Evaluation of High Dose Prednisolone Pharmacokinetics in the Acute and Chronic Setting

Last updated: September 27, 2023
Sponsor: Imperial College London
Overall Status: Active - Recruiting

Phase

N/A

Condition

Asthma

Inflammation

Ulcerative Colitis (Pediatric)

Treatment

No intervention - prednisolone is taken as part if routine clinical care.

Clinical Study ID

NCT05012033
21HH6792
  • Ages 18-75
  • All Genders

Study Summary

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.

Eligibility Criteria

Inclusion

Inclusion Criteria:

  • Aged 18 - 75 years
  • Male or female
  • Participants who are otherwise healthy enough to participate, as determined bypre-study medical history
  • Participants who are able and willing to give written informed consent to participatein the study
  • Group A only: Patients requiring acute (<5 days) high dose (minimum 30mg) oralprednisolone therapy for antiinflammatory purposes in either an inpatient oroutpatient setting.
  • Group B only: Minimum of 1 month duration of high dose prednisolone (>30mg) if in thechronic use group.
  • Group C only: Patients started on high dose methylprednisolone (>3 day course) orprolonged courses of dexamethasone.

Exclusion

Exclusion Criteria:

  • Participants with a diagnosis of Type 1 or Type 2 diabetes mellitus.
  • Unable to give informed consent.
  • Taking supplements or herbal medications that the participant is unwilling or unableto stop prior to and during the study period e.g. St John's Wort (may decreaseprednisolone levels), Cat's claw, Echinacea (immunomodulatory properties).
  • Currently taking medications that alter CYP3A4 metabolism of glucocorticoids that theparticipant is unwilling or unable to stop prior to and during the study period e.g.phenytoin, phenobarbital, rifampicin, rifabutin, carbamazepine, primidone,aminogluethimide, itraconazole, ketoconazole, ciclosporin or ritonavir.
  • Pregnancy. Females of child-bearing age will be asked to provide a urine sample for apregnancy test at each visit.
  • History of any medical, psychological or other condition, or use of any medications,including over-the-counter products, which, in the opinion of the investigators, wouldeither interfere with the study or compromise the safety of the participant.

Study Design

Total Participants: 120
Treatment Group(s): 1
Primary Treatment: No intervention - prednisolone is taken as part if routine clinical care.
Phase:
Study Start date:
April 12, 2023
Estimated Completion Date:
March 26, 2026

Study Description

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.

Connect with a study center

  • Imperial College Healthcare NHS Trust

    London,
    United Kingdom

    Active - Recruiting

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