TMEM237 is mutated in individuals with a Joubert syndrome related disorder and expands the role of the TMEM family at the ciliary transition zone

Lijia Huang; Katarzyna Szymanska; Victor L. Jensen; Andreas R. Janecke; A. Micheil Innes; Erica E. Davis; Patrick Frosk; Chunmei Li; Jason R. Willer; Bernard N. Chodirker; Cheryl R. Greenberg; D. Ross McLeod; Francois P. Bernier; Albert E. Chudley; Thomas Müller; Mohammad Shboul; Clare V. Logan; Catrina M. Loucks; Chandree L. Beaulieu; Rachel V. Bowie; Sandra M. Bell; Jonathan Adkins; Freddi I. Zuniga; Kevin D. Ross; Jian Wang; Matthew R. Ban; Christian Becker; Peter Nürnberg; Stuart Douglas; Cheryl M. Craft; Marie Andree Akimenko; Robert A. Hegele; Carole Ober; Gerd Utermann; Hanno J. Bolz; Dennis E. Bulman; Nicholas Katsanis; Oliver E. Blacque; Dan Doherty; Jillian S. Parboosingh; Michel R. Leroux; Colin A. Johnson; Kym M. Boycott

doi:10.1016/j.ajhg.2011.11.005

TMEM237 is mutated in individuals with a Joubert syndrome related disorder and expands the role of the TMEM family at the ciliary transition zone

Lijia Huang
, Katarzyna Szymanska
, Victor L. Jensen
, Andreas R. Janecke
, A. Micheil Innes
, Erica E. Davis
, Patrick Frosk
, Chunmei Li
, Jason R. Willer
, Bernard N. Chodirker
, Cheryl R. Greenberg
, D. Ross McLeod
, Francois P. Bernier
, Albert E. Chudley
, Thomas Müller
, Mohammad Shboul
, Clare V. Logan
, Catrina M. Loucks
, Chandree L. Beaulieu
, Rachel V. Bowie

Sandra M. Bell, Jonathan Adkins, Freddi I. Zuniga, Kevin D. Ross, Jian Wang, Matthew R. Ban, Christian Becker, Peter Nürnberg, Stuart Douglas, Cheryl M. Craft, Marie Andree Akimenko, Robert A. Hegele, Carole Ober, Gerd Utermann, Hanno J. Bolz, Dennis E. Bulman, Nicholas Katsanis, Oliver E. Blacque, Dan Doherty, Jillian S. Parboosingh, Michel R. Leroux, Colin A. Johnson, Kym M. Boycott

University of Ottawa
Leeds Teaching Hospitals NHS Trust
Simon Fraser University
Innsbruck Medical University
University of Calgary
Duke University
University of Manitoba
Agency for Science, Technology and Research, Singapore
University College Dublin
University of Washington
Doheny Eye Institute
The University of Chicago
Western University
University of Cologne
Bioscientia Institut für Medizinische Diagnostik GmbH

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

169 Scopus citations

Abstract

Joubert syndrome related disorders (JSRDs) have broad but variable phenotypic overlap with other ciliopathies. The molecular etiology of this overlap is unclear but probably arises from disrupting common functional module components within primary cilia. To identify additional module elements associated with JSRDs, we performed homozygosity mapping followed by next-generation sequencing (NGS) and uncovered mutations in TMEM237 (previously known as ALS2CR4). We show that loss of the mammalian TMEM237, which localizes to the ciliary transition zone (TZ), results in defective ciliogenesis and deregulation of Wnt signaling. Furthermore, disruption of Danio rerio (zebrafish) tmem237 expression produces gastrulation defects consistent with ciliary dysfunction, and Caenorhabditis elegans jbts-14 genetically interacts with nphp-4, encoding another TZ protein, to control basal body-TZ anchoring to the membrane and ciliogenesis. Both mammalian and C. elegans TMEM237/JBTS-14 require RPGRIP1L/MKS5 for proper TZ localization, and we demonstrate additional functional interactions between C. elegans JBTS-14 and MKS-2/TMEM216, MKSR-1/B9D1, and MKSR-2/B9D2. Collectively, our findings integrate TMEM237/JBTS-14 in a complex interaction network of TZ-associated proteins and reveal a growing contribution of a TZ functional module to the spectrum of ciliopathy phenotypes.

