[HTML][HTML] Danazol treatment for telomere diseases
DM Townsley, B Dumitriu, D Liu… - … England Journal of …, 2016 - Mass Medical Soc
DM Townsley, B Dumitriu, D Liu, A Biancotto, B Weinstein, C Chen, N Hardy, AD Mihalek…
New England Journal of Medicine, 2016•Mass Medical SocBackground Genetic defects in telomere maintenance and repair cause bone marrow
failure, liver cirrhosis, and pulmonary fibrosis, and they increase susceptibility to cancer.
Historically, androgens have been useful as treatment for marrow failure syndromes. In
tissue culture and animal models, sex hormones regulate expression of the telomerase
gene. Methods In a phase 1–2 prospective study involving patients with telomere diseases,
we administered the synthetic sex hormone danazol orally at a dose of 800 mg per day for a …
failure, liver cirrhosis, and pulmonary fibrosis, and they increase susceptibility to cancer.
Historically, androgens have been useful as treatment for marrow failure syndromes. In
tissue culture and animal models, sex hormones regulate expression of the telomerase
gene. Methods In a phase 1–2 prospective study involving patients with telomere diseases,
we administered the synthetic sex hormone danazol orally at a dose of 800 mg per day for a …
Background
Genetic defects in telomere maintenance and repair cause bone marrow failure, liver cirrhosis, and pulmonary fibrosis, and they increase susceptibility to cancer. Historically, androgens have been useful as treatment for marrow failure syndromes. In tissue culture and animal models, sex hormones regulate expression of the telomerase gene.
Methods
In a phase 1–2 prospective study involving patients with telomere diseases, we administered the synthetic sex hormone danazol orally at a dose of 800 mg per day for a total of 24 months. The goal of treatment was the attenuation of accelerated telomere attrition, and the primary efficacy end point was a 20% reduction in the annual rate of telomere attrition measured at 24 months. The occurrence of toxic effects of treatment was the primary safety end point. Hematologic response to treatment at various time points was the secondary efficacy end point.
Results
After 27 patients were enrolled, the study was halted early, because telomere attrition was reduced in all 12 patients who could be evaluated for the primary end point; in the intention-to-treat analysis, 12 of 27 patients (44%; 95% confidence interval [CI], 26 to 64) met the primary efficacy end point. Unexpectedly, almost all the patients (11 of 12, 92%) had a gain in telomere length at 24 months as compared with baseline (mean increase, 386 bp [95% CI, 178 to 593]); in exploratory analyses, similar increases were observed at 6 months (16 of 21 patients; mean increase, 175 bp [95% CI, 79 to 271]) and 12 months (16 of 18 patients; mean increase, 360 bp [95% CI, 209 to 512]). Hematologic responses occurred in 19 of 24 patients (79%) who could be evaluated at 3 months and in 10 of 12 patients (83%) who could be evaluated at 24 months. Known adverse effects of danazol — elevated liver-enzyme levels and muscle cramps — of grade 2 or less occurred in 41% and 33% of the patients, respectively.
Conclusions
In our study, treatment with danazol led to telomere elongation in patients with telomere diseases. (Funded by the National Institutes of Health; ClinicalTrials.gov number, NCT01441037.)
The New England Journal Of Medicine