TMEM161B regulates cerebral cortical gyration, Sonic Hedgehog signaling, and ciliary structure in the developing central nervous system

Undiagnosed Diseases Network

doi:10.1073/pnas.2209964120

TMEM161B regulates cerebral cortical gyration, Sonic Hedgehog signaling, and ciliary structure in the developing central nervous system

Undiagnosed Diseases Network

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

Abstract

Sonic hedgehog signaling regulates processes of embryonic development across multiple tissues, yet factors regulating context-specific Shh signaling remain poorly understood. Exome sequencing of families with polymicrogyria (disordered cortical folding) revealed multiple individuals with biallelic deleterious variants in TMEM161B, which encodes a multi-pass transmembrane protein of unknown function. Tmem161b null mice demonstrated holoprosencephaly, craniofacial midline defects, eye defects, and spinal cord patterning changes consistent with impaired Shh signaling, but were without limb defects, suggesting a CNS-specific role of Tmem161b. Tmem161b depletion impaired the response to Smoothened activation in vitro and disrupted cortical histogenesis in vivo in both mouse and ferret models, including leading to abnormal gyration in the ferret model. Tmem161b localizes non-exclusively to the primary cilium, and scanning electron microscopy revealed shortened, dysmorphic, and ballooned ventricular zone cilia in the Tmem161b null mouse, suggesting that the Shh-related phenotypes may reflect ciliary dysfunction. Our data identify TMEM161B as a regulator of cerebral cortical gyration, as involved in primary ciliary structure, as a regulator of Shh signaling, and further implicate Shh signaling in human gyral development.

Original language	English (US)
Article number	e2209964120
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	120
Issue number	4
DOIs	https://doi.org/10.1073/pnas.2209964120
State	Published - Jan 24 2023

Keywords

Sonic Hedgehog
cortical gyration
holoprosencephaly
polymicrogyria
primary cilia

ASJC Scopus subject areas

General

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10.1073/pnas.2209964120

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@article{36e508231a3d4cfa8fd2fb445fe8715e,

title = "TMEM161B regulates cerebral cortical gyration, Sonic Hedgehog signaling, and ciliary structure in the developing central nervous system",

abstract = "Sonic hedgehog signaling regulates processes of embryonic development across multiple tissues, yet factors regulating context-specific Shh signaling remain poorly understood. Exome sequencing of families with polymicrogyria (disordered cortical folding) revealed multiple individuals with biallelic deleterious variants in TMEM161B, which encodes a multi-pass transmembrane protein of unknown function. Tmem161b null mice demonstrated holoprosencephaly, craniofacial midline defects, eye defects, and spinal cord patterning changes consistent with impaired Shh signaling, but were without limb defects, suggesting a CNS-specific role of Tmem161b. Tmem161b depletion impaired the response to Smoothened activation in vitro and disrupted cortical histogenesis in vivo in both mouse and ferret models, including leading to abnormal gyration in the ferret model. Tmem161b localizes non-exclusively to the primary cilium, and scanning electron microscopy revealed shortened, dysmorphic, and ballooned ventricular zone cilia in the Tmem161b null mouse, suggesting that the Shh-related phenotypes may reflect ciliary dysfunction. Our data identify TMEM161B as a regulator of cerebral cortical gyration, as involved in primary ciliary structure, as a regulator of Shh signaling, and further implicate Shh signaling in human gyral development.",

keywords = "Sonic Hedgehog, cortical gyration, holoprosencephaly, polymicrogyria, primary cilia",

