Phenotype Spectrum of TRPM3-Associated Disorders

Laura Jolitz; Ingo Helbig; Mark P. Fitzgerald; Sarah McKeown Ruggiero; Stacey Cohen; Chloe Angelini; Elena Vallespin; Vincent Michaud; Anna Gerasimenko; Benjamin Cogne; Bertrand Isidor; Boris Keren; David Dyment; Delphine Heron; Helena Gásdal Karstensen; Inge Cuppen; John Christodoulou; Meredith Wilson; Nicole J. Lake; Saskia Biskup; Steffen Syrbe; Takayasu Mori; Lena Luise Becker; Angela M. Kaindl

doi:10.1002/ana.27141

Phenotype Spectrum of TRPM3-Associated Disorders

Laura Jolitz, Ingo Helbig, Mark P. Fitzgerald, Sarah McKeown Ruggiero, Stacey Cohen, Chloe Angelini, Elena Vallespin, Vincent Michaud, Anna Gerasimenko, Benjamin Cogne, Bertrand Isidor, Boris Keren, David Dyment, Delphine Heron, Helena Gásdal Karstensen, Inge Cuppen, John Christodoulou, Meredith Wilson, Nicole J. Lake, Saskia BiskupSteffen Syrbe, Takayasu Mori, Lena Luise Becker^*, Angela M. Kaindl^*

^*Corresponding author for this work

Neurologen

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

Abstract

Objective: Monoallelic variants in the transient receptor potential melastatin-related type 3 gene (TRPM3) have been associated with neurodevelopmental manifestations, but knowledge on the clinical manifestations and treatment options is limited. We characterized the clinical spectrum, highlighting particularly the epilepsy phenotype, and the effect of treatments. Methods: We analyzed retrospectively the phenotypes and genotypes of 43 individuals with TRPM3 variants, acquired from GeneMatcher and collaborations (n = 21), and through a systematic literature search (n = 22). We included all patients with a pathogenic TRPM3 variant. Results: The median age at the time of the study was 10 years, with a preponderance of girls (60%) versus boys (40%). Frequent findings were developmental delay and/or intellectual disability (93%), global or axial hypotonia (77%), ocular involvement (70%), musculoskeletal anomalies (65%), and dysmorphic features (58%). Epilepsy was diagnosed in 31 patients (72%), classified in all as developmental and epileptic encephalopathy with or without spike wave activation in sleep (DEE/DEE-SWAS). Patients with the variant p.Val1002Met (n = 24) significantly more often had developmental delay and epilepsy. The most effective anti-seizure medication was primidone. All treated patients showed an improvement in seizure frequency, motor and speech development, and/or learning capability with this drug. Interpretation: Developmental delay/intellectual disability and epilepsy are dominant phenotypic features in patients with TRPM3 variants. Given that epilepsy can negatively impact development, screening for awake and sleep electroencephalogram abnormalities and other manifestations are essential to offer early intervention. The TRPM3 channel blocker primidone has shown promising effects and should be considered in every child with a TRPM3 gain-of-function variant. ANN NEUROL 2025;97:561–570.

Original language	English
Pages (from-to)	561-570
Number of pages	10
Journal	Annals of Neurology
Volume	97
Issue number	3
Early online date	3 Jan 2025
DOIs	https://doi.org/10.1002/ana.27141
Publication status	Published - Mar 2025

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Jolitz, L., Helbig, I., Fitzgerald, M. P., McKeown Ruggiero, S., Cohen, S., Angelini, C., Vallespin, E., Michaud, V., Gerasimenko, A., Cogne, B., Isidor, B., Keren, B., Dyment, D., Heron, D., Karstensen, H. G., Cuppen, I., Christodoulou, J., Wilson, M., Lake, N. J., ... Kaindl, A. M. (2025). Phenotype Spectrum of TRPM3-Associated Disorders. Annals of Neurology, 97(3), 561-570. https://doi.org/10.1002/ana.27141

