Functional interpretation of ATAD3A variants in neuro-mitochondrial phenotypes

Zheng Yie Yap; Yo Han Park; Saskia B. Wortmann; Adam C. Gunning; Shlomit Ezer; Sukyeong Lee; Lita Duraine; Ekkehard Wilichowski; Kate Wilson; Johannes A. Mayr; Matias Wagner; Hong Li; Usha Kini; Emily Davis Black; Kristin G. Monaghan; James R. Lupski; Sian Ellard; Dominik S. Westphal; Tamar Harel; Wan Hee Yoon

doi:10.1186/s13073-021-00873-3

Functional interpretation of ATAD3A variants in neuro-mitochondrial phenotypes

Zheng Yie Yap, Yo Han Park, Saskia B. Wortmann, Adam C. Gunning, Shlomit Ezer, Sukyeong Lee, Lita Duraine, Ekkehard Wilichowski, Kate Wilson, Johannes A. Mayr, Matias Wagner, Hong Li, Usha Kini, Emily Davis Black, Kristin G. Monaghan, James R. Lupski, Sian Ellard, Dominik S. Westphal, Tamar Harel, Wan Hee Yoon

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

23 Scopus citations

Abstract

Background: ATPase family AAA-domain containing protein 3A (ATAD3A) is a nuclear-encoded mitochondrial membrane-anchored protein involved in diverse processes including mitochondrial dynamics, mitochondrial DNA organization, and cholesterol metabolism. Biallelic deletions (null), recessive missense variants (hypomorph), and heterozygous missense variants or duplications (antimorph) in ATAD3A lead to neurological syndromes in humans. Methods: To expand the mutational spectrum of ATAD3A variants and to provide functional interpretation of missense alleles in trans to deletion alleles, we performed exome sequencing for identification of single nucleotide variants (SNVs) and copy number variants (CNVs) in ATAD3A in individuals with neurological and mitochondrial phenotypes. A Drosophila Atad3a Gal4 knockin-null allele was generated using CRISPR-Cas9 genome editing technology to aid the interpretation of variants. Results: We report 13 individuals from 8 unrelated families with biallelic ATAD3A variants. The variants included four missense variants inherited in trans to loss-of-function alleles (p.(Leu77Val), p.(Phe50Leu), p.(Arg170Trp), p.(Gly236Val)), a homozygous missense variant p.(Arg327Pro), and a heterozygous non-frameshift indel p.(Lys568del). Affected individuals exhibited findings previously associated with ATAD3A pathogenic variation, including developmental delay, hypotonia, congenital cataracts, hypertrophic cardiomyopathy, and cerebellar atrophy. Drosophila studies indicated that Phe50Leu, Gly236Val, Arg327Pro, and Lys568del are severe loss-of-function alleles leading to early developmental lethality. Further, we showed that Phe50Leu, Gly236Val, and Arg327Pro cause neurogenesis defects. On the contrary, Leu77Val and Arg170Trp are partial loss-of-function alleles that cause progressive locomotion defects and whose expression leads to an increase in autophagy and mitophagy in adult muscles. Conclusion: Our findings expand the allelic spectrum of ATAD3A variants and exemplify the use of a functional assay in Drosophila to aid variant interpretation.

Original language	English
Article number	55
Journal	Genome Medicine
Volume	13
Issue number	1
DOIs	https://doi.org/10.1186/s13073-021-00873-3
State	Published - 1 Dec 2021
Externally published	Yes

Keywords

AAA+ protein
ATAD3A
Autophagy
Autosomal recessive
Disease
Drosophila
Mitochondria
Neurogenesis

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology
Genetics
Genetics(clinical)

Access to Document

10.1186/s13073-021-00873-3

Cite this

Yap, Z. Y., Park, Y. H., Wortmann, S. B., Gunning, A. C., Ezer, S., Lee, S., Duraine, L., Wilichowski, E., Wilson, K., Mayr, J. A., Wagner, M., Li, H., Kini, U., Black, E. D., Monaghan, K. G., Lupski, J. R., Ellard, S., Westphal, D. S., Harel, T., & Yoon, W. H. (2021). Functional interpretation of ATAD3A variants in neuro-mitochondrial phenotypes. Genome Medicine, 13(1), Article 55. https://doi.org/10.1186/s13073-021-00873-3

