首页> 外文期刊>International journal of immunopathology and pharmacology. >Identification of SARS-COV Spike Protein-Derived and HLA-A2-Restricted Human CTL Epitopes by Using a New Muramyl Dipeptide-Derivative Adjuvant
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Identification of SARS-COV Spike Protein-Derived and HLA-A2-Restricted Human CTL Epitopes by Using a New Muramyl Dipeptide-Derivative Adjuvant

机译:通过使用新的Muramyl二肽衍生物佐剂鉴定SARS-COV穗蛋白衍生和HLA-A2限制性人类CTL表位。

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Severe acute respiratory syndrome (SARS) spread during the winter of 2003, and attempt have been made to develop vaccines against SARS corona virus (SARS-CoV). The present study provides a strategy to rapidly identify SARS-CoV-derived antigenic peptides recognized by HLA-A2-restricted cytotoxic T lymphocytes (CTLs). Forty-three candidate peptides having HLA-A2-binding motifs were selected in silico and HLA-A2/Db chimeric MHC class I-transgenic mice were immunized with these peptides and a new derivative of muramyl dipeptide that can induce upregulation of HLA-DR, CD80, CD86, and CD40 in human CD14+ antigen presenting cells, was administered as an adjuvant. Six HLA-A2-restricted mouse CTL epitopes were identified, including two new epitopes which have never been reported before. One of the novel peptides was naturally processed and successfully induced HLA-A2-restricted specific CTLs in both HLA transgenic mice and healthy donors. The method was useful, convenient and efficient for rapid identification of CTL epitopes derived from SARS-CoV proteins and will be possibly applicable for other pathogens to develop a peptide-based vaccine.
机译:严重急性呼吸系统综合症(SARS)在2003年冬季传播,并已尝试开发针对SARS日冕病毒(SARS-CoV)的疫苗。本研究提供了一种策略,可以快速鉴定被HLA-A2限制性细胞毒性T淋巴细胞(CTL)识别的SARS-CoV衍生抗原肽。在计算机上选择了43种具有HLA-A2结合基序的候选肽,并用这些肽和HLA-A2 / D b 嵌合的MHC I类嵌合转基因小鼠免疫了一种新的穆拉基二肽衍生物,可以在人CD14 + 抗原呈递细胞中诱导HLA-DR,CD80,CD86和CD40的上调,作为佐剂给药。确定了六个HLA-A2限制性小鼠CTL表位,包括两个从未报道过的新表位。一种新颖的肽是经过自然加工的,并成功地在HLA转基因小鼠和健康供体中诱导了HLA-A2限制性的特定CTL。该方法对于快速鉴定源自SARS-CoV蛋白的CTL表位是有用,方便和有效的,并且可能适用于其他病原体以开发基于肽的疫苗。

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