首页> 外文期刊>Frontiers in Immunology >Stage of Gestation at Porcine Epidemic Diarrhea Virus Infection of Pregnant Swine Impacts Maternal Immunity and Lactogenic Immune Protection of Neonatal Suckling Piglets
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Stage of Gestation at Porcine Epidemic Diarrhea Virus Infection of Pregnant Swine Impacts Maternal Immunity and Lactogenic Immune Protection of Neonatal Suckling Piglets

机译:怀孕猪的猪流行性腹泻病毒感染的妊娠期影响新生儿乳猪的母体免疫力和致乳源性免疫保护。

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During pregnancy, the maternal immune response changes dramatically over the course of gestation. This has implications for generation of lactogenic immunity and subsequent protection in suckling neonates against enteric viral infections. For example, porcine epidemic diarrhea virus (PEDV) is an alphacoronavirus that causes acute diarrhea in neonatal piglets. Due to the high virulence of PEDV and the na?ve, immature immune system of neonatal suckling piglets, passive lactogenic immunity to PEDV induced during pregnancy, via the gut-mammary gland (MG)-secretory IgA (sIgA) axis, is critical for piglet protection. However, the anti-PEDV immune response during pregnancy and stage of gestation required to optimally stimulate the gut-MG-sIgA axis is undefined. We hypothesize that there is a gestational window in which non-lethal PEDV infection of pregnant gilts influences maximum lymphocyte mucosal trafficking to the MG, resulting in optimal passive lactogenic protection in suckling piglets. To understand how the stages of gestation affect maternal immune responses to PEDV, three groups of gilts were orally infected with PEDV in the first, second or third trimester. Control (mock) gilts were inoculated with medium in the third trimester. To determine if lactogenic immunity correlated with protection, all piglets were PEDV-challenged at 3–5 days postpartum. PEDV infection of gilts at different stages of gestation significantly affected multiple maternal systemic immune parameters prepartum, including cytokines, B cells, PEDV antibodies (Abs), and PEDV antibody secreting cells (ASCs). Pregnant second trimester gilts had significantly higher levels of circulating PEDV IgA and IgG Abs and ASCs and PEDV virus neutralizing (VN) Abs post PEDV infection. Coinciding with the significantly higher PEDV Ab responses in second trimester gilts, the survival rate of their PEDV-challenged piglets was 100%, compared with 87.2, 55.9, and 5.7% for first, third, and mock litters, respectively. Additionally, piglet survival positively correlated with PEDV IgA Abs and ASCs and VN Abs in milk and PEDV IgA and IgG Abs in piglet serum. Our findings have implications for gestational timing of oral attenuated PEDV maternal vaccines, whereby PEDV intestinal infection in the second trimester optimally stimulated the gut-MG-sIgA axis resulting in 100% lactogenic immune protection in suckling piglets.
机译:在怀孕期间,孕妇的免疫反应会在妊娠过程中发生巨大变化。这对乳汁免疫力的产生和哺乳期新生儿的肠道病毒感染的后续保护具有影响。例如,猪流行性腹泻病毒(PEDV)是一种冠状病毒,可引起新生仔猪急性腹泻。由于PEDV的高毒力和新生乳猪的幼稚,未成熟的免疫系统,因此在怀孕期间通过肠-乳腺(MG)-分泌型IgA(sIgA)轴对PEDV产生的被动泌乳原性免疫对于至关重要仔猪保护。但是,尚未确定最佳刺激肠道-MG-sIgA轴所需的妊娠期和妊娠期的抗PEDV免疫反应。我们假设存在一个妊娠窗口,其中妊娠小母猪的非致命性PEDV感染影响向MG的最大淋巴细胞粘膜运输,从而在乳猪中获得最佳的被动产乳保护。为了了解妊娠阶段如何影响母体对PEDV的免疫反应,三组小母猪在妊娠中期,中期或中期口服了PEDV。在妊娠中期,将对照(模拟)小母猪接种培养基。为了确定泌乳原性免疫是否与保护相关,在产后3-5天对所有仔猪进行PEDV攻击。妊娠期不同阶段的小母猪的PEDV感染会显着影响产前的多种母体系统免疫参数,包括细胞因子,B细胞,PEDV抗体(Abs)和PEDV抗体分泌细胞(ASC)。怀孕中期的后备母猪在感染PEDV后具有较高水平的循环PEDV IgA和IgG Abs和ASC和PEDV病毒中和(VN)Abs。与中晚期后备母猪的PEDV Ab应答显着提高相对应,他们受PEDV攻击的仔猪的存活率为100%,而第一胎,第三胎和模拟胎的存活率分别为87.2、55.9和5.7%。此外,仔猪存活率与牛奶中的PEDV IgA Abs和ASCs和VN Abs以及猪血清中PEDV IgA和IgG Abs正相关。我们的发现对口服减毒PEDV母源疫苗的妊娠时机有影响,在妊娠中期,PEDV肠道感染可以最佳地刺激肠道MG-sIgA轴,从而在乳猪中产生100%的乳原性免疫保护作用。

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