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在 B 细胞恶性肿瘤中鉴定出一种替代的 CD20 转录变体,该变体编码一种与利妥昔单抗耐药相关的新型蛋白。

Identification of an alternative CD20 transcript variant in B-cell malignancies coding for a novel protein associated to rituximab resistance.

机构信息

Inserm, Unite Mixte de Recherche (UMR) 645, 25020 Besançon, France.

出版信息

Blood. 2010 Mar 25;115(12):2420-9. doi: 10.1182/blood-2009-06-229112. Epub 2010 Jan 20.

Abstract

Human CD20 is a B-cell lineage-specific marker expressed by normal and leukemic B cells from the pre-B to the plasma-cell stages and is a target for rituximab (RTX) immunotherapy. A CD20 reverse transcriptase-polymerase chain reaction (PCR) on B-cell lines cDNA yielded a short PCR product (DeltaCD20) corresponding to a spliced mRNA transcript linking the exon 3 and exon 7 ends. We established here that this novel, alternatively spliced CD20 transcript is expressed and detectable at various levels in leukemic B cells, lymphoma B cells, in vivo tonsil- or in vitro CD40L-activated B cells, and Epstein-Barr virus (EBV)-transformed B cells, but not in resting CD19(+)- or CD20(+)-sorted B cells from peripheral blood or bone marrow of healthy donors. The truncated CD20 sequence is within the reading frame, codes a protein of 130 amino acids ( approximately 15-17 kDa) lacking large parts of the 4 transmembrane segments, suggesting that DeltaCD20 is a nonanchored membrane protein. We demonstrated the translation into a DeltaCD20 protein which is associated with the membrane CD20 protein and showed its involvement in RTX resistance. Study of patient samples before and after RTX resistance or escape confirms our in vitro findings.

摘要

人 CD20 是 B 细胞谱系特异性标志物,表达于正常和白血病 B 细胞,从前 B 细胞到浆细胞阶段,是利妥昔单抗(RTX)免疫治疗的靶点。B 细胞系 cDNA 的 CD20 逆转录-聚合酶链反应(PCR)产生了一个短的 PCR 产物(DeltaCD20),对应于连接外显子 3 和外显子 7 末端的剪接 mRNA 转录本。我们在这里证实,这种新的、选择性剪接的 CD20 转录本在白血病 B 细胞、淋巴瘤 B 细胞、体内扁桃体或体外 CD40L 激活的 B 细胞和 EBV 转化的 B 细胞中表达,并可检测到不同水平,但在健康供体外周血或骨髓中的静止 CD19(+)-或 CD20(+)-分选 B 细胞中不可检测。截断的 CD20 序列在阅读框内,编码 130 个氨基酸(约 15-17 kDa)的蛋白质,缺失大部分 4 个跨膜区,提示 DeltaCD20 是一种非锚定膜蛋白。我们证明了 DeltaCD20 蛋白的翻译,该蛋白与膜 CD20 蛋白相关,并表明其与 RTX 耐药性有关。对 RTX 耐药或逃逸前后患者样本的研究证实了我们的体外发现。

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