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首页> 外文期刊>Clinical & developmental immunology. >Parenterally Administered Norovirus GII.4 Virus-Like Particle Vaccine Formulated with Aluminum Hydroxide or Monophosphoryl Lipid A Adjuvants Induces Systemic but Not Mucosal Immune Responses in Mice
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Parenterally Administered Norovirus GII.4 Virus-Like Particle Vaccine Formulated with Aluminum Hydroxide or Monophosphoryl Lipid A Adjuvants Induces Systemic but Not Mucosal Immune Responses in Mice

机译:肠胃外给药的诺病毒GII.4与氢氧化铝或单磷虾脂质配制的病毒样颗粒疫苗辅助剂诱导小鼠的系统性但不是粘膜免疫应答

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Norovirus (NoV) is a main cause of acute gastroenteritis across all ages worldwide. NoV vaccine candidates currently in clinical trials are based on noninfectious highly immunogenic virus-like particles (VLPs) delivered intramuscularly (IM). Since NoV is an enteric pathogen, it is likely that mucosal immunity has a significant role in protection from infection in the intestine. Due to the fact that IM delivery of NoV VLPs does not generate mucosal immunity, we investigated whether NoV genotype GII.4 VLPs coadministered with aluminum hydroxide (Al(OH)_(3)) or monophosphoryl lipid A (MPLA) would induce mucosal antibodies in mice. Systemic as well as mucosal IgG and IgA antibodies in serum and intestinal and nasal secretions were measured. As expected, strong serum IgG, IgG1, and IgG2a antibodies as well as a dose sparing effect were induced by both Al(OH)_(3) and MPLA, but no mucosal IgA antibodies were detected. In contrast, IN immunization with GII.4 VLPs without an adjuvant induced systemic as well as mucosal IgA antibody response. These results indicate that mucosal delivery of NoV VLPs is needed for induction of mucosal responses.
机译:诺罗病毒(11月)是全球所有年龄段的急性胃肠炎的主要原因。目前在临床试验中的11月疫苗候选者基于肌肉内(IM)递送的非浮选高度免疫原性病毒样颗粒(VLP)。自11月是一种肠溶病原体,可能粘膜免疫可能在肠道中的感染方面具有重要作用。由于11月vlps的Im递送不会产生粘膜免疫力,我们研究了11种基因型GII.4 VLP是否共用氢氧化铝(Al(OH)_(3))或单磷虾脂质A(MPLA)将诱导粘膜抗体在老鼠中。测定了血清和肠道分泌物中的系统性以及粘膜IgG和IgA抗体。通过预期的,通过Al(OH)_(3)和MPLA诱导强血清IgG,IgG1和IgG2A抗体以及剂量保留效果,但不检测到粘膜IgA抗体。相反,在没有佐剂诱导的系统和粘膜IgA抗体反应的情况下,在没有GII.4 VLP的免疫中。这些结果表明,粘膜反应诱导粘膜反应需要11月VLP的粘膜递送。

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