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甲状腺钠-碘同向转运体与细菌和病毒蛋白的同源性。

Homologies of the thyroid sodium-iodide symporter with bacterial and viral proteins.

作者信息

Benvenga S, Alesci S, Trimarchi F, Facchiano A

机构信息

Cattedra di Endocrinologia, Università di Messina, Italy.

出版信息

J Endocrinol Invest. 1999 Jul-Aug;22(7):535-40. doi: 10.1007/BF03343605.

Abstract

We have demonstrated that Na+/I- symporter (NIS), a novel thyroid autoantigen, has local amino acid sequence homologies with the other thyroid autoantigens: Thyroglobulin (Tg), thyroid peroxidase (TPO) and thyrotropin receptor (TSH-R). These homologies concern the 4th, 5th, 6th extracellular loop and the beginning of the intracellular tail. We have expanded our studies and found that there are significant local homologies with other 11 proteins, most of them of bacterial or viral origin (e.g., Streptococcus or Herpes). These homologies concern the 2nd and 4th extracellular loop, and both the beginning and the end of the intracellular tail. These 11 homologies were retrieved by a computer-assisted search and extracted out of a database containing almost 300,000 amino acid sequences. These homologies were of magnitude greater than those concerning the three thyroid autoantigens [identities=51.1+/-7.3% vs 25.3+/-7.8% (mean+/-SD), p<0.001; similarities=70.6+/-10.7% vs 43.3+/-8.5%; p<0.001]. In addition, extensive, not local, homology was found with a number of unknown proteins from invertebrates (Drosophila melanogaster and Caenorhabditis elegans) and bacteria such as Bacillus subtilis and Xanthobacter. Previously, we had found that NIS has no extensive homology with Tg or TPO or TSH-R. This is the first demonstration of both extensive and local homologies between one thyroid autoantigen (NIS) and microbiological proteins. Taken together with data of the literature on the homologies between other thyroid antigens (Tg, TPO, TSH-R) and bacteria, the homologies we have now found reinforce the view that both bacterial and viral infections may trigger autoimmune thyroid diseases.

摘要

我们已经证明,钠/碘同向转运体(NIS)是一种新型甲状腺自身抗原,与其他甲状腺自身抗原:甲状腺球蛋白(Tg)、甲状腺过氧化物酶(TPO)和促甲状腺激素受体(TSH-R)存在局部氨基酸序列同源性。这些同源性涉及第4、5、6个细胞外环以及细胞内尾端起始部分。我们扩展了研究范围,发现与其他11种蛋白质存在显著的局部同源性,其中大多数来自细菌或病毒(如链球菌或疱疹病毒)。这些同源性涉及第2和第4个细胞外环,以及细胞内尾端的起始和末端。这11种同源性是通过计算机辅助搜索从一个包含近300,000个氨基酸序列的数据库中检索并提取出来的。这些同源性的程度大于与三种甲状腺自身抗原的同源性[同一性=51.1±7.3%对25.3±7.8%(平均值±标准差),p<0.001;相似性=70.6±10.7%对43.3±8.5%;p<0.001]。此外,还发现与一些来自无脊椎动物(黑腹果蝇和秀丽隐杆线虫)以及诸如枯草芽孢杆菌和黄杆菌等细菌的未知蛋白质存在广泛而非局部的同源性。此前,我们发现NIS与Tg、TPO或TSH-R不存在广泛同源性。这是首次证明一种甲状腺自身抗原(NIS)与微生物蛋白质之间存在广泛和局部同源性。结合文献中关于其他甲状腺抗原(Tg、TPO、TSH-R)与细菌之间同源性的数据,我们现在发现的同源性强化了细菌和病毒感染都可能引发自身免疫性甲状腺疾病这一观点。

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