TMEM107 recruits ciliopathy proteins to subdomains of the ciliary transition zone and causes Joubert syndrome

Nils J Lambacher; Ange-Line Bruel; Teunis J P van Dam; Katarzyna Szymańska; Gisela G Slaats; Stefanie Kuhns; Gavin J McManus; Julie E Kennedy; Karl Gaff; Ka Man Wu; Robin van der Lee; Lydie Burglen; Diane Doummar; Jean-Baptiste Rivière; Laurence Faivre; Tania Attié-Bitach; Sophie Saunier; Alistair Curd; Michelle Peckham; R Giles; Colin A Johnson; Martijn A Huynen; Christel Thauvin-Robinet; Oliver E Blacque

doi:10.1038/ncb3273

TMEM107 recruits ciliopathy proteins to subdomains of the ciliary transition zone and causes Joubert syndrome

Nils J Lambacher, Ange-Line Bruel, Teunis J P van Dam, Katarzyna Szymańska, Gisela G Slaats, Stefanie Kuhns, Gavin J McManus, Julie E Kennedy, Karl Gaff, Ka Man Wu, Robin van der Lee, Lydie Burglen, Diane Doummar, Jean-Baptiste Rivière, Laurence Faivre, Tania Attié-Bitach, Sophie Saunier, Alistair Curd, Michelle Peckham, R GilesColin A Johnson, Martijn A Huynen, Christel Thauvin-Robinet, Oliver E Blacque

Research output: Contribution to journal › Letter › Academic › peer-review

Abstract

The transition zone (TZ) ciliary subcompartment is thought to control cilium composition and signalling by facilitating a protein diffusion barrier at the ciliary base. TZ defects cause ciliopathies such as Meckel-Gruber syndrome (MKS), nephronophthisis (NPHP) and Joubert syndrome (JBTS). However, the molecular composition and mechanisms underpinning TZ organization and barrier regulation are poorly understood. To uncover candidate TZ genes, we employed bioinformatics (coexpression and co-evolution) and identified TMEM107 as a TZ protein mutated in oral-facial-digital syndrome and JBTS patients. Mechanistic studies in Caenorhabditis elegans showed that TMEM-107 controls ciliary composition and functions redundantly with NPHP-4 to regulate cilium integrity, TZ docking and assembly of membrane to microtubule Y-link connectors. Furthermore, nematode TMEM-107 occupies an intermediate layer of the TZ-localized MKS module by organizing recruitment of the ciliopathy proteins MKS-1, TMEM-231 (JBTS20) and JBTS-14 (TMEM237). Finally, MKS module membrane proteins are immobile and super-resolution microscopy in worms and mammalian cells reveals periodic localizations within the TZ. This work expands the MKS module of ciliopathy-causing TZ proteins associated with diffusion barrier formation and provides insight into TZ subdomain architecture.

Original language	English
Pages (from-to)	122-31
Number of pages	10
Journal	Nature Cell Biology
Volume	18
Issue number	1
DOIs	https://doi.org/10.1038/ncb3273
Publication status	Published - Jan 2016

Access to Document

10.1038/ncb3273

Cite this

Lambacher, N. J., Bruel, A.-L., van Dam, T. J. P., Szymańska, K., Slaats, G. G., Kuhns, S., McManus, G. J., Kennedy, J. E., Gaff, K., Wu, K. M., van der Lee, R., Burglen, L., Doummar, D., Rivière, J.-B., Faivre, L., Attié-Bitach, T., Saunier, S., Curd, A., Peckham, M., ... Blacque, O. E. (2016). TMEM107 recruits ciliopathy proteins to subdomains of the ciliary transition zone and causes Joubert syndrome. Nature Cell Biology, 18(1), 122-31. https://doi.org/10.1038/ncb3273

@article{875047bc186546008fbd4f2c7c7cf3e5,

title = "TMEM107 recruits ciliopathy proteins to subdomains of the ciliary transition zone and causes Joubert syndrome",

abstract = "The transition zone (TZ) ciliary subcompartment is thought to control cilium composition and signalling by facilitating a protein diffusion barrier at the ciliary base. TZ defects cause ciliopathies such as Meckel-Gruber syndrome (MKS), nephronophthisis (NPHP) and Joubert syndrome (JBTS). However, the molecular composition and mechanisms underpinning TZ organization and barrier regulation are poorly understood. To uncover candidate TZ genes, we employed bioinformatics (coexpression and co-evolution) and identified TMEM107 as a TZ protein mutated in oral-facial-digital syndrome and JBTS patients. Mechanistic studies in Caenorhabditis elegans showed that TMEM-107 controls ciliary composition and functions redundantly with NPHP-4 to regulate cilium integrity, TZ docking and assembly of membrane to microtubule Y-link connectors. Furthermore, nematode TMEM-107 occupies an intermediate layer of the TZ-localized MKS module by organizing recruitment of the ciliopathy proteins MKS-1, TMEM-231 (JBTS20) and JBTS-14 (TMEM237). Finally, MKS module membrane proteins are immobile and super-resolution microscopy in worms and mammalian cells reveals periodic localizations within the TZ. This work expands the MKS module of ciliopathy-causing TZ proteins associated with diffusion barrier formation and provides insight into TZ subdomain architecture.",

