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Clinicogenetic Characterisation of Slc29a3-Related Syndromes: A Case Series, Tracing Ancestral Variants and Molecular Dynamics Simulation Publisher



Biglari S1 ; Shahrooei M2, 3 ; Vahidnezhad F4, 5 ; Youssefian L5, 6 ; Ziaee V7, 8, 9 ; Rezaei N10, 11 ; Moghaddam AS12 ; Sedighzadeh S3 ; Moravej H13 ; Safari Foroushani P14 ; Keivanfar M15, 16 ; Ilkhanipoor H17 ; Hozhabrpour A18, 19 ; Seyedhosseiniaghaheh H20 Show All Authors
Authors
  1. Biglari S1
  2. Shahrooei M2, 3
  3. Vahidnezhad F4, 5
  4. Youssefian L5, 6
  5. Ziaee V7, 8, 9
  6. Rezaei N10, 11
  7. Moghaddam AS12
  8. Sedighzadeh S3
  9. Moravej H13
  10. Safari Foroushani P14
  11. Keivanfar M15, 16
  12. Ilkhanipoor H17
  13. Hozhabrpour A18, 19
  14. Seyedhosseiniaghaheh H20
  15. Mohammadzadeh I21, 22
  16. Naderi M23, 24
  17. Sheikhi Ghayur E25
  18. Mansour Samaei N26, 27, 28
  19. Dorgaleleh S29
  20. Esmaeilzadeh E30
  21. Sherkat R31
  22. Khorram Khorshid HR32
  23. Tabatabaiefar MA1
  24. Hakonarson H5, 33, 34
  25. Vahidnezhad H5, 33, 34, 35

Source: Journal of Medical Genetics Published:2025


Abstract

Background: SLC29A3-related syndromes (SLC29A3-RS) are characterised by severe and multiorgan involvement that has a severe impact on the quality of life of the affected persons and therefore merit further genetic and clinical research. We investigated the clinical and genetic aspects of patients with SLC29A3-RS. Methods: Six pathogenic variants of the SLC29A3 gene were identified in eight families in the current study. RNA sequencing was used for evaluating SLC29A3 variant gene expression and protein stability by molecular dynamics (MD) simulations. This study conducted a Preferred Reporting Items for Systematic Reviews and Meta-Analyses-compliant systematic review of cases across five electronic databases. Results: Genetic analysis revealed six pathogenic variants of the SLC29A3 gene in eight families; one variant was shared among three families, indicating a possible founder effect. The estimated most recent common ancestor for these patients lived approximately 8.5 generations ago. MD studies revealed structural instability in mutant proteins. RNA sequencing also demonstrated that the expression of SLC29A3 was downregulated while the expression of the immune markers CD68 and LYZ was upregulated. A systematic search of 197 patients of different ethnic backgrounds revealed that the following symptoms were frequent findings: hyperpigmentation, hypertrichosis, hearing loss, short stature and hepatomegaly. The age of onset of SLC29A3-RS was 5.53±5.24 years with an IQR of 1.4-8.25 years. Conclusions: The characterisation of the founder variants and the genotype-phenotype correlations helps delineate the phenotype spectrum of SLC29A3-RS, which will facilitate the genetic counselling and screening of the high-risk population. Findings on SLC29A3 variants show the way to proceed in the process of developing the diagnostic and therapeutic methods in the management of SLC29A3-RS. © Author(s) (or their employer(s)) 2025. No commercial re-use. See rights and permissions. Published by BMJ Group.
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