论文信息 - Inhibiting pathologically active ADAM10 rescues synaptic and cognitive decline in Huntington's disease. - 字舞流文

Inhibiting pathologically active ADAM10 rescues synaptic and cognitive decline in Huntington's disease.

A disintegrine and metalloproteinase 10 (ADAM10) is implicated in synaptic function through its interaction with postsynaptic receptors and adhesion molecules. Here, we report that levels of active ADAM10 are increased in Huntington's disease (HD) mouse cortices and striata and in human postmortem caudate. We show that, in the presence of polyglutamine-expanded (polyQ-expanded) huntingtin (HTT), ADAM10 accumulates at the postsynaptic densities (PSDs) and causes excessive cleavage of the synaptic protein N-cadherin (N-CAD). This aberrant phenotype is also detected in neurons from HD patients where it can be reverted by selective silencing of mutant HTT. Consistently, ex vivo delivery of an ADAM10 synthetic inhibitor reduces N-CAD proteolysis and corrects electrophysiological alterations in striatal medium-sized spiny neurons (MSNs) of 2 HD mouse models. Moreover, we show that heterozygous conditional deletion of ADAM10 or delivery of a competitive TAT-Pro-ADAM10709-729 peptide in R6/2 mice prevents N-CAD proteolysis and ameliorates cognitive deficits in the mice. Reduction in synapse loss was also found in R6/2 mice conditionally deleted for ADAM10. Taken together, these results point to a detrimental role of hyperactive ADAM10 at the HD synapse and provide preclinical evidence of the therapeutic potential of ADAM10 inhibition in HD.

A. Caricasole | G. Biella | P. Saftig | G. Sancini | A. Falqui | O. Riess | E. Cattaneo | C. Zuccato | Ottavia Cecchetti | I. Caron | E. Sogne | A. Bresciani | Elisa Battaglia | H. Nguyen | E. Vezzoli | P. Rivetti di Val Cervo | Lisa Seipold | P. Conforti | D. Besusso | Lara Petricca | F. Talpo | Paola Martufi | Margherita Verani

[1] G. Biella,et al. Faulty neuronal determination and cell polarization are reverted by modulating HD early phenotypes , 2018, Proceedings of the National Academy of Sciences.

[2] H. Heinsen,et al. Huntington's disease (HD): the neuropathology of a multisystem neurodegenerative disorder of the human brain , 2016, Brain pathology.

[3] E. Kremmer,et al. Systematic substrate identification indicates a central role for the metalloprotease ADAM10 in axon targeting and synapse function , 2016, eLife.

[4] P. Saftig,et al. The alpha secretase ADAM10: A metalloprotease with multiple functions in the brain , 2015, Progress in Neurobiology.

[5] M. Hayden,et al. HD iPSC-derived neural progenitors accumulate in culture and are susceptible to BDNF withdrawal due to glutamate toxicity. , 2015, Human molecular genetics.

[6] R. Murmu,et al. Altered Sensory Experience Exacerbates Stable Dendritic Spine and Synapse Loss in a Mouse Model of Huntington's Disease , 2015, The Journal of Neuroscience.

[7] J. Brandt,et al. Determinants of functional disability in Huntington's disease: Role of cognitive and motor dysfunction , 2014, Movement disorders : official journal of the Movement Disorder Society.

[8] H. Yin,et al. Huntingtin Is Required for Normal Excitatory Synapse Development in Cortical and Striatal Circuits , 2014, The Journal of Neuroscience.

[9] L. Raymond,et al. Mechanisms of synaptic dysfunction and excitotoxicity in Huntington's disease. , 2014, Drug discovery today.

[10] R. D'Hooge,et al. Postnatal Disruption of the Disintegrin/Metalloproteinase ADAM10 in Brain Causes Epileptic Seizures, Learning Deficits, Altered Spine Morphology, and Defective Synaptic Functions , 2013, The Journal of Neuroscience.

[11] A. Holtmaat,et al. Dendritic Spine Instability Leads to Progressive Neocortical Spine Loss in a Mouse Model of Huntington's Disease , 2013, The Journal of Neuroscience.

