A Dose-dependent Effect of the Novel Inhaled  Corticosteroid Ciclesonide on Airway Responsiveness to Adenosine-5 ′ -Monophosphate in Asthmatic Patients

Taylor, David A.; Jensen, M W; Kanabar, Varsha; Engelstätter, Renate; Steinijans, V W; Barnes, Peter J.; O’Connor, Brian

doi:10.1164/ajrccm.160.1.9809046

Cited by 137 publications

(82 citation statements)

References 19 publications

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“…We performed our challenges in the morning when the airway exhibits enhanced diurnal hyper-responsiveness, so as to coincide with trough protection at the end of the 24-h dosing interval with CIC. Previous data with twice daily CIC have shown a doseresponse against adenosine monophosphate challenge with doses of 100, 400 and 1600 mg daily given each for 2 weeks [21]. In summary, our results showed no significant difference between HFA formulations of once daily CIC 400 mg and twice daily FP 250 mg over 4 weeks for effects on the primary outcome of methacholine hyperresponsiveness in mild-to-moderate asthma.…”

Section: Discussionsupporting

confidence: 47%

Effects of hydrofluoroalkane formulations of ciclesonide 400 µg once daily vs fluticasone 250 µg twice daily on methacholine hyper‐responsiveness in mild‐to‐moderate persistent asthma

Lee

Haggart

Currie

et al. 2004

Brit J Clinical Pharma

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AimsThere are no data comparing the relative efficacy of hydrofluoroalkane (HFA) formulations of ciclesonide (CIC) and fluticasone propionate (FP) on airway hyperresponsiveness, in mild-to-moderate persistent asthma. We therefore elected to evaluate the comparative efficacy of HFA pressurized metered-dose inhaler formulations of CIC and FP, assessing methacholine challenge, in addition to exhaled nitric oxide, lung function, diary cards and quality of life. MethodsNineteen mild-to-moderate asthmatic patients completed the study per protocol in randomized, double-blind, double-dummy, crossover fashion. Patients were required to stop their usual inhaled corticosteroid therapy for the duration of the study. Patients were commenced instead on salmeterol (SM) 50 m g one puff twice daily + montelukast (ML) 10 mg once daily for 2-week washout periods prior to each randomized treatment, in order to prevent dropouts. Patients received 4 weeks of either CIC 200 m g two puffs once daily (08.00 h) + CIC-placebo (PL) two puffs once daily (20.00 h) + FP-PL two puffs twice daily (08.00 h and 20.00 h), or FP 125 m g two puffs twice daily (08.00 h and 20.00 h) + CIC-PL two puffs twice daily (08.00 h and 20.00 h). SM + ML were withheld for 72 h prior to post-washout visits and CIC or FP was withheld for 24 h prior to study visits. ResultsThere was no significant difference between CIC vs. FP for the primary outcome of methacholine P C 20 as doubling dilution (dd) shift from respective baseline; mean difference: 0.4 dd (95% CI -0.4, 1.2). Moreover, there was no difference between treatments for the sequence of CIC first vs FP second; mean difference: 0.2 dd (95% CI -1.3, 1.7) or FP first vs CIC second; mean difference: 0.9 dd (95% CI -0.1, 1.8). There were also no differences for other secondary outcomes between treatments, either respective or irrespective of sequence, as change from baseline. ConclusionsThere were no differences between 4 weeks of CIC 400 m g once daily and FP 250 m g twice daily on methacholine hyper-responsiveness in mild-to-moderate persistent asthma. Longer-term studies are indicated to evaluate their relative efficacy on asthma exacerbations. Ciclesonide vs fluticasone in asthmaBr J Clin Pharmacol 58 :1 27

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Section: Discussionsupporting

confidence: 47%

Effects of hydrofluoroalkane formulations of ciclesonide 400 µg once daily vs fluticasone 250 µg twice daily on methacholine hyper‐responsiveness in mild‐to‐moderate persistent asthma

Lee

Haggart

Currie

et al. 2004

Brit J Clinical Pharma

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“…To date, the dose-dependent effect of ICS on airway eosinophilia has mainly been assessed on induced sputum samples. These studies also indicate that ICS are effective, from low doses onwards, at reducing eosinophil number, and that the dose-response curve is relatively flat [17][18][19][20]. To what extent this is paralleled by changes in mucosal eosinophil number has not been fully established in humans.…”

