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与FVB小鼠癫痫发作相关的神经病理学发现。

Neuropathologic findings associated with seizures in FVB mice.

作者信息

Goelz M F, Mahler J, Harry J, Myers P, Clark J, Thigpen J E, Forsythe D B

机构信息

National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina, USA.

出版信息

Lab Anim Sci. 1998 Feb;48(1):34-7.

PMID:9517887
Abstract

The FVB mouse is used extensively in transgenic research because of its defined inbred background, superior reproductive performance, and prominent pronuclei, which facilitate microinjection of genomic material. Seizures associated with a known mutation and seizure-susceptible inbred strains are well documented in mice; however, to the authors' knowledge, seizures in the FVB strain have not been evaluated. Affected nonmanipulated FVB/N (n = 5) and transgenic FVB/N mice generated, using eight unrelated transgenic constructs (n = 63), were submitted for pathologic examination. Most cases were detected during routine observations in animal rooms; however, seizure induction by tail tattooing, fur clipping, and fire alarms has been observed. The majority of mice were female (62 of 68), with mean age of 5.8 months (range, 2 to 16 months). Observations made during seizure presentation in 12 of 68 mice included facial grimace, chewing automatism, ptyalism with matting of the fur of the ventral aspect of the neck and/or forelimbs, and clonic convulsions that frequently progressed to tonic convulsions and death. Four mice were dead at presentation, with matting of the fur of the neck and forelimbs. The remainder of the mice had nonspecific signs of disease, such as lethargy, moribundity, or matting of the fur. Vendor and in-house animal health surveillance reports indicated that mice were seronegative to all murine pathogens. Results of gross pathologic examination were unremarkable. Microscopic findings were limited to the brain and liver. In all mice, neuronal necrosis was present in the cerebral cortex, hippocampus, and thalamus. Concurrent astrocyte hypertrophy, as evidenced by an increase in glial fibrillary acidic protein staining, was detected. Acute coagulative necrosis of centrilobular hepatocytes was present in the liver of some cases (19 of 68). Infective agents were not detected in selected brain specimens submitted for electron microscopy or in brain and liver specimens evaluated by use of special stains. Cytopathologic effect was not observed in 3T3, Vero, and BHK-21 cell lines inoculated with brain and liver specimens. The ischemic neuronal necrosis observed in these mice is consistent with lesions associated with status epilepticus in humans. The hepatocellular changes are interpreted to be agonal and associated with terminal hypoxia in seizuring animals. These results provide evidence of a previously unrecognized, often lethal epileptic syndrome in FVB mice that may have a major impact on transgenic research and other disciplines using this mouse strain.

摘要

FVB小鼠因其明确的近交系背景、优良的繁殖性能和显著的原核,便于基因组材料的显微注射,而被广泛应用于转基因研究。与已知突变相关的癫痫发作以及癫痫易感近交系小鼠中的癫痫发作在小鼠中已有充分记录;然而,据作者所知,尚未对FVB品系小鼠的癫痫发作情况进行评估。对受影响的未处理FVB/N小鼠(n = 5)和使用8种无关转基因构建体产生的转基因FVB/N小鼠(n = 63)进行了病理检查。大多数病例是在动物房的常规观察中发现的;然而,也观察到通过尾部纹身、剪毛和火警诱导癫痫发作的情况。大多数小鼠为雌性(68只中的62只),平均年龄为5.8个月(范围为2至16个月)。在68只小鼠中的12只癫痫发作时观察到的症状包括面部抽搐、咀嚼自动症、流涎并伴有颈部腹侧和/或前肢皮毛结块,阵挛性惊厥常发展为强直性惊厥并导致死亡。4只小鼠在出现症状时死亡,颈部和前肢皮毛结块。其余小鼠有非特异性疾病体征,如嗜睡、濒死或皮毛结块。供应商和内部动物健康监测报告表明,小鼠对所有鼠类病原体血清学检测均为阴性。大体病理检查结果无明显异常。显微镜检查结果仅限于脑和肝。在所有小鼠中,大脑皮层、海马体和丘脑均出现神经元坏死。同时检测到胶质纤维酸性蛋白染色增加所证实的星形胶质细胞肥大。部分病例(68只中的19只)肝脏出现小叶中心肝细胞急性凝固性坏死。在提交用于电子显微镜检查的选定脑标本中,以及在使用特殊染色评估的脑和肝标本中,均未检测到感染因子。用脑和肝标本接种3T3、Vero和BHK - 21细胞系未观察到细胞病变效应。在这些小鼠中观察到的缺血性神经元坏死与人类癫痫持续状态相关的病变一致。肝细胞变化被解释为濒死期变化,并与癫痫发作动物的终末期缺氧有关。这些结果提供了证据,表明FVB小鼠中存在一种以前未被认识的、通常致命的癫痫综合征,这可能对使用该小鼠品系的转基因研究和其他学科产生重大影响。

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