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通过双重包封在红细胞和自体血浆珠中有效递呈抗原。

Effective antigen delivery via dual entrapment in erythrocytes and autologous plasma beads.

机构信息

a Interdisciplinary Biotechnology Unit , Aligarh Muslim University , Aligarh , India.

出版信息

J Drug Target. 2018 Feb;26(2):162-171. doi: 10.1080/1061186X.2017.1350859. Epub 2017 Jul 12.

Abstract

Fibrin-based polymeric systems have now emerged as efficient carriers of drugs, growth factors, genes, and cells. Earlier, we have reported fibrin-based plasma beads (PB), prepared from clotted whole plasma, as an efficient system for the controlled release of entrapped therapeutics. In the present study, we investigate the dual entrapment in erythrocytes and PB, as potential particulate antigen delivery system in rabbit and mice, with yeast invertase as the model antigen. Preparations used for immunisation include- invertase entrapped in erythrocytes, the same further entrapped in PB, and crosslinked with glutaraldehyde. While route of administration of the antigen only moderately affected the antibody titres, strategies slowing its release from PB increased the antibody titres remarkably, especially after a booster. Entrapment of erythrocytes entrapped antigen in the PB and further crosslinking with glutaraldehyde also resulted in significant alterations of IgG1/IgG2a ratio, indicating a shift towards humoral response. The elicited immune response was more marked in rabbits as compared to that in mice. Considering the well-known toxicity of the adjuvant, comparable antibody titres induced by the erythrocyte-plasma bead system was encouraging in the induction of humoral immunity.

摘要

纤维蛋白基聚合体系统现已成为药物、生长因子、基因和细胞的有效载体。我们之前曾报道过,从凝固的全血血浆中制备的纤维蛋白基血浆珠(PB),是一种用于控制包埋治疗剂释放的有效系统。在本研究中,我们研究了红细胞和 PB 的双重包封,作为兔和小鼠中潜在的微粒抗原递送系统,以酵母转化酶为模型抗原。用于免疫的制剂包括-包封在红细胞中的转化酶、进一步包封在 PB 中的转化酶,并用戊二醛交联。虽然抗原的给药途径仅适度影响抗体滴度,但减缓其从 PB 中释放的策略显著提高了抗体滴度,尤其是在加强免疫后。将红细胞包封的抗原包封在 PB 中,并进一步用戊二醛交联也导致 IgG1/IgG2a 比值发生显著变化,表明向体液免疫反应的转变。与小鼠相比,在兔中引起的免疫反应更为明显。考虑到佐剂的已知毒性,红细胞-血浆珠系统诱导的可比抗体滴度令人鼓舞,可诱导体液免疫。

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