Haploinsufficiency of the forkhead gene Foxf1, a target for sonic hedgehog signaling, causes lung and foregut malformations

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Development 128, 2397-2406 (2001)
© 2001 The Company of Biologists Limited

Haploinsufficiency of the forkhead gene Foxf1, a target for sonic hedgehog signaling, causes lung and foregut malformations

Margit Mahlapuu¹, Sven Enerbäck² and Peter Carlsson¹

¹ Department of Molecular Biology, Göteborg University, The Lundberg Laboratory, Box 462, SE-405 30 Göteborg, Sweden
² Department of Medical Biochemistry, Göteborg University, SE-405 30 Göteborg, Sweden

*Author for correspondence (e-mail: peter.carlsson{at}molbio.gu.se)

Accepted April 10, 2001

The murine Foxf1 gene, encoding a forkhead – or wingedhelix – transcription factor, is expressed in splanchnicmesenchyme during organogenesis. The concentration of expressionto subepithelial mesenchyme suggested that Foxf1 is activatedby paracrine signals from endodermal epithelia. Homozygous Foxf1-nullmice die before embryonic day 10, owing to defects in extra-embryonicmesoderm, and do not provide any information about the roleof Foxf1 in morphogenesis of endodermally derived organs. Weshow that, on CD1 genetic background, Foxf1 heterozygote perinatalmortality is around 90%. The haploinsufficiency causes a variablephenotype that includes lung immaturity and hypoplasia, fusionof right lung lobes, narrowing of esophagus and trachea, esophagealatresia and tracheo-esophageal fistula. Similar malformationsare observed in mutants that are defective in the sonic hedgehog(Shh) signaling pathway, and we show that exogenous Shh activatestranscription of Foxf1 in developing lung. Foxf1 mRNA is absentin the lungs, foregut and sclerotomes of Shh^-/- embryos, butpersists in tissues where indian hedgehog (Ihh) is expressed.In lung organ cultures, activation of Foxf1 by Shh is counteractedby bone morphogenetic protein 4 (BMP4). Fibroblast growth factor(FGF) 10 and FGF7 both decrease Foxf1 expression and we speculatethat this is mediated by transcriptional activation of epithelialBmp4 (in the case of FGF10) and by inhibition of Shh expressionfor FGF7.

Key words: Lung, Mouse, Foregut, Foxf1, forkhead

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				M.-T. Teh, S.-T. Wong, G. W. Neill, L. R. Ghali, M. P. Philpott, and A. G. Quinn FOXM1 Is a Downstream Target of Gli1 in Basal Cell Carcinomas Cancer Res., August 15, 2002; 62(16): 4773 - 4780. [Abstract] [Full Text] [PDF]

				V. V. Kalinichenko, Y. Zhou, D. Bhattacharyya, W. Kim, B. Shin, K. Bambal, and R. H. Costa Haploinsufficiency of the Mouse Forkhead Box f1 Gene Causes Defects in Gall Bladder Development J. Biol. Chem., March 29, 2002; 277(14): 12369 - 12374. [Abstract] [Full Text] [PDF]

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				V. V. Kalinichenko, Y. Zhou, B. Shin, D. B. Stolz, S. C. Watkins, J. A. Whitsett, and R. H. Costa Wild-type levels of the mouse Forkhead Box f1 gene are essential for lung repair Am J Physiol Lung Cell Mol Physiol, June 1, 2002; 282(6): L1253 - L1265. [Abstract] [Full Text] [PDF]