Molecular analysis of inherited disorders of cornification in polish patients show novel variants and functional data and provokes questions on the significance of secondary findings

Katarzyna Wertheim-Tysarowska; Katarzyna Osipowicz; Katarzyna Wozniak; Justyna Sawicka; Adrianna Mika; Anna Kutkowska-Kazmierczak; Katarzyna Niepokój; Agnieszka Sobczynska-Tomaszewska; Bartlomiej Wawrzycki; Aldona Pietrzak; Robert Smigiel; Bartosz Wojtas; Bartlomiej Gielniewski; Alicja Szabelska-Beresewicz; Joanna Zyprych-Walczak; Agnieszka Magdalena Rygiel; Alicja Domaszewicz; Natalia Braun-Walicka; Alicja Grabarczyk; Sylwia Rzonca-Niewczas; Ruszkowska Lidia; Mateusz Dawidziuk; Dominik Domanski; Tomasz Gambin; Monika Jackiewicz; Katarzyna Duk; Barbara Dorozko; Orest Szczygielski; Natalia Krzesniak; Bartlomiej H Noszczyk; Ewa Obersztyn; Jolanta Wierzba; Artur Barczyk; Jennifer Castaneda; Anna Eckersdorf-Mastalerz; Anna Jakubiuk-Tomaszuk; Pawel Wlasienko; Ilona Jaszczuk; Aleksandra Jezela-Stanek; Jakub Klapecki; Michel van Geel; Cezary Kowalewski; Jerzy Bal; Antoni Gostynski

doi:10.1186/s13023-024-03395-4

Molecular analysis of inherited disorders of cornification in polish patients show novel variants and functional data and provokes questions on the significance of secondary findings

Katarzyna Wertheim-Tysarowska^*, Katarzyna Osipowicz, Katarzyna Wozniak, Justyna Sawicka, Adrianna Mika, Anna Kutkowska-Kazmierczak, Katarzyna Niepokój, Agnieszka Sobczynska-Tomaszewska, Bartlomiej Wawrzycki, Aldona Pietrzak, Robert Smigiel, Bartosz Wojtas, Bartlomiej Gielniewski, Alicja Szabelska-Beresewicz, Joanna Zyprych-Walczak, Agnieszka Magdalena Rygiel, Alicja Domaszewicz, Natalia Braun-Walicka, Alicja Grabarczyk, Sylwia Rzonca-NiewczasRuszkowska Lidia, Mateusz Dawidziuk, Dominik Domanski, Tomasz Gambin, Monika Jackiewicz, Katarzyna Duk, Barbara Dorozko, Orest Szczygielski, Natalia Krzesniak, Bartlomiej H Noszczyk, Ewa Obersztyn, Jolanta Wierzba, Artur Barczyk, Jennifer Castaneda, Anna Eckersdorf-Mastalerz, Anna Jakubiuk-Tomaszuk, Pawel Wlasienko, Ilona Jaszczuk, Aleksandra Jezela-Stanek, Jakub Klapecki, Michel van Geel, Cezary Kowalewski, Jerzy Bal, Antoni Gostynski

