COVID-19 Clinical Trial
— DEFEAT-COVIDOfficial title:
Targeting de Novo Pyrimidine Biosynthesis by Leflunomide as a Novel Concept for the Treatment of Corona Virus Disease 2019 (COVID-19)
Verified date | February 2023 |
Source | Ashford and St. Peter's Hospitals NHS Trust |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
The global COVID-19 pandemic has caused unprecedented strain on health care services around the world.The absence of specific anti-viral medications to treat the underlying infection led to a proliferation of clinical studies and trials aimed at re-purposing existing medications. Human dihydroorotate dehydrogenase (DHODH) is vital enzyme utilised by viruses to replicate in the host cell. Leflunomide, a drug that is already licenced to treat rheumatoid arthritis, is a potent inhibitor of the enzyme DHODH. Importantly, this drug has dual anti-viral and anti-inflammatory properties so it targets viral replication and suppresses host inflammatory response which plays a role at more progressive stages of infection. DEFEAT-COVID is a multi-site, international, interventional, pragmatic, parallel group design, open label, randomised CTIMP with a pilot phase that will allow to adapt procedures and assessments if required. A phase III clinical trial of leflunomide for treating COVID-19 has been registered in China, Registration number: ChiCTR2000030058). The current proposal extends the original clinical study of leflunomide in China (People's Hospital of Wuhan University) to the UK through a structured collaboration.
Status | Completed |
Enrollment | 178 |
Est. completion date | July 1, 2022 |
Est. primary completion date | July 1, 2022 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: 1. Age =18 years, 2. Patients with onset of symptoms >15 days, 3. Laboratory (RT-PCR) confirmed infection with 2019-nCoV. Exclusion Criteria: 1. Pregnant or breast feeding, 2. On specific monoclonal antibodies, or other drug trial treatment for COVID-19 within one week prior to study enrolment, 3. Liver function tests >2 fold of upper limits of normal (ULN) reference levels of the respective testing assay, 4. Patients with known hypersensitivity to leflunomide, 5. Patients with severe immunodeficiency syndrome and hypoalbuminaemia. |
Country | Name | City | State |
---|---|---|---|
United Kingdom | Ashford and St Peters Hospital NHS Foundation Trust | Chertsey |
Lead Sponsor | Collaborator |
---|---|
Ashford and St. Peter's Hospitals NHS Trust |
United Kingdom,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Other | Evaluation of patient reported symptoms in follow up | Completion of questionnaires to examine persistence of any COVID-19 related symptoms of COVID-19 persisted | 30 and 90 days after discharge | |
Primary | Time to clinical improvement | TTCI is defined as the time (in days) from initiation of trial treatment (for participants in the treatment arm), or day of randomisation (for participants in the control arm), until the first occurrence of;
an improvement of two points on a seven-category ordinal scale of clinical status categories.All surviving patients who have not reached any TTCI ordinal level by Day 28 will be right-censored at that point. live discharge from hospital. |
28 days from randomisation | |
Primary | Incidence of adverse events | All adverse events within 28 days will be recorded and incidence of serious adverse events (SAEs) and Grade 3 and 4 adverse events (AEs)* will be reported.
*Grade 3 adverse events: Severe or medically significant but not immediately life-threatening; or hospitalisation or prolongation of hospitalisation indicated; or disabling; or limiting self-care activity of daily living. Grade 4 Life-threatening consequences; urgent intervention indicated. |
28 days from randomisation | |
Secondary | Changes in virological load over time | Comparing changes in virological load at predefined time periods by comparing proportions of SARS-CoV-2 negativity by RT-PCR and changes in viral load in upper respiratory tract specimens. | Days 0/1, 7,11 and 15 days post randomisation | |
Secondary | Time to hospital discharge | Number of days from randomisation to discharge | Daily assessments during hospitalisation up to 28 days or discharge | |
Secondary | All-cause mortality | Recorded incidence of mortality due to any cause | From randomisation to the event within 28 days | |
Secondary | Duration of intensive care stay | Time from admission to ITU to discharge to another care environment will be recorded for each patient, noting that the start of this period may ante-date the time of randomisation. | From randomisation to 28 days or discharge | |
Secondary | Duration of invasive and non-invasive ventilation | Time from initiation to withdrawal of mechanical ventilation will be recorded, subdivided by whether the ventilation was invasive. | From randomisation to discharge or 28 days | |
Secondary | Incidence of re-intubation | The proportion of patients requiring re-intubation following a decision to extubate | From randomisation to 28 days or discharge | |
Secondary | Incidence of tracheostomy | The proportion of patients requiring tracheostomy | From randomisation to 28 days or discharge | |
Secondary | Degree of acute lung injury | Proportions of patients with mild, moderate and severe lung impairment based on Berlin definition | At baseline, 15 and 28 days or discharge | |
Secondary | Evaluation of surrogate of inflammation and lung recovery | Ratios of arterial and peripheral oxygen saturation divided by fraction of inspired oxygen:
P/F ratio, (i.e. arterial pO2 divided by the FIO2) S/F ratio, (i.e. oxygen saturation divided by the FIO2) |
Daily measurements from randomisation to discharge or 28 days | |
Secondary | Incidence of inotropic/vasoactive support | The proportion of patients needing inotropic/vasoactive support | From randomisation to discharge or 28 days | |
Secondary | Incidence of acute kidney injury | Proportion of patients diagnosed with acute kidney injury by the KDIGO criteria | From randomisation to discharge or 28 days | |
Secondary | Need for renal replacement therapy | Proportion of patients needing renal replacement therapy | From randomisation to discharge or 28 days | |
Secondary | Characterisation of biomarkers including high sensitivity CRP, ferritin, procalcitonin, troponin, BNP, creatinine and kidney biomarkers. | Measurements of these markers will be collected daily | Daily measurements during hospitalisation to 28 days or discharge | |
Secondary | Changes in cytokine profile including pro- and anti-inflammatory cytokines | Measurements for each of the cytokines will be collected at predetermined time points. | Days 0, 1, 3 and 11 |
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