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马传染性贫血病毒的血细胞凝集作用。

Hemagglutination by equine infectious anemia virus.

作者信息

Sentsui H, Kono Y

出版信息

Infect Immun. 1976 Aug;14(2):325-31. doi: 10.1128/iai.14.2.325-331.1976.

DOI:10.1128/iai.14.2.325-331.1976
PMID:9361
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC420886/
Abstract

Equine infectious anemia (EIA) virus which was propagated on an equine dermal cell line agglutinated guinea pig erythrocytes. Viral fluids containing about 10(7.5) mean tissue culture infective doses/ml showed hemagglutinating (HA) titers ranging from 16 to 32 units/0.05 ml. Results of cesium chloride equilibrium density gradient centrifugation revealed that the hemagglutinin was inseparable from the virus particles. The hemagglutination reaction persisted over a wide range of temperature and pH, and the absence of divalent cations did not decrease its activity. The HA activity was stable at 4 degrees C but not at 56 degreesC. The activity was destroyed by virus-disrupting lipid solvents and moderately sensitive to a proteolytic enzyme. Neuraminidase enhanced HA activity slightly. Phospholipase C had no effect on HA titer, although it completely inactivated infectivity. It was relatively stable to ultraviolet irradiation. Thus, the hemagglutinin appears to be closely associated with virus particles, and its activity is dependent on the presence of its lipids and proteins. Hemagglutination was inhibited by sera from horses infected with EIA virus. Hemagglutinin receptors on the erythrocytes were inactivated by a proteolytic enzyme and formaldehyde but were not influenced by neuraminidase, sodium deoxycholate, or KIO4.

摘要

在马皮肤细胞系上繁殖的马传染性贫血(EIA)病毒能凝集豚鼠红细胞。含有约10(7.5)平均组织培养感染剂量/毫升的病毒液,其血凝(HA)滴度范围为16至32单位/0.05毫升。氯化铯平衡密度梯度离心结果表明,血凝素与病毒颗粒不可分离。血凝反应在很宽的温度和pH范围内持续存在,二价阳离子的缺失并不降低其活性。HA活性在4℃稳定,但在56℃不稳定。该活性可被破坏病毒的脂质溶剂所破坏,且对蛋白水解酶中度敏感。神经氨酸酶可轻微增强HA活性。磷脂酶C对HA滴度无影响,尽管它能完全灭活感染性。它对紫外线照射相对稳定。因此,血凝素似乎与病毒颗粒密切相关,其活性取决于其脂质和蛋白质的存在。感染EIA病毒的马的血清可抑制血凝。红细胞上的血凝素受体可被蛋白水解酶和甲醛灭活,但不受神经氨酸酶、脱氧胆酸钠或KIO4的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f41d/420886/0937b6c6ca05/iai00224-0006-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f41d/420886/65cafc11b694/iai00224-0004-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f41d/420886/0937b6c6ca05/iai00224-0006-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f41d/420886/65cafc11b694/iai00224-0004-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f41d/420886/0937b6c6ca05/iai00224-0006-a.jpg

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