@article{ecee6511a2a54021b59d171dbc6e589f,

title = "Phenotype Spectrum of TRPM3-Associated Disorders",

abstract = "Objective: Monoallelic variants in the transient receptor potential melastatin-related type 3 gene (TRPM3) have been associated with neurodevelopmental manifestations, but knowledge on the clinical manifestations and treatment options is limited. We characterized the clinical spectrum, highlighting particularly the epilepsy phenotype, and the effect of treatments. Methods: We analyzed retrospectively the phenotypes and genotypes of 43 individuals with TRPM3 variants, acquired from GeneMatcher and collaborations (n = 21), and through a systematic literature search (n = 22). We included all patients with a pathogenic TRPM3 variant. Results: The median age at the time of the study was 10 years, with a preponderance of girls (60%) versus boys (40%). Frequent findings were developmental delay and/or intellectual disability (93%), global or axial hypotonia (77%), ocular involvement (70%), musculoskeletal anomalies (65%), and dysmorphic features (58%). Epilepsy was diagnosed in 31 patients (72%), classified in all as developmental and epileptic encephalopathy with or without spike wave activation in sleep (DEE/DEE-SWAS). Patients with the variant p.Val1002Met (n = 24) significantly more often had developmental delay and epilepsy. The most effective anti-seizure medication was primidone. All treated patients showed an improvement in seizure frequency, motor and speech development, and/or learning capability with this drug. Interpretation: Developmental delay/intellectual disability and epilepsy are dominant phenotypic features in patients with TRPM3 variants. Given that epilepsy can negatively impact development, screening for awake and sleep electroencephalogram abnormalities and other manifestations are essential to offer early intervention. The TRPM3 channel blocker primidone has shown promising effects and should be considered in every child with a TRPM3 gain-of-function variant. ANN NEUROL 2025;97:561–570.",

author = "Laura Jolitz and Ingo Helbig and Fitzgerald, {Mark P.} and {McKeown Ruggiero}, Sarah and Stacey Cohen and Chloe Angelini and Elena Vallespin and Vincent Michaud and Anna Gerasimenko and Benjamin Cogne and Bertrand Isidor and Boris Keren and David Dyment and Delphine Heron and Karstensen, {Helena G{\'a}sdal} and Inge Cuppen and John Christodoulou and Meredith Wilson and Lake, {Nicole J.} and Saskia Biskup and Steffen Syrbe and Takayasu Mori and Becker, {Lena Luise} and Kaindl, {Angela M.}",

note = "Publisher Copyright: {\textcopyright} 2025 The Author(s). Annals of Neurology published by Wiley Periodicals LLC on behalf of American Neurological Association.",

year = "2025",

month = mar,

doi = "10.1002/ana.27141",

language = "English",

volume = "97",

pages = "561--570",

journal = "Annals of Neurology",

issn = "0364-5134",

publisher = "John Wiley & Sons Inc.",

number = "3",

}

Jolitz, L, Helbig, I, Fitzgerald, MP, McKeown Ruggiero, S, Cohen, S, Angelini, C, Vallespin, E, Michaud, V, Gerasimenko, A, Cogne, B, Isidor, B, Keren, B, Dyment, D, Heron, D, Karstensen, HG, Cuppen, I, Christodoulou, J, Wilson, M, Lake, NJ, Biskup, S, Syrbe, S, Mori, T, Becker, LL & Kaindl, AM 2025, 'Phenotype Spectrum of TRPM3-Associated Disorders', Annals of Neurology, vol. 97, no. 3, pp. 561-570. https://doi.org/10.1002/ana.27141

TY - JOUR

T1 - Phenotype Spectrum of TRPM3-Associated Disorders

AU - Jolitz, Laura

AU - Helbig, Ingo

AU - Fitzgerald, Mark P.

AU - McKeown Ruggiero, Sarah

AU - Cohen, Stacey

AU - Angelini, Chloe

AU - Vallespin, Elena

AU - Michaud, Vincent

AU - Gerasimenko, Anna

AU - Cogne, Benjamin

AU - Isidor, Bertrand

AU - Keren, Boris

AU - Dyment, David

AU - Heron, Delphine

AU - Karstensen, Helena Gásdal

AU - Cuppen, Inge

AU - Christodoulou, John

AU - Wilson, Meredith

AU - Lake, Nicole J.

