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羊瘙痒病在SCID小鼠脾脏中的复制发生在野生型小鼠骨髓重建之后。

Replication of scrapie in spleens of SCID mice follows reconstitution with wild-type mouse bone marrow.

作者信息

Fraser H, Brown K L, Stewart K, McConnell I, McBride P, Williams A

机构信息

Institute for Animal Health, BBSRC & MRC Neuropathogenesis Unit, Edinburgh, UK.

出版信息

J Gen Virol. 1996 Aug;77 ( Pt 8):1935-40. doi: 10.1099/0022-1317-77-8-1935.

Abstract

SCID mice are resistant to intraperitoneal infection with 10(3) and 10(4) intracerebral ID50 units of ME7 scrapie agent whereas they develop disease after intracerebral challenge. However, higher doses introduced, by intraperitoneal or subcutaneous routes, produce disease. Immunocompetent mice of the same strain (CB20) developed scrapie following either intracerebral or intraperitoneal infection. Bioassay of spleens from SCID mice infected with 10(-1) dilutions of ME7 scrapie by intraperitoneal, intracerebral or abdominal subcutaneous injection showed traces or low levels of infectivity in spleen. However, subcutaneous injection beneath the skin of the neck failed to infect the spleen. CB20 bone marrow reconstitution of SCID mice resulted in the regeneration of a normal lymphoid architecture in the spleen. Spleens from these reconstituted mice, infected intracerebrally with a 10(-1) dilution of ME7 contained high levels of infectivity. These results suggest that the ability to replicate scrapie agent in spleen or lymphoid tissue depends on the restoration of normal lymphoid structure and in particular the presence of differentiated follicular dendritic cells. The possibility that SCID mice can select minor strains of scrapie which are normally unrecognized in cloned ME7 is discussed.

摘要

严重联合免疫缺陷(SCID)小鼠对腹腔注射10³和10⁴脑内半数感染量(ID50)单位的ME7羊瘙痒病病原体具有抵抗力,而脑内接种后它们会发病。然而,通过腹腔或皮下途径引入更高剂量则会引发疾病。同一品系(CB20)的免疫活性小鼠在脑内或腹腔感染后会患上羊瘙痒病。对经腹腔、脑内或腹部皮下注射10⁻¹稀释度ME7羊瘙痒病病原体感染的SCID小鼠的脾脏进行生物测定,结果显示脾脏中有微量或低水平的感染性。然而,在颈部皮肤下进行皮下注射未能感染脾脏。用CB20骨髓重建SCID小鼠导致脾脏中正常淋巴结构的再生。这些重建小鼠经脑内注射10⁻¹稀释度ME7感染后,脾脏中含有高水平的感染性。这些结果表明,在脾脏或淋巴组织中复制羊瘙痒病病原体的能力取决于正常淋巴结构的恢复,特别是分化滤泡树突状细胞的存在。讨论了SCID小鼠能否选择在克隆的ME7中通常未被识别的羊瘙痒病小毒株的可能性。

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