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毛发细胞白血病中肿瘤 B 细胞受体轻链的二次重排导致等位基因排斥缺失。

Lack of allelic exclusion by secondary rearrangements of tumour B-cell receptor light chains in hairy cell leukaemia.

机构信息

Sezione and Unità di Ematologia, Università di Siena & AOUS, Italy.

出版信息

Hematol Oncol. 2011 Mar;29(1):31-7. doi: 10.1002/hon.952.

Abstract

Analyses of the tumour immunoglobulin (Ig) gene (IG) heavy (H) and light chains show heterogeneity of mutational status, but reveal common features of ongoing IGH isotype-switching with multiple IGH isotype expression and preference of IG lambda (IGL) light chain with selective use of IGLJ3. Phenotypic and immunogenetic analyses were performed in a series of 105 HCL patients to estimate prevalence of multiple IG light chain expression by the tumour cells. By phenotype, 3/105 HCL (2.9%) expressed double tumour-related Ig kappa (K) and L light chain proteins. By immunogenetic analysis, functional mutated double IGK(I) /IGK(II) , IGK(I) /IGL(I) and IGL(I) /IGL(II) transcripts were cloned and sequenced in 3/71 (4.2%) HCL. These latter three HCL expressed multiple IGH isotypes with mutated IGHVDJ rearrangements at the time of AID transcript expression. Most interestingly, the three cases had reinduced RAG1 transcript. In the double IGL expresser, single-cell analysis documented co-expression of the tumour-related IGLs in 5/6 cells (83%). In the IGK/IGL co-expresser, evidence of surface IgK/IgL isotype proteins confirmed functionality of the tumour-derived transcripts. The evidence of double light chain expression in single HCs and the new observation of RAG re-induction suggest ongoing selective influences on the BCR that may promote or maintain the HCL clone in the periphery.

摘要

对肿瘤免疫球蛋白(Ig)基因(IG)重链(H)和轻链的分析显示突变状态存在异质性,但揭示了正在进行的 IGH 同种型转换的共同特征,具有多种 IGH 同种型表达和对 IG 入(IGL)轻链的偏好,选择性使用 IGLJ3。对 105 例 HCL 患者进行了表型和免疫遗传学分析,以估计肿瘤细胞中多重 IG 轻链表达的患病率。通过表型,3/105 例 HCL(2.9%)表达了双重肿瘤相关 Ig kappa(K)和 L 轻链蛋白。通过免疫遗传学分析,在 3/71(4.2%)例 HCL 中克隆和测序了功能性突变的双重 IGK(I)/IGK(II)、IGK(I)/IGL(I)和 IGL(I)/IGL(II)转录本。这三个 HCL 在 AID 转录物表达时表达了多种 IGH 同种型,并且具有突变的 IGHVDJ 重排。最有趣的是,这三个病例重新诱导了 RAG1 转录本。在双重 IGL 表达者中,单细胞分析在 5/6 个细胞(83%)中记录到肿瘤相关 IGL 的共表达。在 IGK/IGL 共表达者中,表面 IgK/IgL 同种型蛋白的证据证实了肿瘤衍生转录物的功能。在单个 HC 中双轻链表达的证据以及 RAG 重新诱导的新观察结果表明,BCR 持续受到选择性影响,这可能促进或维持外周的 HCL 克隆。

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