Restricted valency (NPNA)n repeats and junctional epitope-based circumsporozoite protein vaccines against Plasmodium falciparum

被引:13
作者
Langowski, Mark D. [1 ]
Khan, Farhat A. [1 ]
Savransky, Sofya [1 ]
Brown, Dallas R. [1 ]
Balasubramaniyam, Arasu [1 ]
Harrison, William B. [1 ]
Zou, Xiaoyan [2 ]
Beck, Zoltan [3 ,6 ]
Matyas, Gary R. [3 ]
Regules, Jason A. [4 ]
Miller, Robin [5 ]
Soisson, Lorraine A. [5 ]
Batchelor, Adrian H. [1 ]
Dutta, Sheetij [1 ]
机构
[1] Walter Reed Army Inst Res, Struct Vaccinol Lab, Malaria Biol Branch, Silver Spring, MD 20910 USA
[2] Naval Med Res Ctr, Malaria Dept, Silver Spring, MD USA
[3] Walter Reed Army Inst Res, US Mil HIV Res Program, Silver Spring, MD USA
[4] Walter Reed Army Inst Res, Malaria Biol Branch, Silver Spring, MD USA
[5] US Agcy Int Dev, Washington, DC 20523 USA
[6] Pfizer Inc, 401N Middletown Rd, Pearl River, NY 10965 USA
关键词
HEPARAN-SULFATE PROTEOGLYCANS; MONOPHOSPHORYL-LIPID-A; ALL-ATOM REFINEMENT; MALARIA VACCINE; STRUCTURE PREDICTION; PROTECTIVE EFFICACY; IMMUNE-RESPONSES; DOUBLE-BLIND; BINDING; SPOROZOITES;
D O I
10.1038/s41541-022-00430-y
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
The Circumsporozoite Protein (CSP) of Plasmodium falciparum contains an N-terminal region, a conserved Region I (RI), a junctional region, 25-42 copies of major (NPNA) and minor repeats followed by a C-terminal domain. The recently approved malaria vaccine, RTS,S/AS01 contains NPNAx19 and the C-terminal region of CSP. The efficacy of RTS,S against natural infection is low and short-lived, and mapping epitopes of inhibitory monoclonal antibodies may allow for rational improvement of CSP vaccines. Tobacco Mosaic Virus (TMV) was used here to display the junctional epitope (mAb CIS43), Region I (mAb 5D5), NPNAx5, and NPNAx20 epitope of CSP (mAbs 317 and 580). Protection studies in mice revealed that Region I did not elicit protective antibodies, and polyclonal antibodies against the junctional epitope showed equivalent protection to NPNAx5. Combining the junctional and NPNAx5 epitopes reduced immunogenicity and efficacy, and increasing the repeat valency to NPNAx20 did not improve upon NPNAx5. TMV was confirmed as a versatile vaccine platform for displaying small epitopes defined by neutralizing mAbs. We show that polyclonal antibodies against engineered VLPs can recapitulate the binding specificity of the mAbs and immune-focusing by reducing the structural complexity of an epitope may be superior to immune-broadening as a vaccine design approach. Most importantly the junctional and restricted valency NPNA epitopes can be the basis for developing highly effective second-generation malaria vaccine candidates.
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页数:11
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