Comparison of the hypothalamic–pituitary–adrenal axis susceptibility upon single-dose i.m. depot versus long-acting i.v. triamcinolone acetonide therapy: a direct pharmacokinetic correlation

Abraham, Getu; Demiraj, Fioralba; Ungemach, F. R.

doi:10.1677/joe.1.06991

Cited by 15 publications

(10 citation statements)

References 34 publications

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“…Screening should therefore be timed, if possible, at least 1 week after the exogenous glucocorticoid has been tapered to a physiological dose or removed. 13 Prolonged released formulations (intra-articular and epidural, especially triamcinolone), cause low level cortisol and a blunted response to ACTH stimulation for 4-6 weeks, outside of CYP3A4 inhibition 41,42 and likely for longer with it. Test results need to be interpreted with caution and with endocrinology input.…”

Section: Investigation Of Ics/sai and Management Of Highrisk Co-prescmentioning

confidence: 99%

Iatrogenic Cushing’s syndrome due to drug interaction between glucocorticoids and the ritonavir or cobicistat containing HIV therapies

et al. 2016

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Ritonavir and cobicistat, used as pharmacokinetic enhancers in combination with some antiretrovirals (ARVs) for the treatment of HIV, are potent inhibitors of the CYP3A4 isoenzyme. Most glucocorticoids are metabolised via the CYP3A4 pathway and iatrogenic Cushing's syndrome (ICS), with possible secondary adrenal insufficiency (SAI), is a recognised complication following co-administration with ritonavir or cobicistat. A structured approach for identifying and managing potentially affected individuals has not been established. We systematically identified patients with ICS/SAI and found substantial heterogeneity in clinical practice across three large London HIV centres. While this significant drug interaction and its complications are now well-recognised, it is apparent that there is no standardised approach to management or guidance for the general physician. Here we describe the management of ICS/SAI in our current practice, review the available evidence and suggest practice recommendations. KEYWORDS : Adrenal insuffi ciency , cobicistat , Cushing's syndrome , HIV , ritonavir IntroductionRitonavir and cobicistat are pharmacokinetic enhancers used in the treatment of HIV infection. They are extremely potent inhibitors of cytochrome P450 3A4 (CYP3A4) activity. Ritonavir, originally developed as an antiretroviral, is used ABSTRACT Iatrogenic Cushing's syndrome due to drug interaction between glucocorticoids and the ritonavir or cobicistat containing HIV therapies at sub-therapeutic doses, in combination with HIV protease inhibitors (PIs), to significantly increase their concentrations and allow less frequent and lower dosing.1 Cobicistat was developed more recently and is similar in structure. It is used in combination with PIs or elvitegravir (an integrase inhibitor) 2 but has no antiretroviral activity itself. 3 The downside of this pharmacokinetic manipulation is the significant potential for interactions with CYP3A4 substrates, leading to side effects. CYP3A4 is the dominant isoenzyme of the hepatic cytochrome P450 system and is the primary metabolic step for the degradation of endogenous and most prescribed corticosteroids. The metabolism of these can therefore be decreased by inhibitors such as ritonavir/cobicistat. 4 Subsequent increases in exogenous corticosteroid plasma concentrations and half-life can lead to iatrogenic Cushing's syndrome (ICS) 5 and, at supraphysiological levels, to suppression of adrenocorticotropic hormone (ACTH) and endogenous corticosteroid secretion, potentially resulting in secondary adrenal insufficiency (SAI). There is abundant evidence highlighting this issue. 1,[6][7][8][9][10][11] However, a structured approach to identify and manage potentially affected individuals has not been established. We aim to summarise the current management of ICS/SAI in three large HIV patient cohorts, review the available literature and develop practice recommendations. Of note, cobicistat became available after the evaluation period covered; however, all advice for ritonavir is applicable to i...

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Section: Investigation Of Ics/sai and Management Of Highrisk Co-prescmentioning

confidence: 99%

Iatrogenic Cushing’s syndrome due to drug interaction between glucocorticoids and the ritonavir or cobicistat containing HIV therapies

et al. 2016

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“…; Abraham et al . ; Bentz ). Parenteral triamcinolone acetonide has been used in the past for treatment of systemic diseases such as RAO (Lapointe et al .…”

Section: Commonly Used Glucorticoidsmentioning

confidence: 99%

Review of glucocorticoid therapy in horses. Part 1: Pharmacology

Cuming

Groover

Wooldridge

et al. 2016

Equine Veterinary Education

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Summary This article is the first in a three part review series examining glucocorticoid use in treatment of medical conditions and musculoskeletal disorders of the horse. This article provides a review of the structure and function of corticosteroids together with a summary of the available literature pertaining to the pharmacodynamics, pharmacokinetics and indications for use of, and adverse effects associated with, glucocorticoids currently available for use by equine veterinarians.

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“…It was hypothesized that particulate steroid preparations may provide a local depot effect with constant release of the active drug from the administration site over a longer time period compared to non-particulate steroids [53].…”

Section: Efficacy Of Various Steroids In Lumbar Epidural Injectionsmentioning

confidence: 99%

“…The duration of action of intramuscular administered triamcinolone acetonide representing a particulate glucocorticoid was studied in an investigation with dogs and compared to intravenous administered triamcinolone acetonide dihydrogen phosphate (TAA-DHP), which represents the non-particulate steroid [53]. It was shown that a single dose of the particulate glucocorticoid (triamcinolone acetonide) after intramuscular administration revealed a much longer duration of action of up to 4 weeks on the hypothalamicpituitary-adrenal axis activity in dogs than a similar intravenous dose of its analogue, the non-particulate steroid (TAA-DHP) [53].…”

Section: Efficacy Of Various Steroids In Lumbar Epidural Injectionsmentioning

confidence: 99%

“…It was shown that a single dose of the particulate glucocorticoid (triamcinolone acetonide) after intramuscular administration revealed a much longer duration of action of up to 4 weeks on the hypothalamicpituitary-adrenal axis activity in dogs than a similar intravenous dose of its analogue, the non-particulate steroid (TAA-DHP) [53]. The duration of action of the intravenous nonparticulate steroid (TAA-DHP) was only up to 72 h [53], although the potentially longer duration of action of intramuscular administered TAA-DHP was not evaluated in this study.…”

Section: Efficacy Of Various Steroids In Lumbar Epidural Injectionsmentioning

confidence: 99%

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Particulate versus non-particulate steroids for lumbar transforaminal or interlaminar epidural steroid injections: an update

et al. 2014

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Comparison of the hypothalamic–pituitary–adrenal axis susceptibility upon single-dose i.m. depot versus long-acting i.v. triamcinolone acetonide therapy: a direct pharmacokinetic correlation

Cited by 15 publications

References 34 publications

Iatrogenic Cushing’s syndrome due to drug interaction between glucocorticoids and the ritonavir or cobicistat containing HIV therapies

Iatrogenic Cushing’s syndrome due to drug interaction between glucocorticoids and the ritonavir or cobicistat containing HIV therapies

Review of glucocorticoid therapy in horses. Part 1: Pharmacology

Particulate versus non-particulate steroids for lumbar transforaminal or interlaminar epidural steroid injections: an update

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