Effect of Fluticasone/Salmeterol on Chronic Bronchitis Symptoms and Associated Patient Reported Outcomes: a post-hoc analysis of the TORCH trial

Proposal
1640

Title of Proposed Research

Lead Researcher

Victor Kim

Affiliation

Lewis Katz School of Medicine, Temple University.

Funding Source

None

Potential Conflicts of Interest

Funded by NHLBI K23HL094696; Chairman, Critical Care Test Writing Committee, American Board of Internal Medicine; Member, Exam Chairs Committee, American Board of Internal Medicine; Advisory boards for Astra Zeneca, Concert Pharmaceuticals, Gala Therapeutics, CSA Medical

Data Sharing Agreement Date

28 February 2017

Lay Summary

Chronic Obstructive Pulmonary Disease (COPD) affects 12-16 million people in the US and is the third leading cause of death worldwide. COPD encompasses a spectrum of diseases, with chronic bronchitis (CB, defined as chronic cough and phlegm production) at one end and emphysema at the other, with most individuals having some characteristics of both. CB affects 3.4-22.0% of all adults, and CB affects anywhere from 14-74% of COPD patients. CB has been shown in numerous studies to increase COPD “flare-ups” (i.e. exacerbations), increase breathlessness, reduce quality of life and physical functioning, and may increase mortality. Despite this, few studies have analyzed the effects of inhaled medications on CB to date. The TORCH trial randomized patients with COPD to placebo, salmeterol, fluticasone, or fluticasone/salmeterol therapy for three years. The primary endpoint of a decrease in mortality was unfortunately not met, most likely because of a high dropout rate and a less than anticipated level of mortality in the placebo group. The three non-placebo groups did experience improvements in health related quality of life, a reduction in lung function decline, and reduced numbers of exacerbations. However, the study did not classify patients into whether or not they had CB at baseline. Conceptually, the use of an inhaled corticosteroid (i.e. fluticasone) would decrease symptoms of CB because of its known effects on reducing airway inflammation. This has unfortunately never been shown in a large, randomized controlled trial. Therefore, this analysis of previously collected data is paramount to ascertaining whether fluticasone or fluticasone/salmeterol combination reduces CB symptoms and associated COPD-related outcomes. We hypothesize that those receiving fluticasone, whether alone or with salmeterol, will have a greater reduction of CB symptoms and exacerbations in those with CB compared to those without CB. Should our hypothesis be correct, it will revolutionize the way physicians treat patients with CB in the era of personalized medicine. To prove this, we propose the following:1) We will determine which patients in the TORCH trial had CB at study entry using a proven novel definition of CB derived from the Saint George's Respiratory Questionnaire (SGRQ), a validated measure of COPD health related quality of life. We will ascertain how many patients in each of the four arms of the trial had CB. 2) We will compare the various outcomes between those with and without CB in each arm, in order to see if the treatments had a greater benefit in those with CB. As the SGRQ, lung function, exacerbations, side effects, and mortality were tracked at regular intervals, we will be able to determine the effects of therapy in those with and without CB over the course of three years. Additionally, we will be able to determine if there was a greater reduction in cough and phlegm symptoms in those with CB compared to those without CB.

Study Data Provided

[{ "PostingID": 416, "Title": "GSK-SCO30003", "Description": "A multicentre, randomised, double-blind, parallel group, placebo-controlled study to investigate the long-term effects of salmeterol/fluticasone propionate (SERETIDE® inhaler) 50/500mcg BD, salmeterol 50mcg BD and fluticasone propionate 500mcg BD, all delivered via the DISKUS®/ACCUHALER® inhaler, on mortality and morbidity of subjects with chronic obstructive pulmonary disease (COPD) over 3 years of treatment" }]

