Sengers syndrome caused by biallelic TIMM29 variants and RNAi silencing in Drosophila orthologue recapitulates the human phenotype

Adel Shalata; Ann Saada; Mohammed Mahroum; Yarin Hadid; Chaya Furman; Zaher Eldin Shalata; Robert J. Desnick; Avraham Lorber; Asaad Khoury; Adnan Higazi; Avraham Shaag; Varda Barash; Ronen Spiegel; Euvgeni Vlodavsky; Pierre Rustin; Shmuel Pietrokovski; Irena Manov; Dan Gieger; Galit Tal; Adi Salzberg; Hanna Mandel

doi:https://doi.org/10.1186/s40246-025-00723-y

Sengers syndrome caused by biallelic TIMM29 variants and RNAi silencing in Drosophila orthologue recapitulates the human phenotype

Adel Shalata, Ann Saada, Mohammed Mahroum, Yarin Hadid, Chaya Furman, Zaher Eldin Shalata, Robert J. Desnick, Avraham Lorber, Asaad Khoury, Adnan Higazi, Avraham Shaag, Varda Barash, Ronen Spiegel, Euvgeni Vlodavsky, Pierre Rustin, Shmuel Pietrokovski, Irena Manov, Dan Gieger, Galit Tal, Adi SalzbergHanna Mandel

Technion - Israel Institute of Technology, University of Haifa, Weizmann Institute of Science

Research output: Contribution to journal › Review article › peer-review

Abstract

Purpose: Sengers-syndrome (S.S) is a genetic disorder characterized by congenital cataracts, hypertrophic cardiomyopathy, skeletal myopathy and lactic acidosis. All reported cases were genetically caused by biallelic mutations in the AGK gene. We herein report a pathogenic variant in TIMM29 gene, encoding Tim29 protein, as a novel cause of S.S. Notably, AGK and Tim29 proteins are components of the TIM22 complex, which is responsible for importing carrier proteins into the inner mitochondrial membrane. Method: Clinical data of 17 consanguineous patients featuring S.S was obtained. Linkage analysis, and sequencing were used to map and identify the disease-causing gene. Tissues derived from the study participants and a Drosophila melanogaster model were used to evaluate the effects of TIMM29 variant on S.S. Results: The patients presented with a severe phenotype of S.S, markedly elevated serum creatine-phosphokinase, combined mitochondrial-respiratory-chain-complexes deficiency, reduced pyruvate-dehydrogenase complex activity, and reduced adenine nucleotide translocator 1 protein. Histopathological studies showed accumulation of abnormal mitochondria. Homozygosity mapping and gene sequencing revealed a biallelic variant in TIMM29 NM_138358.4:c.514T > C NP_612367.1:p.(Trp172Arg). The knockdown of the Drosophila TIMM29 orthologous gene (CG14270) recapitulated the phenotype and pathology observed in the studied cohort. We expand the clinical phenotype of S.S and provide substantial evidence supporting TIMM29 as the second causal gene of a severe type of S.S, designated as S.S- TIMM29. Conclusion: The present study uncovers several biochemical differences between the two S.S types, including the hyperCPKemia being almost unique for S.S-TIMM29 cohort, the different frequency of MMRCC and PDHc deficiencies among the two S.S types. We propose to designate the S.S associated with TIMM29 homozygous variant as S.S-TIMM29.

Original language	English
Article number	21
Journal	Human Genomics
Volume	19
Issue number	1
DOIs	https://doi.org/10.1186/s40246-025-00723-y
State	Published - Dec 2025

Keywords

AGK
CK
RCC
Sengers syndrome
TIMM29

All Science Journal Classification (ASJC) codes

Drug Discovery
Genetics
Molecular Medicine
Molecular Biology

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https://doi.org/10.1186/s40246-025-00723-y

Cite this

Shalata, A., Saada, A., Mahroum, M., Hadid, Y., Furman, C., Shalata, Z. E., Desnick, R. J., Lorber, A., Khoury, A., Higazi, A., Shaag, A., Barash, V., Spiegel, R., Vlodavsky, E., Rustin, P., Pietrokovski, S., Manov, I., Gieger, D., Tal, G., ... Mandel, H. (2025). Sengers syndrome caused by biallelic TIMM29 variants and RNAi silencing in Drosophila orthologue recapitulates the human phenotype. Human Genomics, 19(1), Article 21. https://doi.org/10.1186/s40246-025-00723-y

