Myocarditis in an FIP-Diseased Cat with FCoV M1058L Mutation: Clinical and Pathological Changes

Animals Pub Date : 2024-06-03 DOI:10.3390/ani14111673
Chiara Guarnieri, L. Bertola, Luca Ferrari, Cecilia Quintavalla, Attilio Corradi, Rosanna Di Lecce
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Abstract

An 8-month-old intact male domestic shorthair cat was referred to the Emergency Service of the Veterinary Teaching Hospital (VTH) of the Department of Veterinary Science of the University of Parma (Italy) from the Parma municipal multi-cat shelter, during the winter season (January 2023), for lethargy, anorexia, hypothermia, and hypoglycemia. At the VTH, upon cardiologic examination, an increase in heart rate, under normal blood pressure conditions, was detected. Signalment, clinical history, basal metabolic panel (BMP), ultrasound investigations, and cytological findings were all consistent with a diagnosis of feline infectious peritonitis (FIP). FIP was confirmed in the effusive abdominal fluid by a molecular genetic test (real-time PCR for feline coronavirus RNA). The molecular genetic investigation also detected an FCoV S gene single-nucleotide mutation: biotype M1058L. At necropsy, an effusive collection was recorded in the abdomen, thoracic cavity, and pericardium sac. White parenchymal nodules, of about 1 mm diameter, were found on the surface and deep in the lungs, liver, kidneys, and heart. Histopathology revealed the typical FIP pyogranulomatous vasculitis and IHC confirmed the presence of the FIP virus (FIPV) antigen. The most relevant histopathological finding was the myocarditis/myocardial necrosis associated with the presence of the S gene-mutated FCoV (M1058L biotype). This is the first case of myocarditis in a cat positive for the FCoV/FIP M1058L biotype. Further studies are necessary to support the mutated FCoV M1058L biotype, as an uncommon, but possible, causative pathogen of myocarditis in FCoV/FIP-positive cats. Studies including several FCoV/FIP M1058L-positive cases could allow us to make a correlation with heart gross pathology, histopathology, and immunolocalization of the FCoV/FIP M1058L biotype in the myocardium. The investigation will potentially allow us to determine the effective tropism of the FCoV/FIP M1058L biotype for myocardiocytes or whether myocardiocyte lesions are evident in the presence of concomitant causes related to the patient, its poor condition, or external environmental distress such as cold season, and whether the aforementioned concomitant events are correlated.
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一只患有FCoV M1058L突变的FIP病猫的心肌炎:临床和病理变化
在冬季(2023 年 1 月),一只 8 个月大的完整雄性短毛猫因嗜睡、厌食、体温过低和低血糖症从帕尔马市立多猫收容所转诊到意大利帕尔马大学兽医科学系兽医教学医院(VTH)急诊科。在 VTH 进行心脏检查时,发现在血压正常的情况下心率加快。信号、临床病史、基础代谢试验(BMP)、超声波检查和细胞学检查结果均符合猫传染性腹膜炎(FIP)的诊断。通过分子基因检测(猫冠状病毒 RNA 实时 PCR),在流出的腹腔液中确诊了 FIP。分子遗传学检查还检测到 FCoV S 基因单核苷酸突变:生物型 M1058L。尸体解剖时,腹部、胸腔和心包囊都有渗出物。在肺部、肝脏、肾脏和心脏的表面和深部发现了直径约 1 毫米的白色实质结节。组织病理学检查发现了典型的 FIP 热肉芽肿性血管炎,IHC 检查证实了 FIP 病毒(FIPV)抗原的存在。最相关的组织病理学发现是心肌炎/心肌坏死,这与 S 基因突变的 FCoV(M1058L 生物型)的存在有关。这是首例对 FCoV/FIP M1058L 生物型检测呈阳性的猫患心肌炎的病例。有必要开展进一步研究,以证实变异的 FCoV M1058L 生物型是 FCoV/FIP 阳性猫心肌炎的一种不常见但可能的致病病原体。通过对几例 FCoV/FIP M1058L 阳性病例的研究,我们可以将心脏大体病理学、组织病理学和 FCoV/FIP M1058L 生物型在心肌中的免疫定位联系起来。这项调查将使我们有可能确定 FCoV/FIP M1058L 生物型对心肌细胞的有效滋养性,或心肌细胞病变是否在与患者有关的并发症、患者状况不佳或外部环境困扰(如寒冷季节)存在的情况下明显,以及上述并发症是否相关。
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