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The over-expression of cell migratory genes in alveolar rhabdomyosarcoma could contribute to metastatic spread.

机译:肺泡横纹肌肉瘤中细胞迁移基因的过度表达可能有助于转移扩散。

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Alveolar (ARMS) and Embryonal (ERMS) rhabdomyosarcoma differ in their response to current treatments. The ARMS subtype has a less favourable prognosis and often presents with widespread metastases, while the less metastatic ERMS has a 5 year survival rate of more than 80 %. In this study we investigate gene expression differences that could contribute to the high frequency of metastasis in ARMS. Microarray analysis identified significant differences in DNA repair, cell cycle and cell migration between the two RMS subtypes. Two genes up regulated in ARMS and involved in cell migration; the engulfment and cell motility gene 1 (ELMO1) and NEL-like 1 gene (NELL1) were selected for further investigation. Over-expression of ELMO1 significantly increased cell invasion from 24.70 ± 7% to 93 ± 5.4% in primary myoblasts and from 29.43 ± 2.1% to 87.33 ± 4.1% in the ERMS cell line RD. siRNA knockout of ELMO1 in the ARMS cell line RH30 significantly reduced cell invasion from 88.2 ± 3.8% to 35.2 ± 2.5%. Over-expression of NELL1 significantly increased myoblast invasion from 23.6 ± 6.9% to 100 ± 0.1%, but had no effect on invasion of the ERMS cell line RD. These findings suggest that ELMO1 may play a key role in ARMS metastasis. NELL1 increased invasion in primary myoblasts, but other factors required for it to enhance motility were not present in the RD ERMS cell line. Impairing ELMO1 function by pharmacological or siRNA knockdown could be a highly effective approach to reduce the metastatic spread of RMS.
机译:肺泡(ARMS)和胚胎(ERMS)横纹肌肉瘤对目前治疗的反应不同。 ARMS亚型的预后较差,通常会出现广泛的转移,而转移性较低的ERMS的5年生存率超过80%。在这项研究中,我们调查了可能导致ARMS转移频率高的基因表达差异。基因芯片分析确定了两种RMS亚型在DNA修复,细胞周期和细胞迁移方面的显着差异。两个基因在ARMS中被上调并参与细胞迁移。选择吞噬和细胞运动基因1(ELMO1)和NEL-like 1基因(NELL1)进行进一步研究。 ELMO1的过表达将原代成肌细胞的细胞浸润从24.70±7%显着提高到93±5.4%,而ERMS细胞系RD从29.43±2.1%增至87.33±4.1%。在ARMS细胞株RH30中ELMO1的siRNA敲除可将细胞侵袭从88.2±3.8%显着降低至35.2±2.5%。 NELL1的过度表达将成肌细胞侵袭从23.6±6.9%显着增加到100±0.1%,但对ERMS细胞系RD的侵袭没有影响。这些发现表明ELMO1可能在ARMS转移中起关键作用。 NELL1增加了对原代成肌细胞的侵袭,但在RD ERMS细胞系中不存在其增强运动性所需的其他因素。通过药理学或siRNA敲低损害ELMO1功能可能是减少RMS转移扩散的高效方法。

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