Telomerase mutations in smokers with severe emphysema
Susan E. Stanley, Julian J.L. Chen, Joshua D. Podlevsky, Jonathan K. Alder, Nadia N. Hansel, Rasika A. Mathias, Xiaodong Qi, Nicholas M. Rafaels, Robert A. Wise, Edwin K. Silverman, Kathleen C. Barnes, Mary Armanios
Susan E. Stanley, Julian J.L. Chen, Joshua D. Podlevsky, Jonathan K. Alder, Nadia N. Hansel, Rasika A. Mathias, Xiaodong Qi, Nicholas M. Rafaels, Robert A. Wise, Edwin K. Silverman, Kathleen C. Barnes, Mary Armanios
View: Text | PDF
Research Article Pulmonology

Telomerase mutations in smokers with severe emphysema

Abstract

Mutations in the essential telomerase genes TERT and TR cause familial pulmonary fibrosis; however, in telomerase-null mice, short telomeres predispose to emphysema after chronic cigarette smoke exposure. Here, we tested whether telomerase mutations are a risk factor for human emphysema by examining their frequency in smokers with chronic obstructive pulmonary disease (COPD). Across two independent cohorts, we found 3 of 292 severe COPD cases carried deleterious mutations in TERT (1%). This prevalence is comparable to the frequency of alpha-1 antitrypsin deficiency documented in this population. The TERT mutations compromised telomerase catalytic activity, and mutation carriers had short telomeres. Telomerase mutation carriers with emphysema were predominantly female and had an increased incidence of pneumothorax. In families, emphysema showed an autosomal dominant inheritance pattern, along with pulmonary fibrosis and other telomere syndrome features, but manifested only in smokers. Our findings identify germline mutations in telomerase as a Mendelian risk factor for COPD susceptibility that clusters in autosomal dominant families with telomere-mediated disease including pulmonary fibrosis.

Authors

Susan E. Stanley, Julian J.L. Chen, Joshua D. Podlevsky, Jonathan K. Alder, Nadia N. Hansel, Rasika A. Mathias, Xiaodong Qi, Nicholas M. Rafaels, Robert A. Wise, Edwin K. Silverman, Kathleen C. Barnes, Mary Armanios

×

Figure 3

Pedigrees of telomere syndrome cases with emphysema.

Options: View larger image (or click on image) Download as PowerPoint
Pedigrees of telomere syndrome cases with emphysema. (A) Pedigrees of em...
(A) Pedigrees of emphysema cases with telomere defects and their relatives’ clinical history. The asterisk denotes individuals with DNA sequence data available and/or telomere length measurement performed. Boldface indicates individuals who carried the mutant gene and/or had very short telomeres (shown in B). DC, dyskeratosis congenita, a telomere syndrome defined by mucocutaneous features; CS, positive smoking history; NS, never-smoker; BMF, bone marrow failure; d., age at death from lung disease; ds, disease. (B) Measurement of lymphocyte telomere length by flow cytometry and FISH shows the short telomere defect in affected members relative to age-matched controls. The nomogram was based on data from 400 controls. (C–F) Apical and mid-lung chest CT cuts from two female cases (2.II.1 [C and D] and 5.II.3 [E and F]) show severe apical emphysema with blebs. In addition, 2.II.1 has a right-sided pneumothorax that arose spontaneously.