^*Corresponding author for this work

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

Abstract

BACKGROUND: The Mendelian Disorders of Cornification (MeDOC) comprise a large number of disorders that present with either localised (palmoplantar keratoderma, PPK) or generalised (ichthyoses) signs. The MeDOC are highly heterogenic in terms of genetics and phenotype. Consequently, diagnostic process is challenging and before implementation of the next generation sequencing, was mostly symptomatic, not causal, which limited research on those diseases. The aim of the study was to genetically characterise a cohort of 265 Polish patients with MeDOC and to get insight into the skin lesions using transcriptome and lipid profile analyses. RESULTS: We detected causal variants in 85% (226/265) patients. In addition to the primary gene defect, a pathogenic variant in another gene involved in MeDOC pathology was identified in 23 cases. We found 150 distinct variants in 33 genes, including 32 novel and 16 recurrent (present in > 5 alleles). In 43 alleles large rearrangements were detected, including deletions in the STS, SPINK5, CERS3 and recurrent duplication of exons 10-14 in TGM1. The RNA analysis using samples collected from 18 MeDOC patients and 22 controls identified 1377 differentially expressed genes - DEG. The gene ontology analysis revealed that 114 biological processes were upregulated in the MeDOC group, including i.e. epithelial cell differentiation, lipid metabolic process; homeostasis; regulation of water loss via skin; peptide cross-linking. The DEG between TGM1 and ALOX12B patients, showed that RNA profile is highly similar, though fatty acid profile in epidermal scrapings of those patients showed differences e.g. for the very long chain fatty acids (VLCFAs; FAs = C20), the very long-chain monounsaturated fatty acids (VLC-MUFAs, FAs = C20:1) and the n6 polyunsaturated fatty acids (n6 PUFAs). CONCLUSION: Our results show that NGS-based analysis is an effective MeDOC diagnostic tool. The Polish MeDOC patients are heterogenic, however recurrent variants are present. The novel variants and high number of TGM1 and SPINK5 copy number variations give further insight into molecular pathology of MeDOC. We show that secondary variants in MeDOC-related genes are present in a significant group of patients, which should be further investigated in the context of phenotype modifiers. Finally, we provide novel RNA and lipid data that characterise molecularly MeDOC epidermis.

Original language	English
Article number	413
Number of pages	14
Journal	Orphanet Journal of Rare Diseases
Volume	19
Issue number	1
DOIs	https://doi.org/10.1186/s13023-024-03395-4
Publication status	Published - 5 Nov 2024

Keywords

Genes
Genodermatoses
Ichthyoses
MeDOC
PPK
RNAseq
Secondary findings
Variants
Humans
Poland
Female
Male
Serine Peptidase Inhibitor Kazal-Type 5/genetics metabolism
Transglutaminases/genetics metabolism
High-Throughput Nucleotide Sequencing
Ichthyosis/genetics metabolism pathology
Mutation/genetics
Adult

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Wertheim-Tysarowska, K., Osipowicz, K., Wozniak, K., Sawicka, J., Mika, A., Kutkowska-Kazmierczak, A., Niepokój, K., Sobczynska-Tomaszewska, A., Wawrzycki, B., Pietrzak, A., Smigiel, R., Wojtas, B., Gielniewski, B., Szabelska-Beresewicz, A., Zyprych-Walczak, J., Rygiel, A. M., Domaszewicz, A., Braun-Walicka, N., Grabarczyk, A., ... Gostynski, A. (2024). Molecular analysis of inherited disorders of cornification in polish patients show novel variants and functional data and provokes questions on the significance of secondary findings. Orphanet Journal of Rare Diseases, 19(1), Article 413. https://doi.org/10.1186/s13023-024-03395-4

@article{d541fd333dc7428f83573f2fa8449ced,

title = "Molecular analysis of inherited disorders of cornification in polish patients show novel variants and functional data and provokes questions on the significance of secondary findings",

abstract = "BACKGROUND: The Mendelian Disorders of Cornification (MeDOC) comprise a large number of disorders that present with either localised (palmoplantar keratoderma, PPK) or generalised (ichthyoses) signs. The MeDOC are highly heterogenic in terms of genetics and phenotype. Consequently, diagnostic process is challenging and before implementation of the next generation sequencing, was mostly symptomatic, not causal, which limited research on those diseases. The aim of the study was to genetically characterise a cohort of 265 Polish patients with MeDOC and to get insight into the skin lesions using transcriptome and lipid profile analyses. RESULTS: We detected causal variants in 85% (226/265) patients. In addition to the primary gene defect, a pathogenic variant in another gene involved in MeDOC pathology was identified in 23 cases. We found 150 distinct variants in 33 genes, including 32 novel and 16 recurrent (present in > 5 alleles). In 43 alleles large rearrangements were detected, including deletions in the STS, SPINK5, CERS3 and recurrent duplication of exons 10-14 in TGM1. The RNA analysis using samples collected from 18 MeDOC patients and 22 controls identified 1377 differentially expressed genes - DEG. The gene ontology analysis revealed that 114 biological processes were upregulated in the MeDOC group, including i.e. epithelial cell differentiation, lipid metabolic process; homeostasis; regulation of water loss via skin; peptide cross-linking. The DEG between TGM1 and ALOX12B patients, showed that RNA profile is highly similar, though fatty acid profile in epidermal scrapings of those patients showed differences e.g. for the very long chain fatty acids (VLCFAs; FAs = C20), the very long-chain monounsaturated fatty acids (VLC-MUFAs, FAs = C20:1) and the n6 polyunsaturated fatty acids (n6 PUFAs). CONCLUSION: Our results show that NGS-based analysis is an effective MeDOC diagnostic tool. The Polish MeDOC patients are heterogenic, however recurrent variants are present. The novel variants and high number of TGM1 and SPINK5 copy number variations give further insight into molecular pathology of MeDOC. We show that secondary variants in MeDOC-related genes are present in a significant group of patients, which should be further investigated in the context of phenotype modifiers. Finally, we provide novel RNA and lipid data that characterise molecularly MeDOC epidermis.",

