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.-Reference-Cited by-同舟云学术

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.

Published:2024-03-11 Issue: Volume: Page:
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Author:

Wertheim-Tysarowska Katarzyna¹^ORCID,Osipowicz Katarzyna²,Woźniak Katarzyna²,Sawicka Justyna¹,Mika Adrianna³,Kutkowska-Kaźmierczak Anna¹,Niepokój Katarzyna¹,Sobczyńska-Tomaszewska Agnieszka⁴,Wawrzycki Bartłomiej⁵,Pietrzak Aldona⁵,Śmigiel Robert⁶,Wojtaś Bartosz⁷,Gielniewski Bartłomiej⁷,Szabelska-Beresewicz Alicja⁸,Zyprych-Walczak Joanna⁸,Rygiel Agnieszka Magdalena¹,Domaszewicz Alicja¹,Braun-Walicka Natalia¹,Grabarczyk Alicja¹,Rzońca-Niewczas Sylwia¹,Lidia Ruszkowska⁹,Dawidziuk Mateusz¹,Domański Dominik¹⁰,Gambin Tomasz¹,Jackiewicz Monika¹,Duk Katarzyna¹,Dorożko Barbara¹,Szczygielski Orest¹,Krześniak Natalia¹¹,Noszczyk Bartłomiej H¹²,Obersztyn Ewa¹,Wierzba Jolanta³,Barczyk Artur¹,Castaneda Jennifer¹,Eckersdorf-Mastalerz Anna¹³,Jakubiuk-Tomaszuk Anna¹⁴,Własienko Paweł¹,Jaszczuk Ilona⁵,Jezela-Stanek Aleksandra¹⁵,Klapecki Jakub¹,Geel Michel van¹⁶,Kowalewski Cezary²,Bal Jerzy¹,Gostyński Antoni¹⁶

Affiliation:

1. Institute of Mother and Child Care: Instytut Matki i Dziecka

2. Medical University of Warsaw: Warszawski Uniwersytet Medyczny

3. Medical University of Gdansk: Gdanski Uniwersytet Medyczny

4. MedGen Medical Center

5. Medical University of Lublin: Uniwersytet Medyczny w Lublinie

6. Wroclaw Medical University: Uniwersytet Medyczny im Piastow Slaskich we Wroclawiu

7. Nencki Institute of Experimental Biology: Instytut Biologii Doswiadczalnej im M Nenckiego Polskiej Akademii Nauk

8. Poznan University of Life Sciences: Uniwersytet Przyrodniczy w Poznaniu

9. Miedzyleski Specialistic Hospital in Warsaw

10. Institute of Biochemistry and Biophysics Polish Academy of Sciences: Instytut Biochemii i Biofizyki Polskiej Akademii Nauk

11. Centre of Postgraduate Medical Education, Prof. W Orlowski Memorial Hospital

12. Centre of Postrgraduate Mdical Education, Porf. W. Orlowski Memorial Hospital

13. Medical Center Fundacja PoMoc

14. Medical Genetics Unit Mastermed

15. National institute of Tuberculosis and Lung Diseases

16. Maastricht University Medical Centre+: Maastricht Universitair Medisch Centrum+

Abstract

Abstract Background: The Mendelian Disorders of Cornification (MeDOC) comprise a large number of disorders that are manifested by either localised (palmoplantar keratoderma, PPK) or generalised (ichthyoses) symptoms. 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 characterize a cohort of 265 Polish patients with MeDOC and to characterise the skin lesions using transcriptome and lipid profile analyses. Results: We detected causal variants in 85% (225/265) patients. In 23 in addition to the primary gene defect, a pathogenic variant in another gene involved in MeDOC pathology was detected. We found 150 distinct variants in 35 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 eg. 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 gives further insight into molecular pathology of MeDOC. We provide evidence 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.

Publisher

Research Square Platform LLC

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