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骨髓瘤VL和VH基因序列揭示了肿瘤细胞中抗原选择的互补印记。

Myeloma VL and VH gene sequences reveal a complementary imprint of antigen selection in tumor cells.

作者信息

Sahota S S, Leo R, Hamblin T J, Stevenson F K

机构信息

Molecular Immunology Group, Tenovus Laboratory, Southampton University Hospitals, UK.

出版信息

Blood. 1997 Jan 1;89(1):219-26.

PMID:8978295
Abstract

In multiple myeloma, sequence studies of VH genes used to encode clonal Ig in neoplastic plasma cells have shown a common pattern of extensive somatic hypermutation. A further consistent feature of these VH sequences is a complete lack of intraclonal variation. These findings indicate that the malignant cell arises at a mature, postfollicular stage of B-cell development. However, only a minority of cases have a distribution of somatic mutations in VH consistent with a prior role for antigen in selecting the B cell of origin. To complement these studies, and to take further the investigation of a role for antigen in the clonal history of myeloma, we have investigated tumor-derived VL sequences from bone marrows of 15 patients. All sequences (9V kappa and 6V lambda A) were potentially functional and 5 of 15 had evidence for N-region additions. All had undergone extensive somatic hypermutation, and showed no intraclonal variation. In 4 of 15 cases, the distribution of mutations revealed a significant (P < .05) clustering of replacement mutations in the CDR sequences, indicating a role for VL in selection by antigen. Comparison with the VH sequences used by the same tumor cells showed that, if significant clustering was present, it was in either VH or VL but not both. Altogether, 10 of 15 V-regions showed evidence for antigen selection, suggesting that the B cell of origin has behaved as a normal germinal center B cell. Deductions concerning a role for antigen selection may require both VH and VL sequences for validation.

摘要

在多发性骨髓瘤中,对用于编码肿瘤性浆细胞中克隆性免疫球蛋白的VH基因进行的序列研究显示,存在广泛体细胞超突变的常见模式。这些VH序列的另一个一致特征是完全缺乏克隆内变异。这些发现表明,恶性细胞起源于B细胞发育的成熟滤泡后阶段。然而,只有少数病例的VH体细胞突变分布与抗原在选择起源B细胞中的先前作用一致。为了补充这些研究,并进一步调查抗原在骨髓瘤克隆历史中的作用,我们研究了15例患者骨髓中肿瘤衍生的VL序列。所有序列(9条Vκ和6条Vλ)都具有潜在功能,15条中有5条有N区添加的证据。所有序列都经历了广泛的体细胞超突变,且无克隆内变异。在15例中的4例中,突变分布显示CDR序列中替换突变有显著(P < 0.05)聚集,表明VL在抗原选择中起作用。与同一肿瘤细胞使用的VH序列比较表明,如果存在显著聚集,则仅在VH或VL中存在,而非两者都有。总共,15个V区中有10个显示出抗原选择的证据,这表明起源B细胞的行为类似于正常生发中心B细胞。关于抗原选择作用的推断可能需要VH和VL序列两者来验证。

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