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Literature DB >> 29222403

Common Pathophysiology in Multiple Mouse Models of Pitt-Hopkins Syndrome.

Courtney Thaxton^1,2, Alexander D Kloth^1,2, Ellen P Clark^1,2, Sheryl S Moy^3,4, Raymond A Chitwood⁵, Benjamin D Philpot^6,2,4.

Abstract

Mutations or deletions of the transcription factor TCF4 are linked to Pitt-Hopkins syndrome (PTHS) and schizophrenia, suggesting that the precise pathogenic mutations dictate cellular, synaptic, and behavioral consequences. Here, we generated two novel mouse models of PTHS, one that mimics the most common pathogenic TCF4 point mutation (human R580W, mouse R579W) and one that deletes three pathogenic arginines, and explored phenotypes of these lines alongside models of pan-cellular or CNS-specific heterozygous Tcf4 disruption. We used mice of both sexes to show that impaired Tcf4 function results in consistent microcephaly, hyperactivity, reduced anxiety, and deficient spatial learning. All four PTHS mouse models demonstrated exaggerated hippocampal long-term potentiation (LTP), consistent with deficits in hippocampus-mediated behaviors. We further examined R579W mutant mice and mice with pan-cellular Tcf4 heterozygosity and found that they exhibited hippocampal NMDA receptor hyperfunction, which likely drives the enhanced LTP. Together, our data pinpoint convergent neurobiological features in PTHS mouse models and provide a foundation for preclinical studies and a rationale for testing whether NMDAR antagonists might be used to treat PTHS.SIGNIFICANCE STATEMENT Pitt-Hopkins syndrome (PTHS) is a rare neurodevelopmental disorder associated with TCF4 mutations/deletions. Despite this genetic insight, there is a need to identify the function of TCF4 in the brain. Toward this goal, we developed two mouse lines, including one harboring the most prevalent pathogenic point mutation, and compared them with two existing models that conditionally delete Tcf4 Our data identify a set of overlapping phenotypes that may serve as outcome measures for preclinical studies of PTHS treatments. We also discovered penetrant enhanced synaptic plasticity across mouse models that may be linked to increased NMDA receptor function. These data reveal convergent neurobiological characteristics of PTHS mouse models and support the further investigation of NMDA receptor antagonists as a possible PTHS treatment.

Entities: Chemical Disease Gene Mutation Species

Keywords: NMDA; Pitt–Hopkins syndrome; TCF4; autism; mouse; schizophrenia

Mesh：

Substances：

Year: 2017 PMID： 29222403 PMCID： PMC5783968 DOI： 10.1523/JNEUROSCI.1305-17.2017

Source DB: PubMed Journal: J Neurosci ISSN： 0270-6474 Impact factor: 6.167

68 in total

1. A behavioral and neuroanatomical assessment of an inbred substrain of 129 mice with behavioral comparisons to C57BL/6J mice.

Authors: S A Balogh; C S McDowell; A J Stavnezer; V H Denenberg
Journal: Brain Res Date: 1999-07-31 Impact factor: 3.252

2. NR2A subunit expression shortens NMDA receptor synaptic currents in developing neocortex.

Authors: A C Flint; U S Maisch; J H Weishaupt; A R Kriegstein; H Monyer
Journal: J Neurosci Date: 1997-04-01 Impact factor: 6.167

3. Mutations in TCF4, encoding a class I basic helix-loop-helix transcription factor, are responsible for Pitt-Hopkins syndrome, a severe epileptic encephalopathy associated with autonomic dysfunction.

Authors: Jeanne Amiel; Marlene Rio; Loic de Pontual; Richard Redon; Valerie Malan; Nathalie Boddaert; Perrine Plouin; Nigel P Carter; Stanislas Lyonnet; Arnold Munnich; Laurence Colleaux
Journal: Am J Hum Genet Date: 2007-03-23 Impact factor: 11.025

4. Haploinsufficiency of TCF4 causes syndromal mental retardation with intermittent hyperventilation (Pitt-Hopkins syndrome).

