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Chromosomal Imbalances in Primary Lymphomas of the Central Nervous System

机译:中枢神经系统原发性淋巴瘤的染色体失衡

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摘要

Twenty-two primary central nervous system lymphomas of immunocompetent adults were studied by comparative genomic hybridization. All were high-grade diffuse large B cell lymphomas. Comparative genomic hybridization revealed an average of 5.5 chromosomal changes per tumor, with gains being more common than losses (3.5 vs. 2.0). The most frequent DNA copy number changes were gains on chromosomes 1, 12, 18 (41% each), 7 (23%), and 11 (18%) and losses involving chromosomes 6 (59%), 18, and 20 (18% each). Commonly involved regions were +12q (41%), +18q (36%), +1q (32%), and +7q (23%), as well as −6q (50%), −6p (18%), −17p, and −18p (14% each). High-level gains were found on 7 chromosomes, mainly involving chromosomes 18q (23%), 12q (18%), and 1q (14%). Minimal common regions of over- and underrepresentation were found on +1q25–31, −6q16–21, +7q11.2, +12p11.2–13, +12q12–14, +12q22–24.1, and +18q12.2–21.3. A significant correlation between loss of DNA copy numbers on chromosome 6q and shorter survival could be established (10.2 vs. 22.3 months; P < 0.05). Our findings suggest that chromosomal imbalances of primary central nervous system lymphomas are similar to those of diffuse large B cell lymphomas at other locations and are probably not related to cerebral presentation; however, they may be prognostically relevant.
机译:通过比较基因组杂交研究了22名具有免疫能力的成年人的原发性中枢神经系统淋巴瘤。均为高度弥漫性大B细胞淋巴瘤。比较基因组杂交显示每个肿瘤平均有5.5个染色体变化,收益多于损失(3.5比2.0)。 DNA拷贝数变化最频繁的是分别在1号,12号,18号(分别占41%),7号(23%)和11号(占18%)上增加,以及与6号(59%),18号和20号染色体有关的丢失(18个)。 %)。共同参与的区域是+ 12q(41%),+ 18q(36%),+ 1q(32%)和+ 7q(23%)以及-6q(50%),-6p(18%), -17p和-18p(各14%)。在7条染色体上发现了高水平的扩增,主要涉及18q(23%),12q(18%)和1q(14%)染色体。在+ 1q25–31,−6q16–21,+ 7q11.2,+ 12p11.2–13,+ 12q12–14,+ 12q22–24.1和+ 18q12.2–11.3上找到了最小的过量代表和共同代表区域。可以确定染色体6q上DNA拷贝数的减少与存活时间的缩短之间存在显着的相关性(10.2对22.3个月; P <0.05)。我们的发现表明,原发性中枢神经系统淋巴瘤的染色体失衡与其他部位的弥漫性大B细胞淋巴瘤的染色体失衡相似,可能与脑部表现无关。但是,它们可能与预后相关。

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