A loss-of-function mutation in the binding domain of HAND1 predicts hypoplasia of the human hearts

doi:10.1093/hmg/ddn027

Human Molecular Genetics Advance Access originally published online on February 14, 2008
Human Molecular Genetics 2008 17(10):1397-1405; doi:10.1093/hmg/ddn027

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A loss-of-function mutation in the binding domain of HAND1 predicts hypoplasia of the human hearts

Stella Marie Reamon-Buettner¹, Yari Ciribilli², Alberto Inga² and Juergen Borlak¹^,*

¹ Molecular Medicine and Medical Biotechnology, Fraunhofer Institute of Toxicology and Experimental Medicine, Nikolai-Fuchs-Strasse 1, D-30625 Hannover, Germany ² Unit of Molecular Mutagenesis, National Cancer Research Institute (IST), Largo R. Benzi, 10, 16132 Genoa, Italy

^* To whom correspondence should be addressed. Tel: +49 5115350559; Fax: +49 5115350573; Email: borlak{at}item.fraunhofer.de

Received November 23, 2007; Revised January 3, 2008; Accepted January 24, 2008

Hypoplasia of the human heart is the most severe form of congenitalheart disease (CHD) and usually lethal during early infancy.It is a leading cause of neonatal loss, especially in infantsdiagnosed with hypoplastic left heart syndrome (HLHS), a conditionwhere the left side of the heart including the aorta, aorticvalve, left ventricle (LV) and mitral valve are underdeveloped.The molecular causes of HLHS are unclear, but the basic helix–loop–helix(bHLH) transcription factor heart and neural crest derivativesexpressed 1 (Hand1), may be a candidate culprit for this condition.The absence of Hand1 in mice resulted in the failure of rightwardlooping of the heart tube, a severely hypoplastic LV and outflowtract abnormalities. Nonetheless, no HAND1 mutations associatedwith human CHD have been reported so far. We sequenced the humanHAND1 gene in heart tissues derived from 31 unrelated patientsdiagnosed with hypoplastic hearts. We detected in 24 of 31 hypoplasticventricles, a common frameshift mutation (A126fs) in the bHLHdomain, which is necessary for DNA binding and combinatorialinteractions. The resulting mutant protein, unlike wild-type(wt) HAND1, was unable to modulate transcription of reporterconstructs containing specific DNA-binding sites. Thus, in hypoplastichuman hearts HAND1 function is impaired.

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