keywords = "Genes, Genodermatoses, Ichthyoses, MeDOC, PPK, RNAseq, Secondary findings, Variants, Humans, Poland, Female, Male, Serine Peptidase Inhibitor Kazal-Type 5/genetics metabolism, Transglutaminases/genetics metabolism, High-Throughput Nucleotide Sequencing, Ichthyosis/genetics metabolism pathology, Mutation/genetics, Adult",

author = "Katarzyna Wertheim-Tysarowska and Katarzyna Osipowicz and Katarzyna Wozniak and Justyna Sawicka and Adrianna Mika and Anna Kutkowska-Kazmierczak and Katarzyna Niepok{\'o}j and Agnieszka Sobczynska-Tomaszewska and Bartlomiej Wawrzycki and Aldona Pietrzak and Robert Smigiel and Bartosz Wojtas and Bartlomiej Gielniewski and Alicja Szabelska-Beresewicz and Joanna Zyprych-Walczak and Rygiel, {Agnieszka Magdalena} and Alicja Domaszewicz and Natalia Braun-Walicka and Alicja Grabarczyk and Sylwia Rzonca-Niewczas and Ruszkowska Lidia and Mateusz Dawidziuk and Dominik Domanski and Tomasz Gambin and Monika Jackiewicz and Katarzyna Duk and Barbara Dorozko and Orest Szczygielski and Natalia Krzesniak and Noszczyk, {Bartlomiej H} and Ewa Obersztyn and Jolanta Wierzba and Artur Barczyk and Jennifer Castaneda and Anna Eckersdorf-Mastalerz and Anna Jakubiuk-Tomaszuk and Pawel Wlasienko and Ilona Jaszczuk and Aleksandra Jezela-Stanek and Jakub Klapecki and {van Geel}, Michel and Cezary Kowalewski and Jerzy Bal and Antoni Gostynski",

year = "2024",

month = nov,

day = "5",

doi = "10.1186/s13023-024-03395-4",

language = "English",

volume = "19",

journal = "Orphanet Journal of Rare Diseases",

issn = "1750-1172",

publisher = "BioMed Central Ltd",

number = "1",

}

Wertheim-Tysarowska, K, Osipowicz, K, Wozniak, K, Sawicka, J, Mika, A, Kutkowska-Kazmierczak, A, Niepokój, K, Sobczynska-Tomaszewska, A, Wawrzycki, B, Pietrzak, A, Smigiel, R, Wojtas, B, Gielniewski, B, Szabelska-Beresewicz, A, Zyprych-Walczak, J, Rygiel, AM, Domaszewicz, A, Braun-Walicka, N, Grabarczyk, A, Rzonca-Niewczas, S, Lidia, R, Dawidziuk, M, Domanski, D, Gambin, T, Jackiewicz, M, Duk, K, Dorozko, B, Szczygielski, O, Krzesniak, N, Noszczyk, BH, Obersztyn, E, Wierzba, J, Barczyk, A, Castaneda, J, Eckersdorf-Mastalerz, A, Jakubiuk-Tomaszuk, A, Wlasienko, P, Jaszczuk, I, Jezela-Stanek, A, Klapecki, J, van Geel, M, Kowalewski, C, Bal, J & Gostynski, A 2024, 'Molecular analysis of inherited disorders of cornification in polish patients show novel variants and functional data and provokes questions on the significance of secondary findings', Orphanet Journal of Rare Diseases, vol. 19, no. 1, 413. https://doi.org/10.1186/s13023-024-03395-4

