SCUBE3 loss-of-function causes a recognizable recessive developmental disorder due to defective bone morphogenetic protein signaling

Genomics England Research Consortium

doi:10.1016/j.ajhg.2020.11.015

SCUBE3 loss-of-function causes a recognizable recessive developmental disorder due to defective bone morphogenetic protein signaling

Genomics England Research Consortium

Department of Physiology

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

31 Citations (Scopus)

Abstract

Signal peptide-CUB-EGF domain-containing protein 3 (SCUBE3) is a member of a small family of multifunctional cell surface-anchored glycoproteins functioning as co-receptors for a variety of growth factors. Here we report that bi-allelic inactivating variants in SCUBE3 have pleiotropic consequences on development and cause a previously unrecognized syndromic disorder. Eighteen affected individuals from nine unrelated families showed a consistent phenotype characterized by reduced growth, skeletal features, distinctive craniofacial appearance, and dental anomalies. In vitro functional validation studies demonstrated a variable impact of disease-causing variants on transcript processing, protein secretion and function, and their dysregulating effect on bone morphogenetic protein (BMP) signaling. We show that SCUBE3 acts as a BMP2/BMP4 co-receptor, recruits the BMP receptor complexes into raft microdomains, and positively modulates signaling possibly by augmenting the specific interactions between BMPs and BMP type I receptors. Scube3^−/− mice showed craniofacial and dental defects, reduced body size, and defective endochondral bone growth due to impaired BMP-mediated chondrogenesis and osteogenesis, recapitulating the human disorder. Our findings identify a human disease caused by defective function of a member of the SCUBE family, and link SCUBE3 to processes controlling growth, morphogenesis, and bone and teeth development through modulation of BMP signaling.

Original language	English
Pages (from-to)	115-133
Number of pages	19
Journal	American Journal of Human Genetics
Volume	108
Issue number	1
DOIs	https://doi.org/10.1016/j.ajhg.2020.11.015
Publication status	Published - Jan 7 2021

Keywords

BMP
BMP receptors
bone morphogenetic protein
genomic sequencing
intracellular signaling
mechanism of disease
morphogenesis
SCUBE
skeletal development

ASJC Scopus subject areas

Genetics
Genetics(clinical)

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.ajhg.2020.11.015

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@article{d75c6db9957b4558ae9aee55bb3b5599,

title = "SCUBE3 loss-of-function causes a recognizable recessive developmental disorder due to defective bone morphogenetic protein signaling",

abstract = "Signal peptide-CUB-EGF domain-containing protein 3 (SCUBE3) is a member of a small family of multifunctional cell surface-anchored glycoproteins functioning as co-receptors for a variety of growth factors. Here we report that bi-allelic inactivating variants in SCUBE3 have pleiotropic consequences on development and cause a previously unrecognized syndromic disorder. Eighteen affected individuals from nine unrelated families showed a consistent phenotype characterized by reduced growth, skeletal features, distinctive craniofacial appearance, and dental anomalies. In vitro functional validation studies demonstrated a variable impact of disease-causing variants on transcript processing, protein secretion and function, and their dysregulating effect on bone morphogenetic protein (BMP) signaling. We show that SCUBE3 acts as a BMP2/BMP4 co-receptor, recruits the BMP receptor complexes into raft microdomains, and positively modulates signaling possibly by augmenting the specific interactions between BMPs and BMP type I receptors. Scube3−/− mice showed craniofacial and dental defects, reduced body size, and defective endochondral bone growth due to impaired BMP-mediated chondrogenesis and osteogenesis, recapitulating the human disorder. Our findings identify a human disease caused by defective function of a member of the SCUBE family, and link SCUBE3 to processes controlling growth, morphogenesis, and bone and teeth development through modulation of BMP signaling.",

keywords = "BMP, BMP receptors, bone morphogenetic protein, genomic sequencing, intracellular signaling, mechanism of disease, morphogenesis, SCUBE, skeletal development",

author = "{Genomics England Research Consortium} and Lin, {Yuh Charn} and Marcello Niceta and Valentina Muto and Barbara Vona and Pagnamenta, {Alistair T.} and Reza Maroofian and Christian Beetz and {van Duyvenvoorde}, Hermine and Dentici, {Maria Lisa} and Peter Lauffer and Sadeq Vallian and Andrea Ciolfi and Simone Pizzi and Peter Bauer and Gr{\"u}ning, {Nana Maria} and Emanuele Bellacchio and {Del Fattore}, Andrea and Stefania Petrini and Ranad Shaheen and Dov Tiosano and Rana Halloun and Ben Pode-Shakked and Albayrak, {Hatice Mutlu} and Emreg{\"u}l I{\c s}ık and Wit, {Jan M.} and Marcus Dittrich and Freire, {Bruna L.} and Bertola, {Debora R.} and Jorge, {Alexander A.L.} and Ortal Barel and Sabir, {Ataf H.} and {Al Tenaiji}, {Amal M.J.} and Taji, {Sulaima M.} and Nouriya Al-Sannaa and Hind Al-Abdulwahed and Digilio, {Maria Cristina} and Melita Irving and Yair Anikster and Bhavani, {Gandham S.L.} and Girisha, {Katta M.} and Thomas Haaf and Taylor, {Jenny C.} and Bruno Dallapiccola and Alkuraya, {Fowzan S.} and Yang, {Ruey Bing} and Marco Tartaglia",

