In a groundbreaking bioRxiv* study, US researchers demonstrate the capability of next-generation bivalent human adenovirus serotype 5 (hAd5) vaccine for inducing both cellular and humoral immunity against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) – using both an S protein sequence optimized for cell surface expression and a conserved nucleocapsid antigen designed to be transported to the endosomal subcellular compartment.
.jpg "Colorized scanning electron micrograph of a cell heavily infected with SARS-CoV-2 virus particles (yellow), isolated from a patient sample. Image captured at the NIAID Integrated Research Facility (IRF) in Fort Detrick, Maryland. Credit: NIAI")
Colorized scanning electron micrograph of a cell heavily infected with SARS-CoV-2 virus particles (yellow), isolated from a patient sample. Image captured at the NIAID Integrated Research Facility (IRF) in Fort Detrick, Maryland. Credit: NIAI
This news article was a review of a preliminary scientific report that had not undergone peer-review at the time of publication. Since its initial publication, the scientific report has now been peer reviewed and accepted for publication in a Scientific Journal. Links to the preliminary and peer-reviewed reports are available in the Sources section at the bottom of this article. View Sources
In response to the ongoing health crisis brought by the coronavirus disease (COVID-19) pandemic, the quest for a safe and effective vaccine that will elicit durable immune responses is of utmost importance.
It is known that SARS-CoV-2 utilizes S protein and its receptor-binding domain (RBD) to interact with angiotensin-converting enzyme 2 (ACE2) to enter human cells. Consequently, most vaccines under development target S protein in order to elicit the production of antibodies against RBD, but also to adequately steer T cell immune response.
Notwithstanding the urgent need for rapid SARS-CoV-2 vaccine development, reliance on only one antigen cargo or immunological pathway (as currently seen in the monovalent vaccines under development) is not without risks. For example, new viral strains with mutations in S protein may emerge and render developed vaccines ineffective.
In order to overcome the aforementioned risk and provide additional antigens, the researchers from ImmunityBio Inc. and Icahn School of Medicine at Mount Sinai in New York have added an optimized N protein sequence, which has a role in viral replication, particle assembly, and release.
![The SARS-CoV-2 virus, spike, the hAd5 [E1-, E2b-, E3-] vector and vaccine candidate constructs. (a) Trimeric spike (S) protein ( ) is displayed on the viral surface; the nucleocapsid (N) protein ( ) is associated with the viral RNA. (b) The Receptor Binding Domain (RBD) is within the S1 region, followed by other functional regions, the transmembrane domain (TM) and the C-terminus (CT), which is within the virus. (c) The second-generation human adenovirus serotype 5 (hAd5) vector used has the E1, E2b, and E3 regions deleted. Constructs are shown for (d) S wild type (S-WT), (e) S-RBD with the Enhanced T-cell Stimulation Domain (S RBD-ETSD), (f) S-Fusion, (g) N-ETSD, and (h) bivalent hAd5 S-Fusion + N-ETSD; LP – Leader peptide.](https://d2jx2rerrg6sh3.cloudfront.net/image-handler/picture/2020/8/%402020.07.29.227595v1.jpg "The SARS-CoV-2 virus, spike, the hAd5 [E1-, E2b-, E3-] vector and vaccine candidate constructs. (a) Trimeric spike (S) protein ( ) is displayed on the viral surface; the nucleocapsid (N) protein ( ) is associated with the viral RNA. (b) The Receptor Binding Domain (RBD) is within the S1 region, followed by other functional regions, the transmembrane domain (TM) and the C-terminus (CT), which is within the virus. (c) The second-generation human adenovirus serotype 5 (hAd5) vector used has the E1, E2b, and E3 regions deleted. Constructs are shown for (d) S wild type (S-WT), (e) S-RBD with the Enhanced T-cell Stimulation Domain (S RBD-ETSD), (f) S-Fusion, (g) N-ETSD, and (h) bivalent hAd5 S-Fusion + N-ETSD; LP – Leader peptide.")
The SARS-CoV-2 virus, spike, the hAd5 [E1-, E2b-, E3-] vector and vaccine candidate constructs. (a) Trimeric spike (S) protein ( ▼) is displayed on the viral surface; the nucleocapsid (N) protein (⬤) is associated with the viral RNA. (b) The Receptor Binding Domain (RBD) is within the S1 region, followed by other functional regions, the transmembrane domain (TM) and the C-terminus (CT), which is within the virus. (c) The second-generation human adenovirus serotype 5 (hAd5) vector used has the E1, E2b, and E3 regions deleted. Constructs are shown for (d) S wild type (S-WT), (e) S-RBD with the Enhanced T-cell Stimulation Domain (S RBD-ETSD), (f) S-Fusion, (g) N-ETSD, and (h) bivalent hAd5 S-Fusion + N-ETSD; LP – Leader peptide.