@article{ea5b33ece35c4912a6acae1d19a5be42,

title = "Sengers syndrome caused by biallelic TIMM29 variants and RNAi silencing in Drosophila orthologue recapitulates the human phenotype",

abstract = "Purpose: Sengers-syndrome (S.S) is a genetic disorder characterized by congenital cataracts, hypertrophic cardiomyopathy, skeletal myopathy and lactic acidosis. All reported cases were genetically caused by biallelic mutations in the AGK gene. We herein report a pathogenic variant in TIMM29 gene, encoding Tim29 protein, as a novel cause of S.S. Notably, AGK and Tim29 proteins are components of the TIM22 complex, which is responsible for importing carrier proteins into the inner mitochondrial membrane. Method: Clinical data of 17 consanguineous patients featuring S.S was obtained. Linkage analysis, and sequencing were used to map and identify the disease-causing gene. Tissues derived from the study participants and a Drosophila melanogaster model were used to evaluate the effects of TIMM29 variant on S.S. Results: The patients presented with a severe phenotype of S.S, markedly elevated serum creatine-phosphokinase, combined mitochondrial-respiratory-chain-complexes deficiency, reduced pyruvate-dehydrogenase complex activity, and reduced adenine nucleotide translocator 1 protein. Histopathological studies showed accumulation of abnormal mitochondria. Homozygosity mapping and gene sequencing revealed a biallelic variant in TIMM29 NM_138358.4:c.514T > C NP_612367.1:p.(Trp172Arg). The knockdown of the Drosophila TIMM29 orthologous gene (CG14270) recapitulated the phenotype and pathology observed in the studied cohort. We expand the clinical phenotype of S.S and provide substantial evidence supporting TIMM29 as the second causal gene of a severe type of S.S, designated as S.S- TIMM29. Conclusion: The present study uncovers several biochemical differences between the two S.S types, including the hyperCPKemia being almost unique for S.S-TIMM29 cohort, the different frequency of MMRCC and PDHc deficiencies among the two S.S types. We propose to designate the S.S associated with TIMM29 homozygous variant as S.S-TIMM29.",

keywords = "AGK, CK, RCC, Sengers syndrome, TIMM29",

author = "Adel Shalata and Ann Saada and Mohammed Mahroum and Yarin Hadid and Chaya Furman and Shalata, {Zaher Eldin} and Desnick, {Robert J.} and Avraham Lorber and Asaad Khoury and Adnan Higazi and Avraham Shaag and Varda Barash and Ronen Spiegel and Euvgeni Vlodavsky and Pierre Rustin and Shmuel Pietrokovski and Irena Manov and Dan Gieger and Galit Tal and Adi Salzberg and Hanna Mandel",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2025.",

year = "2025",

month = dec,

doi = "https://doi.org/10.1186/s40246-025-00723-y",

language = "الإنجليزيّة",

volume = "19",

journal = "Human Genomics",

issn = "1473-9542",

publisher = "BioMed Central Ltd.",

number = "1",

}

Shalata, A, Saada, A, Mahroum, M, Hadid, Y, Furman, C, Shalata, ZE, Desnick, RJ, Lorber, A, Khoury, A, Higazi, A, Shaag, A, Barash, V, Spiegel, R, Vlodavsky, E, Rustin, P, Pietrokovski, S, Manov, I, Gieger, D, Tal, G, Salzberg, A & Mandel, H 2025, 'Sengers syndrome caused by biallelic TIMM29 variants and RNAi silencing in Drosophila orthologue recapitulates the human phenotype', Human Genomics, vol. 19, no. 1, 21. https://doi.org/10.1186/s40246-025-00723-y

TY - JOUR

T1 - Sengers syndrome caused by biallelic TIMM29 variants and RNAi silencing in Drosophila orthologue recapitulates the human phenotype

AU - Shalata, Adel

AU - Saada, Ann

AU - Mahroum, Mohammed

AU - Hadid, Yarin

AU - Furman, Chaya

AU - Shalata, Zaher Eldin

AU - Desnick, Robert J.

