A subcutaneously injected UV-inactivated SARS coronavirus vaccine elicits systemic humoral immunity in mice

doi:10.1093/intimm/dxh143

International Immunology Advance Access originally published online on August 16, 2004
International Immunology 2004 16(10):1423-1430; doi:10.1093/intimm/dxh143

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A subcutaneously injected UV-inactivated SARS coronavirus vaccine elicits systemic humoral immunity in mice

Naomi Takasuka¹, Hideki Fujii¹, Yoshimasa Takahashi¹, Masataka Kasai¹, Shigeru Morikawa², Shigeyuki Itamura⁴, Koji Ishii³, Masahiro Sakaguchi¹, Kazuo Ohnishi¹, Masamichi Ohshima¹, Shu-ichi Hashimoto¹, Takato Odagiri⁴, Masato Tashiro⁴, Hiroshi Yoshikura⁵, Toshitada Takemori¹ and Yasuko Tsunetsugu-Yokota¹

¹ Department of Immunology, ² First, ³ Second and ⁴ Third Departments of Virology, ⁵ National Institute of Infectious Diseases, Toyama 1-23-1, Shinjuku-ku, Tokyo 162-8640, Japan

Correspondence to: Y. Tsunetsugu-Yokota; E-mail: yyokota{at}nih.go.jp

The recent emergence of severe acute respiratory syndrome (SARS)was caused by a novel coronavirus, SARS-CoV. It spread rapidlyto many countries and developing a SARS vaccine is now urgentlyrequired. In order to study the immunogenicity of UV-inactivatedpurified SARS-CoV virion as a vaccine candidate, we subcutaneouslyimmunized mice with UV-inactivated SARS-CoV with or withoutan adjuvant. We chose aluminum hydroxide gel (alum) as an adjuvant,because of its long safety history for human use. We observedthat the UV-inactivated SARS-CoV virion elicited a high levelof humoral immunity, resulting in the generation of long-termantibody secreting and memory B cells. With the addition ofalum to the vaccine formula, serum IgG production was augmentedand reached a level similar to that found in hyper-immunizedmice, though it was still insufficient to elicit serum IgA antibodies.Notably, the SARS-CoV virion itself was able to induce long-termantibody production even without an adjuvant. Anti-SARS-CoVantibodies elicited in mice recognized both the spike and nucleocapsidproteins of the virus and were able to neutralize the virus.Furthermore, the UV-inactivated virion induced regional lymphnode T-cell proliferation and significant levels of cytokineproduction (IL-2, IL-4, IL-5, IFN- ${gamma}$ and TNF- ${alpha}$ ) upon restimulationwith inactivated SARS-CoV virion in vitro. Thus, a whole killedvirion could serve as a candidate antigen for a SARS vaccineto elicit both humoral and cellular immunity.

Keywords: alum, cellular immunity, neutralizing antibody, parenteral administration, vaccination

Transmitting editor: K. Sugamura

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