Ross Kathleen A, Tingle April M, Senapati Sujata, Holden Kaitlyn G, Wannemuehler Michael J, Mallapragada Surya K, Narasimhan Balaji, Kohut Marian L
Nanovaccine Institute, Iowa State University, Ames, IA, 50011, USA.
Immunobiology, Iowa State University, Ames, IA, 50011, USA.
Immun Ageing. 2023 Jun 21;20(1):28. doi: 10.1186/s12979-023-00349-5.
Age-associated impairments of immune response and inflammaging likely contribute to poor vaccine efficacy. An appropriate balance between activation of immune memory and inflammatory response may be more effective in vaccines for older adults; attempts to overcome reduced efficacy have included the addition of adjuvants or increased antigenic dose. Next generation vaccine formulations may also use biomaterials to both deliver and adjuvant vaccine antigens. In the context of aging, it is important to determine the degree to which new biomaterials may enhance antigen-presenting cell (APC) functions without inducing potent inflammatory responses of APCs or other immune cell types (e.g., T cells). However, the effect of newer biomaterials on these cell types from young and older adults remains unknown.
In this pilot study, cells from young and older adults were used to evaluate the effect of novel biomaterials such as polyanhydride nanoparticles (NP) and pentablock copolymer micelles (Mi) and cyclic dinucleotides (CDN; a STING agonist) on cytokine and chemokine secretion in comparison to standard immune activators such as lipopolysaccharide (LPS) and PMA/ionomycin. The NP treatment showed adjuvant-like activity with induction of inflammatory cytokines, growth factors, and select chemokines in peripheral blood mononuclear cells (PBMCs) of both young (n = 6) and older adults (n = 4), yet the degree of activation was generally less than LPS. Treatment with Mi or CDN resulted in minimal induction of cytokines and chemokine secretion with the exception of increased IFN-α and IL-12p70 by CDN. Age-related decreases were observed across multiple cytokines and chemokines, yet IFN-α, IL-12, and IL-7 production by NP or CDN stimulation was equal to or greater than in cells from younger adults. Consistent with these results in aged humans, a combination nanovaccine composed of NP, Mi, and CDN administered to aged mice resulted in a greater percentage of antigen-specific CD4 T cells and greater effector memory cells in draining lymph nodes compared to an imiquimod-adjuvanted vaccine.
Overall, our novel biomaterials demonstrated a modest induction of cytokine secretion with a minimal inflammatory profile. These findings suggest a unique role for biomaterial nanoadjuvants in the development of next generation vaccines for older adults.
与年龄相关的免疫反应损伤和炎症衰老可能导致疫苗效力不佳。在针对老年人的疫苗中,免疫记忆激活和炎症反应之间的适当平衡可能更有效;为克服效力降低所做的尝试包括添加佐剂或增加抗原剂量。下一代疫苗制剂也可能使用生物材料来递送疫苗抗原并作为佐剂。在衰老的背景下,确定新的生物材料在何种程度上可以增强抗原呈递细胞(APC)功能而不诱导APC或其他免疫细胞类型(如T细胞)产生强烈炎症反应非常重要。然而,新型生物材料对年轻人和老年人的这些细胞类型的影响仍然未知。
在这项初步研究中,与标准免疫激活剂如脂多糖(LPS)和佛波酯/离子霉素相比,使用年轻人和老年人的细胞来评估新型生物材料如聚酐纳米颗粒(NP)、五嵌段共聚物胶束(Mi)和环二核苷酸(CDN;一种STING激动剂)对细胞因子和趋化因子分泌的影响。NP处理在年轻(n = 6)和老年成年人(n = 4)的外周血单核细胞(PBMC)中显示出类似佐剂的活性,可诱导炎性细胞因子、生长因子和特定趋化因子,但激活程度通常低于LPS。Mi或CDN处理导致细胞因子和趋化因子分泌的诱导作用最小,CDN除外,它可增加IFN-α和IL-12p70。在多种细胞因子和趋化因子中观察到与年龄相关的下降,但NP或CDN刺激产生的IFN-α、IL-12和IL-7与年轻成年人细胞中的产量相当或更高。与这些在老年人中的结果一致,与咪喹莫德佐剂疫苗相比,给老年小鼠接种由NP、Mi和CDN组成的联合纳米疫苗后,引流淋巴结中抗原特异性CD4 T细胞和效应记忆细胞的百分比更高。
总体而言,我们的新型生物材料显示出适度的细胞因子分泌诱导作用,炎症特征最小。这些发现表明生物材料纳米佐剂在开发针对老年人的下一代疫苗中具有独特作用。
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