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Clinical Trial
. 2025 Mar;4(3):EVIDoa2400252.
doi: 10.1056/EVIDoa2400252. Epub 2025 Feb 25.

Clinical Use of ZSCAN4 for Telomere Elongation in Hematopoietic Stem Cells

Kasiani C Myers  1   2 Stella M Davies  1   2 Carolyn Lutzko  1   3   4 Robin Wahle  3 David D Grier  1   5 Geraldine Aubert  6 Kevin Norris  7   8 Duncan M Baird  7   8 Minako Koga  9 Akihiro C Ko  10 Tomokazu Amano  10 Misa Amano  10 Hong Yu  10 Minoru S H Ko  10
Affiliations
Clinical Trial

Clinical Use of ZSCAN4 for Telomere Elongation in Hematopoietic Stem Cells

Kasiani C Myers et al. NEJM Evid. 2025 Mar.

Abstract

Background: Extremely short telomeres in patients with dyskeratosis congenita and related telomere biology disorders (TBDs) lead to premature cellular senescence and bone marrow failure. Zinc finger and SCAN domain-containing 4 (ZSCAN4) elongates telomeres by recombination.

Methods: We report a clinical study in which EXG34217, the term given for autologous CD34+ hematopoietic stem cells from patients with TBD exposed to a temperature-sensitive Sendai virus vector encoding human ZSCAN4 at 33°C for 24 hours, was infused into patients without preconditioning.

Results: Four patients were enrolled; two experienced successful CD34+ mobilization during the second mobilization attempt and underwent apheresis and EXG34217 infusion, with follow-up of 5 and 24 months (both ongoing). We observed telomere elongation (1.06- to 1.34-fold) in CD34+ cells ex vivo. In one patient, the treatment was associated with a change in the mean absolute neutrophil count (ANC) from 1.78×103 to 3.18×103 cells/μl; the lymphocyte subpopulation telomere length changed from 3.6 to 6.7 kb (50th percentile for age). In the other patient, the treatment was associated with a change in the lowest ANC from 0.6×103/μl to 1.2×103/μl; this has occurred in 5 months without the patient receiving prior intermittent low-dose granulocyte-colony-stimulating factor injections. During mobilization, all patients experienced mild to moderate bone pain or pain after line replacement, and one patient had a blood infection associated with fever and hypoxemia. After EXG34217 infusion, no acute safety issues were noted; in one patient mild to moderate long-term cardiac and pulmonary adverse events were noted; these were similar to symptoms of the patient's underlying conditions.

Conclusions: Although definitive conclusions cannot be drawn from the two EXG34217-treated patients, these results warrant further investigation of CD34+ cells exposed to ZSCAN4 for treating TBDs. (Funded by Elixirgen Therapeutics; ClinicalTrials.gov number, NCT04211714.).

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