# DNA hypomethylation at specific CG-sites within TRAK1 is linked to the neurocognitive profile in Klinefelter syndrome

**Authors:** Helene B. L. Tallaksen, Emma B. Hasselholm, Joel B. Berletch, Gala N. Filippova, Xinxian Deng, Daniel L. Van Dyke, James W. MacDonald, Theo K. Bammler, Simon Chang, Cecilie D. R. Buskbjerg, Claus H. Gravholt, Christine M. Disteche, Jesper Just, Anne Skakkebæk

PMC · DOI: 10.1038/s41380-025-03254-z · Molecular Psychiatry · 2025-09-30

## TL;DR

This study finds that DNA hypomethylation in the TRAK1 gene is linked to neurocognitive issues in Klinefelter syndrome.

## Contribution

The study links specific DNA methylation changes in TRAK1 to neurocognitive impairments in Klinefelter syndrome for the first time.

## Key findings

- DNA hypomethylation at five CG-sites in TRAK1 is observed in males with Klinefelter syndrome.
- TRAK1 hypomethylation correlates with neurocognitive variables and a specific transcript's high expression.
- Neural precursor cells from 47,XXY cells show TRAK1 hypomethylation and transcript upregulation.

## Abstract

Klinefelter syndrome (47,XXY; KS) impacts neurodevelopment. Furthermore, KS is associated with widespread alterations in the epigenome and transcriptome. Whether these epigenetic and transcriptomic alterations can be linked to the neurocognitive phenotype remains to be elucidated. We performed a comprehensive, integrative analysis of the neurocognitive profile and the methylome in blood from males with KS (n = 65) and male controls (n = 63) (Cohort 1). The results were validated in a second cohort of males with KS (n = 22) and male controls (n = 16) in which transcriptome data was also available (Cohort 2). The findings were further validated in neural precursor cells derived from human induced pluripotent stem cells from 47,XXY (n = 3) and 46,XY (n = 3) amniotic cells. In cohort 1, we identified five CG-sites within the TRAK1 gene which were hypomethylated in males with KS compared to male controls. TRAK1 hypomethylation was positively correlated with several neurocognitive variables among males with KS. In cohort 2, we identified a similar methylation pattern and demonstrated that the methylation levels at the five CG-sites were correlated with a high expression level of a specific short TRAK1 transcript (ENST00000341421.7). Neural precursor cells (NPCs) established from 47,XXY amniotic cells also exhibited hypomethylation at the five CG-sites and strong upregulation of ENST00000341421.7 compared to NPCs established from 46,XY amniotic cells. In conclusion, we demonstrate that the DNA methylation level at specific CG-sites within TRAK1, a gene highly expressed in the brain, is correlated with the neurocognitive phenotype of KS, implying a possible epigenetic underpinning for the observed neurocognitive impairments in KS.

## Linked entities

- **Genes:** TRAK1 (trafficking kinesin protein 1) [NCBI Gene 22906]
- **Diseases:** Klinefelter syndrome (MONDO:0006823)

## Full-text entities

- **Genes:** TRAK1 (trafficking kinesin protein 1) [NCBI Gene 22906] {aka DEE68, EIEE68, MILT1, OIP106}
- **Diseases:** neurocognitive impairments (MESH:D019965), 47,XXY (MESH:D007713)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Full text

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## Figures

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## References

1 references — full list in the complete paper: https://tomesphere.com/paper/PMC12916290/full.md

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Source: https://tomesphere.com/paper/PMC12916290