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β-1,3-葡聚糖和霍乱毒素对大鼠血清及黏膜抗体针对溶组织内阿米巴滋养体反应的免疫调节作用

Immunodulation of rat serum and mucosal antibody responses to Entamoeba histolytica trophozoites by beta-1,3-glucan and cholera toxin.

作者信息

Navarro-García F, Pedroso M, López-Revilla R

机构信息

Department of Cell Biology, CINVESTAV-IPN, México DF, 07000, Mexico.

出版信息

Clin Immunol. 2000 Nov;97(2):182-8. doi: 10.1006/clim.2000.4918.

Abstract

Systemic and mucosal and immune responses can be manipulated with immunomodulators. Here we show the modulatory effects of cholera toxin (CT) and beta-1,3-glucan (GLU) on the rat antiamebic serum and fecal antibody responses to one or four intraperitoneal (IP) or intragastric (IG) doses of glutaraldehyde-fixed Entamoeba histolytica trophozoites (GFT). One IP dose of GFT maximized serum IgM and IgG antiamebic antibodies on days 4 and 9, respectively; CT coadministration increased IgM antibodies, whereas IgG titers increased with CT or GLU; coproantibodies were undetectable after GFT alone or coadministered with GLU, whereas CT coadministration maximized fecal IgA antibodies on day 6. One IG dose of GFT alone increased serum IgM and IgG antibodies 2.5 times and no further increases were detected using GLU, whereas CT doubled serum IgG antibodies; GFT did not affect the coproantibody responses, whereas GLU coadministration maximized IgG coproantibody levels on day 6 and CT increased IgG and IgA coproantibody levels on the same day. On the other hand, four IG doses of GFT alone or with GLU induced tolerance, whereas GFT alone via the IP route increased serum antibodies slightly and GLU coadministration increased serum IgG antibody titers 300-fold. CT coadministration by both routes increased IgA coproantibodies, and simultaneous CT+GLU coadministration induced lower responses than either CT or GLU. Different antiamebic immune responses might therefore be attained through the use of different immunization routes and immunomodulators to induce protective immunity against intestinal or extraintestinal amebiasis.

摘要

免疫调节剂可调控全身、黏膜及免疫反应。在此,我们展示了霍乱毒素(CT)和β-1,3-葡聚糖(GLU)对大鼠抗阿米巴血清及粪便抗体反应的调节作用,该反应针对腹腔内(IP)或胃内(IG)给予一或四次戊二醛固定的溶组织内阿米巴滋养体(GFT)。一次IP剂量的GFT分别在第4天和第9天使血清IgM和IgG抗阿米巴抗体达到最大值;联合给予CT可增加IgM抗体,而IgG滴度在联合CT或GLU时增加;单独给予GFT或与GLU联合使用后未检测到粪便抗体,而联合给予CT在第6天使粪便IgA抗体达到最大值。一次IG剂量的GFT单独使血清IgM和IgG抗体增加2.5倍,使用GLU未检测到进一步增加,而联合CT使血清IgG抗体增加一倍;GFT不影响粪便抗体反应,而联合给予GLU在第6天使IgG粪便抗体水平达到最大值,联合CT在同一天增加IgG和IgA粪便抗体水平。另一方面,四次IG剂量的GFT单独或与GLU联合诱导耐受,而通过IP途径单独给予GFT使血清抗体略有增加,联合给予GLU使血清IgG抗体滴度增加300倍。两种途径联合给予CT均增加IgA粪便抗体,同时联合给予CT + GLU诱导的反应低于单独给予CT或GLU。因此,通过使用不同的免疫途径和免疫调节剂来诱导针对肠道或肠外阿米巴病的保护性免疫,可能会获得不同的抗阿米巴免疫反应。

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