Authors: Christiane Zweier; Maarit M Peippo; Juliane Hoyer; Sergio Sousa; Armand Bottani; Jill Clayton-Smith; William Reardon; Jorge Saraiva; Alexandra Cabral; Ina Gohring; Koen Devriendt; Thomy de Ravel; Emilia K Bijlsma; Raoul C M Hennekam; Alfredo Orrico; Monika Cohen; Alexander Dreweke; Andre Reis; Peter Nurnberg; Anita Rauch
Journal: Am J Hum Genet Date: 2007-03-23 Impact factor: 11.025

5. Tcf4 Regulates Synaptic Plasticity, DNA Methylation, and Memory Function.

Authors: Andrew J Kennedy; Elizabeth J Rahn; Brynna S Paulukaitis; Katherine E Savell; Holly B Kordasiewicz; Jing Wang; John W Lewis; Jessica Posey; Sarah K Strange; Mikael C Guzman-Karlsson; Scott E Phillips; Kyle Decker; S Timothy Motley; Eric E Swayze; David J Ecker; Todd P Michael; Jeremy J Day; J David Sweatt
Journal: Cell Rep Date: 2016-08-25 Impact factor: 9.423

6. B-lymphocyte development is regulated by the combined dosage of three basic helix-loop-helix genes, E2A, E2-2, and HEB.

Authors: Y Zhuang; P Cheng; H Weintraub
Journal: Mol Cell Biol Date: 1996-06 Impact factor: 4.272

Review 7. In utero exposure to valproic acid and autism--a current review of clinical and animal studies.

Authors: Florence I Roullet; Jonathan K Y Lai; Jane A Foster
Journal: Neurotoxicol Teratol Date: 2013-02-08 Impact factor: 3.763

8. Molecular characterisation of the 22q13 deletion syndrome supports the role of haploinsufficiency of SHANK3/PROSAP2 in the major neurological symptoms.

Authors: H L Wilson; A C C Wong; S R Shaw; W-Y Tse; G A Stapleton; M C Phelan; S Hu; J Marshall; H E McDermid
Journal: J Med Genet Date: 2003-08 Impact factor: 6.318

9. Neurodevelopmental models of transcription factor 4 deficiency converge on a common ion channel as a potential therapeutic target for Pitt Hopkins syndrome.

Authors: Matthew D Rannals; Stephanie Cerceo Page; Morganne N Campbell; Ryan A Gallo; Brent Mayfield; Brady J Maher
Journal: Rare Dis Date: 2016-08-05

10. Phenotype and natural history in 101 individuals with Pitt-Hopkins syndrome through an internet questionnaire system.

Authors: Channa F de Winter; Melanie Baas; Emilia K Bijlsma; John van Heukelingen; Sue Routledge; Raoul C M Hennekam
Journal: Orphanet J Rare Dis Date: 2016-04-12 Impact factor: 4.123

18 in total

1. Repurposing the Dihydropyridine Calcium Channel Inhibitor Nicardipine as a Na_v1.8 Inhibitor In Vivo for Pitt Hopkins Syndrome.

Authors: Sean Ekins; Ana C Puhl; Audrey Davidow
Journal: Pharm Res Date: 2020-06-11 Impact factor: 4.200

2. Kinesin Kif3b mutation reduces NMDAR subunit NR2A trafficking and causes schizophrenia-like phenotypes in mice.

Authors: Ashwaq Hassan Alsabban; Momo Morikawa; Yosuke Tanaka; Yosuke Takei; Nobutaka Hirokawa
Journal: EMBO J Date: 2019-11-20 Impact factor: 11.598

3. Exploration of group II metabotropic glutamate receptor modulation in mouse models of Rett syndrome and MECP2 Duplication syndrome.

Authors: Sheryl Anne D Vermudez; Aditi Buch; Kelly Weiss; Rocco G Gogliotti; Colleen M Niswender
Journal: Neuropharmacology Date: 2022-03-03 Impact factor: 5.250

Review 4. Evaluation of Na_v1.8 as a therapeutic target for Pitt Hopkins Syndrome.

