首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Comparison of constitutional and tumor-associated 11;22 translocations: nonidentical breakpoints on chromosomes 11 and 22.
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Comparison of constitutional and tumor-associated 11;22 translocations: nonidentical breakpoints on chromosomes 11 and 22.

机译:体质和与肿瘤相关的11; 22易位的比较:11号和22号染色体上的不同断点。

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摘要

Recurring, site-specific chromosomal rearrangements are associated with several human syndromes and malignant disorders. Such nonrandom translocations involving chromosome 22 in band q11 are numerous and found to be associated with a diversity of neoplasms as well as constitutional disorders. Chromosome 11 in bands q23-q24 is similarly involved in several types of tumors as well as in a recurring constitutional reciprocal translocation with chromosome 22. Here we report the use of chromosomal in situ hybridization to compare the translocation breakpoints in the cytologically indistinguishable constitutional t(11;22) and the tumor-related t(11;22) associated with Ewing sarcoma and peripheral neuroepithelioma. We have shown that the breakpoints can be distinguished from each other with respect to the locus encoding the constant region of the Ig lambda light chain (C lambda) at 22q11 and the ETS1 locus at 11q23----q24; ETS1 has been called hu-ets-1 or human c-ets-1. The tumor-associated chromosome 11 breakpoint is also different from those of leukemias with t(9;11) and t(4;11) translocations. Southern-blot analysis showed no rearrangement of ETS1 in these disorders in the region detected by our probe. ETS1 has also been mapped more precisely to 11q23.3----q24 by in situ hybridization to cells from an individual with an 11q23.3----qter deletion.
机译:反复发生的,特定于位点的染色体重排与几种人类综合征和恶性疾病有关。这种涉及q11波段22号染色体的非随机易位现象很多,并且被发现与多种肿瘤以及体质疾病有关。 q23-q24带中的11号染色体同样与几种类型的肿瘤有关,并与22号染色体反复发生宪法性易位。 11; 22)和与肿瘤相关的t(11; 22)与尤因肉瘤和周围神经上皮瘤相关。我们已经表明,对于在22q11处编码Igλ轻链(Cλ)恒定区和在11q23 ---- q24处的ETS1编码区的恒定区而言,可以将断点区分开。 ETS1被称为hu-ets-1或人类c-ets-1。肿瘤相关的11号染色体断裂点也与t(9; 11)和t(4; 11)易位的白血病不同。 Southern印迹分析显示在我们的探针检测到的区域中的这些疾病中,ETS1没有重排。通过与具有11q23.3 ---- qter缺失的个体的细胞原位杂交,ETS1也已更精确地定位到11q23.3 ---- q24。

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