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修饰后的重组人促红细胞生成素,可能降低免疫原性。

Modified recombinant human erythropoietin with potentially reduced immunogenicity.

机构信息

Program in Environmental Toxicology, Chulabhorn Graduate Institute, Bangkok, 10210, Thailand.

Translational Research Unit, Chulabhorn Research Institute, Bangkok, 10210, Thailand.

出版信息

Sci Rep. 2021 Jan 15;11(1):1491. doi: 10.1038/s41598-020-80402-1.

Abstract

Recombinant human erythropoietin (rHuEPO) is a biopharmaceutical drug given to patients who have a low hemoglobin related to chronic kidney disease, cancer or anemia. However, some patients repeatedly receiving rHuEPO develop anti-rHuEPO neutralizing antibodies leading to the development of pure red cell aplasia (PRCA). The immunogenic antibody response activated by rHuEPO is believed to be triggered by T-cells recognizing EPO epitopes bound to MHC molecules displayed on the cell surface of APCs. Previous studies have reported an association between the development of anti-rHuEpo-associated PRCA and the HLA-DRB109 gene, which is reported to be entrenched in the Thai population. In this study, we used computational design to screen for immunogenic hotspots recognized by HLA-DRB109, and predicted seventeen mutants having anywhere between one through four mutations that reduce affinity for the allele, without disrupting the structural integrity and bioactivity. Five out of seventeen mutants were less immunogenic in vitro while retaining similar or slightly reduced bioactivity than rHuEPO. These engineered proteins could be the potential candidates to treat patients who are rHuEpo-dependent and express the HLA-DRB1*09 allele.

摘要

重组人促红细胞生成素(rHuEPO)是一种生物制药药物,用于治疗因慢性肾病、癌症或贫血导致血红蛋白水平低的患者。然而,一些反复接受 rHuEPO 治疗的患者会产生抗 rHuEPO 中和抗体,导致纯红细胞再生障碍性贫血(PRCA)的发生。rHuEPO 激活的免疫原性抗体反应被认为是由 T 细胞识别与 MHC 分子结合的 EPO 表位引发的,这些 MHC 分子在 APC 的细胞表面上表达。先前的研究报告称,抗 rHuEpo 相关 PRCA 的发生与 HLA-DRB109 基因有关,该基因在泰国人群中根深蒂固。在这项研究中,我们使用计算设计筛选 HLA-DRB109 识别的免疫原性热点,并预测了十七种突变体,这些突变体在不破坏结构完整性和生物活性的情况下,其等位基因亲和力降低了一个到四个突变。十七个突变体中有五个在体外的免疫原性较低,而保留了与 rHuEPO 相似或略有降低的生物活性。这些工程蛋白可能是治疗依赖 rHuEPO 并表达 HLA-DRB1*09 等位基因的患者的潜在候选药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/36ce/7810742/c2bb3c0df3b5/41598_2020_80402_Fig1_HTML.jpg

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