A Highly Immunogenic and Protective Middle East Respiratory Syndrome Coronavirus Vaccine Based on a Recombinant Measles Virus Vaccine Platform

Author:

Malczyk Anna H.12,Kupke Alexandra34,Prüfer Steffen1,Scheuplein Vivian A.1,Hutzler Stefan1,Kreuz Dorothea5,Beissert Tim6,Bauer Stefanie5,Hubich-Rau Stefanie7,Tondera Christiane1,Eldin Hosam Shams34,Schmidt Jörg34,Vergara-Alert Júlia34,Süzer Yasemin1,Seifried Janna1,Hanschmann Kay-Martin8,Kalinke Ulrich910,Herold Susanne11,Sahin Ugur67,Cichutek Klaus12,Waibler Zoe25,Eickmann Markus34,Becker Stephan34,Mühlebach Michael D.12

Affiliation:

1. Oncolytic Measles Viruses and Vaccine Vectors, Paul-Ehrlich-Institut, Langen, Germany

2. German Center for Infection Research, Langen, Germany

3. Institut für Virologie, Philipps Universität Marburg, Marburg, Germany

4. German Center for Infection Research, Marburg, Germany

5. Novel Vaccination Strategies and Early Immune Responses, Paul-Ehrlich-Institut, Langen, Germany

6. TRON gGmbH, Mainz, Germany

7. Universitätsmedizin Mainz, Mainz, Germany

8. Biostatistics, Paul-Ehrlich-Institut, Langen, Germany

9. Institute for Experimental Infection Research, TWINCORE, Centre for Experimental and Clinical Infection Research, Hannover, Germany

10. German Center for Infection Research, Hannover, Germany

11. Universities Gießen and Marburg Lung Center, Department of Internal Medicine II, Section of Infectious Diseases, Giessen, Germany

Abstract

ABSTRACT In 2012, the first cases of infection with the Middle East respiratory syndrome coronavirus (MERS-CoV) were identified. Since then, more than 1,000 cases of MERS-CoV infection have been confirmed; infection is typically associated with considerable morbidity and, in approximately 30% of cases, mortality. Currently, there is no protective vaccine available. Replication-competent recombinant measles virus (MV) expressing foreign antigens constitutes a promising tool to induce protective immunity against corresponding pathogens. Therefore, we generated MVs expressing the spike glycoprotein of MERS-CoV in its full-length (MERS-S) or a truncated, soluble variant of MERS-S (MERS-solS). The genes encoding MERS-S and MERS-solS were cloned into the vaccine strain MV vac2 genome, and the respective viruses were rescued (MV vac2 -CoV-S and MV vac2 -CoV-solS). These recombinant MVs were amplified and characterized at passages 3 and 10. The replication of MV vac2 -CoV-S in Vero cells turned out to be comparable to that of the control virus MV vac2 -GFP (encoding green fluorescent protein), while titers of MV vac2 -CoV-solS were impaired approximately 3-fold. The genomic stability and expression of the inserted antigens were confirmed via sequencing of viral cDNA and immunoblot analysis. In vivo , immunization of type I interferon receptor-deficient (IFNAR −/− )-CD46Ge mice with 2 × 10 5 50% tissue culture infective doses of MV vac2 -CoV-S(H) or MV vac2 -CoV-solS(H) in a prime-boost regimen induced robust levels of both MV- and MERS-CoV-neutralizing antibodies. Additionally, induction of specific T cells was demonstrated by T cell proliferation, antigen-specific T cell cytotoxicity, and gamma interferon secretion after stimulation of splenocytes with MERS-CoV-S presented by murine dendritic cells. MERS-CoV challenge experiments indicated the protective capacity of these immune responses in vaccinated mice. IMPORTANCE Although MERS-CoV has not yet acquired extensive distribution, being mainly confined to the Arabic and Korean peninsulas, it could adapt to spread more readily among humans and thereby become pandemic. Therefore, the development of a vaccine is mandatory. The integration of antigen-coding genes into recombinant MV resulting in coexpression of MV and foreign antigens can efficiently be achieved. Thus, in combination with the excellent safety profile of the MV vaccine, recombinant MV seems to constitute an ideal vaccine platform. The present study shows that a recombinant MV expressing MERS-S is genetically stable and induces strong humoral and cellular immunity against MERS-CoV in vaccinated mice. Subsequent challenge experiments indicated protection of vaccinated animals, illustrating the potential of MV as a vaccine platform with the potential to target emerging infections, such as MERS-CoV.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

Reference90 articles.

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