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PhenoScore quantifies phenotypic variation for rare genetic diseases by combining facial analysis with other clinical features using a machine-learning framework

PhenoScore quantifies phenotypic variation for rare genetic diseases by combining facial analysis with other clinical features using a machine-learning framework
PhenoScore quantifies phenotypic variation for rare genetic diseases by combining facial analysis with other clinical features using a machine-learning framework
Several molecular and phenotypic algorithms exist that establish genotype–phenotype correlations, including facial recognition tools. However, no unified framework that investigates both facial data and other phenotypic data directly from individuals exists. We developed PhenoScore: an open-source, artificial intelligence-based phenomics framework, combining facial recognition technology with Human Phenotype Ontology data analysis to quantify phenotypic similarity. Here we show PhenoScore’s ability to recognize distinct phenotypic entities by establishing recognizable phenotypes for 37 of 40 investigated syndromes against clinical features observed in individuals with other neurodevelopmental disorders and show it is an improvement on existing approaches. PhenoScore provides predictions for individuals with variants of unknown significance and enables sophisticated genotype–phenotype studies by testing hypotheses on possible phenotypic (sub)groups. PhenoScore confirmed previously known phenotypic subgroups caused by variants in the same gene for SATB1, SETBP1 and DEAF1 and provides objective clinical evidence for two distinct ADNP-related phenotypes, already established functionally.
1061-4036
1598-1607
Dingemans, Alexander J.M.
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Hinne, Max
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Truijen, Kim M.G.
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Goltstein, Lia
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Jansen, Sandra
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Van Bon, Bregje W.
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Kleefstra, Tjitske
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Campeau, Philippe M.
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Palmer, Elizabeth E.
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Van Esch, Hilde
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Lyon, Gholson J.
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Alkuraya, Fowzan S.
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Baralle, Diana
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Van Der Sluijs, Pleuntje J.
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Santen, Gijs W.E.
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Kooy, R. Frank
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Van Gerven, Marcel A.J.
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Vissers, Lisenka E.L.M.
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De Vries, Bert B.A.
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Dingemans, Alexander J.M.
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Hinne, Max
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Truijen, Kim M.G.
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Goltstein, Lia
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Van Reeuwijk, Jeroen
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De Leeuw, Nicole
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Diets, Illja J.
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Den Hoed, Joery
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Jonis, Noraly
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Vulto-van Silfhout, Anneke T.
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Palmer, Elizabeth E.
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Van Esch, Hilde
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Marom, Ronit
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Baralle, Diana
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Kooy, R. Frank
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De Vries, Bert B.A.
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Dingemans, Alexander J.M., Hinne, Max, Truijen, Kim M.G., Goltstein, Lia, Van Reeuwijk, Jeroen, De Leeuw, Nicole, Schuurs-hoeijmakers, Janneke, Pfundt, Rolph, Diets, Illja J., Den Hoed, Joery, De Boer, Elke, Coenen-van Der Spek, Jet, Jansen, Sandra, Van Bon, Bregje W., Jonis, Noraly, Ockeloen, Charlotte W., Vulto-van Silfhout, Anneke T., Kleefstra, Tjitske, Koolen, David A., Campeau, Philippe M., Palmer, Elizabeth E., Van Esch, Hilde, Lyon, Gholson J., Alkuraya, Fowzan S., Rauch, Anita, Marom, Ronit, Baralle, Diana, Van Der Sluijs, Pleuntje J., Santen, Gijs W.E., Kooy, R. Frank, Van Gerven, Marcel A.J., Vissers, Lisenka E.L.M. and De Vries, Bert B.A. (2023) PhenoScore quantifies phenotypic variation for rare genetic diseases by combining facial analysis with other clinical features using a machine-learning framework. Nature Genetics, 55 (9), 1598-1607. (doi:10.1038/s41588-023-01469-w).

