Heterozygous loss-of-function variants significantly expand the phenotypes associated with loss of GDF11

Undiagnosed Diseases Network

doi:10.1038/s41436-021-01216-8

Heterozygous loss-of-function variants significantly expand the phenotypes associated with loss of GDF11

Undiagnosed Diseases Network

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

Abstract

Purpose: Growth differentiation factor 11 (GDF11) is a key signaling protein required for proper development of many organ systems. Only one prior study has associated an inherited GDF11 variant with a dominant human disease in a family with variable craniofacial and vertebral abnormalities. Here, we expand the phenotypic spectrum associated with GDF11 variants and document the nature of the variants. Methods: We present a cohort of six probands with de novo and inherited nonsense/frameshift (4/6 patients) and missense (2/6) variants in GDF11. We generated gdf11 mutant zebrafish to model loss of gdf11 phenotypes and used an overexpression screen in Drosophila to test variant functionality. Results: Patients with variants in GDF11 presented with craniofacial (5/6), vertebral (5/6), neurological (6/6), visual (4/6), cardiac (3/6), auditory (3/6), and connective tissue abnormalities (3/6). gdf11 mutant zebrafish show craniofacial abnormalities and body segmentation defects that match some patient phenotypes. Expression of the patients’ variants in the fly showed that one nonsense variant in GDF11 is a severe loss-of-function (LOF) allele whereas the missense variants in our cohort are partial LOF variants. Conclusion: GDF11 is needed for human development, particularly neuronal development, and LOF GDF11 alleles can affect the development of numerous organs and tissues.

Original language	English (US)
Pages (from-to)	1889-1900
Number of pages	12
Journal	Genetics in Medicine
Volume	23
Issue number	10
DOIs	https://doi.org/10.1038/s41436-021-01216-8
State	Published - Oct 2021

ASJC Scopus subject areas

Genetics(clinical)

Access to Document

10.1038/s41436-021-01216-8

Cite this

@article{83b56d9733b540a69b70d1c9e40637e9,

title = "Heterozygous loss-of-function variants significantly expand the phenotypes associated with loss of GDF11",

abstract = "Purpose: Growth differentiation factor 11 (GDF11) is a key signaling protein required for proper development of many organ systems. Only one prior study has associated an inherited GDF11 variant with a dominant human disease in a family with variable craniofacial and vertebral abnormalities. Here, we expand the phenotypic spectrum associated with GDF11 variants and document the nature of the variants. Methods: We present a cohort of six probands with de novo and inherited nonsense/frameshift (4/6 patients) and missense (2/6) variants in GDF11. We generated gdf11 mutant zebrafish to model loss of gdf11 phenotypes and used an overexpression screen in Drosophila to test variant functionality. Results: Patients with variants in GDF11 presented with craniofacial (5/6), vertebral (5/6), neurological (6/6), visual (4/6), cardiac (3/6), auditory (3/6), and connective tissue abnormalities (3/6). gdf11 mutant zebrafish show craniofacial abnormalities and body segmentation defects that match some patient phenotypes. Expression of the patients{\textquoteright} variants in the fly showed that one nonsense variant in GDF11 is a severe loss-of-function (LOF) allele whereas the missense variants in our cohort are partial LOF variants. Conclusion: GDF11 is needed for human development, particularly neuronal development, and LOF GDF11 alleles can affect the development of numerous organs and tissues.",

author = "{Undiagnosed Diseases Network} and Ravenscroft, {Thomas A.} and Phillips, {Jennifer B.} and Elizabeth Fieg and Bajikar, {Sameer S.} and Judy Peirce and Jeremy Wegner and Luna, {Alia A.} and Fox, {Eric J.} and Yan, {Yi Lin} and Rosenfeld, {Jill A.} and Jonathan Zirin and Oguz Kanca and Acosta, {Maria T.} and Margaret Adam and Adams, {David R.} and Agrawal, {Pankaj B.} and Alejandro, {Mercedes E.} and Justin Alvey and Laura Amendola and Ashley Andrews and Ashley, {Euan A.} and Azamian, {Mahshid S.} and Bacino, {Carlos A.} and Guney Bademci and Eva Baker and Ashok Balasubramanya and Dustin Baldridge and Jim Bale and Michael Bamshad and Deborah Barbouth and Pinar Bayrak-Toydemir and Anita Beck and Beggs, {Alan H.} and Edward Behrens and Gill Bejerano and Jimmy Bennet and Beverly Berg-Rood and Bernstein, {Jonathan A.} and Berry, {Gerard T.} and Anna Bican and Stephanie Bivona and Elizabeth Blue and John Bohnsack and Carsten Bonnenmann and Devon Bonner and Surendra Dasari and Lanpher, {Brendan C.} and Lanza, {Ian R.} and Eva Morava and Devin Oglesbee",

note = "Publisher Copyright: {\textcopyright} 2021, The Author(s), under exclusive licence to the American College of Medical Genetics and Genomics.",

year = "2021",

month = oct,

doi = "10.1038/s41436-021-01216-8",

language = "English (US)",

volume = "23",

pages = "1889--1900",

journal = "Genetics in Medicine",

issn = "1098-3600",

publisher = "Lippincott Williams and Wilkins",

number = "10",

}

TY - JOUR

T1 - Heterozygous loss-of-function variants significantly expand the phenotypes associated with loss of GDF11

AU - Undiagnosed Diseases Network

AU - Ravenscroft, Thomas A.

