Thorsten T. Ebel scite author profile

Binding sites for transcription factor nuclear factor one (NFI) proteins, encoded by four genes in the mouse, have been characterized from many tissue-specific genes. NFI genes are expressed in unique but overlapping patterns in embryonic and in adult tissues. Nfib is highly expressed in the embryonic lung. Here we show that Nfib null mutants die early postnatally and display severe lung hypoplasia. Heterozygotes do survive, but exhibit delayed pulmonary differentiation. Expression of transforming growth factor beta 1 (TGF-beta1) and sonic hedgehog (Shh) is not down-regulated in mutant lung epithelium at late stages of morphogenesis, which may result in incomplete lung maturation. Our study demonstrates that Nfib is essential for normal lung development, and suggests that it could be involved in the pathogenesis of respiratory distress syndromes in humans.

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Genomic organization, splice products and mouse chromosomal localization of genes for transcription factor Nuclear Factor One

Gründer

Qian

Ebel

et al. 2003

Gene

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A rapid method to deplete endogenous DNA-binding proteins from reticulocyte lysate translation systems

Ebel

Sippel

1995

Nucl Acids Res

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Generation of Transcription Factors in Rabbit Reticulocyte Lysate Depleted of Endogenous DNA-Binding Protein

Kruse

Ebel

Sippel

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Thorsten T. Ebel

Nuclear factor I-B (Nfib) deficient mice have severe lung hypoplasia

Genomic organization, splice products and mouse chromosomal localization of genes for transcription factor Nuclear Factor One

A rapid method to deplete endogenous DNA-binding proteins from reticulocyte lysate translation systems

Generation of Transcription Factors in Rabbit Reticulocyte Lysate Depleted of Endogenous DNA-Binding Protein

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