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骨髓瘤IgE注射对大鼠被动和主动皮肤过敏反应的影响。

Effect of myeloma IgE injections on passive and active cutaneous anaphylaxis in rats.

作者信息

Spiegelberg H L, Canning K M, Scheetz M, Koppel G, Chiller J M

出版信息

J Immunol. 1986 Jan;136(1):131-5.

PMID:3484388
Abstract

The ability of injected rat IgE myeloma protein IR162 to inhibit passive and active cutaneous anaphylaxis in Lewis rats was investigated. IgE injected i.p. 24 hr before the sensitization with IgE anti-ovalbumin (OVA) completely inhibited both IgE- and IgG2a-induced passive cutaneous anaphylactic (PCA) reactions at a dose (2.5 mg/100 g body weight) that resulted in peak serum concentrations of 150 micrograms IgE IR162/ml. Peak IgE IR162 serum concentrations of 20 to 60 micrograms/ml inhibited the PCA reaction in approximately 50% of the rats. Intracutaneous injection of a mixture of myeloma IgE and anti-OVA IgE in a ratio of 100:1 or more also inhibited the PCA reaction. In contrast, the PCA reaction was not inhibited by seven daily doses of IgE beginning 24 hr after passive sensitization. Likewise, the cutaneous anaphylactic reaction elicited in rats 14 days after immunization with OVA and Bordetella pertussis was not prevented by daily injections of myeloma IgE despite a 1000- to 3000-fold excess of the myeloma IgE to anti-OVA IgE serum concentration. The data demonstrate that parenteral administration of myeloma IgE inhibits the PCA reaction only when given before passive sensitization and does not prevent cutaneous anaphylaxis in actively immunized rats. Because myeloma IgE failed to inhibit anaphylactic reactions in actively immunized rats, it is questionable whether administering human IgE-derived synthetic peptides or recombinant DNA-produced IgE fragments will be able to prevent allergic diseases by blocking the IgE Fc receptors on mast cells.

摘要

研究了注射大鼠IgE骨髓瘤蛋白IR162抑制Lewis大鼠被动和主动皮肤过敏反应的能力。在用抗卵清蛋白(OVA)IgE致敏前24小时腹腔注射IgE,以2.5mg/100g体重的剂量可完全抑制IgE和IgG2a诱导的被动皮肤过敏(PCA)反应,该剂量导致血清中IgE IR162的峰值浓度为150μg/ml。IgE IR162血清峰值浓度为20至60μg/ml时,约50%的大鼠PCA反应受到抑制。皮内注射骨髓瘤IgE与抗OVA IgE比例为100:1或更高的混合物也可抑制PCA反应。相比之下,被动致敏后24小时开始连续7天注射IgE,并未抑制PCA反应。同样,用OVA和百日咳博德特氏菌免疫14天后大鼠引发的皮肤过敏反应,尽管骨髓瘤IgE与抗OVA IgE血清浓度相比过量1000至3000倍,但每日注射骨髓瘤IgE并不能预防。数据表明,骨髓瘤IgE仅在被动致敏前给予时才会抑制PCA反应,且不能预防主动免疫大鼠的皮肤过敏反应。由于骨髓瘤IgE未能抑制主动免疫大鼠的过敏反应,因此给予人IgE衍生的合成肽或重组DNA产生的IgE片段是否能够通过阻断肥大细胞上的IgE Fc受体来预防过敏性疾病值得怀疑。

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