Tailoring Subunit Vaccine Immunity with Adjuvant Combinations and Delivery Routes Using the Middle East Respiratory Coronavirus (MERS-CoV) Receptor-Binding Domain as an Antigen

Lan, Jiaming; Deng, Yao; Chen, Hong; Lu, Guangwen; Wang, Wen; Guo, Xiaojuan; Zhang, Lu; Gao, George F.; Tan, Wenjie

doi:10.1371/journal.pone.0112602

Cited by 74 publications

(108 citation statements)

References 35 publications

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“…Other studies showed similar findings of antigenic property of a rRBD protein of MERS-CoV spike (S) [78,[81][82][83]. Moreover, three adjuvants-alum, IFA, CpG and poly (I:C)-in rRBD subunit vaccines were effective in producing RBD-specific cellular and humoral immune responses [84]. Since the N-terminus RBD of (S) glycoprotein is conserved in currently circulating MERS-CoV strains, this terminus is considered a possible vaccine candidate [85].…”

Section: Currently Available Antiviral Agents and Vaccinessupporting

confidence: 55%

An update on Middle East respiratory syndrome: 2 years later

Al‐Tawfiq

Memish

2015

Expert Review of Respiratory Medicine

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Section: Currently Available Antiviral Agents and Vaccinessupporting

confidence: 55%

An update on Middle East respiratory syndrome: 2 years later

Al‐Tawfiq

Memish

2015

Expert Review of Respiratory Medicine

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“…Further, passive immunotherapy using convalescent phase human plasma is being considered in MERS patients after its success in animal models . However, studies also demonstrate that MERS-CoV S protein-derived vaccines induce specific CD8 þ T-cell and virus-neutralizing antibodies, which could contribute to complete protection against MERS-CoV in animal models (Lan et al, 2014;Volz et al, 2015). Based on the investigations of immune memory against SARS-CoV in follow-up studies of recovered patients (discussed above), T-cell responses can provide robust long-term memory and possess a considerable potential for cross-reactivity with heterotypic coronaviruses.…”

Section: Perspectivementioning

confidence: 99%

T-cell immunity of SARS-CoV: Implications for vaccine development against MERS-CoV

et al. 2017

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Over 12 years have elapsed since severe acute respiratory syndrome (SARS) triggered the first global alert for coronavirus infections. Virus transmission in humans was quickly halted by public health measures and human infections of SARS coronavirus (SARS-CoV) have not been observed since. However, other coronaviruses still pose a continuous threat to human health, as exemplified by the recent emergence of Middle East respiratory syndrome (MERS) in humans. The work on SARS-CoV widens our knowledge on the epidemiology, pathophysiology and immunology of coronaviruses and may shed light on MERS coronavirus (MERS-CoV). It has been confirmed that T-cell immunity plays an important role in recovery from SARS-CoV infection. Herein, we summarize T-cell immunological studies of SARS-CoV and discuss the potential cross-reactivity of the SARS-CoV-specific immunity against MERS-CoV, which may provide useful recommendations for the development of broad-spectrum vaccines against coronavirus infections.

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“…Soon after the identification of MERS‐CoV, several groups developed vaccines for preclinical testing. Recombinant receptor‐binding domain (rRBD), residues 367 to 606 of MERS‐CoV spike (S) protein, has been expressed and tested in mice as a vaccine . It induced RBD‐specific immunoglobulin G (IgG) antibody when it was tested with various adjuvants such as alum, CpG, P(I:C), or IFA.…”

Section: Current Mers‐cov Vaccine Candidates Under Developmentmentioning

confidence: 99%

“…It induced RBD‐specific immunoglobulin G (IgG) antibody when it was tested with various adjuvants such as alum, CpG, P(I:C), or IFA. However, only RBD with alum or with alum and CpG was able to induce nAb . This vaccine was then taken further and tested in Rhesus macaques at 2 different dosages, in 3 homologous vaccinations regimen, with 8‐ and 17‐week intervals.…”

Section: Current Mers‐cov Vaccine Candidates Under Developmentmentioning

confidence: 99%

Vaccines against Middle East respiratory syndrome coronavirus for humans and camels

Alharbi

2016

Reviews in Medical Virology

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Middle East respiratory syndrome coronavirus (MERS-CoV) is caused by a novel betacoronavirus that was isolated in late 2012 in Saudi Arabia. The viral infections have been reported in more than 1700 humans, ranging from asymptomatic or mild cases to severe pneumonia with a mortality rate of 40%. It is well documented now that dromedary camels contract the infection and shed the virus without notable symptoms, and such animals had been infected by at least the early 1980s. The mechanism of camel to human transmission is still not clear, but several primary cases have been associated with camel contact. There is no approved antiviral drug or vaccine against MERS-CoV despite the active research in this area. Vaccine candidates have been developed using various platforms and regimens and have been tested in several animal models. Here, this article reviews the published studies on MERS-CoV vaccines with more focus on vaccines tested in large animals, including camels. It is foreseeable that the 1-health approach could be the best way of tackling the MERS-CoV endemic in the Arabian Peninsula, by using the mass vaccination of camels in the affected areas to block camel to human transmission. Camel vaccines can be developed in a faster time with fewer regulations and lower costs and could clear this virus from the Arabian Peninsula if accompanied by efficient public health measures.

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Tailoring Subunit Vaccine Immunity with Adjuvant Combinations and Delivery Routes Using the Middle East Respiratory Coronavirus (MERS-CoV) Receptor-Binding Domain as an Antigen

Cited by 74 publications

References 35 publications

An update on Middle East respiratory syndrome: 2 years later

An update on Middle East respiratory syndrome: 2 years later

T-cell immunity of SARS-CoV: Implications for vaccine development against MERS-CoV

Vaccines against Middle East respiratory syndrome coronavirus for humans and camels

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