Angiotensin-converting enzyme inhibitors may affect pulmonary function in lymphangioleiomyomatosis
Wendy K. Steagall, Mario Stylianou, Gustavo Pacheco-Rodriguez, Joel Moss
Wendy K. Steagall, Mario Stylianou, Gustavo Pacheco-Rodriguez, Joel Moss
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Clinical Research and Public Health Pulmonology Therapeutics

Angiotensin-converting enzyme inhibitors may affect pulmonary function in lymphangioleiomyomatosis

Abstract

INTRODUCTION. A local renin-angiotensin system exists in the pulmonary nodules of lymphangioleiomyomatosis patients. Sirolimus, the standard treatment for lymphangioleiomyomatosis, stabilizes lung function, but all patients do not respond to or tolerate sirolimus. As renin-angiotensin systems may affect tumor growth and metastasis, we questioned if angiotensin-converting enzyme inhibitors affected lymphangioleiomyomatosis disease progression. METHODS. Retrospective study of 426 patients was performed, examining angiotensin-converting enzyme levels, pulmonary function data, and angiotensin-converting enzyme inhibitor treatment. RESULTS. Serum angiotensin-converting enzyme levels were elevated in approximately 33% of patients, increased with duration of disease, and were inversely correlated with pulmonary function. Levels decreased significantly over time with sirolimus treatment. Treatment with angiotensin-converting enzyme inhibitors was reported by approximately 15% of patients and was significantly associated with a slower rate of decline in percentage predicted forced expiratory volume (FEV1) and diffusing capacity of the lungs for carbon monoxide (DLCO) in patients not treated with sirolimus. No significant differences in rates of decline of FEV1 or DLCO were seen in patients treated with both inhibitors and sirolimus versus sirolimus alone. CONCLUSIONS. Angiotensin-converting enzyme inhibitors may slow decline of pulmonary function in patients with lymphangioleiomyomatosis not treated with sirolimus. These inhibitors may be an option or adjunct in the treatment of lymphangioleiomyomatosis. A clinical trial may be warranted to examine this possibility. FUNDING. NIH.

Authors

Wendy K. Steagall, Mario Stylianou, Gustavo Pacheco-Rodriguez, Joel Moss

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Figure 4

Serum ACE activity was inversely correlated with FEV1 and DLCO.

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Serum ACE activity was inversely correlated with FEV1 and DLCO. Serum AC...
Serum ACE activity was inversely correlated with percentage predicted FEV1 (A) and DLCO (B) (both P < 0.001) using mixed-effects models controlling for initial values and sirolimus treatment. Measurements of ACE activity from 330 patients (including both measurements before and during sirolimus treatment; 257 patients never began sirolimus therapy, 59 patients have measurements both before and during therapy, and 14 patients have measurements only during therapy) were compared to the percentage predicted FEV1 or DLCO values recorded at the same visit to the NIH. The trend lines on the graphs were created by Excel and are for visual purposes only, as mathematical models were created for both percentage predicted FEV1 and DLCO. The models for patients not on sirolimus are (i) FEV1 = 18.4895 + (0.9156 × [initial FEV1]) – (0.06942 × [ACE activity]) – 10.4531 – (1.4638 × time); (ii) DLCO = 17.4347 + (0.9044 × [initial DLCO]) – (0.09381 × [ACE activity]) – 8.9540 – (1.4636 × time). During sirolimus therapy, the models are (iii) FEV1 = 18.4895 + (0.9156 × [initial FEV1]) – (0.06942 × [ACE activity]) – (1.4638 × time); (iv) DLCO = 17.4347 + (0.9044 × [initial DLCO]) – (0.09381 × [ACE activity]) – (1.4636 × time).