首页> 美国卫生研究院文献>The American Journal of Tropical Medicine and Hygiene >Triatoma infestans Calreticulin: Gene Cloning and Expression of a Main Domain That Interacts with the Host Complement System
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Triatoma infestans Calreticulin: Gene Cloning and Expression of a Main Domain That Interacts with the Host Complement System

机译:Triatoma infestans Calreticulin:Triatoma infestans Calreticulin:与主体互补系统相互作用的主要域的基因克隆和表达

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摘要

Triatoma infestans is an important hematophagous vector of Chagas disease, a neglected chronic illness affecting approximately 6 million people in Latin America. Hematophagous insects possess several molecules in their saliva that counteract host defensive responses. Calreticulin (CRT), a multifunctional protein secreted in saliva, contributes to the feeding process in some insects. Human CRT (HuCRT) and Trypanosoma cruzi CRT (TcCRT) inhibit the classical pathway of complement activation, mainly by interacting through their central S domain with complement component C1. In previous studies, we have detected CRT in salivary gland extracts from T. infestans. We have called this molecule TiCRT. Given that the S domain is responsible for C1 binding, we have tested its role in the classical pathway of complement activation in vertebrate blood. We have cloned and characterized the complete nucleotide sequence of CRT from T. infestans, and expressed its S domain. As expected, this S domain binds to human C1 and, as a consequence, it inhibits the classical pathway of complement, at its earliest stage of activation, namely the generation of C4b. Possibly, the presence of TiCRT in the salivary gland represents an evolutionary adaptation in hematophagous insects to control a potential activation of complement proteins, present in the massive blood meal that they ingest, with deleterious consequences at least on the anterior digestive tract of these insects.
机译:Triatoma infestans是Chagas病的重要嗜血传播媒介,Chagas病是一种被忽视的慢性病,​​在拉丁美洲影响了约600万人。食血昆虫的唾液中有几个分子可以抵消宿主的防御反应。钙网蛋白(CRT)是唾液中分泌的一种多功能蛋白质,有助于某些昆虫的摄食过程。人类CRT(HuCRT)和克氏锥虫(TcCRT)抑制补体激活的经典途径,主要是通过其中央S结构域与补体成分C1相互作用。在以前的研究中,我们已经在T. infestans唾液腺提取物中检测到了CRT。我们称此分子为TiCRT。鉴于S结构域负责C1结合,我们已经测试了其在脊椎动物血液中补体激活的经典途径中的作用。我们已经克隆并鉴定了来自T. infestans的CRT的完整核苷酸序列,并表达了其S结构域。如所期望的,该S结构域与人C1结合,因此,在其激活的最早阶段即C4b的产生,其抑制了补体的经典途径。唾液腺中TiCRT的存在可能代表着食血昆虫的进化适应,以控制其摄取的大量血粉中存在的补体蛋白的潜在活化,至少对这些昆虫的前消化道具有有害影响。

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