author = "Lambacher, {Nils J} and Ange-Line Bruel and {van Dam}, {Teunis J P} and Katarzyna Szyma{\'n}ska and Slaats, {Gisela G} and Stefanie Kuhns and McManus, {Gavin J} and Kennedy, {Julie E} and Karl Gaff and Wu, {Ka Man} and {van der Lee}, Robin and Lydie Burglen and Diane Doummar and Jean-Baptiste Rivi{\`e}re and Laurence Faivre and Tania Atti{\'e}-Bitach and Sophie Saunier and Alistair Curd and Michelle Peckham and R Giles and Johnson, {Colin A} and Huynen, {Martijn A} and Christel Thauvin-Robinet and Blacque, {Oliver E}",

year = "2016",

month = jan,

doi = "10.1038/ncb3273",

language = "English",

volume = "18",

pages = "122--31",

journal = "Nature Cell Biology",

issn = "1465-7392",

publisher = "Nature Research",

number = "1",

}

Lambacher, NJ, Bruel, A-L, van Dam, TJP, Szymańska, K, Slaats, GG, Kuhns, S, McManus, GJ, Kennedy, JE, Gaff, K, Wu, KM, van der Lee, R, Burglen, L, Doummar, D, Rivière, J-B, Faivre, L, Attié-Bitach, T, Saunier, S, Curd, A, Peckham, M, Giles, R, Johnson, CA, Huynen, MA, Thauvin-Robinet, C & Blacque, OE 2016, 'TMEM107 recruits ciliopathy proteins to subdomains of the ciliary transition zone and causes Joubert syndrome', Nature Cell Biology, vol. 18, no. 1, pp. 122-31. https://doi.org/10.1038/ncb3273

TY - JOUR

T1 - TMEM107 recruits ciliopathy proteins to subdomains of the ciliary transition zone and causes Joubert syndrome

AU - Lambacher, Nils J

AU - Bruel, Ange-Line

AU - van Dam, Teunis J P

AU - Szymańska, Katarzyna

AU - Slaats, Gisela G

AU - Kuhns, Stefanie

AU - McManus, Gavin J

AU - Kennedy, Julie E

AU - Gaff, Karl

AU - Wu, Ka Man

AU - van der Lee, Robin

AU - Burglen, Lydie

AU - Doummar, Diane

AU - Rivière, Jean-Baptiste

AU - Faivre, Laurence

AU - Attié-Bitach, Tania

AU - Saunier, Sophie

AU - Curd, Alistair

AU - Peckham, Michelle

AU - Giles, R

AU - Johnson, Colin A

AU - Huynen, Martijn A

AU - Thauvin-Robinet, Christel

AU - Blacque, Oliver E

PY - 2016/1

Y1 - 2016/1

N2 - The transition zone (TZ) ciliary subcompartment is thought to control cilium composition and signalling by facilitating a protein diffusion barrier at the ciliary base. TZ defects cause ciliopathies such as Meckel-Gruber syndrome (MKS), nephronophthisis (NPHP) and Joubert syndrome (JBTS). However, the molecular composition and mechanisms underpinning TZ organization and barrier regulation are poorly understood. To uncover candidate TZ genes, we employed bioinformatics (coexpression and co-evolution) and identified TMEM107 as a TZ protein mutated in oral-facial-digital syndrome and JBTS patients. Mechanistic studies in Caenorhabditis elegans showed that TMEM-107 controls ciliary composition and functions redundantly with NPHP-4 to regulate cilium integrity, TZ docking and assembly of membrane to microtubule Y-link connectors. Furthermore, nematode TMEM-107 occupies an intermediate layer of the TZ-localized MKS module by organizing recruitment of the ciliopathy proteins MKS-1, TMEM-231 (JBTS20) and JBTS-14 (TMEM237). Finally, MKS module membrane proteins are immobile and super-resolution microscopy in worms and mammalian cells reveals periodic localizations within the TZ. This work expands the MKS module of ciliopathy-causing TZ proteins associated with diffusion barrier formation and provides insight into TZ subdomain architecture.

AB - The transition zone (TZ) ciliary subcompartment is thought to control cilium composition and signalling by facilitating a protein diffusion barrier at the ciliary base. TZ defects cause ciliopathies such as Meckel-Gruber syndrome (MKS), nephronophthisis (NPHP) and Joubert syndrome (JBTS). However, the molecular composition and mechanisms underpinning TZ organization and barrier regulation are poorly understood. To uncover candidate TZ genes, we employed bioinformatics (coexpression and co-evolution) and identified TMEM107 as a TZ protein mutated in oral-facial-digital syndrome and JBTS patients. Mechanistic studies in Caenorhabditis elegans showed that TMEM-107 controls ciliary composition and functions redundantly with NPHP-4 to regulate cilium integrity, TZ docking and assembly of membrane to microtubule Y-link connectors. Furthermore, nematode TMEM-107 occupies an intermediate layer of the TZ-localized MKS module by organizing recruitment of the ciliopathy proteins MKS-1, TMEM-231 (JBTS20) and JBTS-14 (TMEM237). Finally, MKS module membrane proteins are immobile and super-resolution microscopy in worms and mammalian cells reveals periodic localizations within the TZ. This work expands the MKS module of ciliopathy-causing TZ proteins associated with diffusion barrier formation and provides insight into TZ subdomain architecture.

U2 - 10.1038/ncb3273

DO - 10.1038/ncb3273

M3 - Letter

C2 - 26595381

SN - 1465-7392

VL - 18

SP - 122

EP - 131

JO - Nature Cell Biology

JF - Nature Cell Biology

IS - 1

ER -

TMEM107 recruits ciliopathy proteins to subdomains of the ciliary transition zone and causes Joubert syndrome

Abstract

Access to Document

Fingerprint

Cite this