author = "{Undiagnosed Diseases Network} and Akula, {Shyam K.} and Marciano, {Jack H.} and Youngshin Lim and David Exposito-Alonso and Hylton, {Norma K.} and Hwang, {Grace H.} and Neil, {Jennifer E.} and Nicole Dominado and Bunton-Stasyshyn, {Rosie K.} and Song, {Janet H.T.} and Maya Talukdar and Aloisia Schmid and Lydia Teboul and Alisa Mo and Taehwan Shin and Benjamin Finander and Beck, {Samantha G.} and Yeh, {Rebecca C.} and Aoi Otani and Xuyu Qian and DeGennaro, {Ellen M.} and Alkuraya, {Fowzan S.} and Sateesh Maddirevula and Cascino, {Gregory D.} and Caterina Giannini and Burrage, {Lindsay C.} and Rosenfield, {Jill A.} and Shamika Ketkar and Clark, {Gary D.} and Carlos Bacino and Lewis, {Richard A.} and Segal, {Rosalind A.} and Bazan, {J. Fernando} and Smith, {Kelly A.} and Golden, {Jeffrey A.} and Ginam Cho and Walsh, {Christopher A.}",

note = "Funding Information: ACKNOWLEDGMENTS. We are grateful the participant families involved in this study. We are grateful to Annapurna Poduri, Gord Fishell, Lisa Goodrich, Xuecai Ge, Rajat Rohatgi, Jennifer Kong, Lu Wang, and to other members of the Joseph Gleeson Lab for helpful discussions during planning of experiments and data interpretation. We thank Swati P. Iyer for assistance with mice. We are grateful to Andrew C. Kay for design consultation and illustration support. S.K.A. is supported by the Harvard Stem Cell Institute, NIH T32 MH020017 and T32 GM007753, and the Paul and Daisy Soros Fellowship for New Americans. D.E-A. is supported by an EMBO Postdoctoral Fellowship ALTF 336-2022.X.Q.is funded by a Postdoctoral Fellowship from the Helen Hay Whitney Foundation and the HHMI.R.A.S and G.H.H.are supported by Alex{\textquoteright}s Lemonade Stand Foundation,The Swifty Foundation, and the Helen Gurley Pussycat Foundation. Exome sequencing and analysis were provided by the Broad Institute of MIT and Harvard Center for Mendelian Genomics (Broad CMG) and was funded by the National Human Genome Research Institute, the National Eye Institute, and the National Heart, Lung and Blood Institute grant UM1 HG008900. C.A.W. is supported by the NINDS (R01 NS035129) and J.A.G. is supported by the NINDS (R01NS100007). This work was supported by UM1HG006348. C.A.W. is supported by the Allen Discovery Center for Human Brain Evolution through The Paul G. Allen Frontiers Group. C.A.W. is an Investigator of the HHMI. Funding Information: We are grateful the participant families involved in this study. We are grateful to Annapurna Poduri, Gord Fishell, Lisa Goodrich, Xuecai Ge, Rajat Rohatgi, Jennifer Kong, Lu Wang, and to other members of the Joseph Gleeson Lab for helpful discussions during planning of experiments and data interpretation. We thank Swati P. Iyer for assistance with mice. We are grateful to Andrew C. Kay for design consultation and illustration support. S.K.A. is supported by the Harvard Stem Cell Institute, NIH T32 MH020017 and T32 GM007753, and the Paul and Daisy Soros Fellowship for New Americans. D.E-A. is supported by an EMBO Postdoctoral Fellowship ALTF 336-2022. X.Q. is funded by a Postdoctoral Fellowship from the Helen Hay Whitney Foundation and the HHMI. R.A.S and G.H.H. are supported by Alex{\textquoteright}s Lemonade Stand Foundation, The Swifty Foundation, and the Helen Gurley Pussycat Foundation. Exome sequencing and analysis were provided by the Broad Institute of MIT and Harvard Center for Mendelian Genomics (Broad CMG) and was funded by the National Human Genome Research Institute, the National Eye Institute, and the National Heart, Lung and Blood Institute grant UM1 HG008900. C.A.W. is supported by the NINDS (R01 NS035129) and J.A.G. is supported by the NINDS (R01NS100007). This work was supported by UM1HG006348. C.A.W. is supported by the Allen Discovery Center for Human Brain Evolution through The Paul G. Allen Frontiers Group. C.A.W. is an Investigator of the HHMI. Publisher Copyright: Copyright {\textcopyright} 2023 the Author(s).",

year = "2023",

month = jan,

day = "24",

doi = "10.1073/pnas.2209964120",

language = "English (US)",

volume = "120",

journal = "Proceedings of the National Academy of Sciences of the United States of America",

issn = "0027-8424",

publisher = "National Academy of Sciences",

number = "4",

}

TY - JOUR

T1 - TMEM161B regulates cerebral cortical gyration, Sonic Hedgehog signaling, and ciliary structure in the developing central nervous system

AU - Undiagnosed Diseases Network

AU - Akula, Shyam K.

