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北京鸭短嘴侏儒综合征的发现、全基因组测序及舌组织新型鹅细小病毒的免疫组化信号。

Short beak and dwarfism syndrome among Pekin ducks: First detection, full genome sequencing, and immunohistochemical signals of novel goose parvovirus in tongue tissue.

机构信息

Zagazig University, Zagazig, Egypt.

Ministry of Defense, Cairo, Egypt.

出版信息

Vet Pathol. 2024 Sep;61(5):829-838. doi: 10.1177/03009858241249108. Epub 2024 May 7.

Abstract

Novel goose parvovirus (NGPV) is continuously threatening the global duck industry, as it causes short beak and dwarfism syndrome among different duck breeds. In this study, we investigated the viral pathogenesis in the tongue of affected ducks, as a new approach for deeper understanding of the syndrome. Seventy-three, 14- to 60-day-old commercial Pekin ducks were clinically examined. Thirty tissue pools of intestine and tongue (15 per tissue) were submitted for molecular identification. Clinical signs in the examined ducks were suggestive of parvovirus infection. All examined ducks had short beaks. Necrotic, swollen, and congested protruding tongues were recorded in adult ducks (37/73, 51%). Tongue protrusion without any marked congestion or swelling was observed in 20-day-old ducklings (13/73, 18%), and no tongue protrusion was observed in 15-day-old ducklings (23/73, 32%). Microscopically, the protruding tongues of adult ducks showed necrosis of the superficial epithelial layer with vacuolar degeneration. Glossitis was present in the nonprotruding tongues of young ducks, which was characterized by multifocal lymphoplasmacytic aggregates and edema in the propria submucosa. Immunohistochemical examination displayed parvovirus immunolabeling, mainly in the tongue propria submucosa. Based on polymerase chain reaction, goose parvovirus was detected in 9 out of 15 tongue sample pools (60%). Next-generation sequencing confirmed the presence of a variant goose parvovirus that is globally named NGPV and closely related to Chinese NGPV isolates. Novel insights are being gained from the study of NGPV pathogenesis in the tongue based on molecular and immunohistochemical identification.

摘要

新型鹅细小病毒(NGPV)持续威胁着全球养鸭业,因为它会导致不同鸭品种出现短喙和侏儒症。本研究通过研究受感染鸭的舌组织,探讨病毒的发病机制,为深入了解该综合征提供新的方法。对 73 只 14-60 日龄的商业北京鸭进行临床检查。提交了 30 个肠和舌组织池(每个组织 15 个)进行分子鉴定。检查中鸭子的临床症状提示为细小病毒感染。所有受检鸭均有短喙。成年鸭(37/73,51%)出现坏死、肿胀和充血的突出舌。20 日龄雏鸭观察到舌突出但无明显充血或肿胀(13/73,18%),15 日龄雏鸭无舌突出(23/73,32%)。显微镜下,成年鸭的突出舌表现为浅层上皮层坏死伴空泡变性。幼鸭的非突出舌出现舌炎,特征为固有粘膜下多灶性淋巴浆细胞聚集和水肿。免疫组化检查显示,细小病毒免疫标记主要位于舌固有粘膜下。聚合酶链反应检测到 15 个舌样本池中有 9 个(60%)存在鹅细小病毒。下一代测序证实存在一种新型鹅细小病毒,在全球范围内被命名为 NGPV,与中国的 NGPV 分离株密切相关。通过分子和免疫组化鉴定,从 NGPV 发病机制的研究中获得了新的认识。

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