distinct motifs in the intracellular domain of human cd30 differentially activate canonical and alternative transcription factor nf-κb signaling不同的图案在胞内域的人类cd30不同激活规范和替代转录因子nf-κb信号.pdfVIP
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distinct motifs in the intracellular domain of human cd30 differentially activate canonical and alternative transcription factor nf-κb signaling不同的图案在胞内域的人类cd30不同激活规范和替代转录因子nf-κb信号
Distinct Motifs in the Intracellular Domain of Human
CD30 Differentially Activate Canonical and Alternative
Transcription Factor NF-kB Signaling
Sarah L. Buchan*, Aymen Al-Shamkhani*
Cancer Sciences Unit, School of Medicine, University of Southampton, Southampton General Hospital, Southampton, United Kingdom
Abstract
The TNF-receptor superfamily member CD30 is expressed on normal and malignant lymphocytes, including anaplastic large
cell lymphoma (ALCL) cells. CD30 transmits multiple effects, including activation of NF-kB signaling, cell proliferation,
growth arrest and apoptosis. How CD30 generates these pleiotropic effects is currently unknown. Herein we describe ALCL
cells expressing truncated forms of the CD30 intracellular domain that allowed us to identify the key regions responsible for
transmitting its biological effects in lymphocytes. The first region (CD30519–537) activated both the alternative and canonical
NF-kB pathways as detected by p100 and IkBa degradation, IKKb-dependent transcription of both IkBa and the cyclin-
dependent kinase inhibitor p21WAF1/CIP1 and induction of cell cycle arrest. In contrast, the second region of CD30 (CD30538–
595) induced some aspects of canonical NF-kB activation, including transcription of IkBa, but failed to activate the alternative
NF-kB pathway or drive p21WAF1/CIP1-mediated cell-cycle arrest. Direct comparison of canonical NF-kB activation by the two
motifs revealed 4-fold greater p65 nuclear translocation following CD30519–537 engagement. These data reveal that
independent regions of the CD30 cytoplasmic tail regulate the magnitude and type of NF-kB activation and additionally
identify a short motif necessary for CD30-driven growth arrest signals in ALCL cells.
Citation: Buchan SL, Al-Shamkhani A (2012) Distinct Motifs in the Intracellular Domain of
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