CANCER CELL:系统生物学方法将FUT8鉴定为黑色素瘤转移的驱动因素

2017-06-14 MedSci MedSci原创

我们的工作是利用系统生物学方法,尝试确定与黑素瘤患者样品中转移相关的关键糖基化变化并将其映射到酶上,揭示了岩藻糖基转移酶FUT8可以作为预防和治疗转移的抗肿瘤靶标。利用多种最先进的互补方法,我们确定FUT8在黑色素瘤转移中发挥作用,且核心岩藻糖基化是为癌细胞适应新的宿主环境(如转移部位)的重要因素,并确定某些蛋白,其异常核心岩藻糖基化赋予黑素瘤细胞攻击性行为,这些蛋白为特异性靶蛋白。

异常糖基化与黑素瘤进展的关联主要是基于细胞系的分析。在这项研究中,我们提出了基于系统生物学的方法,对血糖变化及相应的与患者样本中黑素瘤转移相关的酶进行分析。核心岩藻糖基化(FUT8)的上调和α-1,2岩藻糖基化(FUT1,FUT2)的下调被鉴定为转移性黑素瘤的特征。利用体外和体内双重研究,我们证明FUT8是黑素瘤转移的驱动因素,当FUT8沉默时,会抑制肿瘤入侵和传播。FUT8的糖蛋白靶标在细胞迁移蛋白中富集,其中就包括粘附分子L1CAM。核心岩藻糖基化影响L1CAM切割和L1CAM支持黑素瘤侵袭的能力。FUT8及其靶标因此可以作为黑素瘤转移的治疗靶点。

意义:我们的工作是利用系统生物学方法,尝试确定与黑素瘤患者样品中转移相关的关键糖基化变化并将其映射到酶上,揭示了岩藻糖基转移酶FUT8可以作为预防和治疗转移的抗肿瘤靶标。利用多种最先进的互补方法,我们确定FUT8在黑色素瘤转移中发挥作用,且核心岩藻糖基化是为癌细胞适应新的宿主环境(如转移部位)的重要因素,并确定某些蛋白,其异常核心岩藻糖基化赋予黑素瘤细胞攻击性行为,这些蛋白为特异性靶蛋白。

亮点:

1.原发性和转移性黑色素瘤显示不同的核心和α-1,2岩藻糖基化

2.FUT8促进黑素瘤转移

3.FUT8由TGIF2进行转录控制

4.FUT8介导的核心岩藻糖基化改变L1CAM蛋白水解切割和细胞侵袭

原文出处:

Praveen Agrawal,Lara K. Mahal, Eva Hernando,et al.A Systems Biology Approach Identifies FUT8 as a Driver of Melanoma Metastasis.[J].Cancer Cell 31, 804–819, June 12, 2017;DOI:http://dx.doi.org/10.1016/j.ccell.2017.05.007


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    2017-09-22 sunylz
  5. 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  6. 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  7. 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    2017-06-14 honghongwuwu

    谢谢分享,学习了

    0

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Sci Signal:新型机器人技术追踪癌症信号通路,及早发现癌症迹象!

恶性黑色素瘤是最常见,也是最危险的癌症类型之一。日前,来自亚历山大大学研究所的研究人员使用创新机器人技术研究棕色色素痣如何以及为什么变成恶性黑色素瘤。这一发现会使未来恶性黑色素瘤的诊断变得十分容易。研究人员还强调,为了避免恶性黑色素瘤,在使用很多化妆品和面霜的时候都应该格外小心。

NEJM:前哨淋巴结转移的黑色素瘤患者治疗手段选择

淋巴结切除可增加前哨淋巴结转移患者区域疾病控制并改善预后但不增加患者黑色素瘤特异性生存率

ASCO2017:黑色素瘤检查点抑制剂经验告诉我们关于其他癌症的免疫治疗?

自从2002年在黑素瘤患者中首次测试检查点抑制剂ipilimumab和tremelimumab之后,癌症免疫治疗领域的试验激增,增加了数百起新的试验,在肿瘤疗法领域的发展也迅猛增加。Ipilimumab,nivolumab和pembrolizumab已经成为治疗转移性黑色素瘤的主要治疗手段,但是更重要的临床发展是美国食品和药物管理局(FDA)批准三种不同的抗PD-1 / -PD-L1药物在非小

Oncologist:黑色素瘤免疫治疗,老少通吃!

针对PD-1/PD-L1的单克隆抗体彻底改变了黑色素瘤的治疗,然而其在各年龄段中的有效性和耐受性的数据有限。麻省总医院癌症中心的Ryan J. Sullivan在近日的The Oncologist上发表文章称,不管年龄如何,黑色素瘤患者都能安全地耐受抗PD-1/PD-L1单克隆抗体治疗,并实现相似的结局。

SCI REP:增加的血小板分布宽度可以预测黑色素瘤患者的不良预后!

总之,血小板分布宽度可以很容易从血常规中获取。该研究结果表明血小板分布宽度是黑色素瘤患者的一个独立的预测因素,也可能是黑色素瘤靶向治疗的一个潜在参数。