A next-generation recombinant vector
In short, the vaccine platform utilized in this study represents a next-generation recombinant human adenovirus serotype 5 (hAd5) vector that harbors deletions in the E1, E2b, and E3 gene regions.
Such vector can primarily be distinguished from other first-generation [E1-, E3-] recombinant Ad5 platforms by having additional deletions in the early gene 2b (E2b) region, which remove the expression of the viral DNA polymerase.
Since these deletions make the hAd5 platform efficacious even in the presence of existing adenovirus immunity, it can enable relatively long-term antigen expression without significant induction of anti-vector immunity. Even more important, this next generation Ad vector has shown to be safe in more than 125 patients with solid tumors.
After vector optimization, this innovative vaccine construct design basically comprised an S-Fusion + N-ETSD sequence. More specifically, the researchers have first designed an enhanced T-cell Stimulation Domain (ETSD) to nucleocapsid antigen (N) to allow the necessary processing and presentation.
Additionally, they have optimized the wild type S protein "S Fusion sequence" to display the highly antigenic RBD region of S protein on the cell surface. This was done to increase the stability and the likelihood of native folding.
Greater protection against SARS-CoV-2
"A key finding of our construct is that N-ETSD, which we show is directed to the endosomal/lysosomal compartment, elicits a CD4+ response, a necessity for induction of memory T cells and helper cells for B cell antibody production", study authors summarize their findings.
The T-cell response to both S and N antigens expressed by hAd5 S-Fusion + N-ETSD included the production of multiple cytokines, such as interferon-gamma and tumor necrosis factor-alpha, which is somewhat consistent with successful antimicrobial immunity against bacterial and viral infections.
Likewise, such polycytokine T-cell responses to SARS-CoV-2 N protein are in line with recovered COVID-19 patients, indicating that the bivalent hAd5 S-Fusion + N-ETSD vaccine may provide vaccine subjects with greater protection against SARS-CoV-2.
In contrast to N protein, the S protein (here expressed as S-Fusion with enhanced RBD cell-surface expression and conformational integrity) generated CD8+ T cells predominantly in this study. Finally, both the T-cell and antibody immune responses to S and N demonstrated a T-helper 1 (Th1) bias.
Robust T and B cell response
"Our results confirmed our vaccine design goal, showing that S-Fusion induced elevated levels of antigen-specific T-cell responses against S compared to wild-type spike protein," emphasize study authors in their bioRxiv paper.
Moreover, the potency of the antibody response generated after vaccinating with hAd5 S-Fusion + N-ETSD revealed evidence of a high neutralization effect, which was achieved even at a high dilution factor.
"Based on these findings, we are advancing this next generation bivalent hAd5 S-Fusion + N-ETSD vaccine as our lead clinical candidate to test for its ability to provide robust, durable cell-mediated and humoral immunity against SARS-CoV-2 infection", conclude study authors.
Additional studies exploring this vaccine construct in oral, sublingual, and intranasal formulations to induce mucosal immunity (alongside cell-mediated and humoral immunity) are already underway. This is another breakthrough in the quest for the current 'Holy Grail' in biomedicine – to discover an ideal COVID-19 vaccine that will generate long-term T and B cell memory response.
This news article was a review of a preliminary scientific report that had not undergone peer-review at the time of publication. Since its initial publication, the scientific report has now been peer reviewed and accepted for publication in a Scientific Journal. Links to the preliminary and peer-reviewed reports are available in the Sources section at the bottom of this article. View Sources
Journal references:
- Preliminary scientific report.
Rice, A. et al. (2020). A Next Generation Bivalent Human Ad5 COVID-19 Vaccine Delivering Both Spike and Nucleocapsid Antigens Elicits Th1 Dominant CD4+, CD8+ T-cell and Neutralizing Antibody Responses. bioRxiv. https://doi.org/10.1101/2020.07.29.227595.
- Peer reviewed and published scientific report.
Gabitzsch, Elizabeth, Jeffrey T. Safrit, Mohit Verma, Adrian Rice, Peter Sieling, Lise Zakin, Annie Shin, et al. 2021. “Dual-Antigen COVID-19 Vaccine Subcutaneous Prime Delivery with Oral Boosts Protects NHP against SARS-CoV-2 Challenge.” Frontiers in Immunology 12 (September). https://doi.org/10.3389/fimmu.2021.729837. https://www.frontiersin.org/articles/10.3389/fimmu.2021.729837/full.
Article Revisions
- Mar 23 2023 - The preprint preliminary research paper that this article was based upon was accepted for publication in a peer-reviewed Scientific Journal. This article was edited accordingly to include a link to the final peer-reviewed paper, now shown in the sources section.
Study shows potential for universal flu vaccine with broad antibody response