AU - Marciano, Jack H.

AU - Lim, Youngshin

AU - Exposito-Alonso, David

AU - Hylton, Norma K.

AU - Hwang, Grace H.

AU - Neil, Jennifer E.

AU - Dominado, Nicole

AU - Bunton-Stasyshyn, Rosie K.

AU - Song, Janet H.T.

AU - Talukdar, Maya

AU - Schmid, Aloisia

AU - Teboul, Lydia

AU - Mo, Alisa

AU - Shin, Taehwan

AU - Finander, Benjamin

AU - Beck, Samantha G.

AU - Yeh, Rebecca C.

AU - Otani, Aoi

AU - Qian, Xuyu

AU - DeGennaro, Ellen M.

AU - Alkuraya, Fowzan S.

AU - Maddirevula, Sateesh

AU - Cascino, Gregory D.

AU - Giannini, Caterina

AU - Burrage, Lindsay C.

AU - Rosenfield, Jill A.

AU - Ketkar, Shamika

AU - Clark, Gary D.

AU - Bacino, Carlos

AU - Lewis, Richard A.

AU - Segal, Rosalind A.

AU - Bazan, J. Fernando

AU - Smith, Kelly A.

AU - Golden, Jeffrey A.

AU - Cho, Ginam

AU - Walsh, Christopher A.

N1 - Funding Information: ACKNOWLEDGMENTS. We are grateful the participant families involved in this study. We are grateful to Annapurna Poduri, Gord Fishell, Lisa Goodrich, Xuecai Ge, Rajat Rohatgi, Jennifer Kong, Lu Wang, and to other members of the Joseph Gleeson Lab for helpful discussions during planning of experiments and data interpretation. We thank Swati P. Iyer for assistance with mice. We are grateful to Andrew C. Kay for design consultation and illustration support. S.K.A. is supported by the Harvard Stem Cell Institute, NIH T32 MH020017 and T32 GM007753, and the Paul and Daisy Soros Fellowship for New Americans. D.E-A. is supported by an EMBO Postdoctoral Fellowship ALTF 336-2022.X.Q.is funded by a Postdoctoral Fellowship from the Helen Hay Whitney Foundation and the HHMI.R.A.S and G.H.H.are supported by Alex’s Lemonade Stand Foundation,The Swifty Foundation, and the Helen Gurley Pussycat Foundation. Exome sequencing and analysis were provided by the Broad Institute of MIT and Harvard Center for Mendelian Genomics (Broad CMG) and was funded by the National Human Genome Research Institute, the National Eye Institute, and the National Heart, Lung and Blood Institute grant UM1 HG008900. C.A.W. is supported by the NINDS (R01 NS035129) and J.A.G. is supported by the NINDS (R01NS100007). This work was supported by UM1HG006348. C.A.W. is supported by the Allen Discovery Center for Human Brain Evolution through The Paul G. Allen Frontiers Group. C.A.W. is an Investigator of the HHMI. Funding Information: We are grateful the participant families involved in this study. We are grateful to Annapurna Poduri, Gord Fishell, Lisa Goodrich, Xuecai Ge, Rajat Rohatgi, Jennifer Kong, Lu Wang, and to other members of the Joseph Gleeson Lab for helpful discussions during planning of experiments and data interpretation. We thank Swati P. Iyer for assistance with mice. We are grateful to Andrew C. Kay for design consultation and illustration support. S.K.A. is supported by the Harvard Stem Cell Institute, NIH T32 MH020017 and T32 GM007753, and the Paul and Daisy Soros Fellowship for New Americans. D.E-A. is supported by an EMBO Postdoctoral Fellowship ALTF 336-2022. X.Q. is funded by a Postdoctoral Fellowship from the Helen Hay Whitney Foundation and the HHMI. R.A.S and G.H.H. are supported by Alex’s Lemonade Stand Foundation, The Swifty Foundation, and the Helen Gurley Pussycat Foundation. Exome sequencing and analysis were provided by the Broad Institute of MIT and Harvard Center for Mendelian Genomics (Broad CMG) and was funded by the National Human Genome Research Institute, the National Eye Institute, and the National Heart, Lung and Blood Institute grant UM1 HG008900. C.A.W. is supported by the NINDS (R01 NS035129) and J.A.G. is supported by the NINDS (R01NS100007). This work was supported by UM1HG006348. C.A.W. is supported by the Allen Discovery Center for Human Brain Evolution through The Paul G. Allen Frontiers Group. C.A.W. is an Investigator of the HHMI. Publisher Copyright: Copyright © 2023 the Author(s).

