Multi-bioresponsive silk fibroin-based nanoparticles with on-demand cytoplasmic drug release capacity for CD44-targeted alleviation of ulcerative colitis

被引:204
作者
Gou, Shuangquan [1 ,2 ,3 ]
Huang, Yamei [2 ]
Wan, Ying [4 ]
Ma, Ya [2 ]
Zhou, Xin [2 ]
Tong, Xiaoling [1 ]
Huang, Jin [5 ]
Kang, Yuejun [2 ]
Pan, Guoqing [1 ]
Dai, Fangyin [1 ]
Xiao, Bo [1 ,2 ,3 ]
机构
[1] Southwest Univ, State Key Lab Silkworm Genome Biol, Chongqing 400715, Peoples R China
[2] Southwest Univ, Sch Mat & Energy, Inst Clean Energy & Adv Mat, Chongqing 400715, Peoples R China
[3] Southwest Univ, Coll Biotechnol, Minist Agr & Rural Affairs, Key Lab Sericultural Biol & Genet Breeding, Chongqing 400715, Peoples R China
[4] Huazhong Univ Sci & Technol, Coll Life Sci & Technol, Wuhan 430074, Hubei, Peoples R China
[5] Southwest Univ, Sch Chem & Chem Engn, Chongqing Key Lab Soft Matter Mat Chem & Funct Mf, Chongqing 400715, Peoples R China
基金
中国国家自然科学基金;
关键词
Multi-bioresponsibility; Silk fibroin; Nanomedicine; Glycoprotein CD44; On-demand drug release; Ulcerative colitis; GUT MICROBIOTA; DELIVERY; STABILIZATION; INFLAMMATION; CURCUMIN; THERAPY; DAMAGE; CD98;
D O I
10.1016/j.biomaterials.2019.05.012
中图分类号
R318 [生物医学工程];
学科分类号
0831 ;
摘要
The requirement for the favorable therapeutics against ulcerative colitis (UC) is that anti-inflammatory drugs can be specifically internalized by macrophages and subsequently be on-demand released to suppress inflammation. Herein, we developed a type of multi-bioresponsive anti-inflammatory drug (curcumin, CUR)-loaded nanoparticles (NPs) that were derived from natural silk fibroin and followed by surface functionalization with chondroitin sulfate (CS). The generated CS-CUR-NPs had a desired average particle size (175.4 nm), a uniform size distribution and negative surface charge (-35.5 mV). Strikingly, these NPs exhibited excellent bioresponsibility when triggered with the intrinsic stimuli (acidity, glutathione and reactive oxygen species) within activated macrophages, indicating that they could conceivably confer the on-demand intracellular drug release. Furthermore, we found that CS functionalization yielded notably targeted drug delivery to macrophages, and thereby enhanced the anti-inflammatory activities of NPs. Most importantly, animal experiments revealed that these nanotherapeutics could remarkably alleviate the symptoms of UC, maintain the homeostasis of intestinal microbiota and improve the survival rate of mice with UC through the route of oral administration or intravenous injection. Our results suggest that these facilely fabricated CS-CUR-NPs, which exhibit excellent biocompatibility, multi-bioresponsive drug release and macrophage-targeted capacity, could be exploited as a promising therapeutic platform for clinical UC treatment.
引用
收藏
页码:39 / 54
页数:16
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