Thalidomide induces limb deformities by perturbing the Bmp/Dkk1/Wnt signaling pathway

doi:10.1096/fj.06-7603com

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Thalidomide induces limb deformities by perturbing the Bmp/Dkk1/Wnt signaling pathway

Jürgen Knobloch, John D. Shaughnessy Jr., and Ulrich Rüther

E-mail contact: ruether@uni-duesseldorf.de

Thalidomide, a sedative originally used to treat morning sicknessand now used to treat leprosy and multiple myeloma, is alsoa teratogen that induces birth defects in humans such as limbtruncations and microphthalmia. However, the teratogenic mechanismof action of this drug remains obscure. Thalidomide induceslimb and eye defects in the chicken embryo at an EC₅₀ of 50µg/kg egg wt and apoptosis in primary human embryonic fibroblasts(HEFs) at an EC₅₀ of 8.9 µM. Using these model systems,we demonstrate by semiquantitative reverse transcriptase-polymerasechain reaction and whole-mount in situ hybridization that thalidomide-inducedoxidative stress enhances signaling through bone morphogeneticproteins (Bmps). This leads to up-regulation of the Bmp targetgene and Wnt antagonist Dickkopf1 (Dkk1) with subsequent inhibitionof canonical Wnt/ ${beta}$ -catenin signaling and increased cell deathas shown by trypan blue and terminal deoxynucleotidyl transferase-mediatednick end labeling staining. Thalidomide-induced cell death wasdramatically reduced in HEFs and in embryonic limb buds by theuse of inhibitors against Bmps, Dkk1, and Gsk3 ${beta}$ , a ${beta}$ -catenin antagonistacting downstream of Dkk1 in the Wnt pathway. Most interestingly,blocking of Dkk1 or Gsk3 ${beta}$ dramatically counteracts thalidomide-inducedlimb truncations and microphthalmia. From this, we concludethat perturbing of Bmp/Dkk1/Wnt signaling is central to theteratogenic effects of thalidomide.--Knobloch, J., Shaughnessy,Jr., J. D., Rüther, U. Thalidomide induces limb deformitiesby perturbing the Bmp/Dkk1/Wnt signaling pathway

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