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溶组织内阿米巴包囊壁的 Jacob2 凝集素结合几丁质,且具有多态性。

The Jacob2 lectin of the Entamoeba histolytica cyst wall binds chitin and is polymorphic.

机构信息

Department of Molecular and Cell Biology, Boston University Goldman School of Dental Medicine, Boston, Massachusetts, USA.

出版信息

PLoS Negl Trop Dis. 2010 Jul 20;4(7):e750. doi: 10.1371/journal.pntd.0000750.

Abstract

BACKGROUND

The infectious and diagnostic form of Entamoeba histolytica (Eh), cause of amebic dysentery and liver abscess, is the quadranucleate cyst. The cyst wall of Entamoeba invadens (Ei), a model for Eh, is composed of chitin fibrils and three sets of chitin-binding lectins that cross-link chitin fibrils (multivalent Jacob lectins), self-aggregate (Jessie lectins), and remodel chitin (chitinase). The goal here was to determine how well the Ei model applies to Entamoeba cysts from humans.

METHODS/RESULTS: An Eh Jacob lectin (EhJacob2) has three predicted chitin-binding domains surrounding a large, Ser-rich spacer. Recombinant EhJacob2 made in transfected Eh trophozoites binds to particulate chitin. Sequences of PCR products using primers flanking the highly polymorphic spacer of EhJacob2 may be used to distinguish Entamoeba isolates. Antibodies to the EhJacob2, EhJessie3, and chitinase each recognize cyst walls of clinical isolates of Entamoeba. While numerous sera from patients with amebic intestinal infections and liver abscess recognize recombinant EhJacob1 and EhJessie3 lectins, few of these sera recognize recombinant EhJacob2.

CONCLUSIONS/SIGNIFICANCE: The EhJacob2 lectin binds chitin and is polymorphic, and Jacob2, Jessie3, and chitinase are present in cyst walls of clinical isolates of Entamoeba. These results suggest there are substantial similarities between cysts of the human pathogen (Eh) and the in vitro model (Ei), even though there are quantitative and qualitative differences in their chitin-binding lectins.

摘要

背景

溶组织内阿米巴的感染和诊断形式(Eh),导致阿米巴痢疾和肝脓肿,是四核包囊。侵袭内阿米巴(Ei)的囊壁,Eh 的模型,由几丁质纤维和三套交联几丁质纤维的几丁质结合凝集素(多价 Jacob 凝集素)、自聚集(Jessie 凝集素)和重塑几丁质(几丁质酶)组成。这里的目标是确定 Ei 模型在多大程度上适用于人类的内阿米巴包囊。

方法/结果:EhJacob2 有三个预测的几丁质结合结构域,围绕一个富含丝氨酸的大间隔区。在转染的 Eh 滋养体中表达的重组 EhJacob2 与颗粒状几丁质结合。使用围绕 EhJacob2 高度多态性间隔区的引物进行 PCR 产物的序列分析,可以用于区分内阿米巴分离株。针对 EhJacob2、EhJessie3 和几丁质酶的抗体都能识别临床分离株的囊壁。虽然许多来自阿米巴肠感染和肝脓肿患者的血清能识别重组 EhJacob1 和 EhJessie3 凝集素,但这些血清中很少能识别重组 EhJacob2。

结论/意义:EhJacob2 凝集素结合几丁质,具有多态性,Jacob2、Jessie3 和几丁质酶存在于临床分离株的囊壁中。这些结果表明,人类病原体(Eh)的包囊与体外模型(Ei)之间存在实质性的相似之处,尽管它们的几丁质结合凝集素有数量和质量上的差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bf49/2907411/5b0b7be0ad24/pntd.0000750.g001.jpg

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