Enhanced design and formulation of nanoparticles for anti-biofilm drug delivery

被引:71
|
作者
Sims, Kenneth R., Jr. [1 ]
Liu, Yuan [2 ]
Hwang, Geelsu [2 ]
Jung, Hoi In [3 ]
Koo, Hyun [2 ,4 ,5 ,6 ]
Benoit, Danielle S. W. [7 ,8 ,9 ,10 ]
机构
[1] Univ Rochester, Sch Med & Dent, Translat Biomed Sci, Rochester, NY USA
[2] Univ Penn, Sch Dent Med, Biofilm Res Lab, Levy Ctr Oral Hlth, Philadelphia, PA 19104 USA
[3] Yonsei Univ, Coll Dent, Dept Prevent Dent & Publ Oral Hlth, Seoul, South Korea
[4] Univ Penn, Sch Dent Med, Dept Orthodont, Philadelphia, PA 19104 USA
[5] Univ Penn, Sch Dent Med, Div Pediat Dent, Philadelphia, PA 19104 USA
[6] Univ Penn, Sch Dent Med, Div Community Oral Hlth, Philadelphia, PA 19104 USA
[7] Univ Rochester, Dept Biomed Engn, Rochester, NY 14627 USA
[8] Univ Rochester, Ctr Oral Biol, Rochester, NY 14627 USA
[9] Univ Rochester, Ctr Musculoskeletal Res, Rochester, NY 14627 USA
[10] Univ Rochester, Dept Chem Engn, Rochester, NY 14627 USA
基金
美国国家科学基金会; 美国国家卫生研究院;
关键词
STREPTOCOCCUS-MUTANS; GLOBAL BURDEN; DIBLOCK COPOLYMER; TT-FARNESOL; IN-VITRO; ANTIBACTERIAL ACTIVITY; STAPHYLOCOCCUS-AUREUS; RAFT POLYMERIZATION; SIRNA DELIVERY; ORAL-DISEASES;
D O I
10.1039/c8nr05784b
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Biofilms are surface-bound, structured microbial communities underpinning persistent bacterial infections. Biofilms often create acidic pH microenvironments, providing opportunities to leverage responsive drug delivery systems to improve antibacterial efficacy. Here, the antibacterial efficacy of novel formulations containing pH-responsive polymer nanoparticle carriers (NPCs) and farnesol, a hydrophobic antibacterial drug, were investigated. Multiple farnesol-loaded NPCs, which varied in overall molecular weight and corona-to-core molecular weight ratios (CCRs), were tested using standard and saturated drug loading conditions. NPCs loaded at saturated conditions exhibited approximate to 300% greater drug loading capacity over standard conditions. Furthermore, saturated loading conditions sustained zero-ordered drug release over 48 hours, which was 3-fold longer than using standard farnesol loading. Anti-biofilm activity of saturated NPC loading was markedly amplified using Streptococcus mutans as a biofilm-forming model organism. Specifically, reductions of approximate to 2-4 log colony forming unit (CFU) were obtained using microplate and saliva-coated hydroxyapatite biofilm assays. Mechanistically, the new formulation reduced total biomass by disrupting insoluble glucan formation and increased NPC-cell membrane localization. Finally, thonzonium bromide, a highly potent, FDA-approved antibacterial drug with similar alkyl chain structure to farnesol, was also loaded into NPCs and used to treat S. mutans biofilms. Similar to farnesol-loaded NPCs, thonzonium bromide-loaded NPCs increased drug loading capacity 2.5-fold, demonstrated nearly zero-order release kinetics over 96 hours, and reduced biofilm cell viability by approximate to 6 log CFU. This work provides foundational insights that may lead to clinical translation of novel topical biofilm-targeting therapies, such as those for oral diseases.
引用
收藏
页码:219 / 236
页数:18
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