FOXI3 pathogenic variants cause one form of craniofacial microsomia

Ke Mao; Christelle Borel; Muhammad Ansar; Angad Jolly; Periklis Makrythanasis; Christine Froehlich; Justyna Iwaszkiewicz; Bingqing Wang; Xiaopeng Xu; Qiang Li; Xavier Blanc; Hao Zhu; Qi Chen; Fujun Jin; Harinarayana Ankamreddy; Sunita Singh; Hongyuan Zhang; Xiaogang Wang; Peiwei Chen; Emmanuelle Ranza; Sohail Aziz Paracha; Syed Fahim Shah; Valentina Guida; Francesca Piceci-Sparascio; Daniela Melis; Bruno Dallapiccola; Maria Cristina Digilio; Antonio Novelli; Monia Magliozzi; Maria Teresa Fadda; Haley Streff; Keren Machol; Richard A. Lewis; Vincent Zoete; Gabriella Maria Squeo; Paolo Prontera; Giorgia Mancano; Giulia Gori; Milena Mariani; Angelo Selicorni; Stavroula Psoni; Helen Fryssira; Sofia Douzgou; Sandrine Marlin; Saskia Biskup; Alessandro De Luca; Giuseppe Merla; Shouqin Zhao; Timothy C. Cox; Andrew K. Groves; James R. Lupski; Qingguo Zhang; Yong Biao Zhang; Stylianos E. Antonarakis

doi:10.1038/s41467-023-37703-6

FOXI3 pathogenic variants cause one form of craniofacial microsomia

Ke Mao
, Christelle Borel
, Muhammad Ansar
, Angad Jolly
, Periklis Makrythanasis
, Christine Froehlich
, Justyna Iwaszkiewicz
, Bingqing Wang
, Xiaopeng Xu
, Qiang Li
, Xavier Blanc
, Hao Zhu
, Qi Chen
, Fujun Jin
, Harinarayana Ankamreddy
, Sunita Singh
, Hongyuan Zhang
, Xiaogang Wang
, Peiwei Chen
, Emmanuelle Ranza

Sohail Aziz Paracha, Syed Fahim Shah, Valentina Guida, Francesca Piceci-Sparascio, Daniela Melis, Bruno Dallapiccola, Maria Cristina Digilio, Antonio Novelli, Monia Magliozzi, Maria Teresa Fadda, Haley Streff, Keren Machol, Richard A. Lewis, Vincent Zoete, Gabriella Maria Squeo, Paolo Prontera, Giorgia Mancano, Giulia Gori, Milena Mariani, Angelo Selicorni, Stavroula Psoni, Helen Fryssira, Sofia Douzgou, Sandrine Marlin, Saskia Biskup, Alessandro De Luca, Giuseppe Merla, Shouqin Zhao, Timothy C. Cox, Andrew K. Groves, James R. Lupski, Qingguo Zhang^*, Yong Biao Zhang^*, Stylianos E. Antonarakis^*

^*此作品的通讯作者

Beihang University
University of Geneva
University of Lausanne
Baylor College of Medicine
National and Kapodistrian University of Athens
Academy of Athens
CeGaT GmbH
Swiss Institute of Bioinformatics
Chinese Academy of Medical Sciences
Xuzhou Medical University
Medigenome
SRM Institute of Science and Technology
Capital Medical University
Khyber Medical University
DHQ Hospital KDA
IRCCS Ospedale Casa Sollievo della Sofferenza - San Giovanni Rotondo (FG)
University of Salerno
IRCCS Ospedale pediatrico Bambino Gesù - Roma
Policlinico Umberto I
University Hospital of Perugia
Meyer Children’s University Hospital
ASST Lariana
University of Manchester
University of Bergen
Université Paris Cité
University of Naples Federico II
University of Missouri at Kansas City
iGE3 Institute of Genetics and Genomes in Geneva

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31 引用（Scopus）

摘要

Craniofacial microsomia (CFM; also known as Goldenhar syndrome), is a craniofacial developmental disorder of variable expressivity and severity with a recognizable set of abnormalities. These birth defects are associated with structures derived from the first and second pharyngeal arches, can occur unilaterally and include ear dysplasia, microtia, preauricular tags and pits, facial asymmetry and other malformations. The inheritance pattern is controversial, and the molecular etiology of this syndrome is largely unknown. A total of 670 patients belonging to unrelated pedigrees with European and Chinese ancestry with CFM, are investigated. We identify 18 likely pathogenic variants in 21 probands (3.1%) in FOXI3. Biochemical experiments on transcriptional activity and subcellular localization of the likely pathogenic FOXI3 variants, and knock-in mouse studies strongly support the involvement of FOXI3 in CFM. Our findings indicate autosomal dominant inheritance with reduced penetrance, and/or autosomal recessive inheritance. The phenotypic expression of the FOXI3 variants is variable. The penetrance of the likely pathogenic variants in the seemingly dominant form is reduced, since a considerable number of such variants in affected individuals were inherited from non-affected parents. Here we provide suggestive evidence that common variation in the FOXI3 allele in trans with the pathogenic variant could modify the phenotypic severity and accounts for the incomplete penetrance.

