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涉及t(6;11)(q27;q23)白血病的带有Ras结合胞质蛋白AF6的嵌合MLL产物定位于细胞核。

Chimeric MLL products with a Ras binding cytoplasmic protein AF6 involved in t(6;11) (q27;q23) leukemia localize in the nucleus.

作者信息

Joh T, Yamamoto K, Kagami Y, Kakuda H, Sato T, Yamamoto T, Takahashi T, Ueda R, Kaibuchi K, Seto M

机构信息

Laboratory of Chemotherapy, Aichi Cancer Center Research Institute, Nagoya, Japan.

出版信息

Oncogene. 1997 Oct 2;15(14):1681-7. doi: 10.1038/sj.onc.1201332.

Abstract

In infantile leukemias and therapy-related leukemias, the MLL gene is frequently found to be disrupted and fused to various translocation partner genes, such as AF4/FEL, LTG9/AF9 and LTG19/ENL as a result of 11q23 translocations. We previously showed that the N-terminal portion common to various chimeric MLL products, as well as to MLL-LTG9 and MLL-LTG19, localizes in the nuclei, and therefore suggested that it might play an important role in leukemogenesis. In the present study, MLL-AF6 chimeric products found in the t(6;11)(q27;q23) translocation were analysed since AF6, a Ras-binding protein, exhibits a different subcellular localization from that of LTG9/AF9 and LTG19/ENL. Immunofluorescence staining data and cell fractionation analyses demonstrated that MLL-AF6 chimeric products localize in the nuclei despite the fact that AF6 itself localizes in the cytoplasm, confirming the importance of the nuclear localization of chimeric MLL products. The region in the N-terminal portion of MLL responsible for this nuclear localization was examined and found to be a region containing AT-hook motifs.

摘要

在婴儿白血病和治疗相关白血病中,经常发现MLL基因因11q23易位而被破坏,并与各种易位伙伴基因融合,如AF4/FEL、LTG9/AF9和LTG19/ENL。我们之前表明,各种嵌合MLL产物以及MLL-LTG9和MLL-LTG19共有的N端部分定位于细胞核,因此提示其可能在白血病发生中起重要作用。在本研究中,分析了在t(6;11)(q27;q23)易位中发现的MLL-AF6嵌合产物,因为Ras结合蛋白AF6的亚细胞定位与LTG9/AF9和LTG19/ENL不同。免疫荧光染色数据和细胞分级分离分析表明,尽管AF6本身定位于细胞质,但MLL-AF6嵌合产物定位于细胞核,这证实了嵌合MLL产物核定位的重要性。对MLL N端部分中负责这种核定位的区域进行了检查,发现是一个含有AT钩基序的区域。

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