W.M. Clouston scite author profile

The B-cell POU homeodomain protein Oct-2 contains two transcriptional activation domains, one N terminal and the other C terminal of the central DNA-binding POU domain. The synergistic action of these two activation domains makes Oct-2 a more potent activator of mRNA promoters than the related broadly expressed octamer motif-binding protein Oct-1, which contains an N-terminal but not a C-terminal Oct-2-like activation domain. Both Oct-2 mRNA promoter activation domains were delineated by truncation analysis: the N-terminal Q domain is a 66-amino-acid region rich in glutamines, and the C-terminal P domain is a 42-amino-acid region rich in prolines. The Q and P domains synergized with each other or duplicates of themselves, independently of their N-terminal or C-terminal position relative to the POU domain. The C-terminal P domain, which differentiates Oct-2 from Oct-i, also activated transcription in conjunction with the heterologous GAL4 DNA-binding domain. Oct-2 thus contains three modular functional units, the DNA-binding POU domain and the two P and Q activation domains. An electrophoretic mobility shift assay with a variety of these Oct-2 activators revealed a distinct complex called QA that was dependent on the presence of an active glutamine-rich activation domain and migrated more slowly than the Oct-2-DNA complexes. Formation of the QA complex is consistent with interaction of the glutamine-rich activation domains with a regulatory protein important for the process of transcriptional activation.

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Apoptosis, lymphocytotoxicity and the containment of viral infections

Clouston

Kerr

1985

Medical Hypotheses

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Acromegaly first diagnosed in pregnancy: The role of bromocriptine therapy

Yap

Clouston

Mortimer

et al. 1990

American Journal of Obstetrics and Gynecology

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Molecular cloning of the mouse angiotensinogen gene

et al. 1988

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W.M. Clouston

The Oct-2 glutamine-rich and proline-rich activation domains can synergize with each other or duplicates of themselves to activate transcription.

Apoptosis, lymphocytotoxicity and the containment of viral infections

Acromegaly first diagnosed in pregnancy: The role of bromocriptine therapy

Molecular cloning of the mouse angiotensinogen gene

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