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使用同基因细胞类型的重建组织中的I型超敏反应。

Type 1 hypersensitivity reactions in reconstructed tissues using syngeneic cell types.

作者信息

Baird A W, Cuthbert A W, MacVinish L J

机构信息

Department of Pharmacology, University of Cambridge.

出版信息

Br J Pharmacol. 1987 Aug;91(4):857-69. doi: 10.1111/j.1476-5381.1987.tb11285.x.

Abstract
  1. Type 1 hypersensitivity reactions in response to antigen challenge have been measured as short circuit current (SCC) responses in reconstructed tissues consisting of syngeneic cell types. 2. In all instances reconstructed tissues consisted of an epithelial monolayer grown on collagen-coated Millipore filters and a pad of peritoneal cells. Monolayers were formed of either HCA-7 or HCA-7-Col 1 cells derived from a human adenocarcinoma. Peritoneal cells were derived from rats or guinea-pigs sensitized to either ovalbumin or beta-lactoglobulin. 3. The SCC responses of the monolayers were dependent upon the 'concentration' of peritoneal cells in the reconstructed tissue. The threshold concentration was 0.4 X 10(6) cells when rat peritoneal cells are combined with an epithelial monolayer of 0.2 cm2. 4. The SCC responses in response to antigen challenge were selectively inhibited by the H1-receptor antagonist, mepyramine. Similarly the effects of exogenously applied histamine were antagonised by mepyramine. 5. The responses to antigen challenge were not inhibited by tetrodotoxin in reconstructed tissues. This result is in contrast to that with isolated intestinal epithelia from sensitized animals where tetrodotoxin inhibits the SCC responses to external field stimulation and to challenge with antigens. The consequences of these results for understanding the mechanisms of epithelial Type 1 hypersensitivity reactions are discussed. Suggestions are made to illustrate how the methods developed here may be employed to ask questions about the nature of mediators released and the types of cell responsible in human disease conditions.
摘要
  1. 针对抗原激发的I型超敏反应已通过由同基因细胞类型组成的重建组织中的短路电流(SCC)反应进行测量。2. 在所有情况下,重建组织均由生长在胶原包被的微孔滤膜上的上皮单层和一层腹膜细胞组成。单层由源自人腺癌的HCA - 7或HCA - 7 - Col 1细胞形成。腹膜细胞源自对卵清蛋白或β - 乳球蛋白致敏的大鼠或豚鼠。3. 单层的SCC反应取决于重建组织中腹膜细胞的“浓度”。当大鼠腹膜细胞与0.2平方厘米的上皮单层结合时,阈值浓度为0.4×10⁶个细胞。4. 抗原激发后的SCC反应被H1受体拮抗剂美吡拉敏选择性抑制。同样,外源性应用组胺的作用也被美吡拉敏拮抗。5. 重建组织中对抗原激发的反应不受河豚毒素抑制。这一结果与致敏动物的离体肠上皮情况相反,在离体肠上皮中河豚毒素会抑制对外部电场刺激和抗原激发的SCC反应。讨论了这些结果对于理解上皮I型超敏反应机制的意义。还提出了一些建议,以说明如何利用这里开发的方法来探讨人类疾病状态下释放的介质的性质以及负责的细胞类型等问题。

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