[HTML][HTML] Bcl10 is involved in t (1; 14)(p22; q32) of MALT B cell lymphoma and mutated in multiple tumor types
TG Willis, DM Jadayel, MQ Du, H Peng, AR Perry… - Cell, 1999 - cell.com
Cell, 1999•cell.com
MALT B cell lymphomas with t (1; 14)(p22; q32) showed a recurrent breakpoint upstream of
the promoter of a novel gene, Bcl10. Bcl10 is a cellular homolog of the equine herpesvirus-2
E10 gene: both contain an amino-terminal caspase recruitment domain (CARD)
homologous to that found in several apoptotic molecules. Bcl10 and E10 activated NF-κ B
but caused apoptosis of 293 cells. Bcl10 expressed in a MALT lymphoma exhibited a
frameshift mutation resulting in truncation distal to the CARD. Truncated Bcl10 activated NF …
the promoter of a novel gene, Bcl10. Bcl10 is a cellular homolog of the equine herpesvirus-2
E10 gene: both contain an amino-terminal caspase recruitment domain (CARD)
homologous to that found in several apoptotic molecules. Bcl10 and E10 activated NF-κ B
but caused apoptosis of 293 cells. Bcl10 expressed in a MALT lymphoma exhibited a
frameshift mutation resulting in truncation distal to the CARD. Truncated Bcl10 activated NF …
Abstract
MALT B cell lymphomas with t(1;14)(p22;q32) showed a recurrent breakpoint upstream of the promoter of a novel gene, Bcl10. Bcl10 is a cellular homolog of the equine herpesvirus-2 E10 gene: both contain an amino-terminal caspase recruitment domain (CARD) homologous to that found in several apoptotic molecules. Bcl10 and E10 activated NF-κ B but caused apoptosis of 293 cells. Bcl10 expressed in a MALT lymphoma exhibited a frameshift mutation resulting in truncation distal to the CARD. Truncated Bcl10 activated NF-κ B but did not induce apoptosis. Wild-type Bcl10 suppressed transformation, whereas mutant forms had lost this activity and displayed gain-of-function transforming activity. Similar mutations were detected in other tumor types, indicating that Bcl10 may be commonly involved in the pathogenesis of human malignancy.
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