[12] C. Calaminus,et al. A Novel Transgenic Rat Model for Spinocerebellar Ataxia Type 17 Recapitulates Neuropathological Changes and Supplies In Vivo Imaging Biomarkers , 2013, The Journal of Neuroscience.

[13] Mei Kwan,et al. Comprehensive Behavioral and Molecular Characterization of a New Knock-In Mouse Model of Huntington’s Disease: zQ175 , 2012, PloS one.

[14] Jack R Glaser,et al. Characterization of Neurophysiological and Behavioral Changes, MRI Brain Volumetry and 1H MRS in zQ175 Knock-In Mouse Model of Huntington's Disease , 2012, PloS one.

[15] S. Horvath,et al. Network Organization of the Huntingtin Proteomic Interactome in Mammalian Brain , 2012, Neuron.

[16] C. Korth,et al. C-terminal fragment of N-cadherin accelerates synapse destabilization by amyloid-β. , 2012, Brain : a journal of neurology.

[17] J. Gusella,et al. An evolutionary recent neuroepithelial cell adhesion function of huntingtin implicates ADAM10-Ncadherin , 2012, Nature Neuroscience.

[18] R. Weinberg,et al. Synaptic Autoregulation by Metalloproteases and γ-Secretase , 2011, The Journal of Neuroscience.

[19] C. Mulle,et al. Synaptic Localization and Activity of ADAM10 Regulate Excitatory Synapses through N-Cadherin Cleavage , 2010, The Journal of Neuroscience.

[20] M. Giustetto,et al. Blocking ADAM10 synaptic trafficking generates a model of sporadic Alzheimer's disease. , 2010, Brain : a journal of neurology.

[21] L. Raymond,et al. Early synaptic pathophysiology in neurodegeneration: insights from Huntington's disease , 2010, Trends in Neurosciences.

[22] G. Weskamp,et al. The Disintegrin/Metalloproteinase ADAM10 Is Essential for the Establishment of the Brain Cortex , 2010, The Journal of Neuroscience.

[23] A. Ludwig,et al. Improved Synthesis of ADAM10 Inhibitor GI254023X , 2010, Neurodegenerative Diseases.

[24] F. Fahrenholz,et al. Differential gene expression in ADAM10 and mutant ADAM10 transgenic mice , 2009, BMC Genomics.

[25] C. Behl,et al. Effects of neuron-specific ADAM10 modulation in an in vivo model of acute excitotoxic stress , 2008, Neuroscience.

[26] S. Warren,et al. Polyglutamine domain modulates the TBP-TFIIB interaction: implications for its normal function and neurodegeneration , 2007, Nature Neuroscience.

[27] L. Rüttiger,et al. Nuclear Localization of Ataxin-3 Is Required for the Manifestation of Symptoms in SCA3: In Vivo Evidence , 2007, The Journal of Neuroscience.

[28] Carlos Cepeda,et al. The corticostriatal pathway in Huntington's disease , 2007, Progress in Neurobiology.

[29] A. Jeromin,et al. Synapse-Associated Protein-97 Mediates α-Secretase ADAM10 Trafficking and Promotes Its Activity , 2007, The Journal of Neuroscience.

[30] Carlos Cepeda,et al. Transient and Progressive Electrophysiological Alterations in the Corticostriatal Pathway in a Mouse Model of Huntington's Disease , 2003, The Journal of Neuroscience.

[31] B. de Strooper,et al. The disintegrin/metalloprotease ADAM 10 is essential for Notch signalling but not for alpha-secretase activity in fibroblasts. , 2002, Human molecular genetics.

[32] S. W. Davies,et al. Exon 1 of the HD Gene with an Expanded CAG Repeat Is Sufficient to Cause a Progressive Neurological Phenotype in Transgenic Mice , 1996, Cell.

[33] Manish S. Shah,et al. A novel gene containing a trinucleotide repeat that is expanded and unstable on Huntington's disease chromosomes , 1993, Cell.

[34] A. Jeromin,et al. Synapse-associated protein-97 mediates alpha-secretase ADAM10 trafficking and promotes its activity. , 2007, The Journal of neuroscience : the official journal of the Society for Neuroscience.