PY - 2023/1/24

Y1 - 2023/1/24

N2 - Sonic hedgehog signaling regulates processes of embryonic development across multiple tissues, yet factors regulating context-specific Shh signaling remain poorly understood. Exome sequencing of families with polymicrogyria (disordered cortical folding) revealed multiple individuals with biallelic deleterious variants in TMEM161B, which encodes a multi-pass transmembrane protein of unknown function. Tmem161b null mice demonstrated holoprosencephaly, craniofacial midline defects, eye defects, and spinal cord patterning changes consistent with impaired Shh signaling, but were without limb defects, suggesting a CNS-specific role of Tmem161b. Tmem161b depletion impaired the response to Smoothened activation in vitro and disrupted cortical histogenesis in vivo in both mouse and ferret models, including leading to abnormal gyration in the ferret model. Tmem161b localizes non-exclusively to the primary cilium, and scanning electron microscopy revealed shortened, dysmorphic, and ballooned ventricular zone cilia in the Tmem161b null mouse, suggesting that the Shh-related phenotypes may reflect ciliary dysfunction. Our data identify TMEM161B as a regulator of cerebral cortical gyration, as involved in primary ciliary structure, as a regulator of Shh signaling, and further implicate Shh signaling in human gyral development.

AB - Sonic hedgehog signaling regulates processes of embryonic development across multiple tissues, yet factors regulating context-specific Shh signaling remain poorly understood. Exome sequencing of families with polymicrogyria (disordered cortical folding) revealed multiple individuals with biallelic deleterious variants in TMEM161B, which encodes a multi-pass transmembrane protein of unknown function. Tmem161b null mice demonstrated holoprosencephaly, craniofacial midline defects, eye defects, and spinal cord patterning changes consistent with impaired Shh signaling, but were without limb defects, suggesting a CNS-specific role of Tmem161b. Tmem161b depletion impaired the response to Smoothened activation in vitro and disrupted cortical histogenesis in vivo in both mouse and ferret models, including leading to abnormal gyration in the ferret model. Tmem161b localizes non-exclusively to the primary cilium, and scanning electron microscopy revealed shortened, dysmorphic, and ballooned ventricular zone cilia in the Tmem161b null mouse, suggesting that the Shh-related phenotypes may reflect ciliary dysfunction. Our data identify TMEM161B as a regulator of cerebral cortical gyration, as involved in primary ciliary structure, as a regulator of Shh signaling, and further implicate Shh signaling in human gyral development.

KW - Sonic Hedgehog

KW - cortical gyration

KW - holoprosencephaly

KW - polymicrogyria

KW - primary cilia

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U2 - 10.1073/pnas.2209964120

DO - 10.1073/pnas.2209964120

M3 - Article

C2 - 36669111

AN - SCOPUS:85146892425

SN - 0027-8424

VL - 120

JO - Proceedings of the National Academy of Sciences of the United States of America

JF - Proceedings of the National Academy of Sciences of the United States of America

IS - 4

M1 - e2209964120

ER -

TMEM161B regulates cerebral cortical gyration, Sonic Hedgehog signaling, and ciliary structure in the developing central nervous system

Abstract

Keywords

ASJC Scopus subject areas

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