成人t细胞白血病细胞中不依赖税收的IkappaB激酶激活。

Noriko Hironaka, Kanako Mochida, Naoki Mori, Michiyuki Maeda, Naoki Yamamoto, Shoji Yamaoka
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摘要

成人t细胞白血病(ATL)是一种致命的t细胞恶性肿瘤,在感染人类t细胞白血病病毒I型(HTLV-I)后长期发生。我们之前报道过核因子- kappab (NF-kappaB)在ATL细胞中被组成性激活,尽管几乎检测不到病毒蛋白的表达,包括已知持续激活NF-kappaB的Tax。在这里,我们证明不表达可检测的Tax蛋白的ATL细胞表现出组成IkappaB激酶(IKK)活性。转染研究显示IKK1的显性阴性形式,而不是IKK2或NF-kappaB必需调节剂(NEMO),抑制ATL细胞中的组成型NF-kappaB活性。这种IKK活性伴随着p52的表达升高,表明最近描述的NF-kappaB激活的非规范途径在ATL细胞中起作用。我们最终发现,在htlv -i感染的T细胞中,无论Tax表达如何,IkappaBalpha的超抑制形式(SR-IkappaBalpha)对NF-kappaB的特异性抑制都会导致细胞死亡,这为NF-kappaB在ATL细胞存活中发挥重要作用提供了明确的证据。总之,IKK复合物在ATL细胞中通过不同于税收介导的IKK激活的细胞机制被组成性激活。进一步阐明这种细胞机制将有助于建立治疗ATL的基本原理。
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Tax-independent constitutive IkappaB kinase activation in adult T-cell leukemia cells.

Adult T-cell leukemia (ATL) is a fatal T-cell malignancy that arises long after infection with human T-cell leukemia virus type I (HTLV-I). We reported previously that nuclear factor-kappaB (NF-kappaB) was constitutively activated in ATL cells, although expression of the viral proteins was barely detectable, including Tax, which was known to persistently activate NF-kappaB. Here we demonstrate that ATL cells that do not express detectable Tax protein exhibit constitutive IkappaB kinase (IKK) activity. Transfection studies revealed that a dominant-negative form of IKK1, and not of IKK2 or NF-kappaB essential modulator (NEMO), suppressed constitutive NF-kappaB activity in ATL cells. This IKK activity was accompanied by elevated expression of p52, suggesting that the recently described noncanonical pathway of NF-kappaB activation operates in ATL cells. We finally show that specific inhibition of NF-kappaB by a super-repressor form of IkappaBalpha (SR-IkappaBalpha) in HTLV-I-infected T cells results in cell death regardless of Tax expression, providing definitive evidence of an essential role for NF-kappaB in the survival of ATL cells. In conclusion, the IKK complex is constitutively activated in ATL cells through a cellular mechanism distinct from that of Tax-mediated IKK activation. Further elucidation of this cellular mechanism should contribute to establishing a rationale for treatment of ATL.

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