Disordered breathing in a Pitt-Hopkins syndrome model involves Phox2b-expressing parafacial neurons and aberrant Nav1.8 expression

C. M. Cleary; S. James; B. J. Maher; D. K. Mulkey

doi:10.1038/s41467-021-26263-2

Disordered breathing in a Pitt-Hopkins syndrome model involves Phox2b-expressing parafacial neurons and aberrant Nav1.8 expression

C. M. Cleary, S. James, B. J. Maher, D. K. Mulkey

School of Medicine

Research output: Contribution to journal › Article › peer-review

Abstract

Pitt-Hopkins syndrome (PTHS) is a rare autism spectrum-like disorder characterized by intellectual disability, developmental delays, and breathing problems involving episodes of hyperventilation followed by apnea. PTHS is caused by functional haploinsufficiency of the gene encoding transcription factor 4 (Tcf4). Despite the severity of this disease, mechanisms contributing to PTHS behavioral abnormalities are not well understood. Here, we show that a Tcf4 truncation (Tcf4^tr/+) mouse model of PTHS exhibits breathing problems similar to PTHS patients. This behavioral deficit is associated with selective loss of putative expiratory parafacial neurons and compromised function of neurons in the retrotrapezoid nucleus that regulate breathing in response to tissue CO₂/H⁺. We also show that central Nav1.8 channels can be targeted pharmacologically to improve respiratory function at the cellular and behavioral levels in Tcf4^tr/+ mice, thus establishing Nav1.8 as a high priority target with therapeutic potential in PTHS.

Original language	English (US)
Article number	5962
Journal	Nature communications
Volume	12
Issue number	1
DOIs	https://doi.org/10.1038/s41467-021-26263-2
State	Published - Dec 1 2021

ASJC Scopus subject areas

General Physics and Astronomy
General Chemistry
General Biochemistry, Genetics and Molecular Biology

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10.1038/s41467-021-26263-2

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title = "Disordered breathing in a Pitt-Hopkins syndrome model involves Phox2b-expressing parafacial neurons and aberrant Nav1.8 expression",

abstract = "Pitt-Hopkins syndrome (PTHS) is a rare autism spectrum-like disorder characterized by intellectual disability, developmental delays, and breathing problems involving episodes of hyperventilation followed by apnea. PTHS is caused by functional haploinsufficiency of the gene encoding transcription factor 4 (Tcf4). Despite the severity of this disease, mechanisms contributing to PTHS behavioral abnormalities are not well understood. Here, we show that a Tcf4 truncation (Tcf4tr/+) mouse model of PTHS exhibits breathing problems similar to PTHS patients. This behavioral deficit is associated with selective loss of putative expiratory parafacial neurons and compromised function of neurons in the retrotrapezoid nucleus that regulate breathing in response to tissue CO2/H+. We also show that central Nav1.8 channels can be targeted pharmacologically to improve respiratory function at the cellular and behavioral levels in Tcf4tr/+ mice, thus establishing Nav1.8 as a high priority target with therapeutic potential in PTHS.",

author = "Cleary, {C. M.} and S. James and Maher, {B. J.} and Mulkey, {D. K.}",

note = "Funding Information: We thank Huda Zoghbi for encouraging us to pursue this research topic. We thank Ji-Young Lee and Yong-Ki Park for help with metabolic analysis, Alex Jackson for guidance with the open field assay, and Thiago Moreira for assistance using electromyography to measure respiratory muscle activity. We also thank William Flynn and Paul Robson for single cell RNA sequencing assistance. This work was supported by the following National Institutes of Health Grants: HL104101 (D.K.M.), HL137094 (D.K.M.), NS099887 (D.K.M.), MH104593 (B.J.M.) and MH110487 (B.J.M.) and F31HL142227 (C.M.C.). This work was also supported in part by funding from the Pitt Hopkins Research Foundation (B.J.M.). Publisher Copyright: {\textcopyright} 2021, The Author(s).",

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N1 - Funding Information: We thank Huda Zoghbi for encouraging us to pursue this research topic. We thank Ji-Young Lee and Yong-Ki Park for help with metabolic analysis, Alex Jackson for guidance with the open field assay, and Thiago Moreira for assistance using electromyography to measure respiratory muscle activity. We also thank William Flynn and Paul Robson for single cell RNA sequencing assistance. This work was supported by the following National Institutes of Health Grants: HL104101 (D.K.M.), HL137094 (D.K.M.), NS099887 (D.K.M.), MH104593 (B.J.M.) and MH110487 (B.J.M.) and F31HL142227 (C.M.C.). This work was also supported in part by funding from the Pitt Hopkins Research Foundation (B.J.M.). Publisher Copyright: © 2021, The Author(s).

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N2 - Pitt-Hopkins syndrome (PTHS) is a rare autism spectrum-like disorder characterized by intellectual disability, developmental delays, and breathing problems involving episodes of hyperventilation followed by apnea. PTHS is caused by functional haploinsufficiency of the gene encoding transcription factor 4 (Tcf4). Despite the severity of this disease, mechanisms contributing to PTHS behavioral abnormalities are not well understood. Here, we show that a Tcf4 truncation (Tcf4tr/+) mouse model of PTHS exhibits breathing problems similar to PTHS patients. This behavioral deficit is associated with selective loss of putative expiratory parafacial neurons and compromised function of neurons in the retrotrapezoid nucleus that regulate breathing in response to tissue CO2/H+. We also show that central Nav1.8 channels can be targeted pharmacologically to improve respiratory function at the cellular and behavioral levels in Tcf4tr/+ mice, thus establishing Nav1.8 as a high priority target with therapeutic potential in PTHS.

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Disordered breathing in a Pitt-Hopkins syndrome model involves Phox2b-expressing parafacial neurons and aberrant Nav1.8 expression

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