Record type: Article

Abstract

Several molecular and phenotypic algorithms exist that establish genotype–phenotype correlations, including facial recognition tools. However, no unified framework that investigates both facial data and other phenotypic data directly from individuals exists. We developed PhenoScore: an open-source, artificial intelligence-based phenomics framework, combining facial recognition technology with Human Phenotype Ontology data analysis to quantify phenotypic similarity. Here we show PhenoScore’s ability to recognize distinct phenotypic entities by establishing recognizable phenotypes for 37 of 40 investigated syndromes against clinical features observed in individuals with other neurodevelopmental disorders and show it is an improvement on existing approaches. PhenoScore provides predictions for individuals with variants of unknown significance and enables sophisticated genotype–phenotype studies by testing hypotheses on possible phenotypic (sub)groups. PhenoScore confirmed previously known phenotypic subgroups caused by variants in the same gene for SATB1, SETBP1 and DEAF1 and provides objective clinical evidence for two distinct ADNP-related phenotypes, already established functionally.

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Accepted/In Press date: 5 July 2023
e-pub ahead of print date: 7 August 2023
Published date: 1 September 2023
Additional Information: Funding Information: We are grateful to all families and clinicians who agreed to participate and provide clinical and genotypic information. R.F.K. acknowledges financial support from the Research Fund of the University of Antwerp (Methusalem-OEC grant GENOMED). The work of G.J.L. is supported by New York State Office for People with Developmental Disabilities (OPWDD) and NIH NIGMS R35-GM-133408. E.E.P. is supported by a National Health and Medical Research Council Investigator Grant (award 2021/GNT2008166). Furthermore, we are grateful to the Dutch Organization for Health Research and Development—ZON-MW grants 912-12-109 (to B.B.A.d.V. and L.E.L.M.V.), Donders Junior researcher grant 2019 (to B.B.A.d.V. and L.E.L.M.V.) and Aspasia grant 015.014.066 (to L.E.L.M.V.). The aims of this study contribute to the Solve-RD project (to L.E.L.M.V.), which has received funding from the European Unions Horizon 2020 research and innovation program under grant agreement 779257. The funders had no role in study design, data collection and analysis, decision to publish or preparation of the manuscript. Publisher Copyright: © 2023, The Author(s), under exclusive licence to Springer Nature America, Inc.

Identifiers

Local EPrints ID: 480825
URI: http://eprints.soton.ac.uk/id/eprint/480825
ISSN: 1061-4036
PURE UUID: 1c2871b4-9b04-48b4-9991-f9db55b861fd
ORCID for Diana Baralle: ORCID iD orcid.org/0000-0003-3217-4833

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Date deposited: 10 Aug 2023 16:30
Last modified: 13 Aug 2024 04:01

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Contributors

Author: Alexander J.M. Dingemans
Author: Max Hinne
Author: Kim M.G. Truijen
Author: Lia Goltstein
Author: Jeroen Van Reeuwijk
Author: Nicole De Leeuw
Author: Janneke Schuurs-hoeijmakers
Author: Rolph Pfundt
Author: Illja J. Diets
Author: Joery Den Hoed
Author: Elke De Boer
Author: Jet Coenen-van Der Spek
Author: Sandra Jansen
Author: Bregje W. Van Bon
Author: Noraly Jonis
Author: Charlotte W. Ockeloen
Author: Anneke T. Vulto-van Silfhout
Author: Tjitske Kleefstra
Author: David A. Koolen
Author: Philippe M. Campeau
Author: Elizabeth E. Palmer
Author: Hilde Van Esch
Author: Gholson J. Lyon
Author: Fowzan S. Alkuraya
Author: Anita Rauch
Author: Ronit Marom
Author: Diana Baralle ORCID iD
Author: Pleuntje J. Van Der Sluijs
Author: Gijs W.E. Santen
Author: R. Frank Kooy
Author: Marcel A.J. Van Gerven
Author: Lisenka E.L.M. Vissers
Author: Bert B.A. De Vries

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