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免疫球蛋白A缺乏个体结肠微生物群中大肠杆菌的甘露糖特异性黏附素表达降低。

Decreased expression of mannose-specific adhesins by Escherichia coli in the colonic microflora of immunoglobulin A-deficient individuals.

作者信息

Friman V, Adlerberth I, Connell H, Svanborg C, Hanson L A, Wold A E

机构信息

Department of Clinical Immunology, Gotëborg University, Sweden.

出版信息

Infect Immun. 1996 Jul;64(7):2794-8. doi: 10.1128/iai.64.7.2794-2798.1996.

Abstract

Most Escherichia coli isolates can express type 1 fimbriae with mannose-specific adhesins. These adhesins bind to the oligosaccharide chains of secretory immunoglobulin A (IgA). Thus, in addition to specific antibody activity, secretory IgA possesses a broad reactivity with bacteria expressing type 1 fimbriae. The absence of secretory IgA in colonic secretions, as seen in IgA deficiency, might therefore alter the ability of type 1-fimbriated E. coli to colonize the large intestines of these individuals. In the present study, 10 E. coli isolates from each of 17 IgA-deficient and 17 age-matched control individuals were assessed for the carriage of the fim gene cluster by DNA-DNA hybridization and for the expression of type 1 fimbriae by hemagglutination of guinea pig erythrocytes. The contribution of type 1-fimbria-mediated adherence to HT-29 colonic cells was also analyzed. The proportion of fim+ E. coli isolates was lower in IgA-deficient than in control individuals (74 versus 94%, P < 0.05), as was the proportion of isolates expressing type 1 fimbriae in vitro (69% versus 85%, P < 0.05). The median mannose-sensitive adherence to HT-29 cells was lower for isolates from IgA-deficient individuals than from the controls (9 versus 26 bacteria per cell, P < 0.05). Isolates expressing type 1 fimbriae showed lower adherence to HT-29 cells when they were derived from IgA-deficient individuals than when they were derived from control individuals (15 versus 27 bacteria per cell, P < 0.05). The results suggest that the interaction of type 1 fimbriae with secretory IgA contributes to the large intestinal colonization by these bacteria.

摘要

大多数大肠杆菌分离株可表达带有甘露糖特异性黏附素的1型菌毛。这些黏附素与分泌型免疫球蛋白A(IgA)的寡糖链结合。因此,除了具有特异性抗体活性外,分泌型IgA还对表达1型菌毛的细菌具有广泛的反应性。在IgA缺乏症患者的结肠分泌物中缺乏分泌型IgA,这可能会改变1型菌毛化大肠杆菌在这些个体大肠中定殖的能力。在本研究中,通过DNA-DNA杂交评估了来自17名IgA缺乏症患者和17名年龄匹配的对照个体的10株大肠杆菌分离株中fim基因簇的携带情况,并通过豚鼠红细胞血凝试验评估了1型菌毛的表达情况。还分析了1型菌毛介导的黏附对HT-29结肠细胞的作用。IgA缺乏症患者中fim+大肠杆菌分离株的比例低于对照个体(分别为74%和94%,P<0.05),体外表达1型菌毛的分离株比例也较低(分别为69%和85%,P<0.05)。IgA缺乏症患者分离株对HT-29细胞的甘露糖敏感黏附中位数低于对照个体(分别为每个细胞9个和26个细菌,P<0.05)。当表达1型菌毛的分离株来自IgA缺乏症患者时,其对HT-29细胞的黏附低于来自对照个体的分离株(分别为每个细胞15个和27个细菌,P<0.05)。结果表明,1型菌毛与分泌型IgA的相互作用有助于这些细菌在大肠中的定殖。

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