Analysis of the MILES cohort reveals determinants of disease progression and treatment response in lymphangioleiomyomatosis

Abstract

IntroductionThe Multicenter International Lymphangioleiomyomatosis (LAM) Efficacy of Sirolimus (MILES) trial revealed that sirolimus stabilised lung function in patients with moderately severe LAM. The purpose of this study was to further examine the MILES cohort for the effects of racial, demographic, clinical and physiological patient characteristics on disease progression and treatment response in LAM.MethodsMILES subjects were stratified on the basis of menopausal status (pre-menopausal/post-menopausal), race (Asian/Caucasian), bronchodilator responsiveness (present/absent), initial forced expiratory volume in 1 s (FEV1; 51–70%versus≤50% predicted) and tuberous sclerosis complex (TSC) association (yes/no). A linear mixed effects model was used to compare slope differences, and nonparametric tests were used to compare medians and proportions between treatment groups in each stratum.ResultsIn the MILES placebo group, pre-menopausal patients declined 5-fold faster than post-menopausal patients (mean±seFEV1slope −17±3versus−3±3 mL·month−1; p=0.003). Upon treatment with sirolimus, both the pre-menopausal (−17±3versus−1±2 mL·month−1; p<0.0001) and post-menopausal patients (−3±3versus6±3 mL·month−1; p=0.04) exhibited a beneficial response in mean±seFEV1slope compared with the placebo group. Race, LAM subtype, bronchodilator responsiveness or baseline FEV1did not impact the rate of disease progression in the placebo group or treatment response in the sirolimus group. Menopausal status and race had differential effects on the adverse event profile of sirolimus. Baseline serum vascular endothelial growth factor (VEGF)-D >600 pg·mL−1identified subgroups of patients who were more likely to decline on placebo and respond to treatment with sirolimus.ConclusionsIn LAM patients, treatment with sirolimus is beneficial regardless of menopausal status, race, bronchodilator responsiveness, baseline FEV1or TSC association. Serum VEGF-D and menopausal status can help inform therapeutic decisions.