Joint Department of Biomedical Engineering, University of North Carolina-Chapel Hill and North Carolina State University, Raleigh, NC, United States.
Comparative Medicine Institute, North Carolina State University, Raleigh, NC, United States.
Front Immunol. 2022 May 3;13:858904. doi: 10.3389/fimmu.2022.858904. eCollection 2022.
Despite the remarkable efficacy of currently approved COVID-19 vaccines, there are several opportunities for continued vaccine development against SARS-CoV-2 and future lethal respiratory viruses. In particular, restricted vaccine access and hesitancy have limited immunization rates. In addition, current vaccines are unable to prevent breakthrough infections, leading to prolonged virus circulation. To improve access, a subunit vaccine with enhanced thermostability was designed to eliminate the need for an ultra-cold chain. The exclusion of infectious and genetic materials from this vaccine may also help reduce vaccine hesitancy. In an effort to prevent breakthrough infections, intranasal immunization to induce mucosal immunity was explored. A prototype vaccine comprised of receptor-binding domain (RBD) polypeptides formulated with additional immunoadjuvants in a chitosan (CS) solution induced high levels of RBD-specific antibodies in laboratory mice after 1 or 2 immunizations. Antibody responses were durable with high titers persisting for at least five months following subcutaneous vaccination. Serum anti-RBD antibodies contained both IgG1 and IgG2a isotypes suggesting that the vaccine induced a mixed Th1/Th2 response. RBD vaccination without CS formulation resulted in minimal anti-RBD responses. The addition of CpG oligonucleotides to the CS plus RBD vaccine formulation increased antibody titers more effectively than interleukin-12 (IL-12). Importantly, generated antibodies were cross-reactive against RBD mutants associated with SARS-CoV-2 variants of concern, including alpha, beta and delta variants, and inhibited binding of RBD to its cognate receptor angiotensin converting enzyme 2 (ACE2). With respect to stability, vaccines did not lose activity when stored at either room temperature (21-22°C) or 4°C for at least one month. When delivered intranasally, vaccines induced RBD-specific mucosal IgA antibodies, which may protect against breakthrough infections in the upper respiratory tract. Altogether, data indicate that the designed vaccine platform is versatile, adaptable and capable of overcoming key constraints of current COVID-19 vaccines.
尽管目前批准的 COVID-19 疫苗具有显著的疗效,但针对 SARS-CoV-2 和未来致命呼吸道病毒,仍有几个机会可以继续开发疫苗。特别是,疫苗接种的限制和犹豫导致免疫接种率有限。此外,目前的疫苗无法预防突破性感染,导致病毒持续传播。为了改善接种途径,设计了一种具有增强热稳定性的亚单位疫苗,以消除对超冷链的需求。该疫苗排除了传染性和遗传物质,这也可能有助于减少疫苗犹豫。为了预防突破性感染,探索了鼻内免疫以诱导黏膜免疫。一种由受体结合域(RBD)多肽组成的原型疫苗,与壳聚糖(CS)溶液中的其他免疫佐剂一起配制,在经过 1 或 2 次免疫后,可在实验室小鼠中诱导高水平的 RBD 特异性抗体。抗体反应具有持久性,在皮下接种后至少 5 个月内保持高滴度。血清抗 RBD 抗体包含 IgG1 和 IgG2a 同种型,表明疫苗诱导了混合的 Th1/Th2 反应。没有 CS 制剂的 RBD 疫苗接种导致最小的抗 RBD 反应。CpG 寡核苷酸的添加到 CS 加 RBD 疫苗配方中比白细胞介素-12(IL-12)更有效地增加抗体滴度。重要的是,产生的抗体与与 SARS-CoV-2 变体相关的 RBD 突变体交叉反应,包括 alpha、beta 和 delta 变体,并抑制 RBD 与其同源受体血管紧张素转换酶 2(ACE2)的结合。就稳定性而言,疫苗在室温(21-22°C)或 4°C 下储存至少一个月时不会失去活性。当经鼻内递送时,疫苗会诱导 RBD 特异性黏膜 IgA 抗体,这可能有助于预防上呼吸道的突破性感染。总之,数据表明,设计的疫苗平台具有多功能性、适应性,并能够克服当前 COVID-19 疫苗的关键限制。
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