AU - Phillips, Jennifer B.

AU - Fieg, Elizabeth

AU - Bajikar, Sameer S.

AU - Peirce, Judy

AU - Wegner, Jeremy

AU - Luna, Alia A.

AU - Fox, Eric J.

AU - Yan, Yi Lin

AU - Rosenfeld, Jill A.

AU - Zirin, Jonathan

AU - Kanca, Oguz

AU - Acosta, Maria T.

AU - Adam, Margaret

AU - Adams, David R.

AU - Agrawal, Pankaj B.

AU - Alejandro, Mercedes E.

AU - Alvey, Justin

AU - Amendola, Laura

AU - Andrews, Ashley

AU - Ashley, Euan A.

AU - Azamian, Mahshid S.

AU - Bacino, Carlos A.

AU - Bademci, Guney

AU - Baker, Eva

AU - Balasubramanya, Ashok

AU - Baldridge, Dustin

AU - Bale, Jim

AU - Bamshad, Michael

AU - Barbouth, Deborah

AU - Bayrak-Toydemir, Pinar

AU - Beck, Anita

AU - Beggs, Alan H.

AU - Behrens, Edward

AU - Bejerano, Gill

AU - Bennet, Jimmy

AU - Berg-Rood, Beverly

AU - Bernstein, Jonathan A.

AU - Berry, Gerard T.

AU - Bican, Anna

AU - Bivona, Stephanie

AU - Blue, Elizabeth

AU - Bohnsack, John

AU - Bonnenmann, Carsten

AU - Bonner, Devon

AU - Dasari, Surendra

AU - Lanpher, Brendan C.

AU - Lanza, Ian R.

AU - Morava, Eva

AU - Oglesbee, Devin

PY - 2021/10

Y1 - 2021/10

N2 - Purpose: Growth differentiation factor 11 (GDF11) is a key signaling protein required for proper development of many organ systems. Only one prior study has associated an inherited GDF11 variant with a dominant human disease in a family with variable craniofacial and vertebral abnormalities. Here, we expand the phenotypic spectrum associated with GDF11 variants and document the nature of the variants. Methods: We present a cohort of six probands with de novo and inherited nonsense/frameshift (4/6 patients) and missense (2/6) variants in GDF11. We generated gdf11 mutant zebrafish to model loss of gdf11 phenotypes and used an overexpression screen in Drosophila to test variant functionality. Results: Patients with variants in GDF11 presented with craniofacial (5/6), vertebral (5/6), neurological (6/6), visual (4/6), cardiac (3/6), auditory (3/6), and connective tissue abnormalities (3/6). gdf11 mutant zebrafish show craniofacial abnormalities and body segmentation defects that match some patient phenotypes. Expression of the patients’ variants in the fly showed that one nonsense variant in GDF11 is a severe loss-of-function (LOF) allele whereas the missense variants in our cohort are partial LOF variants. Conclusion: GDF11 is needed for human development, particularly neuronal development, and LOF GDF11 alleles can affect the development of numerous organs and tissues.

AB - Purpose: Growth differentiation factor 11 (GDF11) is a key signaling protein required for proper development of many organ systems. Only one prior study has associated an inherited GDF11 variant with a dominant human disease in a family with variable craniofacial and vertebral abnormalities. Here, we expand the phenotypic spectrum associated with GDF11 variants and document the nature of the variants. Methods: We present a cohort of six probands with de novo and inherited nonsense/frameshift (4/6 patients) and missense (2/6) variants in GDF11. We generated gdf11 mutant zebrafish to model loss of gdf11 phenotypes and used an overexpression screen in Drosophila to test variant functionality. Results: Patients with variants in GDF11 presented with craniofacial (5/6), vertebral (5/6), neurological (6/6), visual (4/6), cardiac (3/6), auditory (3/6), and connective tissue abnormalities (3/6). gdf11 mutant zebrafish show craniofacial abnormalities and body segmentation defects that match some patient phenotypes. Expression of the patients’ variants in the fly showed that one nonsense variant in GDF11 is a severe loss-of-function (LOF) allele whereas the missense variants in our cohort are partial LOF variants. Conclusion: GDF11 is needed for human development, particularly neuronal development, and LOF GDF11 alleles can affect the development of numerous organs and tissues.

UR - http://www.scopus.com/inward/record.url?scp=85107767922&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85107767922&partnerID=8YFLogxK

U2 - 10.1038/s41436-021-01216-8

DO - 10.1038/s41436-021-01216-8

M3 - Article

C2 - 34113007

AN - SCOPUS:85107767922

SN - 1098-3600

VL - 23

SP - 1889

EP - 1900

JO - Genetics in Medicine

JF - Genetics in Medicine

IS - 10

ER -

Heterozygous loss-of-function variants significantly expand the phenotypes associated with loss of GDF11

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this