This is a pilot study to investigate serum prednisolone profiles in: * Patients on high doses of prednisolone for any inflammatory disorder, both in the acute and chronic setting. * Patients stepping up from or down to prednisolone therapy in association with a course of high dose methyl-prednisolone or dexamethasone. The study will comprise 3 groups, including those started on high doses of prednisolone acutely in an inpatient or outpatient setting, participants on chronically high doses, and those receiving a several week course of high dose methylprednisolone or dexamethasone. The study aims to measure prednisolone levels at a number of time points to investigate serum profile differences in those receiving prednisolone acutely compared with longer term steroid use. Further samples will be taken to characterise additional metabolic changes.
Prednisolone is an anti-inflammatory drug widely used to reduce inflammation and immune activation in a number of medical conditions, including asthma, allergy, inflammatory and auto-immune conditions. Its therapeutic actions, however, are accompanied by several adverse side effects, which are more frequent following high doses and long term treatments. The aim is therefore to use the lowest effective dose or highest dose for the shortest treatment required. It has been observed in a select number of patients on replacement prednisolone doses for adrenal insufficiency (AI) that serum prednisolone levels change over time, despite patients remaining on the same dose. It is currently unclear whether serum levels of prednisolone match the doses in patients taking high dose prednisolone, both in the acute and chronic setting, and whether the way in which prednisolone is metabolised is altered after receiving high doses for prolonged periods of time. The rationale for the use of particular doses for particular conditions is not clear, and has been developed historically in the absence of individual patient data. It is possible that more tailored dosing of prednisolone will result in reduced side effects, and that the minimum possible dose may be weight related. In addition, genetic and epigenetic factors may also play a role in the efficacy of prednisolone and in the risk of developing side effects, accounting for some of the inter-individual variation in drug response. Further characterising this may help to create an evidence base to tailor anti-inflammatory doses and weaning regimens of synthetic glucocorticoids that avoid deleterious effects.
Study Type
OBSERVATIONAL
Enrollment
120
Prednisolone given orally prior to taking timed samples for levels
Imperial College Healthcare NHS Trust
London, United Kingdom
RECRUITINGTo elucidate differences in prednisolone pharmacokinetics (in patients receiving high dose prednisolone acutely and in the chronic setting).
This will be assessed by determination of Cmax
Time frame: Pharmacokinetics measurements taken at the first and second visits. This will be of variable duration depending on duration of steroid treatment (5 days up to 2 years)
To elucidate differences in prednisolone pharmacokinetics (in patients receiving high dose
This will be assessed by determination of Tmax
Time frame: Pharmacokinetics measurements taken at the first and second visits. This will be of variable duration depending on duration of steroid treatment (5 days up to 2 years)
To elucidate differences in prednisolone pharmacokinetics (in patients receiving high dose
This will be assessed by determination of prednisolone half life and area under the curve values.
Time frame: Pharmacokinetics measurements taken at the first and second visits. This will be of variable duration depending on duration of steroid treatment (5 days up to 2 years)
To elucidate differences in prednisolone pharmacokinetics (in patients receiving high dose
This will be assessed by determination of urinary steroid profiles.
Time frame: Pharmacokinetics measurements taken at the first and second visits. This will be of variable duration depending on duration of steroid treatment (5 days up to 2 years)
To elucidate further differences in metabolic profiles and glucocorticoid axis
Assessed by review of bloods, including full blood count (FBC), renal profile, liver function tests (LFTs), creatine kinase (CK), Adrenocorticotropic hormone (ACTH), cortisol, cortisol binding globulin (CBG) and bicarbonate.
Time frame: Time points post prednisolone dose at 1st and 2nd visits. This will be of variable duration depending on duration of steroid treatment (5 days up to 2 years)
Exploratory Outcomes
Metabolomic and metagenomic changes in plasma and urine to investigate inter-individual variation in prednisolone Immunology profiles - assessed by measurement and assessment of soluble immunological analytes and isolated white cell populations metabolism
Time frame: Time points post prednisolone dose at 1st and 2nd visits. This will be of variable duration depending on duration of steroid treatment (5 days up to 2 years)
Surrogate markers and risk factors for cardiovascular disease
Anthropometric markers such as blood pressure
Time frame: On 1st and 2nd visits
Surrogate markers and risk factors for cardiovascular disease
Anthropometric markers such as heart rate
Time frame: On 1st and 2nd visits
Surrogate markers and risk factors for cardiovascular disease
Anthropometric markers such as BMI
Time frame: On 1st and 2nd visits. This will be of variable duration depending on duration of steroid treatment (5 days up to 2 years)
Surrogate markers and risk factors for cardiovascular disease
Anthropometric markers such aswaist-hip circumference ratio.
Time frame: On 1st and 2nd visits. This will be of variable duration depending on duration of steroid treatment (5 days up to 2 years)
This platform is for informational purposes only and does not constitute medical advice. Always consult a qualified healthcare professional.