Defective IκBα in Hodgkin cell lines with constitutively active NF-κB

Wood, Katrina; Roff, Marilynn A.; Hay, Ronald T.

doi:10.1038/sj.onc.1201735

Cited by 123 publications

(92 citation statements)

References 39 publications

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“…In agreement with a recent publication (Wood et al, 1998), we did not detect full length IkBa protein in L428 or KMH-2 cells. Disruption of wild type IkBa (wtIkBa) expression in both cell lines resulted from point mutations, which cause expression of truncated IkBa (data not shown).…”

Section: Discussionsupporting

confidence: 93%

Molecular mechanisms of constitutive NF-κB/Rel activation in Hodgkin/Reed-Sternberg cells

et al. 1999

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A common characteristic of malignant cells derived from patients with Hodgkin's disease (HD) is a high level of constitutive nuclear NF-kB/Rel activity, which stimulates proliferation and confers resistance to apoptosis. We have analysed the mechanisms that account for NF-kB activation in a panel of Hodgkin/Reed-Sternberg (H-RS) cell lines. Whereas two cell lines (L428 and KMH-2) expressed inactive IkBa, no signi®cant changes in NF-kB or IkB expression were seen in other H-RS cells (L591, L1236 and HDLM-2). Constitutive NF-kB was susceptible to inhibition by recombinant IkBa, suggesting that neither mutations in the NF-kB genes nor posttranslational modi®cations of NF-kB were involved. Endogenous IkBa was bound to p65 and displayed a very short half-life. IkBa degradation could be blocked by inhibitors of the NF-kB activating pathway. Proteasomal inhibition caused an accumulation of phosphorylated IkBa and a reduction of NF-kB activity in HDLM-2 and L1236 cells. By in vitro kinase assays we demonstrate constitutive IkB kinase (IKK) activity in H-RS cells, indicating ongoing signal transduction. Furthermore, H-RS cells secrete one or more factor(s) that were able to trigger NF-kB activation. We conclude that aberrant activation of IKK's, and in some cases defective IkBs, lead to constitutive nuclear NF-kB activity, which in turn results in a growth advantage of Hodgkin's disease tumor cells.

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Section: Discussionsupporting

confidence: 93%

Molecular mechanisms of constitutive NF-κB/Rel activation in Hodgkin/Reed-Sternberg cells

et al. 1999

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“…This latter model would be consistent with the complete loss of p100 NF-kB-2 seen in the HUT78 CTCL cells, as well as with the lymphoid hyperplasia observed in mice in which targeted gene deletions were performed to`knock-out' p100 while retaining p52 gene expression (Ishikawa et al, 1997). A model invoking loss of IkB-like activity would also be consistent with older reports that inhibition of IkBa by antisense approaches resulted in transformation of NIH3T3 cells (Beauparlant et al, 1994), and with reports of IkBa mutations in patients with Hodgkin's disease (Cabannes et al, 1999;Krappmann et al, 1999;Wood et al, 1998). This model is also reminiscent of one reported mechanism by which HTLV-1 Tax leads to increased NF-kB activity (Kanno et al, 1994).…”

Section: Discussionsupporting

confidence: 84%

Transcriptional regulatory effects of lymphoma-associated NFKB2/lyt10 protooncogenes

Kim

Thakur

et al. 2000

Oncogene

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“…In several of these HL cells and perhaps as many as 10% of HL HRS cell biopsy samples, the lack of IkBa is due to loss-of-function mutations (e.g., small insertions, deletions or nonsense) in one allele of the IKBA gene couples with the deletion or inactivation of the second IKBA allele (Wood et al, 1998;Cabannes et al, 1999;Jungnickel et al, 2000;Emmerich et al, , 2003. As a consequence of the constitutive NF-kB signaling, several NF-kB target genes are overexpressed in HL cells, including ones encoding antiapoptotic proteins (such as A1, c-IAP2, TRAF1 and Bcl-X L ) and growth-promoting proteins (including cyclin D2, CD86 and CD40) (Hinz et al, 2001).…”

Section: Multiple Familial Trichoepitheliomamentioning

confidence: 99%