note = "Funding Information: The authors wish to thank the participating families and Drs. R.A.J. Nievelstein (University Medical Center Utrecht) and D. Barbuti (Ospedale Pediatrico Bambino Ges{\`u}) for radiological advice. The authors would also thank Prof. Kassim Javaid and other members of musculoskeletal GeCIP (Genomics England). This research used data and findings generated by the 100,000 Genomes Project. This work was supported by grants from: Fondazione Bambino Ges{\`u} (Vite Coraggiose to M.T.) and Italian Ministry of Health ( CCR-2017-23669081 to M.T., Ricerca Corrente 2019 to M.N., and Ricerca Corrente 2019 and 2020 to M.L.D.), Academia Sinica and Ministry of Science and Technology of Taiwan ( 109-3111-Y-001-001 , 109-2320-B-001-012-MY3 , 107-3111-Y-001-048 , 107-0210-01-19-01 , 107-2320-B-001-015-MY3 , 106-2320-B-001-017-MY3 , 106-0210-01-15-02 to R.-B.Y. and 107-2321-B-001-036-MY3 to Y.-C.L.), S{\~a}o Paulo Research Foundation ( FAPESP 2013/03236-5 to A.A.L.J. and 2018/10893-6 to B.L.F.), University of T{\"u}bingen Intramural Funding ( fort{\"u}ne 2545-1-0 to B.V.), Ministry of Science, Research and Art Baden-W{\"u}rttemberg (to B.V.), and Department of Science and Technology, Government of India ( SB/SO/HS/005/2014 to K.M.G.). The 100,000 Genomes Project is funded by the National Institute for Health Research and NHS England. The 100,000 Genomes Project is managed by Genomics England Limited and uses data provided by patients and collected by the National Health Service as part of their care and support. See supplemental information for consortium details. Additional support was from the Wellcome Trust ( 203141/Z/16/Z ) and the NIHR Biomedical Research Centre Oxford (to A.T.P. and J.C.T.). Funding Information: The authors wish to thank the participating families and Drs. R.A.J. Nievelstein (University Medical Center Utrecht) and D. Barbuti (Ospedale Pediatrico Bambino Ges?) for radiological advice. The authors would also thank Prof. Kassim Javaid and other members of musculoskeletal GeCIP (Genomics England). This research used data and findings generated by the 100,000 Genomes Project. This work was supported by grants from: Fondazione Bambino Ges? (Vite Coraggiose to M.T.) and Italian Ministry of Health (CCR-2017-23669081 to M.T. Ricerca Corrente 2019 to M.N. and Ricerca Corrente 2019 and 2020 to M.L.D.), Academia Sinica and Ministry of Science and Technology of Taiwan (109-3111-Y-001-001, 109-2320-B-001-012-MY3, 107-3111-Y-001-048, 107-0210-01-19-01, 107-2320-B-001-015-MY3, 106-2320-B-001-017-MY3, 106-0210-01-15-02 to R.-B.Y. and 107-2321-B-001-036-MY3 to Y.-C.L.), S?o Paulo Research Foundation (FAPESP 2013/03236-5 to A.A.L.J. and 2018/10893-6 to B.L.F.), University of T?bingen Intramural Funding (fort?ne 2545-1-0 to B.V.), Ministry of Science, Research and Art Baden-W?rttemberg (to B.V.), and Department of Science and Technology, Government of India (SB/SO/HS/005/2014 to K.M.G.). The 100,000 Genomes Project is funded by the National Institute for Health Research and NHS England. The 100,000 Genomes Project is managed by Genomics England Limited and uses data provided by patients and collected by the National Health Service as part of their care and support. See supplemental information for consortium details. Additional support was from the Wellcome Trust (203141/Z/16/Z) and the NIHR Biomedical Research Centre Oxford (to A.T.P. and J.C.T.). Publisher Copyright: {\textcopyright} 2020 American Society of Human Genetics",

year = "2021",

month = jan,

day = "7",

doi = "10.1016/j.ajhg.2020.11.015",

language = "English",

volume = "108",

pages = "115--133",

journal = "American Journal of Human Genetics",

issn = "0002-9297",

publisher = "Cell Press",

number = "1",

}

TY - JOUR

T1 - SCUBE3 loss-of-function causes a recognizable recessive developmental disorder due to defective bone morphogenetic protein signaling

AU - Genomics England Research Consortium

AU - Lin, Yuh Charn

AU - Niceta, Marcello

AU - Muto, Valentina

AU - Vona, Barbara

AU - Pagnamenta, Alistair T.

