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A NOVEL UNCONVENTIONAL ANTIGEN MPD5 ELICITS ANTI-TUMOR HUMORAL IMMUNE RESPONSES IN A SUBSET OF PATIENTS WITH POLYCYTHEMIA VERA

机译:一种新的非常规抗原MPD5引发了多发性紫癜患者亚型的抗肿瘤体液免疫反应

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摘要

In an effort to define the antigenic mechanism that contributes to beneficial therapeutic outcomes in patients with polycythemia vera (PV), we screened a human testis cDNA library with serological cloning derived from sera of three PV patients who had undergone therapeutic-induced remission. As a result, we identified a novel antigen, MPD5, which belongs to the group of cryptic antigens with unconventional genomic intron/exon structure. Moreover, MPD5 elicited IgG antibody responses in a subset of PV patients who had benefited from a variety of therapies—including IFN-α, Hydroxyurea, Imatinib mesylate, Anagrelide, and phlebotomy—but not in untreated PV patients or healthy donors, suggesting that MPD5 is a PV-associated, therapy-related antigen. In the granulocytes of PV patients who are responsive to therapy, upregulated MPD5 expression may serve to enhance immune responses. These findings provide new insight into the mechanism underlying regulation of the self-antigen repertoire that elicits anti-tumor immune responses in patients with myeloproliferative diseases, indicating the potential of these self-antigens as targets of novel immunotherapy.
机译:为了确定有助于真性红细胞增多症(PV)患者有益治疗结果的抗原机制,我们筛选了人类睾丸cDNA文库,其血清学克隆来源于三名接受治疗性缓解的PV患者的血清。结果,我们鉴定出一种新型抗原MPD5,其属于具有非常规基因组内含子/外显子结构的隐性抗原。此外,MPD5在部分受益于多种疗法的PV患者子集中引发IgG抗体反应,这些疗法包括IFN-α,羟基脲,甲磺酸伊马替尼,阿那格雷和静脉放血,但未治疗的PV患者或健康供体中却没有。是与PV相关的治疗相关抗原。在对治疗有反应的PV患者的粒细胞中,MPD5表达上调可能有助于增强免疫反应。这些发现提供了对自我抗原库调节的潜在机制的新见解,该机制引发了骨髓增生性疾病患者的抗肿瘤免疫反应,表明这些自我抗原作为新型免疫疗法的靶标的潜力。

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