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针对溶组织内阿米巴半乳糖结合凝集素的单克隆抗体可增强黏附作用。

Monoclonal antibodies directed against the galactose-binding lectin of Entamoeba histolytica enhance adherence.

作者信息

Petri W A, Snodgrass T L, Jackson T F, Gathiram V, Simjee A E, Chadee K, Chapman M D

机构信息

Department of Medicine, University of Virginia, Charlottesville 22908.

出版信息

J Immunol. 1990 Jun 15;144(12):4803-9.

PMID:1693641
Abstract

The Entamoeba histolytica galactose-binding lectin is a surface glycoprotein composed of 170- and 35-kDa subunits. Inhibition of this lectin with galactose or anti-170 kDa subunit polyclonal antibody blocks amebic adherence to target cells and colonic mucin glycoproteins. We describe the properties of 10 mAb with specificity for the 170-kDa subunit. Based on competitive binding studies, six nonoverlapping antigenic determinants on the lectin were identified. The effect of the mAb on adherence of amebic trophozoites to both Chinese hamster ovary (CHO) cells and human colonic mucins was measured. Antilectin antibodies directed against epitopes 1 and 2 enhanced adherence, with the number of amebae having at least three adherent CHO cells increasing with the addition of epitope 1 mAb from 26 +/- 9 to 88 +/- 2% and the binding of colonic mucins increasing from 34 +/- 1 to 164 +/- 3 pg/10(5) amebae. Antibody-enhanced adherence remained 90 to 100% galactose inhibitable, occurred at 4 degrees C and was not Fc mediated. Univalent Fab fragments of epitope 1 mAb augmented mucin binding by 238% and CHO cell adherence by 338%. The binding of purified lectin to CHO cells was increased from 1.1 +/- 0.1 to 2.4 +/- 0.3 ng/10(3) CHO cells by mAb directed to epitope 1, demonstrating that enhanced adherence was due to direct activation of the lectin. mAb to epitope 3 bound to the lectin only upon its solubilization from the membrane and had no effect on adherence. Adherence to CHO cells and mucins was inhibited from 50 to 75% by mAb to epitopes 4 and 5; epitope 6 mAb inhibited amebic adherence to CHO cells but not mucins. The pooled sera from 10 patients with amebic liver abscess blocked the binding to the 170-kDa subunit of mAb directed to all six epitopes. Striking individual variations in the effects of immune sera on adherence were observed. Although the sera of all 44 South African patients with amebic liver abscess had high titer anti-lectin antibodies, 16 patients' sera significantly (more than 3 SEM) enhanced adherence whereas 25 patients' sera significantly inhibited adherence. Antilectin antibodies exert profound functional effects on the interaction of E. histolytica with target cells and human colonic mucins. Exploration of the clinical consequences of adherence-enhancing and inhibitory antibody responses may give insight into the role of antilectin antibodies in immunity to invasive amebiasis.

摘要

溶组织内阿米巴半乳糖结合凝集素是一种表面糖蛋白,由170 kDa和35 kDa亚基组成。用半乳糖或抗170 kDa亚基多克隆抗体抑制这种凝集素可阻断阿米巴对靶细胞和结肠粘蛋白糖蛋白的粘附。我们描述了10种对170 kDa亚基具有特异性的单克隆抗体的特性。基于竞争性结合研究,确定了凝集素上6个不重叠的抗原决定簇。测定了单克隆抗体对阿米巴滋养体与中国仓鼠卵巢(CHO)细胞和人结肠粘蛋白粘附的影响。针对表位1和2的抗凝集素抗体增强了粘附,随着表位1单克隆抗体的加入,至少有3个粘附CHO细胞的阿米巴数量从26±9%增加到88±2%,结肠粘蛋白的结合从34±1 pg/10⁵阿米巴增加到164±3 pg/10⁵阿米巴。抗体增强的粘附仍有90%至100%可被半乳糖抑制,在4℃时发生且不是由Fc介导的。表位1单克隆抗体的单价Fab片段使粘蛋白结合增加了238%,CHO细胞粘附增加了338%。针对表位1的单克隆抗体使纯化的凝集素与CHO细胞的结合从1.1±0.1 ng/10³ CHO细胞增加到2.4±0.3 ng/10³ CHO细胞,表明增强的粘附是由于凝集素的直接激活。针对表位3的单克隆抗体仅在凝集素从膜上溶解后才与之结合,对粘附没有影响。针对表位4和5的单克隆抗体可使与CHO细胞和粘蛋白的粘附抑制50%至75%;表位6单克隆抗体可抑制阿米巴对CHO细胞的粘附,但对粘蛋白无抑制作用。10例阿米巴肝脓肿患者的混合血清可阻断针对所有6个表位的单克隆抗体与170 kDa亚基的结合。观察到免疫血清对粘附作用的显著个体差异。尽管所有44例南非阿米巴肝脓肿患者的血清都有高滴度的抗凝集素抗体,但16例患者的血清显著(超过3个标准误)增强了粘附,而25例患者的血清显著抑制了粘附。抗凝集素抗体对溶组织内阿米巴与靶细胞和人结肠粘蛋白的相互作用具有深远的功能影响。探索增强和抑制粘附的抗体反应的临床后果可能有助于深入了解抗凝集素抗体在侵袭性阿米巴病免疫中的作用。

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