Chimeric nanobody-decorated liposomes by self-assembly

被引:12
|
作者
Rahman, Md. Mofizur [1 ,2 ]
Wang, Jing [3 ,4 ]
Wang, Guosheng [1 ,5 ]
Su, Zhipeng [6 ]
Li, Yizeng [7 ]
Chen, Yundi [1 ]
Meng, Jinguo [6 ]
Yao, Yao [6 ]
Wang, Lefei [6 ]
Wilkens, Stephan [8 ]
Tan, Jifu [9 ]
Luo, Juntao [10 ]
Zhang, Tao [11 ]
Zhu, Chuandong [1 ,12 ]
Cho, Sung Hyun [13 ]
Wang, Lixue [1 ,12 ]
Lee, Luke P. [14 ,15 ,16 ,17 ,18 ]
Wan, Yuan [1 ]
机构
[1] SUNY Binghamton, Dept Biomed Engn, Pq Lab BiomeDx Rx, Binghamton, NY 13902 USA
[2] Daffodil Int Univ, Dept Pharm, Dhaka, Bangladesh
[3] Nanjing Univ, Med Sch, Nanjing Drum Tower Hosp, Dept Hematol,Affiliated Hosp, Nanjing, Peoples R China
[4] Nanjing Drum Tower Hosp Grp, Yizheng Hosp, Dept Oncol & Hematol, Yizheng, Peoples R China
[5] Tongji Univ, Shanghai East Hosp, Dept Pulm & Crit Care Med, Sch Med, Shanghai, Peoples R China
[6] Nanjing Regenecore Biotech Co Ltd, Nanjing, Peoples R China
[7] SUNY Binghamton, Dept Biomed Engn, Biophys & Math Biol Lab, Binghamton, NY USA
[8] SUNY Upstate Med Univ, Dept Biochem & Mol Biol, Syracuse, NY USA
[9] Northern Illinois Univ, Dept Mech Engn, De Kalb, IL USA
[10] SUNY Upstate Med Univ, Dept Pharmacol, Syracuse, NY USA
[11] SUNY Binghamton, Sch Pharm & Pharmaceut Sci, Johnson City, NY USA
[12] Nanjing Univ Chinese Med, Hosp Nanjing 2, Dept Radiotherapy, Nanjing, Jiangsu, Peoples R China
[13] Penn State Univ, Huck Inst Life Sci, University Pk, PA USA
[14] Harvard Univ, Harvard Med Sch, Cambridge, MA 02138 USA
[15] Brigham & Womens Hosp, Dept Med, Boston, MA 02115 USA
[16] Univ Calif Berkeley, Dept Elect Engn & Comp Sci, Dept Bioengn, Berkeley, CA 94720 USA
[17] Sungkyunkwan Univ, Inst Quantum Biophys, Dept Biophys, Suwon, South Korea
[18] Ewha Womans Univ, Dept Chem & Nanosci, Seoul, South Korea
基金
美国国家卫生研究院;
关键词
TRANSMEMBRANE DOMAIN; LIPID-COMPOSITION; MEDIATED FUSION; DRUG-DELIVERY; MODEL; PROTEIN; VISUALIZATION; MEMBRANES; APTAMERS; PHASE;
D O I
10.1038/s41565-024-01620-6
中图分类号
TB3 [工程材料学];
学科分类号
0805 ; 080502 ;
摘要
Liposomes as drug vehicles have advantages, such as payload protection, tunable carrying capacity and improved biodistribution. However, due to the dysfunction of targeting moieties and payload loss during preparation, immunoliposomes have yet to be favoured in commercial manufacturing. Here we report a chemical modification-free biophysical approach for producing immunoliposomes in one step through the self-assembly of a chimeric nanobody (cNB) into liposome bilayers. cNB consists of a nanobody against human epidermal growth factor receptor 2 (HER2), a flexible peptide linker and a hydrophobic single transmembrane domain. We determined that 64% of therapeutic compounds can be encapsulated into 100-nm liposomes, and up to 2,500 cNBs can be anchored on liposomal membranes without steric hindrance under facile conditions. Subsequently, we demonstrate that drug-loaded immunoliposomes increase cytotoxicity on HER2-overexpressing cancer cell lines by 10- to 20-fold, inhibit the growth of xenograft tumours by 3.4-fold and improve survival by more than twofold. Manufacturing complexities, low yield and stability issues have hampered the clinical translation and scaling-up of immunoliposomes to meet the needs of pharmaceutical-grade products. The authors propose a one-step method of incorporating chimeric nanobodies tagged to hydrophobic linkers into liposomes, allowing targeted delivery of small-molecule anti-cancer drugs to tumours.
引用
收藏
页码:818 / 824
页数:14
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