@article{42213f537eb74308968a370a38e07709,

title = "Functional interpretation of ATAD3A variants in neuro-mitochondrial phenotypes",

abstract = "Background: ATPase family AAA-domain containing protein 3A (ATAD3A) is a nuclear-encoded mitochondrial membrane-anchored protein involved in diverse processes including mitochondrial dynamics, mitochondrial DNA organization, and cholesterol metabolism. Biallelic deletions (null), recessive missense variants (hypomorph), and heterozygous missense variants or duplications (antimorph) in ATAD3A lead to neurological syndromes in humans. Methods: To expand the mutational spectrum of ATAD3A variants and to provide functional interpretation of missense alleles in trans to deletion alleles, we performed exome sequencing for identification of single nucleotide variants (SNVs) and copy number variants (CNVs) in ATAD3A in individuals with neurological and mitochondrial phenotypes. A Drosophila Atad3a Gal4 knockin-null allele was generated using CRISPR-Cas9 genome editing technology to aid the interpretation of variants. Results: We report 13 individuals from 8 unrelated families with biallelic ATAD3A variants. The variants included four missense variants inherited in trans to loss-of-function alleles (p.(Leu77Val), p.(Phe50Leu), p.(Arg170Trp), p.(Gly236Val)), a homozygous missense variant p.(Arg327Pro), and a heterozygous non-frameshift indel p.(Lys568del). Affected individuals exhibited findings previously associated with ATAD3A pathogenic variation, including developmental delay, hypotonia, congenital cataracts, hypertrophic cardiomyopathy, and cerebellar atrophy. Drosophila studies indicated that Phe50Leu, Gly236Val, Arg327Pro, and Lys568del are severe loss-of-function alleles leading to early developmental lethality. Further, we showed that Phe50Leu, Gly236Val, and Arg327Pro cause neurogenesis defects. On the contrary, Leu77Val and Arg170Trp are partial loss-of-function alleles that cause progressive locomotion defects and whose expression leads to an increase in autophagy and mitophagy in adult muscles. Conclusion: Our findings expand the allelic spectrum of ATAD3A variants and exemplify the use of a functional assay in Drosophila to aid variant interpretation.",

keywords = "AAA+ protein, ATAD3A, Autophagy, Autosomal recessive, Disease, Drosophila, Mitochondria, Neurogenesis",

author = "Yap, \{Zheng Yie\} and Park, \{Yo Han\} and Wortmann, \{Saskia B.\} and Gunning, \{Adam C.\} and Shlomit Ezer and Sukyeong Lee and Lita Duraine and Ekkehard Wilichowski and Kate Wilson and Mayr, \{Johannes A.\} and Matias Wagner and Hong Li and Usha Kini and Black, \{Emily Davis\} and Monaghan, \{Kristin G.\} and Lupski, \{James R.\} and Sian Ellard and Westphal, \{Dominik S.\} and Tamar Harel and Yoon, \{Wan Hee\}",

note = "Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = dec,

day = "1",

doi = "10.1186/s13073-021-00873-3",

language = "English",

volume = "13",

journal = "Genome Medicine",

issn = "1756-994X",

publisher = "BioMed Central Ltd.",

number = "1",

}

Yap, ZY, Park, YH, Wortmann, SB, Gunning, AC, Ezer, S, Lee, S, Duraine, L, Wilichowski, E, Wilson, K, Mayr, JA, Wagner, M, Li, H, Kini, U, Black, ED, Monaghan, KG, Lupski, JR, Ellard, S, Westphal, DS, Harel, T & Yoon, WH 2021, 'Functional interpretation of ATAD3A variants in neuro-mitochondrial phenotypes', Genome Medicine, vol. 13, no. 1, 55. https://doi.org/10.1186/s13073-021-00873-3

TY - JOUR

T1 - Functional interpretation of ATAD3A variants in neuro-mitochondrial phenotypes

AU - Yap, Zheng Yie

AU - Park, Yo Han

AU - Wortmann, Saskia B.

AU - Gunning, Adam C.

AU - Ezer, Shlomit

AU - Lee, Sukyeong

AU - Duraine, Lita

AU - Wilichowski, Ekkehard

AU - Wilson, Kate

AU - Mayr, Johannes A.

AU - Wagner, Matias

AU - Li, Hong

AU - Kini, Usha

AU - Black, Emily Davis

AU - Monaghan, Kristin G.

AU - Lupski, James R.

AU - Ellard, Sian

AU - Westphal, Dominik S.

