Advanced search
Publication Cover
Rare Diseases Volume 4, 2016 - Issue 1
Journal homepage
1,967
Views
20
CrossRef citations to date
0
Altmetric
Addendum

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

Matthew D. RannalsDepartment of Neurobiology, School of Medicine, University of Pittsburgh, Pittsburgh, PA, USA
,
Stephanie Cerceo PageLieber Institute for Brain Development, Johns Hopkins Medical Campus, Baltimore, MD, USA
,
Morganne N. CampbellLieber Institute for Brain Development, Johns Hopkins Medical Campus, Baltimore, MD, USA
,
Ryan A. GalloLieber Institute for Brain Development, Johns Hopkins Medical Campus, Baltimore, MD, USA
,
Brent MayfieldLieber Institute for Brain Development, Johns Hopkins Medical Campus, Baltimore, MD, USA
&
Brady J. MaherLieber Institute for Brain Development, Johns Hopkins Medical Campus, Baltimore, MD, USA;Department of Psychiatry and Behavioral Sciences, Johns Hopkins School of Medicine, Baltimore, MD, USA;Department of Neuroscience, Johns Hopkins School of Medicine, Baltimore, MD, USACorrespondence[email protected]
Article: e1220468 | Received 01 Jun 2016, Accepted 28 Jul 2016, Published online: 30 Aug 2016
 
Sample our Medicine, Dentistry, Nursing & Allied Health journals, sign in here to start your FREE access for 14 days

ABSTRACT

The clinically pleiotropic gene, Transcription Factor 4 (TCF4), is a broadly expressed basic helix-loop-helix (bHLH) transcription factor linked to multiple neurodevelopmental disorders, including schizophrenia, 18q deletion syndrome, and Pitt Hopkins syndrome (PTHS). In vivo suppression of Tcf4 by shRNA or mutation by CRISPR/Cas9 in the developing rat prefrontal cortex resulted in attenuated action potential output. To explain this intrinsic excitability deficit, we demonstrated that haploinsufficiency of TCF4 lead to the ectopic expression of two ion channels, Scn10a and Kcnq1. These targets of TCF4 regulation were identified through molecular profiling experiments that used translating ribosome affinity purification to enrich mRNA from genetically manipulated neurons.

Using a mouse model of PTHS (Tcf4+/tr), we observed a similar intrinsic excitability deficit, however the underlying mechanism appeared slightly different than our rat model - as Scn10a expression was similarly increased but Kcnq1 expression was decreased. Here, we show that the truncated TCF4 protein expressed in our PTHS mouse model binds to wild-type TCF4 protein, and we suggest the difference in Kcnq1 expression levels between these two rodent models appears to be explained by a dominant-negative function of the truncated TCF4 protein. Despite the differences in the underlying molecular mechanisms, we observed common underlying intrinsic excitability deficits that are consistent with ectopic expression of Scn10a. The converging molecular function of TCF4 across two independent rodent models indicates SCN10a is a potential therapeutic target for Pitt-Hopkins syndrome.

This article refers to:

Disclosure of potential conflicts of interest

No potential conflicts of interest were disclosed.

Funding

This work was supported by NIH grant (R56MH104593) and Pitt-Hopkins Research Foundation Award to B.J.M.

Download PDF

Related research

People also read lists articles that other readers of this article have read.

Recommended articles lists articles that we recommend and is powered by our AI driven recommendation engine.

Cited by lists all citing articles based on Crossref citations.
Articles with the Crossref icon will open in a new tab.