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系统同源中和抗体不足以评估疫苗对高毒力 PEDV 和 PRRSV 共感染的保护效力。

Systemic Homologous Neutralizing Antibodies Are Inadequate for the Evaluation of Vaccine Protective Efficacy against Coinfection by High Virulent PEDV and PRRSV.

机构信息

College of Veterinary Medicine, Yangzhou Universitygrid.268415.c, Yangzhou, Jiangsu, China.

National Research Center for Veterinary Medicine, Luoyang, Henan, China.

出版信息

Microbiol Spectr. 2022 Apr 27;10(2):e0257421. doi: 10.1128/spectrum.02574-21. Epub 2022 Mar 22.

Abstract

G2 porcine epidemic diarrhea virus (G2 PEDV) and highly pathogenic porcine reproductive and respiratory syndrome virus 2 (HP-PRRSV2) are two of the most prevalent swine pathogens in China's swine herds, and their coinfection occurs commonly. Several PED and PRRS vaccines have been utilized in China for decades, and systemic homologous neutralizing antibodies (shnAbs) in serum are frequently used to evaluate the protective efficacy of PED and PRRS vaccines. To develop a vaccine candidate against G2 PEDV and HP-PRRSV2 coinfection, in this study, we generated a chimeric virus (rJSTZ1712-12-S) expressing S protein of G2 PEDV using an avirulent HP-PRRSV2 rJSTZ1712-12 infectious clone as the viral vector. The rJSTZ1712-12-S strain has similar replication efficacies as the parental rJSTZ1712-12 virus. In addition, animal inoculation indicated that rJSTZ1712-12-S is not pathogenic to piglets and can induce shnAbs against both G2 PEDV and HP-PRRSV2 isolates after prime-boost immunization. However, passive transfer study in neonatal piglets deprived of sow colostrum showed that rJSTZ1712-12-S-induced shnAbs may only decrease PEDV and PRRSV viremia but cannot confer sufficient protection against dual challenge of high virulent G2 PEDV XJ1904-34 strain and HP-PRRSV2 XJ17-5 isolate. Overall, this study provides the first evidence that shnAbs confer insufficient protection against PEDV and PRRSV coinfection and are inadequate for the evaluation of protective efficacy of PED and PRRS bivalent vaccine (especially for the PED vaccine). Porcine epidemic diarrhea virus (PEDV) and porcine reproductive and respiratory syndrome virus (PRRSV) coinfection occurs commonly and can synergistically reduce feed intake and pig growth. Vaccination is an effective strategy utilized for PED and PRRS control, and systemic homologous neutralizing antibodies (shnAbs) in serum are commonly used for protective efficacy evaluation of PED and PRRS vaccines. Currently, no commercial vaccine is available against PEDV and PRRSV coinfection. This study generated a chimeric vaccine candidate against the coinfection of prevalent PEDV and PRRSV in China. The chimeric strain can induce satisfied shnAbs against both PEDV and PRRSV after prime-boost inoculation in pigs. But the shnAbs cannot confer sufficient protection against PEDV and PRRSV coinfection in neonatal piglets. To the best of our knowledge, these findings provide the first evidence that shnAbs confer insufficient protection against PEDV and PRRSV coinfection and are inadequate for evaluating PED and PRRS bivalent vaccine protective efficacy.

摘要

猪流行性腹泻病毒(G2 PEDV)和高致病性猪繁殖与呼吸综合征病毒 2 型(HP-PRRSV2)是中国猪群中两种最常见的猪病原体,它们的合并感染很常见。几十年来,中国已经使用了几种 PED 和 PRRS 疫苗,血清中的系统同源中和抗体(shnAbs)常用于评估 PED 和 PRRS 疫苗的保护效力。为了开发针对 G2 PEDV 和 HP-PRRSV2 合并感染的疫苗候选物,本研究使用无毒的 HP-PRRSV2 rJSTZ1712-12 感染性克隆作为病毒载体,生成了表达 G2 PEDV S 蛋白的嵌合病毒(rJSTZ1712-12-S)。rJSTZ1712-12-S 株的复制效率与亲本 rJSTZ1712-12 病毒相似。此外,动物接种表明,rJSTZ1712-12-S 对仔猪无致病性,并且在初次免疫加强免疫后可诱导针对 G2 PEDV 和 HP-PRRSV2 分离株的 shnAbs。然而,在缺乏母猪初乳的新生仔猪的被动转移研究中表明,rJSTZ1712-12-S 诱导的 shnAbs 可能仅降低 PEDV 和 PRRSV 的病毒血症,但不能提供针对高毒力 G2 PEDV XJ1904-34 株和 HP-PRRSV2 XJ17-5 分离株双重挑战的充分保护。总体而言,这项研究首次提供了证据表明,shnAbs 不能提供针对 PEDV 和 PRRS 合并感染的充分保护,并且不足以评估 PED 和 PRRS 二价疫苗的保护效力(特别是对于 PED 疫苗)。猪流行性腹泻病毒(PEDV)和猪繁殖与呼吸综合征病毒(PRRSV)合并感染很常见,会协同降低饲料摄入量和猪的生长速度。疫苗接种是控制 PED 和 PRRS 的有效策略,血清中的系统同源中和抗体(shnAbs)常用于评估 PED 和 PRRS 疫苗的保护效力。目前,尚无针对 PEDV 和 PRRSV 合并感染的商业疫苗。本研究生成了针对中国流行的 PEDV 和 PRRSV 合并感染的嵌合疫苗候选物。嵌合株在猪中进行初次免疫加强接种后,可诱导针对 PEDV 和 PRRSV 的满意 shnAbs。但在新生仔猪中,shnAbs 不能提供针对 PEDV 和 PRRSV 合并感染的充分保护。据我们所知,这些发现首次提供了证据表明,shnAbs 不能提供针对 PEDV 和 PRRSV 合并感染的充分保护,并且不足以评估 PED 和 PRRS 二价疫苗的保护效力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/450a/9045284/5d6712c243a0/spectrum.02574-21-f001.jpg

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