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首页> 外文期刊>Journal of Clinical Microbiology >Molecular Model for Studying the Uncultivated Fungal Pathogen Lacazia loboi
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Molecular Model for Studying the Uncultivated Fungal Pathogen Lacazia loboi

机译:研究未栽培真菌病原菌Lacazia loboi的分子模型

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Lacazia loboi is an uncultivated fungal pathogen of humans and dolphins that causes cutaneous and subcutaneous infections only in the tropical areas of the Americas. It was recently found by phylogenetic analysis that this unusual pathogen is closely related to Paracoccidioides brasiliensis and to the other fungal dimorphic members of the order Onygenales. That original phylogenetic study used universal primers to amplify well-known genes. However, this approach cannot be applied to the study of other proteins. We have developed a strategy for studying the gene encoding the gp43 homologous protein of P. brasiliensis in L. loboi. The gp43 protein was selected because it has been found that this P. brasiliensis antigen strongly reacts when it is used to test sera from patients with lacaziosis. The principle behind this idea was to obtain the gp43 amino acid sequence of P. brasiliensis and other homologous fungal sequences from GenBank and design primers from their aligned conserved regions. These sets of primers were used to amplify the selected regions with genomic DNA extracted from the yeast-like cells of L. loboi from experimentally infected mice. Using this approach, we amplified 483 bp of the L. loboi gp43-like gene. These sequences had 85% identity at the nucleotide level and 75% identity with the deduced amino acid sequences of the P. brasiliensis gp43 protein. The identity of the 483-bp DNA fragment was confirmed by phylogenetic analysis. This analysis revealed that the L. loboi gp43-like deduced amino acid sequence formed a strongly supported (100%) sister group with several P. brasiliensis gp43 sequences and that this taxon in turn was linked to the other fungal sequences used in this analysis. This study shows that the use of a molecular model for investigation of the genes encoding important proteins in L. loboi is feasible.
机译: Lacazia loboi 是人类和海豚的未经培养的真菌病原体,仅在美洲的热带地区引起皮肤和皮下感染。最近通过系统发育分析发现,这种不寻常的病原体与巴西寄生巴拉克西门虫(emacoparaciccides brasiliensis)以及Onygenales 顺序的其他真菌二态成员密切相关。最初的系统发育研究使用通用引物来扩增众所周知的基因。但是,这种方法不能应用于其他蛋白质的研究。我们已经开发出一种策略,用于研究编码 P的gp43同源蛋白的基因。 L中的brasiliensis 。 loboi 。选择gp43蛋白是因为已发现该 P。巴西来宾抗原可用于测试患有败血症的患者的血清。这个想法背后的原理是获得 P的gp43氨基酸序列。 GenBank的巴西巴西人(Brasiliensis)和其他同源真菌序列,以及从其对齐的保守区设计引物。这些引物组用于从 L的酵母样细胞中提取的基因组DNA扩增所选区域。来自实验感染小鼠的叶。使用这种方法,我们扩增了483 bp的 L。 loboi gp43样基因。这些序列在核苷酸水平具有85%的同一性,并且与推导的 P的氨基酸序列具有75%的同一性。巴西巴西人gp43蛋白。通过系统发育分析证实了483bp DNA片段的身份。该分析表明 L。 loboi gp43样推导的氨基酸序列形成了一个具有多个 P的强支持(100%)姊妹基团。 brasiliensis gp43序列,并且该分类单元又与本分析中使用的其他真菌序列相关。这项研究表明,使用分子模型研究 L中编码重要蛋白质的基因。 loboi 是可行的。

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