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将卵清蛋白包封于脂质体中可使小鼠产生不同程度的口服免疫效果。

Ovalbumin encapsulation into liposomes results in distinct degrees of oral immunization in mice.

作者信息

Alves A C, Ramaldes G A, Oliveira M C, Cardoso V N, Mota-Santos T A, Faria A M C, Gontijo C M

机构信息

Departamento de Produtos Farmacêuticos, Faculdade de Farmácia, Universidade Federal de Minas Gerais, Belo Horizonte, MG, Brazil.

出版信息

Cell Immunol. 2008;254(1):63-73. doi: 10.1016/j.cellimm.2008.07.001. Epub 2008 Aug 15.

Abstract

Oral administration of protein antigens, such as ovalbumin, may result in induction of either tolerance or immunization. To avoid oral tolerance, there are new strategies to protect the antigens from degradation within the gastrointestinal tract and to allow them to reach inductive immunological sites. One such strategy is the usage of liposomes. Different parameters may influence the stability of liposomes in the gastrointestinal tract. Herein, we studied the immunological consequences of oral administration of liposome-encapsulated ovalbumin in different strains of mice using different liposomes. Our data demonstrated that ovalbumin liposomes improved the induction of oral immunization and the degree of improvement depended on the liposome type and on the strain of mice used. The mechanism responsible for this differential effect of liposomes depended on the site of antigen release and absorption. Therefore, some liposomes might be suitable as adjuvants for oral immunization, others for oral tolerance induction.

摘要

口服蛋白质抗原,如卵清蛋白,可能会导致诱导耐受或免疫。为避免口服耐受,有一些新策略可保护抗原在胃肠道内不被降解,并使其能够到达诱导免疫的部位。其中一种策略是使用脂质体。不同参数可能会影响脂质体在胃肠道中的稳定性。在此,我们使用不同的脂质体,研究了在不同品系小鼠中口服脂质体包裹的卵清蛋白的免疫后果。我们的数据表明,卵清蛋白脂质体改善了口服免疫的诱导,改善程度取决于脂质体类型和所用小鼠品系。脂质体这种差异效应的机制取决于抗原释放和吸收的部位。因此,一些脂质体可能适合作为口服免疫的佐剂,另一些则适合诱导口服耐受。

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