AU - Maroofian, Reza

AU - Beetz, Christian

AU - van Duyvenvoorde, Hermine

AU - Dentici, Maria Lisa

AU - Lauffer, Peter

AU - Vallian, Sadeq

AU - Ciolfi, Andrea

AU - Pizzi, Simone

AU - Bauer, Peter

AU - Grüning, Nana Maria

AU - Bellacchio, Emanuele

AU - Del Fattore, Andrea

AU - Petrini, Stefania

AU - Shaheen, Ranad

AU - Tiosano, Dov

AU - Halloun, Rana

AU - Pode-Shakked, Ben

AU - Albayrak, Hatice Mutlu

AU - Işık, Emregül

AU - Wit, Jan M.

AU - Dittrich, Marcus

AU - Freire, Bruna L.

AU - Bertola, Debora R.

AU - Jorge, Alexander A.L.

AU - Barel, Ortal

AU - Sabir, Ataf H.

AU - Al Tenaiji, Amal M.J.

AU - Taji, Sulaima M.

AU - Al-Sannaa, Nouriya

AU - Al-Abdulwahed, Hind

AU - Digilio, Maria Cristina

AU - Irving, Melita

AU - Anikster, Yair

AU - Bhavani, Gandham S.L.

AU - Girisha, Katta M.

AU - Haaf, Thomas

AU - Taylor, Jenny C.

AU - Dallapiccola, Bruno

AU - Alkuraya, Fowzan S.

AU - Yang, Ruey Bing

AU - Tartaglia, Marco

N1 - Funding Information: The authors wish to thank the participating families and Drs. R.A.J. Nievelstein (University Medical Center Utrecht) and D. Barbuti (Ospedale Pediatrico Bambino Gesù) for radiological advice. The authors would also thank Prof. Kassim Javaid and other members of musculoskeletal GeCIP (Genomics England). This research used data and findings generated by the 100,000 Genomes Project. This work was supported by grants from: Fondazione Bambino Gesù (Vite Coraggiose to M.T.) and Italian Ministry of Health ( CCR-2017-23669081 to M.T., Ricerca Corrente 2019 to M.N., and Ricerca Corrente 2019 and 2020 to M.L.D.), Academia Sinica and Ministry of Science and Technology of Taiwan ( 109-3111-Y-001-001 , 109-2320-B-001-012-MY3 , 107-3111-Y-001-048 , 107-0210-01-19-01 , 107-2320-B-001-015-MY3 , 106-2320-B-001-017-MY3 , 106-0210-01-15-02 to R.-B.Y. and 107-2321-B-001-036-MY3 to Y.-C.L.), São Paulo Research Foundation ( FAPESP 2013/03236-5 to A.A.L.J. and 2018/10893-6 to B.L.F.), University of Tübingen Intramural Funding ( fortüne 2545-1-0 to B.V.), Ministry of Science, Research and Art Baden-Württemberg (to B.V.), and Department of Science and Technology, Government of India ( SB/SO/HS/005/2014 to K.M.G.). The 100,000 Genomes Project is funded by the National Institute for Health Research and NHS England. The 100,000 Genomes Project is managed by Genomics England Limited and uses data provided by patients and collected by the National Health Service as part of their care and support. See supplemental information for consortium details. Additional support was from the Wellcome Trust ( 203141/Z/16/Z ) and the NIHR Biomedical Research Centre Oxford (to A.T.P. and J.C.T.). Funding Information: The authors wish to thank the participating families and Drs. R.A.J. Nievelstein (University Medical Center Utrecht) and D. Barbuti (Ospedale Pediatrico Bambino Ges?) for radiological advice. The authors would also thank Prof. Kassim Javaid and other members of musculoskeletal GeCIP (Genomics England). This research used data and findings generated by the 100,000 Genomes Project. This work was supported by grants from: Fondazione Bambino Ges? (Vite Coraggiose to M.T.) and Italian Ministry of Health (CCR-2017-23669081 to M.T. Ricerca Corrente 2019 to M.N. and Ricerca Corrente 2019 and 2020 to M.L.D.), Academia Sinica and Ministry of Science and Technology of Taiwan (109-3111-Y-001-001, 109-2320-B-001-012-MY3, 107-3111-Y-001-048, 107-0210-01-19-01, 107-2320-B-001-015-MY3, 106-2320-B-001-017-MY3, 106-0210-01-15-02 to R.-B.Y. and 107-2321-B-001-036-MY3 to Y.-C.L.), S?o Paulo Research Foundation (FAPESP 2013/03236-5 to A.A.L.J. and 2018/10893-6 to B.L.F.), University of T?bingen Intramural Funding (fort?ne 2545-1-0 to B.V.), Ministry of Science, Research and Art Baden-W?rttemberg (to B.V.), and Department of Science and Technology, Government of India (SB/SO/HS/005/2014 to K.M.G.). The 100,000 Genomes Project is funded by the National Institute for Health Research and NHS England. The 100,000 Genomes Project is managed by Genomics England Limited and uses data provided by patients and collected by the National Health Service as part of their care and support. See supplemental information for consortium details. Additional support was from the Wellcome Trust (203141/Z/16/Z) and the NIHR Biomedical Research Centre Oxford (to A.T.P. and J.C.T.). Publisher Copyright: © 2020 American Society of Human Genetics