AU - Harel, Tamar

AU - Yoon, Wan Hee

PY - 2021/12/1

Y1 - 2021/12/1

N2 - Background: ATPase family AAA-domain containing protein 3A (ATAD3A) is a nuclear-encoded mitochondrial membrane-anchored protein involved in diverse processes including mitochondrial dynamics, mitochondrial DNA organization, and cholesterol metabolism. Biallelic deletions (null), recessive missense variants (hypomorph), and heterozygous missense variants or duplications (antimorph) in ATAD3A lead to neurological syndromes in humans. Methods: To expand the mutational spectrum of ATAD3A variants and to provide functional interpretation of missense alleles in trans to deletion alleles, we performed exome sequencing for identification of single nucleotide variants (SNVs) and copy number variants (CNVs) in ATAD3A in individuals with neurological and mitochondrial phenotypes. A Drosophila Atad3a Gal4 knockin-null allele was generated using CRISPR-Cas9 genome editing technology to aid the interpretation of variants. Results: We report 13 individuals from 8 unrelated families with biallelic ATAD3A variants. The variants included four missense variants inherited in trans to loss-of-function alleles (p.(Leu77Val), p.(Phe50Leu), p.(Arg170Trp), p.(Gly236Val)), a homozygous missense variant p.(Arg327Pro), and a heterozygous non-frameshift indel p.(Lys568del). Affected individuals exhibited findings previously associated with ATAD3A pathogenic variation, including developmental delay, hypotonia, congenital cataracts, hypertrophic cardiomyopathy, and cerebellar atrophy. Drosophila studies indicated that Phe50Leu, Gly236Val, Arg327Pro, and Lys568del are severe loss-of-function alleles leading to early developmental lethality. Further, we showed that Phe50Leu, Gly236Val, and Arg327Pro cause neurogenesis defects. On the contrary, Leu77Val and Arg170Trp are partial loss-of-function alleles that cause progressive locomotion defects and whose expression leads to an increase in autophagy and mitophagy in adult muscles. Conclusion: Our findings expand the allelic spectrum of ATAD3A variants and exemplify the use of a functional assay in Drosophila to aid variant interpretation.

AB - Background: ATPase family AAA-domain containing protein 3A (ATAD3A) is a nuclear-encoded mitochondrial membrane-anchored protein involved in diverse processes including mitochondrial dynamics, mitochondrial DNA organization, and cholesterol metabolism. Biallelic deletions (null), recessive missense variants (hypomorph), and heterozygous missense variants or duplications (antimorph) in ATAD3A lead to neurological syndromes in humans. Methods: To expand the mutational spectrum of ATAD3A variants and to provide functional interpretation of missense alleles in trans to deletion alleles, we performed exome sequencing for identification of single nucleotide variants (SNVs) and copy number variants (CNVs) in ATAD3A in individuals with neurological and mitochondrial phenotypes. A Drosophila Atad3a Gal4 knockin-null allele was generated using CRISPR-Cas9 genome editing technology to aid the interpretation of variants. Results: We report 13 individuals from 8 unrelated families with biallelic ATAD3A variants. The variants included four missense variants inherited in trans to loss-of-function alleles (p.(Leu77Val), p.(Phe50Leu), p.(Arg170Trp), p.(Gly236Val)), a homozygous missense variant p.(Arg327Pro), and a heterozygous non-frameshift indel p.(Lys568del). Affected individuals exhibited findings previously associated with ATAD3A pathogenic variation, including developmental delay, hypotonia, congenital cataracts, hypertrophic cardiomyopathy, and cerebellar atrophy. Drosophila studies indicated that Phe50Leu, Gly236Val, Arg327Pro, and Lys568del are severe loss-of-function alleles leading to early developmental lethality. Further, we showed that Phe50Leu, Gly236Val, and Arg327Pro cause neurogenesis defects. On the contrary, Leu77Val and Arg170Trp are partial loss-of-function alleles that cause progressive locomotion defects and whose expression leads to an increase in autophagy and mitophagy in adult muscles. Conclusion: Our findings expand the allelic spectrum of ATAD3A variants and exemplify the use of a functional assay in Drosophila to aid variant interpretation.

KW - AAA+ protein

KW - ATAD3A

KW - Autophagy

KW - Autosomal recessive

KW - Disease

KW - Drosophila

KW - Mitochondria

KW - Neurogenesis

UR - https://www.scopus.com/pages/publications/85104271279

U2 - 10.1186/s13073-021-00873-3

DO - 10.1186/s13073-021-00873-3

M3 - Article

C2 - 33845882

AN - SCOPUS:85104271279

SN - 1756-994X

VL - 13

JO - Genome Medicine

JF - Genome Medicine

IS - 1

M1 - 55

ER -

Functional interpretation of ATAD3A variants in neuro-mitochondrial phenotypes

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this