源语言	英语
文章编号	2026
期刊	Nature Communications
卷	14
期	1
DOI	https://doi.org/10.1038/s41467-023-37703-6
出版状态	已出版 - 12月 2023

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Mao, K., Borel, C., Ansar, M., Jolly, A., Makrythanasis, P., Froehlich, C., Iwaszkiewicz, J., Wang, B., Xu, X., Li, Q., Blanc, X., Zhu, H., Chen, Q., Jin, F., Ankamreddy, H., Singh, S., Zhang, H., Wang, X., Chen, P., ... Antonarakis, S. E. (2023). FOXI3 pathogenic variants cause one form of craniofacial microsomia. Nature Communications, 14(1), 文章 2026. https://doi.org/10.1038/s41467-023-37703-6

@article{57054541249c4689aeb86e8eb0cccb3a,

title = "FOXI3 pathogenic variants cause one form of craniofacial microsomia",

abstract = "Craniofacial microsomia (CFM; also known as Goldenhar syndrome), is a craniofacial developmental disorder of variable expressivity and severity with a recognizable set of abnormalities. These birth defects are associated with structures derived from the first and second pharyngeal arches, can occur unilaterally and include ear dysplasia, microtia, preauricular tags and pits, facial asymmetry and other malformations. The inheritance pattern is controversial, and the molecular etiology of this syndrome is largely unknown. A total of 670 patients belonging to unrelated pedigrees with European and Chinese ancestry with CFM, are investigated. We identify 18 likely pathogenic variants in 21 probands (3.1\%) in FOXI3. Biochemical experiments on transcriptional activity and subcellular localization of the likely pathogenic FOXI3 variants, and knock-in mouse studies strongly support the involvement of FOXI3 in CFM. Our findings indicate autosomal dominant inheritance with reduced penetrance, and/or autosomal recessive inheritance. The phenotypic expression of the FOXI3 variants is variable. The penetrance of the likely pathogenic variants in the seemingly dominant form is reduced, since a considerable number of such variants in affected individuals were inherited from non-affected parents. Here we provide suggestive evidence that common variation in the FOXI3 allele in trans with the pathogenic variant could modify the phenotypic severity and accounts for the incomplete penetrance.",

author = "Ke Mao and Christelle Borel and Muhammad Ansar and Angad Jolly and Periklis Makrythanasis and Christine Froehlich and Justyna Iwaszkiewicz and Bingqing Wang and Xiaopeng Xu and Qiang Li and Xavier Blanc and Hao Zhu and Qi Chen and Fujun Jin and Harinarayana Ankamreddy and Sunita Singh and Hongyuan Zhang and Xiaogang Wang and Peiwei Chen and Emmanuelle Ranza and Paracha, \{Sohail Aziz\} and Shah, \{Syed Fahim\} and Valentina Guida and Francesca Piceci-Sparascio and Daniela Melis and Bruno Dallapiccola and Digilio, \{Maria Cristina\} and Antonio Novelli and Monia Magliozzi and Fadda, \{Maria Teresa\} and Haley Streff and Keren Machol and Lewis, \{Richard A.\} and Vincent Zoete and Squeo, \{Gabriella Maria\} and Paolo Prontera and Giorgia Mancano and Giulia Gori and Milena Mariani and Angelo Selicorni and Stavroula Psoni and Helen Fryssira and Sofia Douzgou and Sandrine Marlin and Saskia Biskup and \{De Luca\}, Alessandro and Giuseppe Merla and Shouqin Zhao and Cox, \{Timothy C.\} and Groves, \{Andrew K.\} and Lupski, \{James R.\} and Qingguo Zhang and Zhang, \{Yong Biao\} and Antonarakis, \{Stylianos E.\}",

note = "Publisher Copyright: {\textcopyright} 2023, The Author(s).",

year = "2023",

month = dec,

doi = "10.1038/s41467-023-37703-6",

language = "英语",

volume = "14",

journal = "Nature Communications",

issn = "2041-1723",

publisher = "Nature Research",

number = "1",

}

Mao, K, Borel, C, Ansar, M, Jolly, A, Makrythanasis, P, Froehlich, C, Iwaszkiewicz, J, Wang, B, Xu, X, Li, Q, Blanc, X, Zhu, H, Chen, Q, Jin, F, Ankamreddy, H, Singh, S, Zhang, H, Wang, X, Chen, P, Ranza, E, Paracha, SA, Shah, SF, Guida, V, Piceci-Sparascio, F, Melis, D, Dallapiccola, B, Digilio, MC, Novelli, A, Magliozzi, M, Fadda, MT, Streff, H, Machol, K, Lewis, RA, Zoete, V, Squeo, GM, Prontera, P, Mancano, G, Gori, G, Mariani, M, Selicorni, A, Psoni, S, Fryssira, H, Douzgou, S, Marlin, S, Biskup, S, De Luca, A, Merla, G, Zhao, S, Cox, TC, Groves, AK, Lupski, JR, Zhang, Q, Zhang, YB & Antonarakis, SE 2023, 'FOXI3 pathogenic variants cause one form of craniofacial microsomia', Nature Communications, 卷 14, 号码 1, 2026. https://doi.org/10.1038/s41467-023-37703-6

