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t(8;21)急性髓系白血病细胞的单核苷酸多态性基因组阵列分析

Single nucleotide polymorphism genomic arrays analysis of t(8;21) acute myeloid leukemia cells.

作者信息

Akagi Tadayuki, Shih Lee-Yung, Ogawa Seishi, Gerss Joachim, Moore Stephen R, Schreck Rhona, Kawamata Norihiko, Liang Der-Cherng, Sanada Masashi, Nannya Yasuhito, Deneberg Stefan, Zachariadis Vasilios, Nordgren Ann, Song Jee Hoon, Dugas Martin, Lehmann Sören, Koeffler H Phillip

机构信息

Department of Stem Cell Biology, Graduate School of Medical Science, Kanazawa University, 13-1 Takara-machi, Kanazawa, Ishikawa, Japan.

出版信息

Haematologica. 2009 Sep;94(9):1301-6. doi: 10.3324/haematol.2009.005744.

DOI:10.3324/haematol.2009.005744
PMID:19734423
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2738725/
Abstract

Translocation of chromosomes 8 and 21, t(8;21), resulting in the AML1-ETO fusion gene, is associated with acute myeloid leukemia. We searched for additional genomic abnormalities in this acute myeloid leukemia subtype by performing single nucleotide polymorphism genomic arrays (SNP-chip) analysis on 48 newly diagnosed cases. Thirty-two patients (67%) had a normal genome by SNP-chip analysis (Group A), and 16 patients (33%) had one or more genomic abnormalities including copy number changes or copy number neutral loss of heterozygosity (Group B). Two samples had copy number neutral loss of heterozygosity on chromosome 6p including the PIM1 gene; and one of these cases had E135K mutation of Pim1. Interestingly, 38% of Group B and only 13% of Group A samples had a KIT-D816 mutation, suggesting that genomic alterations are often associated with a KIT-D816 mutation. Importantly, prognostic analysis revealed that overall survival and event-free survival of individuals in Group B were significantly worse than those in Group A.

摘要

8号和21号染色体易位,即t(8;21),会产生AML1-ETO融合基因,这与急性髓系白血病相关。我们通过对48例新诊断病例进行单核苷酸多态性基因组阵列(SNP芯片)分析,来寻找这种急性髓系白血病亚型中的其他基因组异常情况。通过SNP芯片分析,32例患者(67%)基因组正常(A组),16例患者(33%)存在一种或多种基因组异常,包括拷贝数改变或拷贝数中性杂合性缺失(B组)。两个样本在6号染色体短臂包括PIM1基因处存在拷贝数中性杂合性缺失;其中1例病例存在Pim1基因的E135K突变。有趣的是,B组38%的样本和A组仅13%的样本存在KIT-D816突变,这表明基因组改变常与KIT-D816突变相关。重要的是,预后分析显示,B组个体的总生存期和无事件生存期明显差于A组。

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