Martin Goller scite author profile

The murine poly(C)-binding protein (mCBP) was previously shown to belong to the group of K-homology (KH) proteins by virtue of its homology to hnRNP-K. We have isolated cDNA-splice variants of mCBP which differ by two variable regions of 93 bp and/or 39 +/- 3 bp respectively. Both variable regions are located between the second and third KH-domain of mCBP. The characterization of a partial genomic clone enabled us to propose a model for the generation of the second variable region by the use of a putative alternative splice signal. The mCBP mRNA is expressed ubiquitously and the protein is found predominantly in the nucleus with the exception of the nucleoli. We have identified five proteins which interact with mCBP in the yeast two hybrid system: mouse y-box protein 1 (msy-1), y-box-binding protein, hnRNP-L, filamin and splicing factor 9G8. The interaction between mCBP and splicing factor 9G8 was confirmed in vivo. These results suggest a function of mCBP in RNA metabolism.

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A recombination hotspot in the LTR of a mouse retrotransposon identified in an in vitro system

Edelmann

Kröger

Goller

et al. 1989

Cell

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Hormone-regulatable neoplastic transformation induced by a Jun-estrogen receptor chimera

Kruse

Iacovoni

Goller

et al. 1997

Proc. Natl. Acad. Sci. U.S.A.

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The v-jun oncogene encodes a nuclear DNA binding protein that functions as a transcription factor and is part of the activator protein 1 complex. Oncogenic transformation by v-jun is thought to be mediated by the aberrant expression of specific target genes. To identify such Junregulated genes and to explore the mechanisms by which Jun affects their expression, we have fused the full-length v-Jun and an amino-terminally truncated form of v-Jun to the hormone-binding domain of the human estrogen receptor. The two chimeric proteins function as ligand-inducible transactivators. Expression of the fusion proteins in chicken embryo fibroblasts causes estrogen-dependent transformation.

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Murine protein which binds preferentially to oligo-C-rich single-stranded nucleic acids

et al. 1994

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Martin Goller

Heparin-binding epidermal growth factor-like growth factor, a v-Jun target gene, induces oncogenic transformation

The mouse poly(C)-binding protein exists in multiple isoforms and interacts with several RNA-binding proteins

A recombination hotspot in the LTR of a mouse retrotransposon identified in an in vitro system

Hormone-regulatable neoplastic transformation induced by a Jun-estrogen receptor chimera

Murine protein which binds preferentially to oligo-C-rich single-stranded nucleic acids

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