Authors: Keri Martinowich; Debamitra Das; Srinidhi Rao Sripathy; Yishan Mai; Rakaia F Kenney; Brady J Maher
Journal: Mol Psychiatry Date: 2022-10-12 Impact factor: 13.437

5. Transcription Factor 4 loss-of-function is associated with deficits in progenitor proliferation and cortical neuron content.

Authors: Antonio P Camargo; Janaina S de Souza; Vinicius M A Carvalho; Ryan A Szeto; Erin LaMontagne; Fabio Papes; José R Teixeira; Simoni H Avansini; Sandra M Sánchez-Sánchez; Thiago S Nakahara; Carolina N Santo; Wei Wu; Hang Yao; Barbara M P Araújo; Paulo E N F Velho; Gabriel G Haddad; Alysson R Muotri
Journal: Nat Commun Date: 2022-05-02 Impact factor: 17.694

Common Pathophysiology in Multiple Mouse Models of Pitt-Hopkins Syndrome.

1. A behavioral and neuroanatomical assessment of an inbred substrain of 129 mice with behavioral comparisons to C57BL/6J mice.

2. NR2A subunit expression shortens NMDA receptor synaptic currents in developing neocortex.

3. Mutations in TCF4, encoding a class I basic helix-loop-helix transcription factor, are responsible for Pitt-Hopkins syndrome, a severe epileptic encephalopathy associated with autonomic dysfunction.

4. Haploinsufficiency of TCF4 causes syndromal mental retardation with intermittent hyperventilation (Pitt-Hopkins syndrome).

5. Tcf4 Regulates Synaptic Plasticity, DNA Methylation, and Memory Function.

6. B-lymphocyte development is regulated by the combined dosage of three basic helix-loop-helix genes, E2A, E2-2, and HEB.

Review 7. In utero exposure to valproic acid and autism--a current review of clinical and animal studies.

8. Molecular characterisation of the 22q13 deletion syndrome supports the role of haploinsufficiency of SHANK3/PROSAP2 in the major neurological symptoms.

9. Neurodevelopmental models of transcription factor 4 deficiency converge on a common ion channel as a potential therapeutic target for Pitt Hopkins syndrome.

10. Phenotype and natural history in 101 individuals with Pitt-Hopkins syndrome through an internet questionnaire system.

1. Repurposing the Dihydropyridine Calcium Channel Inhibitor Nicardipine as a Na_v1.8 Inhibitor In Vivo for Pitt Hopkins Syndrome.

2. Kinesin Kif3b mutation reduces NMDAR subunit NR2A trafficking and causes schizophrenia-like phenotypes in mice.

3. Exploration of group II metabotropic glutamate receptor modulation in mouse models of Rett syndrome and MECP2 Duplication syndrome.

Review 4. Evaluation of Na_v1.8 as a therapeutic target for Pitt Hopkins Syndrome.

5. Transcription Factor 4 loss-of-function is associated with deficits in progenitor proliferation and cortical neuron content.

6. Transcription factor 4 controls positioning of cortical projection neurons through regulation of cell adhesion.

Review 7. Molecular and Cellular Function of Transcription Factor 4 in Pitt-Hopkins Syndrome.

8. Tcf4 regulates dendritic spine density and morphology in the adult brain.

9. Region and Cell Type Distribution of TCF4 in the Postnatal Mouse Brain.

10. Pitt-Hopkins Syndrome: Clinical and Molecular Findings of a 5-Year-Old Patient.

Review 7. In utero exposure to valproic acid and autism--a current review of clinical and animal studies.

Review 4. Evaluation of Nav1.8 as a therapeutic target for Pitt Hopkins Syndrome.

Review 7. Molecular and Cellular Function of Transcription Factor 4 in Pitt-Hopkins Syndrome.

Review 4. Evaluation of Na_v1.8 as a therapeutic target for Pitt Hopkins Syndrome.