Clonal Deleterious Mutations in the Iκbα Gene in the Malignant Cells in Hodgkin's Lymphoma

Jungnickel, Berit; Staratschek‐Jox, Andrea; Bräuninger, Andreas; Spieker, Tilmann; Wolf, Jürgen; Diehl, Volker; Hansmann, Martin‐Leo; Rajewsky, Klaus; Küppers, Ralf

doi:10.1084/jem.191.2.395

Cited by 259 publications

(184 citation statements)

References 26 publications

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“…Constitutive (NF)-B activity is likely to be involved in apoptosis resistance, because (NF)-B activates genes involved in apoptosis resistance, cell activation and proliferation, as well as cytokines and chemokines involved in immunosuppression. 11,12 In summary, our results show that a TP53 gene mutation can be an early transforming event, likely to be important in the resistance to apoptosis of the RS precursors. However, even after the enrichment for RS cells and the use of a highly sensitive mutation detection technique we found TP53 gene mutations in only 3 of 26 (11.5%) HL-involved tissue samples.…”

Section: Discussionmentioning

confidence: 68%

“…14,15,34 Because of the low incidence of TP53 mutations in HL and the finding that TP53 gene mutations are not restricted to EBVnegative cases, other important steps in the resistance of RS precursors to apoptosis have to be considered. One alternative is based on a recent study 11 in which mutations in the I B␣ gene were found in 2 of 3 EBV-negative cases and no mutations were found in 2 EBV-positive cases. Mutations of the I B␣ protein, which normally functions as the inhibitor of (NF)-B protein, leads to increased levels of (NF)-B protein.…”

Section: Discussionmentioning

confidence: 99%

“…However, other transforming events such I B␣ gene mutations resulting in over-expression of NF-B as possible explanation of the rescue of these cells from apoptosis have been demonstrated. 11,12 The frequent finding of immunohistochemically detectable p53 protein expression in the nuclei of RS cells 4,13,14 suggests a possible role for p53 protein in the rescue of RS precursors from apoptosis. Wild-type p53 protein has the ability to intervene in cell proliferation and is necessary to maintain the integrity of the DNA.…”

mentioning

confidence: 99%

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TP53 gene mutations in Hodgkin lymphoma are infrequent and not associated with absence of Epstein-Barr virus

Maggio

Stekelenburg

Berg³

et al. 2001

Int. J. Cancer

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Epstein-Barr virus (EBV) infection probably has a role in this transforming event, which renders RS precursors resistance to apoptosis, as clonal EBV genomes can be detected in RS cells of classical HL in 30 -50% of cases. 3,4 EBV-encoded LMP-1 protein, known to be expressed in RS cells, is known for its immortalizing activity. 1,4 -6 EBV encoded EBNA-1 protein is also thought to have transforming capacity. 7,8 Moreover EBV is involved in immune suppression. 9,10 The major subset of HL of the nodular sclerosis subtype among the Western population is, however, frequently EBV negative. The distinct epidemiology of these cases has led to various speculations about their pathogenesis, but no other viruses have been identified to date. However, other transforming events such I B␣ gene mutations resulting in over-expression of NF-B as possible explanation of the rescue of these cells from apoptosis have been demonstrated. 11,12 The frequent finding of immunohistochemically detectable p53 protein expression in the nuclei of RS cells 4,13,14 suggests a possible role for p53 protein in the rescue of RS precursors from apoptosis. Wild-type p53 protein has the ability to intervene in cell proliferation and is necessary to maintain the integrity of the DNA.An aberrant p53 protein with lack of transcriptional activity can result in the survival of genetically unstable cells susceptible to malignant transformation. 15 A mutation in the TP53 gene is often associated with detectable p53 protein expression, because it stabilizes the protein as a consequence of conformational change. Several studies have demonstrated that a TP53 gene mutation causes impairment of p53 protein-mediated trans-activation. For HL a few studies have reported the presence of TP53 gene mutations in RS cells in only a minority of cases. 14,16,17 The low percentages of TP53 gene mutations (Ͻ10%) detected could be the result of the paucity of RS cells in the specimens, which may lead to false-negative findings. In general, higher TP53 gene mutation percentages were reported in studies with enrichment for RS cells. 13,18 -20 One exception was reported in a recent study in which even with enrichment no mutations were found. 21 Because TP53 gene mutations and EBV both can play a role in the resistance of RS precursors to apoptosis, the question arises whether these 2 potentially transforming events exclude each other. Chen et al. 13 found TP53 gene mutations in 6 of 16 EBVnegative cases and no mutations in 7 EBV-positive cases. This finding suggests that in some of the EBV-negative cases a TP53 gene mutation may be fundamental for the inhibition of apoptosis.To gain more insight in the frequency of TP53 gene mutations in HL and to test the hypothesis of an inverse correlation between the presence of TP53 gene mutations and EBV, we analyzed 67 cases of HL-involved tissues. All HL-involved tissues were analyzed for the presence of immunohistochemically detectable p53 protein and the presence of EBV. We enriched 15 EBV-positive and 11 EBV-negative HL-involved ti...