Molecular analysis of inherited disorders of cornification in polish patients show novel variants and functional data and provokes questions on the significance of secondary findings. / Wertheim-Tysarowska, Katarzyna; Osipowicz, Katarzyna; Wozniak, Katarzyna et al.
In: Orphanet Journal of Rare Diseases, Vol. 19, No. 1, 413, 05.11.2024.

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

TY - JOUR

T1 - Molecular analysis of inherited disorders of cornification in polish patients show novel variants and functional data and provokes questions on the significance of secondary findings

AU - Wertheim-Tysarowska, Katarzyna

AU - Osipowicz, Katarzyna

AU - Wozniak, Katarzyna

AU - Sawicka, Justyna

AU - Mika, Adrianna

AU - Kutkowska-Kazmierczak, Anna

AU - Niepokój, Katarzyna

AU - Sobczynska-Tomaszewska, Agnieszka

AU - Wawrzycki, Bartlomiej

AU - Pietrzak, Aldona

AU - Smigiel, Robert

AU - Wojtas, Bartosz

AU - Gielniewski, Bartlomiej

AU - Szabelska-Beresewicz, Alicja

AU - Zyprych-Walczak, Joanna

AU - Rygiel, Agnieszka Magdalena

AU - Domaszewicz, Alicja

AU - Braun-Walicka, Natalia

AU - Grabarczyk, Alicja

AU - Rzonca-Niewczas, Sylwia

AU - Lidia, Ruszkowska

AU - Dawidziuk, Mateusz

AU - Domanski, Dominik

AU - Gambin, Tomasz

AU - Jackiewicz, Monika

AU - Duk, Katarzyna

AU - Dorozko, Barbara

AU - Szczygielski, Orest

AU - Krzesniak, Natalia

AU - Noszczyk, Bartlomiej H

AU - Obersztyn, Ewa

AU - Wierzba, Jolanta

AU - Barczyk, Artur

AU - Castaneda, Jennifer

AU - Eckersdorf-Mastalerz, Anna

AU - Jakubiuk-Tomaszuk, Anna

AU - Wlasienko, Pawel

AU - Jaszczuk, Ilona

AU - Jezela-Stanek, Aleksandra

AU - Klapecki, Jakub

AU - van Geel, Michel

AU - Kowalewski, Cezary

AU - Bal, Jerzy

AU - Gostynski, Antoni

PY - 2024/11/5

Y1 - 2024/11/5

N2 - BACKGROUND: The Mendelian Disorders of Cornification (MeDOC) comprise a large number of disorders that present with either localised (palmoplantar keratoderma, PPK) or generalised (ichthyoses) signs. The MeDOC are highly heterogenic in terms of genetics and phenotype. Consequently, diagnostic process is challenging and before implementation of the next generation sequencing, was mostly symptomatic, not causal, which limited research on those diseases. The aim of the study was to genetically characterise a cohort of 265 Polish patients with MeDOC and to get insight into the skin lesions using transcriptome and lipid profile analyses. RESULTS: We detected causal variants in 85% (226/265) patients. In addition to the primary gene defect, a pathogenic variant in another gene involved in MeDOC pathology was identified in 23 cases. We found 150 distinct variants in 33 genes, including 32 novel and 16 recurrent (present in > 5 alleles). In 43 alleles large rearrangements were detected, including deletions in the STS, SPINK5, CERS3 and recurrent duplication of exons 10-14 in TGM1. The RNA analysis using samples collected from 18 MeDOC patients and 22 controls identified 1377 differentially expressed genes - DEG. The gene ontology analysis revealed that 114 biological processes were upregulated in the MeDOC group, including i.e. epithelial cell differentiation, lipid metabolic process; homeostasis; regulation of water loss via skin; peptide cross-linking. The DEG between TGM1 and ALOX12B patients, showed that RNA profile is highly similar, though fatty acid profile in epidermal scrapings of those patients showed differences e.g. for the very long chain fatty acids (VLCFAs; FAs = C20), the very long-chain monounsaturated fatty acids (VLC-MUFAs, FAs = C20:1) and the n6 polyunsaturated fatty acids (n6 PUFAs). CONCLUSION: Our results show that NGS-based analysis is an effective MeDOC diagnostic tool. The Polish MeDOC patients are heterogenic, however recurrent variants are present. The novel variants and high number of TGM1 and SPINK5 copy number variations give further insight into molecular pathology of MeDOC. We show that secondary variants in MeDOC-related genes are present in a significant group of patients, which should be further investigated in the context of phenotype modifiers. Finally, we provide novel RNA and lipid data that characterise molecularly MeDOC epidermis.

