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慢性髓性白血病中的变异Ph易位

Variant Ph translocations in chronic myeloid leukemia.

作者信息

Heim S, Billström R, Kristoffersson U, Mandahl N, Strömbeck B, Mitelman F

出版信息

Cancer Genet Cytogenet. 1985 Nov;18(3):215-27. doi: 10.1016/0165-4608(85)90086-x.

Abstract

Variant translocations were found in eight of 142 consecutive patients with Ph-positive, chronic myeloid leukemia encountered in our laboratory during the last decade. Two patients had simple, two-way variant translocations: t(17;22)(p13;q11) and t(16;22)(q24;q11). Both of these patients had an additional translocation involving chromosomes #9: t(7;9)(q22;q34) and t(9;17)(q34;q21), respectively. Complex variant translocations were found in four cases: t(2;9;22)(p23q12;q34;q11), t(3;9;22)(p21;q34;q11), t(9;12;22)(q34;q13;q11q13), and t(13;17;22)(p11;p11q21;q11). In two cases, the only discernable cytogenetic aberration was del(22)(q11). A review of the chromosomal breakpoints involved in this series and in 185 cases of variant Ph translocations previously reported in the literature reveals that a disproportionately large number of breakpoints are located in light-staining regions of G-banded chromosomes. Furthermore, the breakpoints in simple variant translocations are more often located in terminal chromosomal regions, whereas, the breakpoints in complex translocations typically affect nonterminal bands. No obvious correlation was detected between variant Ph translocation breakpoints and either fragile sites, oncogene locations, or consistent chromosome breakpoints in other malignancies.

摘要

在过去十年间,我们实验室接诊的142例Ph阳性慢性髓性白血病患者中,有8例发现了变异易位。2例患者出现简单的双向变异易位:t(17;22)(p13;q11)和t(16;22)(q24;q11)。这2例患者均还有一个涉及9号染色体的额外易位,分别为t(7;9)(q22;q34)和t(9;17)(q34;q21)。4例发现了复杂变异易位:t(2;9;22)(p23q12;q34;q11)、t(3;9;22)(p21;q34;q11)、t(9;12;22)(q34;q13;q11q13)和t(13;17;22)(p11;p11q21;q11)。2例中,唯一可识别的细胞遗传学异常为del(22)(q11)。回顾本系列病例以及先前文献报道的185例变异Ph易位病例中涉及的染色体断点发现,大量断点位于G带染色体的浅染区域。此外,简单变异易位中的断点更常位于染色体末端区域,而复杂易位中的断点通常影响非末端带。未检测到变异Ph易位断点与脆性位点、癌基因位置或其他恶性肿瘤中一致的染色体断点之间存在明显相关性。

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