Comparing Treatment Efficacy With Mepolizumab and Omalizumab in Severe Asthma - "Choosebetweenamab".

Study Description

Brief Summary

Mepolizumab is an anti-interleukin-5 ( IL-5) monoclonal antibody that neutralizes IL-5 and reduces eosinophil counts in both sputum and blood. Omalizumab is an anti-immunoglobulin E (IgE) monoclonal antibody (mAb) used in the treatment of severe allergic eosinophilic asthma

The investigators propose that in patients with the dual phenotypes of severe allergic and eosinophilic asthma, that Mepolizumab is as effective as Omalizumab. However, this trial will also identify key clinical biomarkers that will clarify which patients will respond best to each of these interventions.

This study will be the first direct clinical comparison of these agents and will apply expert clinical characterization, along with cutting edge biotechnology to better inform treatment choices for severe asthma. This is an important and urgent management problem facing the Australian pharmaceutical scheme, where imprecision in prescribing will result in reduced clinical effectiveness as well as substantial and sustained costs.

Detailed Description

'Choosebetweenamab' will compare active treatment arms (Mepolizumab and Omalizumab) for efficacy and adverse events in a Phase 4, parallel arm, randomized controlled trail setting with computer generated randomization (permuted block randomization, with block sizes of 4 or 6, stratified by baseline eosinophil count using a median split). There is no placebo control. Particpants will not be blinded but masking will be used for people assessing outcomes and analyzing data.

'Chossebetweenamab' will also include a secondary outcome substudy (ISS 11066) to assess biomarkers of efficacy response to treatment using single cell sequencing of peripheral blood cells. Blood samples are taken from the randomized patients in each treatment arm (Mepolizumab and Omalizumab) at baseline and gene expression changes assessed using transcriptomic single cell sequencing of patient white blood cells. The data generated from this will be compared to the clinical outcomes of 'Choosebetweenamab' at all follow-up time points. Single cell gene expression and cell type cluster patterning will be compared to the primary and secondary outcomes to identify baseline predictors (gene and cell type) of treatment efficacy.

Study Design

Outcome Measures

Primary Outcome Measures

1. ACQ5 [Assessed after 6 months treatment]

   The primary outcome will be Asthma control questionairre (ACQ)5, adjusted for baseline ACQ5

Secondary Outcome Measures

1. Exacerbations [every month up to 6 months after treatment commenced]

   Number of Exacerbations, requiring change in oral corticosteroids, with either a course of prednisone for at least 3 days, or in those on regular OCS an increase in dose of at least 50% for at least 3 days. Patient reported monthly

2. Time to first exacerbation reported, by patient or health provider [every month up to 6 months after treatment commenced]

   Time to first exacerbation reported, by patient or health provider

3. Hospital admissions [every month up to 6 months after treatment commenced]

   Number of admissions to hospital patient reported

4. Oral corticosteroids [every month up to 6 months after treatment commenced]

   Reduction in dose of regular OCS, confirmed by health care provider and patient reported

5. Spirometry [every month up to 6 months after treatment commenced]

   Change in spirometry, FEV1., measured at time treatment commences and 6 months after treatment

6. Continuing treatment [6 months post intervention]

   Proportion continuing on Australian PBS treatment (successful treatment). The number at the conclusion of the 6 months that will continue treatment. reported by health provider

7. Adverse events [every month up to 6 months after treatment commenced]

   Adverse events; i.e. injection site reaction, reported. Headaches, reported, rash, reported, allergic reaction, reported. Any other relevant adverse event report. Patient and health care provider reported

8. Emergency department presentation [every month up to 6 months after treatment commenced]

   Number of emergency department presentations, patient and health care provider reported

9. Overall dose of oral corticosteroids [6 months post intervention]

   Overall dose of systemic corticosteroids used during the 6 months after treatment commences. Patients and health care provided

10. Change in gene expression measured by single cell RNA sequencing of peripheral blood cells (ISS 11066) [Measured prior to treatment and clinical outcomes at 6 months after treatment]

    ISS 11066 is a substudy of Choosebetweenamab using transcriptomic single cell sequencing of patient white blood cells from both treatment groups at baseline. The data generated from this will be compared to the above clinical outcomes at all follow-up time points. Single cell gene expression and cell type cluster patterning delineated through bioinformatic data processing will be inputted with clinical outcomes into a GLM to identify baseline predictors (gene and cell type) of treatment effect

Eligibility Criteria

Criteria

Inclusion Criteria:

• Participants must have a duration of asthma of greater than one year.

• They must have confirmed asthma defined as: (i) forced expiratory volume (FEV1) reversibility greater than or equal to 12%, and greater than or equal to 200 mL at baseline within 30 minutes after administration of salbutamol (200 to 400 micrograms), or (ii) airway hyperresponsiveness defined as a greater than 20% decline in FEV1 during a direct bronchial provocation test or greater than 15% decline during an indirect bronchial provocation test, or (iii) peak expiratory flow (PEF) variability of greater than 15% between the two highest and two lowest peak expiratory flow rates during 14 days.

• They must have evidence of poor asthma control despite optimal ICS and long acting beta agonist (LABA), be treated by a respiratory physician or immunologist, and have demonstrated acceptable adherence and inhaler technique. Poor control is defined as: evidence of an FEV1 <80% of predicted in the last year on at least one occasion; treatment with OCS, either daily for at least 6 weeks, or a cumulative dose of OCS of at least 500 mg prednisolone equivalent in the previous 12 months, unless contraindicated or not tolerated.

• In addition they must demonstrate an: (a) an Asthma Control Questionnaire (ACQ-5)38 score of at least 2.0, as assessed in the previous month, and (b) while receiving optimised asthma therapy in the past 12 months, experienced at least 1 admission to hospital for a severe asthma exacerbation, or 1 severe asthma exacerbation, requiring documented use of OCS initiated or increased for at least 3 days, or parenteral corticosteroids prescribed/supervised by a physician.

• They must also demonstrate evidence of a dual allergic/ eosinophilic phenotype. This is defined as: a total serum IgE >30IU/mL, past or current evidence of atopy documented by skin prick testing or radioallergosorbent assay, and the participant must have a blood eosinophil count greater than or equal to 300 cells per microlitre in the last 6 weeks.

Exclusion Criteria:

• Do not fulfil inclusion criteria

• Unable to attend appointments

• Significant psychiatric illness

Contacts and Locations

Locations

Sponsors and Collaborators

• University of Newcastle, Australia
• GlaxoSmithKline

Investigators

• Principal Investigator: Peter Wark, MBBS/PhD, University of Newcastle and Hunter New England Health

Study Documents (Full-Text)

• Informed Consent Form - Jul 17, 2019
• Study Protocol - Jun 19, 2020

More Information

Publications