Original language	English
Pages (from-to)	713-730
Number of pages	18
Journal	American Journal of Human Genetics
Volume	89
Issue number	6
DOIs	https://doi.org/10.1016/j.ajhg.2011.11.005
State	Published - 9 Dec 2011
Externally published	Yes

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10.1016/j.ajhg.2011.11.005

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Huang, L., Szymanska, K., Jensen, V. L., Janecke, A. R., Innes, A. M., Davis, E. E., Frosk, P., Li, C., Willer, J. R., Chodirker, B. N., Greenberg, C. R., McLeod, D. R., Bernier, F. P., Chudley, A. E., Müller, T., Shboul, M., Logan, C. V., Loucks, C. M., Beaulieu, C. L., ... Boycott, K. M. (2011). TMEM237 is mutated in individuals with a Joubert syndrome related disorder and expands the role of the TMEM family at the ciliary transition zone. American Journal of Human Genetics, 89(6), 713-730. https://doi.org/10.1016/j.ajhg.2011.11.005

@article{fa0e3e94c5f942e0872e6dcda5f32bd2,

title = "TMEM237 is mutated in individuals with a Joubert syndrome related disorder and expands the role of the TMEM family at the ciliary transition zone",

abstract = "Joubert syndrome related disorders (JSRDs) have broad but variable phenotypic overlap with other ciliopathies. The molecular etiology of this overlap is unclear but probably arises from disrupting common functional module components within primary cilia. To identify additional module elements associated with JSRDs, we performed homozygosity mapping followed by next-generation sequencing (NGS) and uncovered mutations in TMEM237 (previously known as ALS2CR4). We show that loss of the mammalian TMEM237, which localizes to the ciliary transition zone (TZ), results in defective ciliogenesis and deregulation of Wnt signaling. Furthermore, disruption of Danio rerio (zebrafish) tmem237 expression produces gastrulation defects consistent with ciliary dysfunction, and Caenorhabditis elegans jbts-14 genetically interacts with nphp-4, encoding another TZ protein, to control basal body-TZ anchoring to the membrane and ciliogenesis. Both mammalian and C. elegans TMEM237/JBTS-14 require RPGRIP1L/MKS5 for proper TZ localization, and we demonstrate additional functional interactions between C. elegans JBTS-14 and MKS-2/TMEM216, MKSR-1/B9D1, and MKSR-2/B9D2. Collectively, our findings integrate TMEM237/JBTS-14 in a complex interaction network of TZ-associated proteins and reveal a growing contribution of a TZ functional module to the spectrum of ciliopathy phenotypes.",

author = "Lijia Huang and Katarzyna Szymanska and Jensen, \{Victor L.\} and Janecke, \{Andreas R.\} and Innes, \{A. Micheil\} and Davis, \{Erica E.\} and Patrick Frosk and Chunmei Li and Willer, \{Jason R.\} and Chodirker, \{Bernard N.\} and Greenberg, \{Cheryl R.\} and McLeod, \{D. Ross\} and Bernier, \{Francois P.\} and Chudley, \{Albert E.\} and Thomas M{\"u}ller and Mohammad Shboul and Logan, \{Clare V.\} and Loucks, \{Catrina M.\} and Beaulieu, \{Chandree L.\} and Bowie, \{Rachel V.\} and Bell, \{Sandra M.\} and Jonathan Adkins and Zuniga, \{Freddi I.\} and Ross, \{Kevin D.\} and Jian Wang and Ban, \{Matthew R.\} and Christian Becker and Peter N{\"u}rnberg and Stuart Douglas and Craft, \{Cheryl M.\} and Akimenko, \{Marie Andree\} and Hegele, \{Robert A.\} and Carole Ober and Gerd Utermann and Bolz, \{Hanno J.\} and Bulman, \{Dennis E.\} and Nicholas Katsanis and Blacque, \{Oliver E.\} and Dan Doherty and Parboosingh, \{Jillian S.\} and Leroux, \{Michel R.\} and Johnson, \{Colin A.\} and Boycott, \{Kym M.\}",

year = "2011",

month = dec,

day = "9",

doi = "10.1016/j.ajhg.2011.11.005",

language = "English",

volume = "89",

pages = "713--730",

journal = "American Journal of Human Genetics",

issn = "0002-9297",

publisher = "Cell Press",

number = "6",

}

Huang, L, Szymanska, K, Jensen, VL, Janecke, AR, Innes, AM, Davis, EE, Frosk, P, Li, C, Willer, JR, Chodirker, BN, Greenberg, CR, McLeod, DR, Bernier, FP, Chudley, AE, Müller, T, Shboul, M, Logan, CV, Loucks, CM, Beaulieu, CL, Bowie, RV, Bell, SM, Adkins, J, Zuniga, FI, Ross, KD, Wang, J, Ban, MR, Becker, C, Nürnberg, P, Douglas, S, Craft, CM, Akimenko, MA, Hegele, RA, Ober, C, Utermann, G, Bolz, HJ, Bulman, DE, Katsanis, N, Blacque, OE, Doherty, D, Parboosingh, JS, Leroux, MR, Johnson, CA & Boycott, KM 2011, 'TMEM237 is mutated in individuals with a Joubert syndrome related disorder and expands the role of the TMEM family at the ciliary transition zone', American Journal of Human Genetics, vol. 89, no. 6, pp. 713-730. https://doi.org/10.1016/j.ajhg.2011.11.005

TY - JOUR

T1 - TMEM237 is mutated in individuals with a Joubert syndrome related disorder and expands the role of the TMEM family at the ciliary transition zone

AU - Huang, Lijia

AU - Szymanska, Katarzyna

AU - Jensen, Victor L.

