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预测的乳房链球菌黏附分子(SUAM)的抗原区域参与黏附和内化到乳腺上皮细胞。

Predicted antigenic regions of Streptococcus uberis adhesion molecule (SUAM) are involved in adherence to and internalization into mammary epithelial cells.

机构信息

Department of Animal Science, The University of Tennessee, Knoxville, TN 37996, USA.

出版信息

Vet Microbiol. 2011 Mar 24;148(2-4):323-8. doi: 10.1016/j.vetmic.2010.09.017. Epub 2010 Oct 20.

Abstract

Streptococcus uberis is a significant cause of bovine mastitis throughout the world. Previous work from our laboratory demonstrated that S. uberis adhesion molecule (SUAM) is an important factor in adherence to and internalization of S. uberis into bovine mammary epithelial cells. Antibodies directed against SUAM significantly reduced bacterial adherence to and internalization into bovine mammary epithelial cells implying that SUAM is surface exposed. Objectives of this research were to: (1) predict surface exposed peptides, and (2) select peptide sequences for production of synthetic peptides with the final aim of evaluating their role in adherence and internalization and immunogenic potential. The Kyte/Doolittle hydropathicity prediction method; Chou/Fasman β-turn prediction method; and output from Coils, Paircoil and MultiCoil scores for prediction of secondary and tertiary structures were used. Prediction algorithms resulted in identification of five overlapping regions of the SUAM sequence with the most hydrophilic valleys and the highest peaks for β-turns. The five 15-mer SUAM epitopes selected by bioinformatic analysis were produced to evaluate the immunogenic value and pathogenic role of these putative domains. Peptides were bound to fluorescent latex beads, incubated with MAC-T bovine mammary epithelial cells, and internalization into MAC-T cells was evaluated using confocal laser and transmission electron microscopy. All peptides evaluated induced some degree of internalization of fluorescent beads into MAC-T cells; however, 2 peptides induced significantly more internalization of fluorescent beads than the other peptides evaluated. These peptides, designated III and IV, were located in the central region of SUAM, between two coiled-coil regions. Convalescent sera were tested against these biotinylated peptides for SUAM specific immune response using an indirect ELISA format. Among the 5 peptides evaluated, peptides I, II and V elicited significant serological response suggesting that the N-terminal region (peptide I), central region (peptide II) and C-terminal region (peptide V) are immunodominant epitopes of SUAM. Results will be useful to design immunotherapeutic tools based on immunodominant epitopes.

摘要

停乳链球菌是引起全世界奶牛乳腺炎的重要原因。我们实验室的先前工作表明,停乳链球菌黏附素(SUAM)是停乳链球菌黏附和内化到牛乳腺上皮细胞的重要因素。针对 SUAM 的抗体显著降低了细菌对牛乳腺上皮细胞的黏附和内化,这意味着 SUAM 是表面暴露的。本研究的目的是:(1)预测表面暴露的肽,(2)选择肽序列以生产具有最终目的的合成肽,评估它们在黏附和内化以及免疫原性中的作用。使用 Kyte/Doolittle 亲水性预测方法;Chou/Fasman β-转角预测方法;以及 Coils、Paircoil 和 MultiCoil 评分的输出,预测二级和三级结构。预测算法确定了 SUAM 序列中五个重叠区域,这些区域具有最亲水的山谷和最高的β-转角峰。通过生物信息学分析选择了 5 个 15 -mer SUAM 表位,以评估这些假定结构域的免疫原性价值和致病作用。将肽与荧光乳胶珠结合,与 MAC-T 牛乳腺上皮细胞孵育,并使用共聚焦激光和透射电子显微镜评估肽进入 MAC-T 细胞的内化。评估的所有肽都诱导了一定程度的荧光珠内化到 MAC-T 细胞中;然而,有 2 个肽诱导的荧光珠内化程度明显高于评估的其他肽。这些肽,命名为 III 和 IV,位于 SUAM 的中心区域,在两个卷曲螺旋区域之间。使用间接 ELISA 格式,用生物素化肽检测恢复期血清针对 SUAM 的特异性免疫反应。在评估的 5 个肽中,肽 I、II 和 V 引起了显著的血清学反应,这表明 N 末端区域(肽 I)、中心区域(肽 II)和 C 末端区域(肽 V)是 SUAM 的免疫优势表位。结果将有助于基于免疫优势表位设计免疫治疗工具。

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