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Cationic DDA/TDB liposome as a mucosal vaccine adjuvant for uptake by dendritic cells in vitro induces potent humoural immunity

机译:阳离子DDA / TDB脂质体作为粘膜疫苗佐剂,用于在体外的树突状细胞吸收诱导有效的静脉抗免疫力

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摘要

The cationic dimethyldioctadecylammonium/trehalose 6,6,9-dibehenate (DDA/TDB) liposome is as a strong adjuvant system for vaccines, with remarkable immunostimulatory activity. The mucosal administration of vaccines is a potential strategy for inducing earlier and stronger mucosal immune responses to infectious diseases. In this study, we assessed whether the intranasal administration of cationic DDA/TDB liposomes combined with influenza antigen A (H3N2) can be used as a highly efficacious vaccine to induce mucosal and systemic antibody responses. Confocal laser scanning microscopy and a flow-cytometric analysis showed that the uptake of the cationic DDA/TDB liposome carrier was significantly higher than that of neutral 1,2-distearoyl-sn-glycero-3-phosphocholine/cholesterol (DSPC/Chol) or cationic 1,2-dioleoyl-3-trimethylammonium-propane/3-(N-[N,N-dimethylaminoethane]-carbamoyl (DOTAP/DC-Chol) liposomes. Our results indicate that the cationic DDA/TDB liposome is more effective in facilitating its uptake by dendritic cells (DCs) in vitro than the DSPC/Chol or DOTAP/DC-Chol liposome. DCs treated with DDA/TDB liposomes strongly expressed CD80, CD86, and MHC II molecules, whereas those treated with DSPC/Chol or DOTAP/DC-Chol liposomes did not. C57BL/6 mice intranasally immunized with H3N2-encapsulating cationic DDA/TDB liposomes had significantly higher H3N2-specific s-IgA levels in their nasal wash fluid than those treated with other formulations. The DDA/TDB liposomes also simultaneously enhanced the serum IgG IgG2a, IgG1, and IgG2b antibody responses. In summary, DDA/TDB liposomes effectively facilitated their uptake by DCs and DCs maturation in vitro, and induced significantly higher mucosal IgA, systemic IgG, IgG1, and IgG2b antibody titres than other formulations after their intranasal administration in vivo. These results indicate that DDA/TDB liposomes are a promising antigen delivery carrier for clinical antiviral applications.
机译:阳离子二甲基二烯烃基铵/海藻糖6,6,9-二庚酸酯(DDA / TDB)脂质体是用于疫苗的强佐剂系统,具有显着的免疫刺激活性。疫苗的粘膜施用是对传染病的早期和更强烈的粘膜免疫反应诱导潜在的策略。在这项研究中,我们评估了与流感抗原A(H3N2)组合的鼻内施用阳离子DDA / TDB脂质体(H3N2)可用作诱导粘膜和全身抗体应答的高度有效疫苗。共聚焦激光扫描显微镜和流量分析显示,阳离子DDA / TDB脂质体载体的摄取显着高于中性1,2- Distearoyl-Sn-甘油-3-普膦醇/胆固醇(DSPC / CHOL)或阳离子1,2-Dioleyl-3-三甲基铵 - 丙烷/ 3-(N- [N,N-二甲基氨基乙烷] -Carbamyl(DOTAP / DC-CHOL)脂质体。我们的结果表明,阳离子DDA / TDB脂质体更有效促进树枝状细胞(DCS)的吸收,比DSPC / CHOL或DOTAP / DC-CHOL脂质体。用DDA / TDB脂质体处理的DCS强烈表达CD80,CD86和MHC II分子,而用DSPC / CHOL处理的DCS或dotap / dc-chol脂质体没有。用H3N2包封的阳离子DDA / TDB脂质体鼻内免疫的C57BL / 6小鼠在其鼻腔洗液中具有显着高于其鼻腔洗液的H3N2特异性S-IgA水平,而不是用其他配方处理的水平。DDA / TDB脂质体还同时增强了血清IgG IgG2a,IgG1和IgG 2B抗体反应。总之,DDA / TDB脂质体有效地促进了DCS和DCS成熟在体外DC和DCS成熟的摄取,并且在体内鼻内给药后的其他制剂中诱导显着高的粘膜IgA,全身IgG,IgG1和IgG2B抗体滴度。这些结果表明DDA / TDB脂质体是临床抗病毒应用的有望抗原输送载体。

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  • 作者单位

    Ningxia Med Univ Sch Pharm Dept Pharmaceut 1160 Shengli South St Yinchuan 750004 Peoples R;

    Ningxia Med Univ Sch Pharm Dept Pharmaceut 1160 Shengli South St Yinchuan 750004 Peoples R;

    Ningxia Med Univ Sch Pharm Dept Pharmaceut 1160 Shengli South St Yinchuan 750004 Peoples R;

    Ningxia Med Univ Sch Pharm Dept Pharmaceut 1160 Shengli South St Yinchuan 750004 Peoples R;

    Ningxia Med Univ Sch Pharm Dept Pharmaceut 1160 Shengli South St Yinchuan 750004 Peoples R;

    Ningxia Med Univ Sch Pharm Dept Pharmaceut 1160 Shengli South St Yinchuan 750004 Peoples R;

    Ningxia Med Univ Sch Pharm Dept Pharmaceut 1160 Shengli South St Yinchuan 750004 Peoples R;

    Ningxia Med Univ Sch Pharm Dept Pharmaceut 1160 Shengli South St Yinchuan 750004 Peoples R;

    Ningxia Med Univ Sch Pharm Dept Pharmaceut 1160 Shengli South St Yinchuan 750004 Peoples R;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医用一般科学;
  • 关键词

    Cationic liposome; intranasal immunization; mucosal antibody response; quantum dots; vaccine adjuvant;

    机译:阳离子脂质体;鼻内免疫;粘膜抗体应答;量子点;疫苗佐剂;
  • 入库时间 2022-08-20 01:25:56

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