AU - Janecke, Andreas R.

AU - Innes, A. Micheil

AU - Davis, Erica E.

AU - Frosk, Patrick

AU - Li, Chunmei

AU - Willer, Jason R.

AU - Chodirker, Bernard N.

AU - Greenberg, Cheryl R.

AU - McLeod, D. Ross

AU - Bernier, Francois P.

AU - Chudley, Albert E.

AU - Müller, Thomas

AU - Shboul, Mohammad

AU - Logan, Clare V.

AU - Loucks, Catrina M.

AU - Beaulieu, Chandree L.

AU - Bowie, Rachel V.

AU - Bell, Sandra M.

AU - Adkins, Jonathan

AU - Zuniga, Freddi I.

AU - Ross, Kevin D.

AU - Wang, Jian

AU - Ban, Matthew R.

AU - Becker, Christian

AU - Nürnberg, Peter

AU - Douglas, Stuart

AU - Craft, Cheryl M.

AU - Akimenko, Marie Andree

AU - Hegele, Robert A.

AU - Ober, Carole

AU - Utermann, Gerd

AU - Bolz, Hanno J.

AU - Bulman, Dennis E.

AU - Katsanis, Nicholas

AU - Blacque, Oliver E.

AU - Doherty, Dan

AU - Parboosingh, Jillian S.

AU - Leroux, Michel R.

AU - Johnson, Colin A.

AU - Boycott, Kym M.

PY - 2011/12/9

Y1 - 2011/12/9

N2 - Joubert syndrome related disorders (JSRDs) have broad but variable phenotypic overlap with other ciliopathies. The molecular etiology of this overlap is unclear but probably arises from disrupting common functional module components within primary cilia. To identify additional module elements associated with JSRDs, we performed homozygosity mapping followed by next-generation sequencing (NGS) and uncovered mutations in TMEM237 (previously known as ALS2CR4). We show that loss of the mammalian TMEM237, which localizes to the ciliary transition zone (TZ), results in defective ciliogenesis and deregulation of Wnt signaling. Furthermore, disruption of Danio rerio (zebrafish) tmem237 expression produces gastrulation defects consistent with ciliary dysfunction, and Caenorhabditis elegans jbts-14 genetically interacts with nphp-4, encoding another TZ protein, to control basal body-TZ anchoring to the membrane and ciliogenesis. Both mammalian and C. elegans TMEM237/JBTS-14 require RPGRIP1L/MKS5 for proper TZ localization, and we demonstrate additional functional interactions between C. elegans JBTS-14 and MKS-2/TMEM216, MKSR-1/B9D1, and MKSR-2/B9D2. Collectively, our findings integrate TMEM237/JBTS-14 in a complex interaction network of TZ-associated proteins and reveal a growing contribution of a TZ functional module to the spectrum of ciliopathy phenotypes.

AB - Joubert syndrome related disorders (JSRDs) have broad but variable phenotypic overlap with other ciliopathies. The molecular etiology of this overlap is unclear but probably arises from disrupting common functional module components within primary cilia. To identify additional module elements associated with JSRDs, we performed homozygosity mapping followed by next-generation sequencing (NGS) and uncovered mutations in TMEM237 (previously known as ALS2CR4). We show that loss of the mammalian TMEM237, which localizes to the ciliary transition zone (TZ), results in defective ciliogenesis and deregulation of Wnt signaling. Furthermore, disruption of Danio rerio (zebrafish) tmem237 expression produces gastrulation defects consistent with ciliary dysfunction, and Caenorhabditis elegans jbts-14 genetically interacts with nphp-4, encoding another TZ protein, to control basal body-TZ anchoring to the membrane and ciliogenesis. Both mammalian and C. elegans TMEM237/JBTS-14 require RPGRIP1L/MKS5 for proper TZ localization, and we demonstrate additional functional interactions between C. elegans JBTS-14 and MKS-2/TMEM216, MKSR-1/B9D1, and MKSR-2/B9D2. Collectively, our findings integrate TMEM237/JBTS-14 in a complex interaction network of TZ-associated proteins and reveal a growing contribution of a TZ functional module to the spectrum of ciliopathy phenotypes.

UR - https://www.scopus.com/pages/publications/83455253776

U2 - 10.1016/j.ajhg.2011.11.005

DO - 10.1016/j.ajhg.2011.11.005

M3 - Article

C2 - 22152675

AN - SCOPUS:83455253776

SN - 0002-9297

VL - 89

SP - 713

EP - 730

JO - American Journal of Human Genetics

JF - American Journal of Human Genetics

IS - 6

ER -

TMEM237 is mutated in individuals with a Joubert syndrome related disorder and expands the role of the TMEM family at the ciliary transition zone

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