Literature DB >> 12060751

Integration of Runx and Smad regulatory signals at transcriptionally active subnuclear sites.

Sayyed K Zaidi1, Andrew J Sullivan, Andre J van Wijnen, Janet L Stein, Gary S Stein, Jane B Lian.   

Abstract

Runx factors control lineage commitment and are transcriptional effectors of Smad signaling. Genetic defects in these pathways interfere with normal development. The in situ localization of Runx and Smad proteins must impact the mechanisms by which these proteins function together in gene regulation. We show that the integration of Runx and Smad signals is mediated by in situ interactions at specific foci within the nucleus. Activated Smads are directed to these subnuclear foci only in the presence of Runx proteins. Smad-Runx complexes are associated in situ with the nuclear matrix, and this association requires the intranuclear targeting signal of Runx factors. The convergence of Smad and Runx proteins at these sites supports transcription as reflected by BrUTP labeling and functional cooperativity between the proteins. Thus, Runx-mediated intranuclear targeting of Smads is critical for the integration of two distinct pathways essential for fetal development.

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Year:  2002        PMID: 12060751      PMCID: PMC123018          DOI: 10.1073/pnas.112664499

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  40 in total

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Journal:  Genes Cells       Date:  1999-12       Impact factor: 1.891

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Authors:  S McNeil; C Zeng; K S Harrington; S Hiebert; J B Lian; J L Stein; A J van Wijnen; G S Stein
Journal:  Proc Natl Acad Sci U S A       Date:  1999-12-21       Impact factor: 11.205

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Review 10.  Intranuclear trafficking of transcription factors: implications for biological control.

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2.  Mitotic partitioning and selective reorganization of tissue-specific transcription factors in progeny cells.

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Review 5.  The dynamic organization of gene-regulatory machinery in nuclear microenvironments.

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Review 6.  Nuclear microenvironments support physiological control of gene expression.

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10.  Differentiation of human fetal multipotential neural progenitor cells to astrocytes reveals susceptibility factors for JC virus.

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