atrophic enteritis

  • 文章类型: Journal Article
    肠扩张综合征(IDS)是一种节段性肠病,其特征是回肠和空肠(Meckel憩室)的交界处扩张。IDS严重影响家禽业,导致产卵的慢性和不可逆转的下降,降低饲料转化效率,增加死亡率。描述了白蛋鸡IDS的临床和病理特征,并进行了病毒分子和宏基因组研究。50至60天大的鸡粘膜苍白,冷漠,抑郁症,荷叶边的羽毛,腹泻,伴随着产卵损失20%,20%的鸟类扑杀,和5%的死亡率。尸检的主要发现是明显的肠道扩张伴肠道淤滞,Meckel憩室区域的狭窄远端空肠,和未消化的食物。显微镜分析显示明显的萎缩性淋巴浆细胞性和嗜异性肠炎伴增生隐窝,溃疡,和嗜异性和淋巴浆细胞性神经周炎。分子分析一致地检测到鸡细小病毒在肠道的三个部分的存在,胰腺,和proventricuus,以及鸡的肠道内容物中的大疱病毒。伴有神经周炎和肠淤滞的萎缩性肠炎与肠吸收不良和继发细菌感染的临床表现有关。我们的数据提供了有关IDS的有用信息,并强调了进一步研究以确定每种检测到的病毒在该综合征中的特定作用的重要性。研究重点IDS呈现空肠直至Meckel憩室的病理性扩张。IDS导致体重减轻,鸡蛋产量下降,以及增加扑杀和死亡率。通过PCR测定一致地检测鸡细小病毒(ChPV)。通过病毒宏基因组学始终检测到鸡大疱疹病毒(ChMV)。
    UNASSIGNED: IDS presented pathognomonic dilatation of the jejunum up to Meckel\'s diverticulum.IDS caused weight loss, decreased egg production, and increased culling and mortality.Chicken parvovirus (ChPV) was consistently detected through PCR assays.Chicken megrivirus (ChMV) was consistently detected through viral metagenomics.
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  • 文章类型: Journal Article
    Sheep-associated malignant catarrhal fever (SA-MCF) is a severe, frequently fatal, lymphoproliferative disease that affects a wide variety of ruminants and is caused by ovine gammaherpesvirus 2 (OvHV-2), a member of the MCF virus (MCFV) complex. The typical clinical manifestations of SA-MCF are well known and easily recognized by veterinarians, resulting in clinical diagnosis of MCF when characteristic clinical signs are present. This article describes the findings observed in cattle infected with OvHV-2 but without typical clinical manifestations of SA-MCF. Three calves with episodes of diarrhea before death and a yearling that died suddenly were investigated. Gross alterations were not suggestive of SA-MCF. Histopathology revealed a combination of proliferating vascular lesions (PVLs) and necrotizing vasculitis in three animals (two calves and the yearling); with PVLs being identified only at the carotid rete mirabile of two calves infected with OvHV-2. Additional significant histopathologic lesions included atrophic enteritis, portal lymphocytic hepatitis, interstitial pneumonia, suppurative bacterial bronchopneumonia, and pulmonary hemorrhage. An immunohistochemical assay designed to identify only antigens of MCFV revealed, positive, intralesional, intracytoplasmic immunoreactivity within epithelial cells of multiple tissues of all animals with PVLs. PCR assays amplified OvHV-2 DNA from multiple tissues of the animals that contained MCFV proteins, confirming the MCFV identified as OvHV-2. Additionally, bovine coronavirus (BCoV) nucleic acids were amplified from tissues of all animals, including the animal not infected by OvHV-2. Collectively, these findings confirmed the participation of OvHV-2 in the development of the disease patterns observed in these animals that were concomitantly infected by BCoV and provide additional confirmation that cattle can be subclinically infected with OvHV-2. Consequently, the real occurrence of OvHV-2-related disease may be more elevated than reported, since asymptomatic or subclinically infected animals are not likely to be investigated for OvHV-2. Furthermore, PVLs should be included as possible histologic indicators of OvHV-2-related diseases in ruminants.
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  • 文章类型: Journal Article
    Porcine deltacoronavirus (PDCoV) was first identified in Hong Kong in 2009-2010 and reported in United States swine for the first time in February 2014. However, diagnostic tools other than polymerase chain reaction for PDCoV detection were lacking and Koch\'s postulates had not been fulfilled to confirm the pathogenic potential of PDCoV. In the present study, PDCoV peptide-specific rabbit antisera were developed and used in immunofluorescence and immunohistochemistry assays to assist PDCoV diagnostics. The pathogenicity and pathogenesis of PDCoV was investigated following orogastric inoculation of 5-day-old piglets with a plaque-purified PDCoV cell culture isolate (3 × 10(4) TCID50 per pig). The PDCoV-inoculated piglets developed mild to moderate diarrhea, shed increasing amount of virus in rectal swabs from 2 to 7 days post inoculation, and developed macroscopic and microscopic lesions in small intestines with viral antigen confirmed by immunohistochemistry staining. This study experimentally confirmed PDCoV pathogenicity and characterized PDCoV pathogenesis in neonatal piglets.
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