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Section: Discussionmentioning

confidence: 68%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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TP53 gene mutations in Hodgkin lymphoma are infrequent and not associated with absence of Epstein-Barr virus

Maggio

Stekelenburg

Berg³

et al. 2001

Int. J. Cancer

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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%

Mutations in the NF-κB signaling pathway: implications for human disease

2006

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“…The constitutive NF-kB activity seen in most haematological disorders occurs through several mechanisms, including the chromosomal translocation and subsequent overexpression of BCL-3 in a subset of human B-cell chronic lymphotic leukaemias (McKeithan et al, 1987) and mutations of the IkBa gene that impair its inhibitory function in some cases of Hodgkin's lymphomas (Cabannes et al, 1999;Emmerich et al, 1999;Jungnickel et al, 2000). Gene amplification of NIK or loss of function mutations for inhibitory signalling molecules such as TRAF3 and CYLD have been reported in multiple myelomas (Annunziata et al, 2007;Keats et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

Matrix Metalloproteinase-9 gene induction by a truncated oncogenic NF-κB2 protein involves the recruitment of MLL1 and MLL2 H3K4 histone methyltransferase complexes

et al. 2009

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Constitutive nuclear factor (NF)-jB activation in haematological malignancies is caused in several cases by loss of function mutations within the coding sequence of NF-jB inhibitory molecules such as IjBa or p100. Hut-78, a truncated form of p100, constitutively generates p52 and contributes to the development of T-cell lymphomas but the molecular mechanism underlying this oncogenic potential remains unclear. We show here that MMP9 gene expression is induced through the alternative NF-jB-activating pathway in fibroblasts and also on Hut-78 or p52 overexpression in fibroblasts as well as in lymphoma cells. p52 is critical for Hut-78-mediated MMP9 gene induction as a Hut-78 mutant as well as other truncated NF-jB2 proteins that are not processed into p52 failed to induce the expression of this metalloproteinase. Conversely, MMP9 gene expression is impaired in p52-depleted HUT-78 cells. Interestingly, MLL1 and MLL2 H3K4 methyltransferase complexes are tethered by p52 on the MMP9 but not on the IjBa promoter, and the H3K4 trimethyltransferase activity recruited on the MMP9 promoter is impaired in p52-depleted HUT-78 cells. Moreover, MLL1 and MLL2 are associated with Hut-78 in a native chromatin-enriched extract. Thus, we identified a molecular mechanism by which the recruitment of a H3K4 histone methyltransferase complex on the promoter of a NF-jB-dependent gene induces its expression and potentially the invasive potential of lymphoma cells harbouring constitutive activity of the alternative NF-jB-activating pathway.

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Clonal Deleterious Mutations in the Iκbα Gene in the Malignant Cells in Hodgkin's Lymphoma

Cited by 259 publications

References 26 publications

TP53 gene mutations in Hodgkin lymphoma are infrequent and not associated with absence of Epstein-Barr virus

TP53 gene mutations in Hodgkin lymphoma are infrequent and not associated with absence of Epstein-Barr virus

Mutations in the NF-κB signaling pathway: implications for human disease

Matrix Metalloproteinase-9 gene induction by a truncated oncogenic NF-κB2 protein involves the recruitment of MLL1 and MLL2 H3K4 histone methyltransferase complexes

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