Study to evaluate effect of oral mini pulse corticosteroid therapy for unstable vitiligo on hypothalamic pituitary adrenal axis suppression

Preema Sinha , Aradhana Sood , Bhasker Mukherjee , Anwita Sinha , Sukriti Baveja , Vikas Pathania
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Abstract

Background

The treatment of vitiligo is difficult and usually requires prolonged therapy. All exogenous glucocorticoid therapies can lead to the hypothalamic–pituitary–adrenal axis (HPA) suppression. Steroid therapy in the form of an intermittent pulse therapy is a much safer option than daily administration. Very few studies have been carried out to evaluate the effect of oral minipulse prednisolone (OMP) on HPA axis, and there are no concrete guidelines regarding the tapering of steroids after OMP, if needed at all. This study is a pilot study to evaluate the effect of use of OMP on HPA axis suppression in unstable vitiligo.

Methods

It is an observational prospective study approved by the Institutional Ethics Committee (IEC) of institution carried out on 30 patients with unstable vitiligo being initiated on OMP between the ages of 20–50 yrs carried out at a tertiary care hospital of Western Maharashtra for a period of one year. Inclusion criteria was all new cases of unstable vitiligo attending dermatology OPD with patients in the age group 20–50 years. Patients treated with systemic corticosteroids in the last six months, on prolonged topical steroid therapy, patients on any other immunosuppressive therapy, patients having contraindications for exhibiting systemic steroids were excluded from the study.

Results

Thirty steroid-naive patients (11 women, 19 men) with a median duration of vitiligo of 10.67 months duration were evaluated. A total of 19 (63.3%) were males and 11 (36.6%) were females with mean age 29.13 years. Serum cortisol levels at baseline, one week, and the end of therapy were 291.1 nmol/L, 288.7 nmol/L, and 304 nmol/L, respectively. Acton Prolongatum (ACTH) stimulated serum cortisol levels at baseline, one week, and the end of therapy were 658.3 nmol/L, 626.1 nmol/L, and 630.1 nmol/L, respectively. Time taken to achieve stability was a mean of 4.41 months post-initiation of OMP in 22/25(73.3%) patients. In 4/30 (13.3%) patients, no stability was achieved at six months of follow-up.

Conclusions

This pilot study has shown that there is no suppression of serum cortisol levels by OMP prednisolone if taken in a weekly dose. OMP steroid therapy is not very effective to achieve a decent level of repigmentation alone; hence, they should be used in combination with other modalities like topical steroids or phototherapy to achieve better repigmentation. The patients did not develop any systemic or cutaneous side effects due to the drug; hence, prednisolone can be considered a safe drug for pulse therapy.
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评价口服小脉冲皮质类固醇治疗不稳定型白癜风对下丘脑-垂体-肾上腺轴抑制的影响
白癜风的治疗很困难,通常需要长时间的治疗。所有外源性糖皮质激素治疗均可导致下丘脑-垂体-肾上腺轴(HPA)抑制。间歇脉冲治疗形式的类固醇治疗比每日给药安全得多。很少有研究评估口服小脉冲强的松龙(OMP)对HPA轴的影响,并且没有关于OMP后类固醇逐渐减少的具体指南,如果需要的话。本研究是一项评估使用OMP对不稳定白癜风患者HPA轴抑制作用的初步研究。方法:这是一项经机构伦理委员会(IEC)批准的观察性前瞻性研究,研究对象为30例年龄在20-50岁之间的不稳定白癜风患者,在西马哈拉施特拉邦的一家三级医院进行为期一年的OMP治疗。纳入标准是所有在皮肤科门诊就诊的不稳定白癜风新病例,患者年龄在20-50岁之间。在过去6个月内接受全身性皮质类固醇治疗的患者,长期局部类固醇治疗的患者,接受任何其他免疫抑制治疗的患者,有全身性类固醇禁忌症的患者被排除在研究之外。结果30例初治白癜风患者(女性11例,男性19例)中位病程10.67个月。男性19例(63.3%),女性11例(36.6%),平均年龄29.13岁。基线、一周和治疗结束时血清皮质醇水平分别为291.1 nmol/L、288.7 nmol/L和304 nmol/L。在基线、治疗一周和治疗结束时,ACTH刺激血清皮质醇水平分别为658.3 nmol/L、626.1 nmol/L和630.1 nmol/L。22/25例(73.3%)患者在开始使用OMP后达到稳定所需的平均时间为4.41个月。在4/30(13.3%)的患者中,在6个月的随访中没有达到稳定。结论:本初步研究表明,每周服用OMP强的松龙对血清皮质醇水平没有抑制作用。OMP类固醇治疗不是很有效,以达到一个体面的水平的重新着色单独;因此,它们应该与其他方式结合使用,如局部类固醇或光疗,以达到更好的重新着色。患者未因药物产生任何全身或皮肤副作用;因此,强的松龙可以被认为是一种安全的脉冲治疗药物。
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来源期刊
Medical Journal Armed Forces India
Medical Journal Armed Forces India Medicine-Medicine (all)
CiteScore
3.40
自引率
0.00%
发文量
206
期刊介绍: This journal was conceived in 1945 as the Journal of Indian Army Medical Corps. Col DR Thapar was the first Editor who published it on behalf of Lt. Gen Gordon Wilson, the then Director of Medical Services in India. Over the years the journal has achieved various milestones. Presently it is published in Vancouver style, printed on offset, and has a distribution exceeding 5000 per issue. It is published in January, April, July and October each year.
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