Statistical Analysis Plan

Subjects: We will determine if the subjects at study entry had CB based on a novel definition that is comparable to the classic definition from the cough and phlegm questions in the SGRQ (15). The subjects will be classified as CB+ if they answer “almost every day” or “most days a week” to the 2 following questions: “Over the last 4 weeks I have coughed” and “Over the last 4 weeks I have brought up phlegm (sputum).” The groups (SGRQ CB+ vs. SGRQ CB-) in each arm will be compared using descriptive statistics; the groups will be tested for normality and if normally distributed will be compared with t test, and if non-normal will be compared with Mann Whitney U test or the data will be log transformed to make the distribution normal. Categorical variables will be compared with a chi squared test. Primary Endpoint: The primary endpoints are exacerbation frequency and time-to-first exacerbation. Our primary goal is to determine if SGRQ CB+ subjects receiving fluticasone with or without salmeterol have a greater reduction in exacerbation frequency in comparison to those receiving salmeterol alone or placebo. We also wish to determine if the reduction in exacerbations is greater in SGRQ CB+ subjects compared to SGRQ CB- subjects in each arm. Therefore, we will compare the exacerbation frequency in SGRQ CB+ subjects in the four arms of the study (fluticasone/salmeterol, fluticasone, salmeterol, or placebo). We will also compare the exacerbation frequency in SGRQ CB- subjects in the four arms. Finally, we will compare the exacerbation frequency in SGRQ CB+ subjects and SGRQ CB- subjects in each arm (i.e. SGRQ CB+ exacerbation frequency vs. SGRQ CB- exacerbation frequency in the fluticasone/salmeterol arm, in the fluticasone arm, in the salmeterol arm, and in the placebo arm). The frequency of exacerbations will be analyzed with a generalized linear model (assuming a negative binomial distribution, which accounts for variability among patients in the number and frequency of exacerbations), with the number of exacerbations as the outcome of interest and the logarithm of time during which treatment was received as an offset variable. Time to first exacerbation will also be a primary endpoint. Kaplan-Meier analysis will be performed using log-rank test to compare exacerbation-free survival curves between groups. A cox proportional hazards model will be used to develop hazard ratios for time to first exacerbation, using several known risk factors for exacerbations as covariates. Rate ratios will be calculated comparing the various groups (i.e. the four arms in SGRQ CB+ patients, the four arms in SGRQ CB- patients, and SGRQ CB+ vs. SGRQ CB- patients in each arm).Secondary Endpoints: The secondary endpoints are SGRQ scores, lung function and mortality. Total scores, as well as subscores (symptoms, activity, and impact) of the SGRQ and post-bronchodilator FEV1 will be analyzed as changes from baseline values with the use of repeated-measures analysis of covariance (ANCOVA). Estimated differences between treatments at each visit will be averaged with equal weights to determine the overall treatment effect during the 3-year study period. All efficacy analyses will be performed according to the intention-to-treat principle. Comparisons other than those between the combination regimen and placebo and between the combination regimen and salmeterol alone will be exploratory. The difference in times to death from any cause in each arm between the CB+ group and CB- group will be analyzed with the log-rank test (with stratification according to smoking status) and Cox regression. We will use CB status and smoking status as time varying covariates in our Cox regression models. We will also test for interactions between CB status and treatment arm in our Cox regression analyses.We understand now that CB may be a time varying covariate; recent evidence has shown that CB can wax and wane, particularly in relationship to smoking status (16, 17). To account for this, we will perform an analysis similar to the Evaluation of COPD Longitudinally to Identify Predictive Surrogate Endpoints (ECLIPSE) trial (18) (see publication for more detail). We will assess the stability of the SGRQ CB+ phenotype over time in each arm. We will determine how many subjects in each arm that were SGRQ CB+ at study initiation who were still SGRQ CB+ at years 1, 2, and 3 using a repeated measures analysis. We hypothesize that in those in the fluticasone arms will be more likely to have converted to SGRQ CB- in follow-up years compared to the salmeterol alone or placebo arms.Power analysis: According to our recent publication, 45.6% of the 2148 subjects in COPDGene with an FEV1=60% predicted (similar to the population in the TORCH trial) were SGRQ CB+ (15). Using the SGRQ CB definition at study initiation, we found that the SGRQ CB+ group had a greater exacerbation frequency compared to the SGRQ CB- group in longitudinal follow-up (1.11±1.62 vs. 0.77±1.17 exacerbations/patient/year, p<0.0001; mean±SD 4.44±1.75 years followed).SGRQ CB+ was statistically significant in multivariable linear regression using other covariates associated with exacerbations (ß coeff 0.266, SE 0.066, p<0.0001). The calculated effect size is 0.24 from these data. There were approximately 1,500 subjects in each arm of the TORCH trial. Using G-power to estimate the sample size, we will need 734 subjects in each arm to have 90% power with a of 0.05 to detect an effect size of 0.24. Therefore, there should be enough subjects in each arm to adequately detect at least a similar difference between SGRQ CB+ and SGRQ CB- groups.

Publication Citation

https://www.atsjournals.org/doi/abs/10.1164/ajrccm-conference.2018.197.1_MeetingAbstracts.A7727