# Bone Marrow Failure Associated With Short Telomeres and Digenic Variants of Uncertain Significance in Telomere Biology Genes

**Authors:** Akhila Vadivelan, Geraldine Aubert, Julian A. Martinez, Alan Ikeda, Satiro De Oliveira, Theodore B. Moore, Vivian Chang

PMC · DOI: 10.1155/crig/2075063 · Case Reports in Genetics · 2025-10-16

## TL;DR

Two patients with bone marrow failure had short telomeres and inherited genetic variants in telomere-related genes, suggesting a possible digenic cause.

## Contribution

The study highlights digenic inheritance of telomere biology disorders through variants of uncertain significance.

## Key findings

- Two patients with bone marrow failure had very low telomere length and inherited VUS in multiple telomere genes.
- Parents of the patients also showed low telomere length but no symptoms, indicating possible asymptomatic carrier status.
- The findings suggest that synergistic VUS in different genes may lead to a penetrant disease phenotype.

## Abstract

Telomere Biology Disorders (TBD) are a group of heritable disorders characterized by short telomeres. We report two patients that presented with bone marrow failure (BMF), who were identified to have low telomere length (TL) and variants of uncertain significance (VUS) in two different telomere genes inherited from their parents. At age 6, Patient 1 had stage 4 neuroblastoma. He was treated with chemotherapy, surgery, immunotherapy, and autologous stem cell rescue. At age 10, he developed pancytopenia. Bone marrow biopsy revealed hypocellular marrow and der (1; 7), associated with myelodysplastic syndrome. Germline genetic evaluation showed a pathogenic variant in DNAJC21 (from father) and VUS in NAF1 (c.1375C > T) (from father) and RTEL1 (c.533T > C) (from mother). The patient was found to have very low TL (VLTL) (< 1st percentile) in 4/6 white blood cell subsets. The patient's mother was found to have borderline low TL (VLTL) ( 1 and < 10th percentiles) in 4/6 subsets and VLTL in 1/6 subsets. Father had VLTL in 1/6 but normal TL in other subsets. Neither parent reported any symptoms of TBD. Patient 2 presented with a depressed skull fracture at age 15. He was found incidentally to have pancytopenia. Bone marrow biopsy showed hypocellular marrow and no cytogenetic abnormalities. The patient had VLTL in all 6/6 subsets. Genetic evaluation showed VUSs in TERT (c.3158-80G > A) (from mother), TINF2 (c.814T > C) (from mother) and SRP72 (c.1928C > T) (from father). Mother was also found to have VLTL in all 6 subsets but has reported good health except for premature graying of hair. These two patients presented with BMF, identified to have VUSs in more than one TBD-associated gene with functional evidence of shortened telomeres, highlighting the potential for a digenic mode of inheritance. Synergy between two VUSs could contribute to a penetrant phenotype and resulting in earlier or more severe onset of disease.

## Linked entities

- **Genes:** DNAJC21 (DnaJ heat shock protein family (Hsp40) member C21) [NCBI Gene 134218], NAF1 (nuclear assembly factor 1 ribonucleoprotein) [NCBI Gene 92345], RTEL1 (regulator of telomere elongation helicase 1) [NCBI Gene 51750], TERT (telomerase reverse transcriptase) [NCBI Gene 7015], TINF2 (TERF1 interacting nuclear factor 2) [NCBI Gene 26277], SRP72 (signal recognition particle 72) [NCBI Gene 6731]
- **Diseases:** myelodysplastic syndrome (MONDO:0018881), neuroblastoma (MONDO:0005072)

## Full-text entities

- **Genes:** SRP72 (signal recognition particle 72) [NCBI Gene 6731] {aka BMFF, BMFS1, HEL103}, DNAJC21 (DnaJ heat shock protein family (Hsp40) member C21) [NCBI Gene 134218] {aka BMFS3, DNAJA5, GS3, JJJ1}, NAF1 (nuclear assembly factor 1 ribonucleoprotein) [NCBI Gene 92345] {aka PFBMFT7}, RTEL1 (regulator of telomere elongation helicase 1) [NCBI Gene 51750] {aka C20orf41, DKCA4, DKCB5, NHL, PFBMFT3, RTEL}, TERT (telomerase reverse transcriptase) [NCBI Gene 7015] {aka CMM9, DKCA2, DKCB4, EST2, PFBMFT1, TCS1}, TINF2 (TERF1 interacting nuclear factor 2) [NCBI Gene 26277] {aka DKCA3, DKCA5, TIN2}
- **Diseases:** depressed skull fracture (MESH:D020204), pancytopenia (MESH:D010198), heritable (MESH:D065627), hypocellular marrow (MESH:D001855), myelodysplastic syndrome (MESH:D009190), TBD (MESH:C536801), BMF (MESH:D000080983), neuroblastoma (MESH:D009447)
- **Species:** Homo sapiens (human, species) [taxon 9606]
- **Mutations:** c.1375C > T, c.3158-80G > A, c.533T > C, c.1928C > T, c.814T > C

## Full text

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## Figures

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## References

38 references — full list in the complete paper: https://tomesphere.com/paper/PMC12549202/full.md

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Source: https://tomesphere.com/paper/PMC12549202