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Uric acid and the vaccine adjuvant activity of aluminium (oxy)hydroxide nanoparticles

机译:尿酸和铝(氧化氢)氢氧化物纳米颗粒的疫苗佐剂活性

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In an effort to improve the adjuvanticity of insoluble aluminium salts, we discovered that the adjuvant activity of aluminium salt nanoparticles is significantly stronger than aluminium salt microparticles, likely related to nanoparticle’s stronger ability to directly activate NACHT, LRR and PYD domains-containing protein 3 (NLRP3) inflammasome as the nanoparticles are more efficiently taken up by phagocytic cells. Endogenous signals such as uric acid from cell damage or death caused by the cytotoxicity of aluminium salts are thought to indirectly activate inflammasome, prompting us to hypothesise that the potent adjuvant activity of aluminium salt nanoparticles is also related to their ability to stimulate uric acid production. In the present study, we prepared aluminium (oxy)hydroxide nanoparticles (~ 30–100 nm) and microparticles (X 50 , 9.43 μm) and showed that intraperitoneal injection of mice with the nanoparticles, absorbed with ovalbumin, led to a significant increase in uric acid level in the peritoneal lavage, whereas the microparticles did not. The aluminium (oxy)hydroxide nanoparticles’ ability to stimulate uric acid production was also confirmed in cell culture. We concluded that the stronger adjuvant activity of insoluble aluminium (oxy)hydroxide nanoparticles, relative to microparticles, may be attributed at least in part to their stronger ability to induce endogenous danger signals such as uric acid. ? 2018 Informa UK Limited, trading as Taylor & Francis Group.
机译:为了提高不溶性铝盐的佐性,我们发现铝盐纳米粒子的佐剂活性比铝盐微粒显着强,可能与纳米粒子的直接激活含Nacht,LRR和PyD结构域的蛋白质3的能力有关( NLRP3)氨基颗粒作为植物细胞更有效地吸收的NLRP3。诸如由铝盐细胞毒性引起的细胞损伤或死亡的内源性信号被认为是间接激活炎症,促使我们假设铝盐纳米粒子的有效佐剂活性与其刺激尿酸产生的能力也有关。在本研究中,我们制备了铝(氧)氢氧化铝纳米颗粒(〜30-100nm)和微粒(×50,9.43μm)并显示腹腔注射用纳米胺吸收的纳米颗粒,导致显着增加腹膜灌洗液中的尿酸水平,而微粒没有。在细胞培养中也证实了铝(氧)氢氧化铝纳米粒子刺激尿酸产生的能力。我们得出结论,相对于微粒的不溶性铝(氧氧化铝纳米粒子的佐剂活性较强,可至少部分地归因于诱导尿酸如尿酸的内源性危险信号的较强能力。还2018年Informa UK Limited,贸易为泰勒&弗朗西斯集团。

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