TY - JOUR

T1 - FOXI3 pathogenic variants cause one form of craniofacial microsomia

AU - Mao, Ke

AU - Borel, Christelle

AU - Ansar, Muhammad

AU - Jolly, Angad

AU - Makrythanasis, Periklis

AU - Froehlich, Christine

AU - Iwaszkiewicz, Justyna

AU - Wang, Bingqing

AU - Xu, Xiaopeng

AU - Li, Qiang

AU - Blanc, Xavier

AU - Zhu, Hao

AU - Chen, Qi

AU - Jin, Fujun

AU - Ankamreddy, Harinarayana

AU - Singh, Sunita

AU - Zhang, Hongyuan

AU - Wang, Xiaogang

AU - Chen, Peiwei

AU - Ranza, Emmanuelle

AU - Paracha, Sohail Aziz

AU - Shah, Syed Fahim

AU - Guida, Valentina

AU - Piceci-Sparascio, Francesca

AU - Melis, Daniela

AU - Dallapiccola, Bruno

AU - Digilio, Maria Cristina

AU - Novelli, Antonio

AU - Magliozzi, Monia

AU - Fadda, Maria Teresa

AU - Streff, Haley

AU - Machol, Keren

AU - Lewis, Richard A.

AU - Zoete, Vincent

AU - Squeo, Gabriella Maria

AU - Prontera, Paolo

AU - Mancano, Giorgia

AU - Gori, Giulia

AU - Mariani, Milena

AU - Selicorni, Angelo

AU - Psoni, Stavroula

AU - Fryssira, Helen

AU - Douzgou, Sofia

AU - Marlin, Sandrine

AU - Biskup, Saskia

AU - De Luca, Alessandro

AU - Merla, Giuseppe

AU - Zhao, Shouqin

AU - Cox, Timothy C.

AU - Groves, Andrew K.

AU - Lupski, James R.

AU - Zhang, Qingguo

AU - Zhang, Yong Biao

AU - Antonarakis, Stylianos E.

PY - 2023/12

Y1 - 2023/12

N2 - Craniofacial microsomia (CFM; also known as Goldenhar syndrome), is a craniofacial developmental disorder of variable expressivity and severity with a recognizable set of abnormalities. These birth defects are associated with structures derived from the first and second pharyngeal arches, can occur unilaterally and include ear dysplasia, microtia, preauricular tags and pits, facial asymmetry and other malformations. The inheritance pattern is controversial, and the molecular etiology of this syndrome is largely unknown. A total of 670 patients belonging to unrelated pedigrees with European and Chinese ancestry with CFM, are investigated. We identify 18 likely pathogenic variants in 21 probands (3.1%) in FOXI3. Biochemical experiments on transcriptional activity and subcellular localization of the likely pathogenic FOXI3 variants, and knock-in mouse studies strongly support the involvement of FOXI3 in CFM. Our findings indicate autosomal dominant inheritance with reduced penetrance, and/or autosomal recessive inheritance. The phenotypic expression of the FOXI3 variants is variable. The penetrance of the likely pathogenic variants in the seemingly dominant form is reduced, since a considerable number of such variants in affected individuals were inherited from non-affected parents. Here we provide suggestive evidence that common variation in the FOXI3 allele in trans with the pathogenic variant could modify the phenotypic severity and accounts for the incomplete penetrance.

AB - Craniofacial microsomia (CFM; also known as Goldenhar syndrome), is a craniofacial developmental disorder of variable expressivity and severity with a recognizable set of abnormalities. These birth defects are associated with structures derived from the first and second pharyngeal arches, can occur unilaterally and include ear dysplasia, microtia, preauricular tags and pits, facial asymmetry and other malformations. The inheritance pattern is controversial, and the molecular etiology of this syndrome is largely unknown. A total of 670 patients belonging to unrelated pedigrees with European and Chinese ancestry with CFM, are investigated. We identify 18 likely pathogenic variants in 21 probands (3.1%) in FOXI3. Biochemical experiments on transcriptional activity and subcellular localization of the likely pathogenic FOXI3 variants, and knock-in mouse studies strongly support the involvement of FOXI3 in CFM. Our findings indicate autosomal dominant inheritance with reduced penetrance, and/or autosomal recessive inheritance. The phenotypic expression of the FOXI3 variants is variable. The penetrance of the likely pathogenic variants in the seemingly dominant form is reduced, since a considerable number of such variants in affected individuals were inherited from non-affected parents. Here we provide suggestive evidence that common variation in the FOXI3 allele in trans with the pathogenic variant could modify the phenotypic severity and accounts for the incomplete penetrance.

UR - https://www.scopus.com/pages/publications/85152272417

U2 - 10.1038/s41467-023-37703-6

DO - 10.1038/s41467-023-37703-6

M3 - 文章

C2 - 37041148

AN - SCOPUS:85152272417

SN - 2041-1723

VL - 14

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 2026

ER -

FOXI3 pathogenic variants cause one form of craniofacial microsomia

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