AB - BACKGROUND: The Mendelian Disorders of Cornification (MeDOC) comprise a large number of disorders that present with either localised (palmoplantar keratoderma, PPK) or generalised (ichthyoses) signs. The MeDOC are highly heterogenic in terms of genetics and phenotype. Consequently, diagnostic process is challenging and before implementation of the next generation sequencing, was mostly symptomatic, not causal, which limited research on those diseases. The aim of the study was to genetically characterise a cohort of 265 Polish patients with MeDOC and to get insight into the skin lesions using transcriptome and lipid profile analyses. RESULTS: We detected causal variants in 85% (226/265) patients. In addition to the primary gene defect, a pathogenic variant in another gene involved in MeDOC pathology was identified in 23 cases. We found 150 distinct variants in 33 genes, including 32 novel and 16 recurrent (present in > 5 alleles). In 43 alleles large rearrangements were detected, including deletions in the STS, SPINK5, CERS3 and recurrent duplication of exons 10-14 in TGM1. The RNA analysis using samples collected from 18 MeDOC patients and 22 controls identified 1377 differentially expressed genes - DEG. The gene ontology analysis revealed that 114 biological processes were upregulated in the MeDOC group, including i.e. epithelial cell differentiation, lipid metabolic process; homeostasis; regulation of water loss via skin; peptide cross-linking. The DEG between TGM1 and ALOX12B patients, showed that RNA profile is highly similar, though fatty acid profile in epidermal scrapings of those patients showed differences e.g. for the very long chain fatty acids (VLCFAs; FAs = C20), the very long-chain monounsaturated fatty acids (VLC-MUFAs, FAs = C20:1) and the n6 polyunsaturated fatty acids (n6 PUFAs). CONCLUSION: Our results show that NGS-based analysis is an effective MeDOC diagnostic tool. The Polish MeDOC patients are heterogenic, however recurrent variants are present. The novel variants and high number of TGM1 and SPINK5 copy number variations give further insight into molecular pathology of MeDOC. We show that secondary variants in MeDOC-related genes are present in a significant group of patients, which should be further investigated in the context of phenotype modifiers. Finally, we provide novel RNA and lipid data that characterise molecularly MeDOC epidermis.

KW - Genes

KW - Genodermatoses

KW - Ichthyoses

KW - MeDOC

KW - PPK

KW - RNAseq

KW - Secondary findings

KW - Variants

KW - Humans

KW - Poland

KW - Female

KW - Male

KW - Serine Peptidase Inhibitor Kazal-Type 5/genetics metabolism

KW - Transglutaminases/genetics metabolism

KW - High-Throughput Nucleotide Sequencing

KW - Ichthyosis/genetics metabolism pathology

KW - Mutation/genetics

KW - Adult

U2 - 10.1186/s13023-024-03395-4

DO - 10.1186/s13023-024-03395-4

M3 - Article

SN - 1750-1172

VL - 19

JO - Orphanet Journal of Rare Diseases

JF - Orphanet Journal of Rare Diseases

IS - 1

M1 - 413

ER -

Molecular analysis of inherited disorders of cornification in polish patients show novel variants and functional data and provokes questions on the significance of secondary findings

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Keywords

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