生物应用中的各种要求。制备了由二硫键稳定的螺旋纳米纤维组成的水凝胶,并进一步注射用于抗肿瘤治疗。结果表明,螺旋纤维水凝胶在不添加抗原、免疫调节因子和佐剂的情况下,可以激活T细胞反应,有效抑制肿瘤生长。因此,由小肽和生物大分子自组装而成的可注射水凝胶具有很大的生物医学应用潜力,特别是开发一种新型的抗肿瘤免疫反应材料。
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来源期刊
Biomacromolecules
Biomacromolecules 化学-高分子科学
CiteScore
10.60
自引率
4.80%
发文量
417
审稿时长
1.6 months
期刊介绍: Biomacromolecules is a leading forum for the dissemination of cutting-edge research at the interface of polymer science and biology. Submissions to Biomacromolecules should contain strong elements of innovation in terms of macromolecular design, synthesis and characterization, or in the application of polymer materials to biology and medicine. Topics covered by Biomacromolecules include, but are not exclusively limited to: sustainable polymers, polymers based on natural and renewable resources, degradable polymers, polymer conjugates, polymeric drugs, polymers in biocatalysis, biomacromolecular assembly, biomimetic polymers, polymer-biomineral hybrids, biomimetic-polymer processing, polymer recycling, bioactive polymer surfaces, original polymer design for biomedical applications such as immunotherapy, drug delivery, gene delivery, antimicrobial applications, diagnostic imaging and biosensing, polymers in tissue engineering and regenerative medicine, polymeric scaffolds and hydrogels for cell culture and delivery.
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