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钙网蛋白在体内具有肽结合活性,并且能够引发针对结合肽的细胞毒性T淋巴细胞反应。

Calreticulin displays in vivo peptide-binding activity and can elicit CTL responses against bound peptides.

作者信息

Nair S, Wearsch P A, Mitchell D A, Wassenberg J J, Gilboa E, Nicchitta C V

机构信息

Center for Cellular and Genetic Therapy, Department of Surgery, Department of Cell Biology, Duke University Medical Center, Durham, NC 27710, USA.

出版信息

J Immunol. 1999 Jun 1;162(11):6426-32.

PMID:10352256
Abstract

Calreticulin is an endoplasmic reticulum (ER) chaperone that displays lectin activity and contributes to the folding pathways for nascent glycoproteins. Calreticulin also participates in the reactions yielding assembly of peptides onto nascent MHC class I molecules. By chemical and immunological criteria, we identify calreticulin as a peptide-binding protein and provide data indicating that calreticulin can elicit CTL responses to components of its bound peptide pool. In an adoptive immunotherapy protocol, dendritic cells pulsed with calreticulin isolated from B16/F10.9 murine melanoma, E.G7-OVA, or EL4 thymoma tumors elicited a CTL response to as yet unknown tumor-derived Ags or the known OVA Ag. To evaluate the relative efficacy of calreticulin in eliciting CTL responses, the ER chaperones GRP94/gp96, BiP, ERp72, and protein disulfide isomerase were purified in parallel from B16/F10.9, EL4, and E.G7-OVA tumors, and the capacity of the proteins to elicit CTL responses was compared. In both the B16/F10.9 and E.G7-OVA models, calreticulin was as effective as or more effective than GRP94/gp96 in eliciting CTL responses. Little to no activity was observed for BiP, ERp72, and protein disulfide isomerase. The observed antigenic activity of calreticulin was recapitulated in in vitro experiments, in which it was observed that pulsing of bone marrow dendritic cells with E.G7-OVA-derived calreticulin elicited sensitivity to lysis by OVA-specific CD8+ T cells. These data identify calreticulin as a peptide-binding protein and indicate that calreticulin-bound peptides can be re-presented on dendritic cell class I molecules for recognition by CD8+ T cells.

摘要

钙网蛋白是一种内质网(ER)伴侣蛋白,具有凝集素活性,有助于新生糖蛋白的折叠途径。钙网蛋白还参与将肽组装到新生MHC I类分子上的反应。通过化学和免疫学标准,我们确定钙网蛋白为一种肽结合蛋白,并提供数据表明钙网蛋白可引发针对其结合肽库成分的CTL反应。在一项过继免疫治疗方案中,用从B16/F10.9小鼠黑色素瘤、E.G7-OVA或EL4胸腺瘤肿瘤中分离出的钙网蛋白脉冲处理的树突状细胞引发了针对尚未知的肿瘤衍生抗原或已知OVA抗原的CTL反应。为了评估钙网蛋白在引发CTL反应中的相对效力,从B16/F10.9、EL4和E.G7-OVA肿瘤中平行纯化了内质网伴侣蛋白GRP94/gp96、BiP、ERp72和蛋白二硫键异构酶,并比较了这些蛋白引发CTL反应的能力。在B16/F10.9和E.G7-OVA模型中,钙网蛋白在引发CTL反应方面与GRP94/gp96一样有效或更有效。BiP、ERp72和蛋白二硫键异构酶几乎没有活性。钙网蛋白的抗原活性在体外实验中得到重现,在该实验中观察到用E.G7-OVA衍生的钙网蛋白脉冲处理骨髓树突状细胞可引发对OVA特异性CD8+ T细胞裂解的敏感性。这些数据确定钙网蛋白为一种肽结合蛋白,并表明钙网蛋白结合的肽可在树突状细胞I类分子上重新呈递以供CD8+ T细胞识别。

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