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首页> 外文期刊>Colloids and Surfaces, B. Biointerfaces >Stabilised aluminium phosphate nanoparticles used as vaccine adjuvant
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Stabilised aluminium phosphate nanoparticles used as vaccine adjuvant

机译:稳定的铝磷酸铝纳米颗粒用作疫苗辅助剂

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Aluminium phosphate is a commonly used adjuvant consisting of heterogeneously sized aggregates up to several micrometers. However, aluminium phosphate nanoparticles may exhibit an improved adjuvant effect. In this study, nanoparticles were made by sonication of commercially available aluminium phosphate adjuvant, resulting in particles with a size (Z-average diameter) between 200-300 nm and a point of zero charge of 4.5. To prevent reaggregation, which occurred within 14 days, a screening of excipients was performed to identify stabilisers effective under physiological conditions (pH 7.4, 290 mOsm). The amino acids threonine, asparagine, and L-alanyl-L-1-aminoethylphosphonic acid (LAPA) stabilised sonicated aluminium phosphate. Particle sizes remained stable between 400-600 nm at 37 degrees C during 106 days. Contrarily, arginine induced strong reaggregation to a particle size larger than 1000 nm. The stability of aluminium phosphate nanoparticles was strongly affected by the pH. Aggregation mainly occurred below pH 7. The adsorption capacity, a potentially relevant parameter for adjuvants, was slightly reduced in the presence of asparagine, when using a model antigen (lysozyme). LAPA, arginine, threonine and aspartic acid reduced protein adsorption significantly. The adjuvant effect of aluminium phosphate nanoparticles was studied by immunisation of mice with diphtheria toxoid adjuvanted with the aluminium phosphate nanoparticles. The presence of LAPA, threonine, aspartic acid or asparagine did not alter diphtheria toxoid-specific antibody or toxin-neutralising antibody titres. Arginine increased diphtheria toxoid-specific antibody titres but not toxin-neutralising antibody titres. In conclusion, aluminium phosphate nanoparticles were stabilised by particular amino acids and induced an adjuvant effect comparable to that of aluminium phosphate microparticles.
机译:磷酸铝是一种常用的佐剂,其由非均相尺寸的聚集体组成,高达几微米。然而,磷酸铝纳米铝可以表现出改善的佐剂效果。在该研究中,通过超声处理市售的磷酸铝佐剂进行纳米颗粒,导致尺寸(Z平均直径)的颗粒在200-300nm之间,零电荷点为4.5。为了防止在14天内发生的重新聚合,进行赋形剂的筛选以鉴定在生理条件下有效的稳定剂(pH7.4,290mOsm)。氨基酸苏氨酸,天冬酰胺和L-丙氨酸-1-1-氨基乙基膦酸(LAPA)稳定的超声波磷酸铝。在106天内,粒度保持在37℃的400-600nm之间。相反,精氨酸诱导强烈的重新聚集到大于1000nm的粒径。磷酸铝纳米铝的稳定性受到pH的强烈影响。主要发生在pH 7以下的聚集体7.使用模型抗原(溶菌酶)时,吸附容量是副酰胺存在的潜在相关参数,在天冬酰胺存在下略微降低。 LAPA,精氨酸,苏氨酸和天冬氨酸显着降低蛋白质吸附。通过用磷酸铝纳米铝溶液佐剂,通过小鼠免疫小鼠研究磷酸铝纳米粒子的佐剂效应。 LAPA,苏氨酸,天冬氨酸或天冬酰胺的存在没有改变白喉类毒素特异性抗体或毒素中和抗体滴度。精氨酸增加了白喉类毒素特异性抗体滴度,但不是毒素中和抗体滴度。总之,通过特定氨基酸稳定磷酸铝纳米粒子,并诱导与磷酸铝微粒相当的佐剂效果。

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