Farooqi Ahsan S, Dagg Rebecca A, Choi L Mi Rim, Shay Jerry W, Reynolds C Patrick, Lau Loretta M S
Cancer Center, Department of Cell Biology and Biochemistry, Texas Tech University Health Sciences Center, Lubbock, TX, USA.
J Neurooncol. 2014 Aug;119(1):17-26. doi: 10.1007/s11060-014-1456-8. Epub 2014 May 3.
Alternative lengthening of telomeres (ALT) is a telomerase-independent telomere length maintenance mechanism that enables the unlimited proliferation of a subset of cancer cells. Some neuroblastoma (NB) tumors appear to maintain telomere length by activating ALT. Of 40 NB cell lines, we identified four potential ALT cell lines (CHLA-90, SK-N-FI, LA-N-6, and COG-N-291) that were telomerase-negative and had long telomeres (a feature of ALT cells). All four cell lines lacked MYCN amplification and were p53 non-functional upon irradiation. Two of these cell lines (CHLA-90 and SK-N-FI) were positive for C-circles (telomeric DNA circles) and ALT-associated promyelocytic leukemia nuclear bodies, both of which are phenotypic characteristics of ALT. Mutation of ATRX (associated with ALT in tumors) was only found in CHLA-90. Thus, the ALT phenotype in NB may not be limited to tumors with ATRX mutations but is associated with a lack of MYCN amplification and alterations in the p53 pathway.
端粒替代延长(ALT)是一种不依赖端粒酶的端粒长度维持机制,可使一部分癌细胞实现无限增殖。一些神经母细胞瘤(NB)肿瘤似乎通过激活ALT来维持端粒长度。在40种NB细胞系中,我们鉴定出四种潜在的ALT细胞系(CHLA-90、SK-N-FI、LA-N-6和COG-N-291),这些细胞系端粒酶阴性且具有长端粒(ALT细胞的一个特征)。所有四种细胞系均无MYCN扩增,且在辐射后p53功能丧失。其中两种细胞系(CHLA-90和SK-N-FI)C环(端粒DNA环)和ALT相关的早幼粒细胞白血病核体呈阳性,这两者都是ALT的表型特征。仅在CHLA-90中发现了与肿瘤中ALT相关的ATRX突变。因此,NB中的ALT表型可能不限于具有ATRX突变的肿瘤,而是与缺乏MYCN扩增和p53途径改变有关。
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