AU - Biskup, Saskia

AU - Syrbe, Steffen

AU - Mori, Takayasu

AU - Becker, Lena Luise

AU - Kaindl, Angela M.

PY - 2025/3

Y1 - 2025/3

N2 - Objective: Monoallelic variants in the transient receptor potential melastatin-related type 3 gene (TRPM3) have been associated with neurodevelopmental manifestations, but knowledge on the clinical manifestations and treatment options is limited. We characterized the clinical spectrum, highlighting particularly the epilepsy phenotype, and the effect of treatments. Methods: We analyzed retrospectively the phenotypes and genotypes of 43 individuals with TRPM3 variants, acquired from GeneMatcher and collaborations (n = 21), and through a systematic literature search (n = 22). We included all patients with a pathogenic TRPM3 variant. Results: The median age at the time of the study was 10 years, with a preponderance of girls (60%) versus boys (40%). Frequent findings were developmental delay and/or intellectual disability (93%), global or axial hypotonia (77%), ocular involvement (70%), musculoskeletal anomalies (65%), and dysmorphic features (58%). Epilepsy was diagnosed in 31 patients (72%), classified in all as developmental and epileptic encephalopathy with or without spike wave activation in sleep (DEE/DEE-SWAS). Patients with the variant p.Val1002Met (n = 24) significantly more often had developmental delay and epilepsy. The most effective anti-seizure medication was primidone. All treated patients showed an improvement in seizure frequency, motor and speech development, and/or learning capability with this drug. Interpretation: Developmental delay/intellectual disability and epilepsy are dominant phenotypic features in patients with TRPM3 variants. Given that epilepsy can negatively impact development, screening for awake and sleep electroencephalogram abnormalities and other manifestations are essential to offer early intervention. The TRPM3 channel blocker primidone has shown promising effects and should be considered in every child with a TRPM3 gain-of-function variant. ANN NEUROL 2025;97:561–570.

AB - Objective: Monoallelic variants in the transient receptor potential melastatin-related type 3 gene (TRPM3) have been associated with neurodevelopmental manifestations, but knowledge on the clinical manifestations and treatment options is limited. We characterized the clinical spectrum, highlighting particularly the epilepsy phenotype, and the effect of treatments. Methods: We analyzed retrospectively the phenotypes and genotypes of 43 individuals with TRPM3 variants, acquired from GeneMatcher and collaborations (n = 21), and through a systematic literature search (n = 22). We included all patients with a pathogenic TRPM3 variant. Results: The median age at the time of the study was 10 years, with a preponderance of girls (60%) versus boys (40%). Frequent findings were developmental delay and/or intellectual disability (93%), global or axial hypotonia (77%), ocular involvement (70%), musculoskeletal anomalies (65%), and dysmorphic features (58%). Epilepsy was diagnosed in 31 patients (72%), classified in all as developmental and epileptic encephalopathy with or without spike wave activation in sleep (DEE/DEE-SWAS). Patients with the variant p.Val1002Met (n = 24) significantly more often had developmental delay and epilepsy. The most effective anti-seizure medication was primidone. All treated patients showed an improvement in seizure frequency, motor and speech development, and/or learning capability with this drug. Interpretation: Developmental delay/intellectual disability and epilepsy are dominant phenotypic features in patients with TRPM3 variants. Given that epilepsy can negatively impact development, screening for awake and sleep electroencephalogram abnormalities and other manifestations are essential to offer early intervention. The TRPM3 channel blocker primidone has shown promising effects and should be considered in every child with a TRPM3 gain-of-function variant. ANN NEUROL 2025;97:561–570.

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U2 - 10.1002/ana.27141

DO - 10.1002/ana.27141

M3 - Article

C2 - 39749750

AN - SCOPUS:85214423835

SN - 0364-5134

VL - 97

SP - 561

EP - 570

JO - Annals of Neurology

JF - Annals of Neurology

IS - 3

ER -

Phenotype Spectrum of TRPM3-Associated Disorders

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