Inserm, U955, 8 rue du Général Sarrail, Créteil, 94010, France.
BMC Med. 2013 Apr 4;11:99. doi: 10.1186/1741-7015-11-99.
Long-term biodistribution of nanomaterials used in medicine is largely unknown. This is the case for alum, the most widely used vaccine adjuvant, which is a nanocrystalline compound spontaneously forming micron/submicron-sized agglomerates. Although generally well tolerated, alum is occasionally detected within monocyte-lineage cells long after immunization in presumably susceptible individuals with systemic/neurologic manifestations or autoimmune (inflammatory) syndrome induced by adjuvants (ASIA).
On the grounds of preliminary investigations in 252 patients with alum-associated ASIA showing both a selective increase of circulating CCL2, the major monocyte chemoattractant, and a variation in the CCL2 gene, we designed mouse experiments to assess biodistribution of vaccine-derived aluminum and of alum-particle fluorescent surrogates injected in muscle. Aluminum was detected in tissues by Morin stain and particle induced X-ray emission) (PIXE) Both 500 nm fluorescent latex beads and vaccine alum agglomerates-sized nanohybrids (Al-Rho) were used.
Intramuscular injection of alum-containing vaccine was associated with the appearance of aluminum deposits in distant organs, such as spleen and brain where they were still detected one year after injection. Both fluorescent materials injected into muscle translocated to draining lymph nodes (DLNs) and thereafter were detected associated with phagocytes in blood and spleen. Particles linearly accumulated in the brain up to the six-month endpoint; they were first found in perivascular CD11b+ cells and then in microglia and other neural cells. DLN ablation dramatically reduced the biodistribution. Cerebral translocation was not observed after direct intravenous injection, but significantly increased in mice with chronically altered blood-brain-barrier. Loss/gain-of-function experiments consistently implicated CCL2 in systemic diffusion of Al-Rho particles captured by monocyte-lineage cells and in their subsequent neurodelivery. Stereotactic particle injection pointed out brain retention as a factor of progressive particle accumulation.
Nanomaterials can be transported by monocyte-lineage cells to DLNs, blood and spleen, and, similarly to HIV, may use CCL2-dependent mechanisms to penetrate the brain. This occurs at a very low rate in normal conditions explaining good overall tolerance of alum despite its strong neurotoxic potential. However, continuously escalating doses of this poorly biodegradable adjuvant in the population may become insidiously unsafe, especially in the case of overimmunization or immature/altered blood brain barrier or high constitutive CCL-2 production.
在医学中使用的纳米材料的长期生物分布在很大程度上是未知的。明矾就是这种情况,明矾是最广泛使用的疫苗佐剂,它是一种自发形成微米/亚微米大小团聚物的纳米晶化合物。虽然通常具有良好的耐受性,但在具有全身/神经表现或由佐剂引起的自身免疫(炎症)综合征的易感个体中,明矾在免疫后很长时间内偶尔会在单核细胞谱系细胞中被检测到。
基于在 252 名与明矾相关的 ASIA 患者的初步研究,这些患者均表现为循环 CCL2(主要的单核细胞趋化因子)选择性增加,以及 CCL2 基因发生变化,我们设计了小鼠实验来评估疫苗衍生的铝和注射到肌肉中的明矾颗粒荧光代用品的生物分布。通过 Morin 染色和粒子诱导 X 射线发射 (PIXE) 检测组织中的铝。使用了 500nm 荧光乳胶珠和疫苗明矾纳米杂化物 (Al-Rho) 大小的纳米杂交体。
肌肉内注射含明矾的疫苗与远处器官(如脾脏和大脑)中铝沉积物的出现有关,在注射后一年仍能检测到。两种注射到肌肉中的荧光材料均转移到引流淋巴结 (DLNs),然后在血液和脾脏中与吞噬细胞一起被检测到。颗粒在线性积累在大脑中,直到六个月的终点;它们首先在血管周围的 CD11b+细胞中发现,然后在小胶质细胞和其他神经细胞中发现。DLN 消融显著减少了生物分布。直接静脉内注射后未观察到脑转移,但在慢性改变血脑屏障的小鼠中显著增加。CCL2 在单核细胞谱系细胞捕获的 Al-Rho 颗粒的全身扩散及其随后的神经传递中具有重要作用。立体定向颗粒注射指出脑保留是颗粒逐渐积累的一个因素。
纳米材料可以被单核细胞谱系细胞运送到 DLNs、血液和脾脏,并且与 HIV 类似,可能使用 CCL2 依赖的机制穿透大脑。在正常情况下,这种情况发生的概率非常低,这解释了尽管明矾具有很强的神经毒性潜力,但仍能很好地耐受。然而,这种生物降解性差的佐剂在人群中的剂量不断增加可能会变得潜在不安全,特别是在过度免疫或不成熟/改变的血脑屏障或高组成型 CCL-2 产生的情况下。
Zotero 插件