A G220V substitution within the N-terminal transcription regulating domain of HOXD13 causes a variant synpolydactyly phenotype

doi:10.1093/hmg/ddn410

Human Molecular Genetics Advance Access originally published online on December 5, 2008
Human Molecular Genetics 2009 18(5):847-860; doi:10.1093/hmg/ddn410

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A G220V substitution within the N-terminal transcription regulating domain of HOXD13 causes a variant synpolydactyly phenotype

Sebastian Fantini¹^,, Giulia Vaccari¹^,, Nathalie Brison², Philippe Debeer³, Przemko Tylzanowski² and Vincenzo Zappavigna¹^,*

¹ Department of Animal Biology, University of Modena and Reggio Emilia, Via Campi 213/D, 41100 Modena, Italy ² Laboratory of Skeletal Development and Joint Disorders, University of Leuven, Herestraat 49, 3000 Leuven, Belgium ³ Division of Orthopedics, Department of Musculoskeletal Sciences, University of Leuven, Heresstraat 49, 3000 Leuven, Belgium

^* To whom correspondence should be addressed. Tel: +39 0592055537; Fax: +39 0592055548; Email: zappavigna.vincenzo{at}unimore.it

Received November 10, 2008; Accepted December 3, 2008

The 5' members of the HoxD gene cluster (paralogous groups 9–13)are crucial for correct vertebrate limb patterning. Mutationsin the HOXD13 gene have been found to cause synpolydactyly (SPD)and other limb malformations in human. We report the identificationin a Greek family of a variant form of SPD caused by a novelmissense mutation that substitutes glycine for valine in position220 (G220V) of HOXD13. This mutation represents the first substitutionof an amino acid located outside of the HOXD13 homeodomain thatcauses autopodal limb malformations. We have characterized thismutation at the molecular level and found that the G220V substitutioncauses a significant impairment of the capacity of HOXD13 tobind DNA and regulate transcription. HOXD13(G220V) was foundto be deficient in both activating and repressing transcriptionthrough HOXD13-responsive regulatory elements. In accordancewith these results, a comparison of the activities of HOXD13and HOXD13(G220V) in vivo, using retrovirus-mediated misexpressionin developing chick limbs, showed that the G220V mutation impairsthe capacity of HOXD13 to perturb the development of proximallimb skeletal elements and to ectopically activate the transcriptionof the Hand2 target gene. We moreover show that the G220V mutationcompromises the stability of the HOXD13 protein within cellsand causes its partial accumulation in the cytosol in the formof subtle aggregates. Taken together, our results establishthat the G220V substitution does not produce a dominant-negativeeffect or a gain-of-function, but represents a dominant loss-of-functionmutation revealing haploinsufficiency of HOXD13 in human.

The authors wish it to be known that, in their opinion, thefirst two authors should be regarded as joint First Authors.

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