Section: Discussionmentioning

confidence: 94%

Dose-related effect of inhaled fluticasone on allergen-induced airway changes in rats

Vanacker¹,

Palmans²,

Pauwels³

et al. 2002

Eur Respir J

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To examine whether fluticasone propionate (FP) dose-dependently inhibits inflammatory as well as structural changes, Brown Norway rats were sensitised to ovalbumin (OA) on day 0 and 7. From day 14-28, rats were exposed to aerosolised OA (1%) or phosphate buffered saline every 2 days. Thirty minutes before each allergen exposure, animals were pre-treated with aerosolised placebo or FP (0.1, 1 or 10 mg) or prednisolone 3 mg?kg -1 i.p.At day 29, 0.1 mg FP had no measurable effect, either on inflammatory or structural changes, such as goblet cell hyperplasia and airway wall thickening. The allergeninduced increase in eosinophilic inflammation in bronchoalveolar lavage fluid and in the airway mucosa, as well as increased fibronectin deposition, were inhibited by treatment with FP from a dose of 1 mg onwards. Inhibition of goblet cell hyperplasia and thickening of the airway wall required 10 mg inhaled FP. At this dose, systemic effects were observed. However, for a comparable degree of systemic activity, prednisolone was far less effective at preventing airway changes.The dose of inhaled fluticasone propionate required to inhibit allergen-induced structural alterations was higher than to prevent eosinophil influx, and caused systemic side-effects. However, for a similar systemic activity, prednisolone was ineffective in preventing airway remodelling.

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“…The first clinical data on ciclesonide have already been published and have demonstrated that ciclesonide reduces airway responsiveness to adenosine-5Ј-monophosphate in a dose-dependent manner when compared with placebo in patients with mildto-moderate asthma. A reduction in eosinophils was also observed in induced sputum from the same patients (Taylor et al, 1999). Another study has shown that ciclesonide produces a significant inhibition of early and late phase reaction after allergen challenge (Dahl et al, 1998).…”

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confidence: 75%

Preclinical Profile of Ciclesonide, a Novel Corticosteroid for the Treatment of Asthma

Belvisi¹,

Bundschuh²,

Stoeck³

et al. 2005

J Pharmacol Exp Ther

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Ciclesonide is a novel, inhaled corticosteroid under development for the treatment of asthma. Ciclesonide is activated to desisobutyryl-ciclesonide (des-CIC) in the lungs to provide potent anti-inflammatory activity. The investigations herein compared the activity of ciclesonide with fluticasone in animal models to assess efficacy/potency as an airway anti-inflammatory and the comparative side effect potential to consider the therapeutic ratio of each compound. In radioligand binding assays, des-CIC and fluticasone exhibited comparable high-affinity binding to the glucocorticoid receptor, whereas ciclesonide exhibited 100-fold less binding affinity. In the Brown Norway rat model of antigen-induced airway eosinophilia and in a model of Sephadex-induced lung edema, ciclesonide and fluticasone exhibited comparable efficacy. Interestingly, following 7-day intratracheal administration, ciclesonide elicited adrenal involution with a potency that was 44-fold less than fluticasone. Furthermore, ciclesonide was 22-fold less active than fluticasone in eliciting hypoplasia of the femoral growth plate. These data support the concept that ciclesonide acts as a parent compound that, when delivered to the airways, can be transformed into the active metabolite des-CIC, resulting in local high anti-inflammatory activity. Furthermore, ciclesonide possesses equivalent anti-inflammatory efficacy through pulmonary activation with a significantly improved safety profile in preclinical animal models compared with fluticasone.

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A Dose-dependent Effect of the Novel Inhaled Corticosteroid Ciclesonide on Airway Responsiveness to Adenosine-5 ′ -Monophosphate in Asthmatic Patients

Cited by 137 publications

References 19 publications

Effects of hydrofluoroalkane formulations of ciclesonide 400 µg once daily vs fluticasone 250 µg twice daily on methacholine hyper‐responsiveness in mild‐to‐moderate persistent asthma

Effects of hydrofluoroalkane formulations of ciclesonide 400 µg once daily vs fluticasone 250 µg twice daily on methacholine hyper‐responsiveness in mild‐to‐moderate persistent asthma

Dose-related effect of inhaled fluticasone on allergen-induced airway changes in rats

Preclinical Profile of Ciclesonide, a Novel Corticosteroid for the Treatment of Asthma

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