AU - Lorber, Avraham

AU - Khoury, Asaad

AU - Higazi, Adnan

AU - Shaag, Avraham

AU - Barash, Varda

AU - Spiegel, Ronen

AU - Vlodavsky, Euvgeni

AU - Rustin, Pierre

AU - Pietrokovski, Shmuel

AU - Manov, Irena

AU - Gieger, Dan

AU - Tal, Galit

AU - Salzberg, Adi

AU - Mandel, Hanna

PY - 2025/12

Y1 - 2025/12

N2 - Purpose: Sengers-syndrome (S.S) is a genetic disorder characterized by congenital cataracts, hypertrophic cardiomyopathy, skeletal myopathy and lactic acidosis. All reported cases were genetically caused by biallelic mutations in the AGK gene. We herein report a pathogenic variant in TIMM29 gene, encoding Tim29 protein, as a novel cause of S.S. Notably, AGK and Tim29 proteins are components of the TIM22 complex, which is responsible for importing carrier proteins into the inner mitochondrial membrane. Method: Clinical data of 17 consanguineous patients featuring S.S was obtained. Linkage analysis, and sequencing were used to map and identify the disease-causing gene. Tissues derived from the study participants and a Drosophila melanogaster model were used to evaluate the effects of TIMM29 variant on S.S. Results: The patients presented with a severe phenotype of S.S, markedly elevated serum creatine-phosphokinase, combined mitochondrial-respiratory-chain-complexes deficiency, reduced pyruvate-dehydrogenase complex activity, and reduced adenine nucleotide translocator 1 protein. Histopathological studies showed accumulation of abnormal mitochondria. Homozygosity mapping and gene sequencing revealed a biallelic variant in TIMM29 NM_138358.4:c.514T > C NP_612367.1:p.(Trp172Arg). The knockdown of the Drosophila TIMM29 orthologous gene (CG14270) recapitulated the phenotype and pathology observed in the studied cohort. We expand the clinical phenotype of S.S and provide substantial evidence supporting TIMM29 as the second causal gene of a severe type of S.S, designated as S.S- TIMM29. Conclusion: The present study uncovers several biochemical differences between the two S.S types, including the hyperCPKemia being almost unique for S.S-TIMM29 cohort, the different frequency of MMRCC and PDHc deficiencies among the two S.S types. We propose to designate the S.S associated with TIMM29 homozygous variant as S.S-TIMM29.

AB - Purpose: Sengers-syndrome (S.S) is a genetic disorder characterized by congenital cataracts, hypertrophic cardiomyopathy, skeletal myopathy and lactic acidosis. All reported cases were genetically caused by biallelic mutations in the AGK gene. We herein report a pathogenic variant in TIMM29 gene, encoding Tim29 protein, as a novel cause of S.S. Notably, AGK and Tim29 proteins are components of the TIM22 complex, which is responsible for importing carrier proteins into the inner mitochondrial membrane. Method: Clinical data of 17 consanguineous patients featuring S.S was obtained. Linkage analysis, and sequencing were used to map and identify the disease-causing gene. Tissues derived from the study participants and a Drosophila melanogaster model were used to evaluate the effects of TIMM29 variant on S.S. Results: The patients presented with a severe phenotype of S.S, markedly elevated serum creatine-phosphokinase, combined mitochondrial-respiratory-chain-complexes deficiency, reduced pyruvate-dehydrogenase complex activity, and reduced adenine nucleotide translocator 1 protein. Histopathological studies showed accumulation of abnormal mitochondria. Homozygosity mapping and gene sequencing revealed a biallelic variant in TIMM29 NM_138358.4:c.514T > C NP_612367.1:p.(Trp172Arg). The knockdown of the Drosophila TIMM29 orthologous gene (CG14270) recapitulated the phenotype and pathology observed in the studied cohort. We expand the clinical phenotype of S.S and provide substantial evidence supporting TIMM29 as the second causal gene of a severe type of S.S, designated as S.S- TIMM29. Conclusion: The present study uncovers several biochemical differences between the two S.S types, including the hyperCPKemia being almost unique for S.S-TIMM29 cohort, the different frequency of MMRCC and PDHc deficiencies among the two S.S types. We propose to designate the S.S associated with TIMM29 homozygous variant as S.S-TIMM29.

KW - AGK

KW - CK

KW - RCC

KW - Sengers syndrome

KW - TIMM29

UR - http://www.scopus.com/inward/record.url?scp=85219643920&partnerID=8YFLogxK

U2 - https://doi.org/10.1186/s40246-025-00723-y

DO - https://doi.org/10.1186/s40246-025-00723-y

M3 - مقالة مرجعية

C2 - 40022150

SN - 1473-9542

VL - 19

JO - Human Genomics

JF - Human Genomics

IS - 1

M1 - 21

ER -

Sengers syndrome caused by biallelic TIMM29 variants and RNAi silencing in Drosophila orthologue recapitulates the human phenotype

Abstract

Keywords

All Science Journal Classification (ASJC) codes

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