PY - 2021/1/7

Y1 - 2021/1/7

N2 - Signal peptide-CUB-EGF domain-containing protein 3 (SCUBE3) is a member of a small family of multifunctional cell surface-anchored glycoproteins functioning as co-receptors for a variety of growth factors. Here we report that bi-allelic inactivating variants in SCUBE3 have pleiotropic consequences on development and cause a previously unrecognized syndromic disorder. Eighteen affected individuals from nine unrelated families showed a consistent phenotype characterized by reduced growth, skeletal features, distinctive craniofacial appearance, and dental anomalies. In vitro functional validation studies demonstrated a variable impact of disease-causing variants on transcript processing, protein secretion and function, and their dysregulating effect on bone morphogenetic protein (BMP) signaling. We show that SCUBE3 acts as a BMP2/BMP4 co-receptor, recruits the BMP receptor complexes into raft microdomains, and positively modulates signaling possibly by augmenting the specific interactions between BMPs and BMP type I receptors. Scube3−/− mice showed craniofacial and dental defects, reduced body size, and defective endochondral bone growth due to impaired BMP-mediated chondrogenesis and osteogenesis, recapitulating the human disorder. Our findings identify a human disease caused by defective function of a member of the SCUBE family, and link SCUBE3 to processes controlling growth, morphogenesis, and bone and teeth development through modulation of BMP signaling.

AB - Signal peptide-CUB-EGF domain-containing protein 3 (SCUBE3) is a member of a small family of multifunctional cell surface-anchored glycoproteins functioning as co-receptors for a variety of growth factors. Here we report that bi-allelic inactivating variants in SCUBE3 have pleiotropic consequences on development and cause a previously unrecognized syndromic disorder. Eighteen affected individuals from nine unrelated families showed a consistent phenotype characterized by reduced growth, skeletal features, distinctive craniofacial appearance, and dental anomalies. In vitro functional validation studies demonstrated a variable impact of disease-causing variants on transcript processing, protein secretion and function, and their dysregulating effect on bone morphogenetic protein (BMP) signaling. We show that SCUBE3 acts as a BMP2/BMP4 co-receptor, recruits the BMP receptor complexes into raft microdomains, and positively modulates signaling possibly by augmenting the specific interactions between BMPs and BMP type I receptors. Scube3−/− mice showed craniofacial and dental defects, reduced body size, and defective endochondral bone growth due to impaired BMP-mediated chondrogenesis and osteogenesis, recapitulating the human disorder. Our findings identify a human disease caused by defective function of a member of the SCUBE family, and link SCUBE3 to processes controlling growth, morphogenesis, and bone and teeth development through modulation of BMP signaling.

KW - BMP

KW - BMP receptors

KW - bone morphogenetic protein

KW - genomic sequencing

KW - intracellular signaling

KW - mechanism of disease

KW - morphogenesis

KW - SCUBE

KW - skeletal development

UR - http://www.scopus.com/inward/record.url?scp=85098151529&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85098151529&partnerID=8YFLogxK

U2 - 10.1016/j.ajhg.2020.11.015

DO - 10.1016/j.ajhg.2020.11.015

M3 - Article

C2 - 33308444

AN - SCOPUS:85098151529

SN - 0002-9297

VL - 108

SP - 115

EP - 133

JO - American Journal of Human Genetics

JF - American Journal of Human Genetics

IS - 1

ER -

SCUBE3 loss-of-function causes a recognizable recessive developmental disorder due to defective bone morphogenetic protein signaling

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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