Abstract
Since 2010, newly identified variants of porcine epidemic diarrhoea virus (PEDV) have caused high mortality in neonatal piglets which has devastated the swine industry. The spike (S) glycoprotein of PEDV contains multiple neutralizing epitopes and is a major target for PEDV neutralization and vaccine development. To understand the antigenicity of the new PEDV variant, we characterized the neutralizing epitopes of a new genotype 2b PEDV isolate from Taiwan, PEDV Pintung 52 (PEDV-PT), by the generation of neutralizing monoclonal antibodies (NmAbs). Two NmAbs, P4B-1, and E10E-1–10 that recognized the ectodomain of the full-length recombinant PEDV S protein and exhibited neutralizing ability against the PEDV-PT virus were selected. Recombinant truncated S proteins were used to identify the target sequences for the NmAbs and P4B-1 was shown to recognize the C-terminus of CO-26K equivalent epitope (COE) at amino acids (a.a.) 575–639 of the PEDV S. Interestingly, E10E-1–10 could recognize a novel neutralizing epitope at a.a. 435–485 within the S1A domain of the PEDV S protein, whose importance and function are yet to be determined. Moreover, both NmAbs could not bind to linearized S proteins, indicating that only conformational epitopes are recognized. This data could improve our understanding of the antigenic structures of the PEDV S protein and facilitate future development of novel epitope-based vaccines.
Highlights
porcine epidemic diarrhoea virus (PEDV) is a single-stranded RNA virus, approximately 28 kb in size, which belongs to the genus Alphacoronavirus[8]
Several sequences of the new variant PEDV spike genes have been decoded[6,21] and multiple domain architectures of the PEDV S protein have been predicted by three-dimensional structures of alphacoronaviruses[16], the effects of genetic mutations on the antigenicity of PEDV remains poorly understood
We generated a panel of monoclonal antibody (mAb) using PEDV Pintung 52 (PEDV-PT) viral particles
Summary
PEDV is a single-stranded RNA virus, approximately 28 kb in size, which belongs to the genus Alphacoronavirus[8]. The S1B domain is a common location for receptor binding in coronaviruses and can be a potential neutralizing target for the new PEDV variant capable of eliciting the production of cross-neutralizing antibodies against different PEDV strains[17]. No neutralizing epitope has been identified in the S1A domain of the historic or the new PEDV variant strains. The neutralizing epitopes of the PEDV-PT S protein, recognized by two of the NmAbs, were characterized using a series of C-terminal truncated recombinant PEDV-PT S proteins under native and denaturing conditions. This approach allows us to identify conformational epitopes of PEDV-PT strain and helps in understanding the antigenicity and pathogenesis of the G2b PEDV
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