CCL28 Enhances HSV-2 gB-Specific Th1-Polarized Immune Responses against Lethal Vaginal Challenge in Mice.
Yan YanKai HuMing FuXu DengXinmeng GuanSukun LuoMudan ZhangYalan LiuQinxue HuPublished in: Vaccines (2022)
Plasmid DNA (pDNA) represents a promising "genetic vaccine platform" capable of overcoming major histocompatibility complex barriers. We previously demonstrated that low-to-moderate doses of mucosae-associated epithelial chemokine (MEC or CCL28) as an immunomodulatory adjuvant can trigger effective and long-lasting systemic and mucosal HSV-2 gD-specific immune responses, whereas mice immunized with gD in combination with high-dose CCL28 showed toxicity and lost their immunoprotective effects after lethal HSV-2 challenge. The exact causes underlying high-dose, CCL28-induced lesions remain unknown. In an intramuscularly immunized mouse model, we investigated the immune-enhancement mechanisms of low-dose CCL28 as a molecular adjuvant combined with the relatively weak immunogen HSV-2 gB. Compared with the plasmid gB antigen group, we found that a low-dose of plasmid CCL28 (pCCL28) codelivered with pgB induced increased levels of gB-specific serum IgG and vaginal fluid IgA, serum neutralizing antibodies (NAb), Th1-polarized IgG2a, and cytokine IL-2 (>5-fold). Furthermore, low-dose pCCL28 codelivery with pgB enhanced CCL28/CCR10-axis responsive CCR10 - plus CCR10 + B-cell (~1.2-fold) and DC pools (~4-fold) in the spleen, CCR10 - plus CCR10 + T-cell pools (~2-fold) in mesenteric lymph nodes (MLNs), and the levels of IgA-ASCs in colorectal mucosal tissues, leading to an improved protective effect against a lethal dose of HSV-2 challenge. Findings in this study provide a basis for the development of CCL28-adjuvant vaccines against viral mucosal infections.
Keyphrases
- low dose
- high dose
- liver injury
- liver fibrosis
- drug induced
- dendritic cells
- immune response
- escherichia coli
- regulatory t cells
- early stage
- herpes simplex virus
- mouse model
- stem cell transplantation
- lymph node
- diabetic rats
- metabolic syndrome
- type diabetes
- single molecule
- high glucose
- high resolution
- advanced non small cell lung cancer
- single cell
- skeletal muscle
- high throughput
- rectal cancer
- molecular dynamics
- neoadjuvant chemotherapy