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The monoclonal antibody HCM31 specifically recognises the Sd^a tetrasaccharide in goblet cell mucin

机译:单克隆抗体HCM31特异性识别杯状细胞粘蛋白中的Sd ^ a四糖

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Rat small intestinal goblet cell mucins reacting with monoclonal antibody HCM31 increase significantly during regeneration from experimental mucosal damage and at the period of expulsion of parasitic nematode, Nippostrongylus brasiliensis (N.b). The reduction in reactivity of HCM31 with mucin upon neuraminidase treatment, suggested that HCM31 recognizes sialylated oligosaccharide on mucin. HCM31-reactive sialomucins are therefore considered to play an important role in the physiological and pathological changes in the gastrointestinal mucosa. To determine the epitope for HCM31, oligosaccharide-alditols reacted with HCM31 were obtained from the small intestinal mucins of N.b-infected rats and purified by ion-exchange chromatography followed by normal-phase HPLC. Two HCM31-reactive oligosaccharide-alditols were obtained. Analyses using tandem mass spectrometry and NMR spectroscopy showed that these oligosaccharides were core 4 mucin-type oligosaccharides having a common tetrasaccharide sequence, NeuAc@a2-3(GalNAc@b1-4)Gal@b1-4GlcNAc@b- (Sd^a blood group antigen). These structures were not found in the small intestinal mucin oligosaccharides from uninfected rats. This epitope specificity of HCM31 was also confirmed using previously established anti-GM2 and anti-Sd^a antibodies. Taken together, these results strongly suggest that HCM31 specifically recognizes mucin-type oligosaccharides with the Sd^a tetrasaccharide sequence. Immunohistochemical examination of human gastrointestinal tracts showed that HCM31 site-specifically stained the goblet cells in normal sigmoid colon and normal rectum, but the goblet cells stained with HCM31 were reduced in the corresponding cancer tissues. HCM31 seems to be useful for diagnosis of colonic cancer and for examining the function of secretory-type mucin with Sd^a antigen.
机译:与单克隆抗体HCM31反应的大鼠小肠杯状细胞粘蛋白在实验性粘膜损伤的再生过程中以及在寄生线虫巴西拟夜蛾(Nippostrongylus brasiliensis)排出期间显着增加(N.b)。神经氨酸酶处理后,HCM31与粘蛋白的反应性降低,表明HCM31识别粘蛋白上的唾液酸化寡糖。因此,认为HCM31反应性唾液铝蛋白在胃肠道粘膜的生理和病理变化中起重要作用。为了确定HCM31的表位,从N.b感染的大鼠的小肠粘蛋白中获得了与HCM31反应的寡糖-醛糖醇,并通过离子交换色谱,然后进行正相HPLC纯化。获得了两种HCM31反应性低聚糖-醛糖醇。使用串联质谱和NMR光谱分析表明,这些寡糖是具有共同四糖序列NeuAc @ a2-3(GalNAc @ b1-4)Gal @ b1-4GlcNAc @ b-(Sd ^ a血液)的核心4种粘蛋白型寡糖。组抗原)。在未感染大鼠的小肠粘蛋白低聚糖中未发现这些结构。还使用先前建立的抗GM2和抗Sd 1a抗体证实了HCM31的这种表位特异性。综上所述,这些结果强烈暗示HCM31特异性识别具有Sd a四糖序列的粘蛋白型寡糖。对人胃肠道的免疫组织化学检查显示,HCM31定点染色了正常乙状结肠和正常直肠中的杯状细胞,但用HCM31染色的杯状细胞在相应的癌组织中却减少了。 HCM31似乎对于诊断结肠癌和检查具有Sd 1a抗原的分泌型粘蛋白的功能是有用的。

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