在南非一家结核病/艾滋病毒流行的三级医院中,需要住院治疗的违规药物和皮肤药物不良反应的范围。

IF 3.3 Q2 ALLERGY
Frontiers in allergy Pub Date : 2024-11-28 eCollection Date: 2024-01-01 DOI:10.3389/falgy.2024.1481281
S P P Konyana, N F Teixeira, L Pirjol, B Thwala, W Nkoyane, M Porter, F Gxolo, E Phillips, R Lehloenya, A Mankahla, J Peter
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引用次数: 0

摘要

皮肤免疫介导的药物不良反应在人类免疫缺陷病毒(PWH)患者中更为普遍。严重皮肤药物不良反应(SCAR)是皮肤药物不良反应(CADRs)中危及生命的一个子集,在人类免疫缺陷病毒和结核病流行的环境中是一个重要的公共卫生问题。然而,在非洲需要住院治疗的CADR数据有限。本研究的目的是描述流行病学、犯罪药物和需要进入南非三级皮肤科服务的cadr的结果。方法:对2015年7月30日至2022年12月15日期间在南非东开普省姆塔塔纳尔逊曼德拉学术医院住院的所有cadr患者进行回顾性文件夹审查。将这些数据与2021年3月3日至2024年4月9日期间CADR入院的前瞻性纳入数据进行比较,这些数据是免疫介导的药物不良反应(IMARI)登记和生物库以及AFRISCAR联盟的一部分。在可能的情况下,分别通过RegiSCAR、Naranjo和/或ALDEN评分进行表型和药物因果关系评估。结果:CADR入院122例:回顾性和前瞻性队列分别为89例和33例。最常见的SCAR表型为Stevens-Johnson综合征/中毒性表皮坏死松解症(SJS/TEN),占59.8%(73/122),尽管其他已证实的SCAR表型包括嗜酸性粒细胞增加和全身症状的药物反应(DRESS),急性全身性脓疱病(AGEP)和全身性固定大疱性药疹(GBFDE)。皮肤表现包括典型和非典型疤痕特征,背景Fitzpatrick肤色为IV型及以上。在回顾性队列中,16.9%(15/89)的表型由于缺乏照片而无法分类。总中位(IQR)年龄为38(25-50)岁,50.8%(62/122)为男性,60.7%(74/122)为PWH[中位(IQR) cd4t细胞计数267(76-470)个细胞/mm3]。最常见的药物为复方新诺明,占24.6% (30/122);13.9%(17/122)接受抗逆转录病毒治疗。24.7%(22/89)的回顾性队列患者未发现不良药物。回顾性队列验证SCAR的中位(IQR)住院时间为13(8-21)天,前瞻性队列为19(13-28)天(p = 0.03)。非scar的中位住院时间(IQR)在回顾性队列中为9(5-13)天,在前瞻性队列中为11(9-16)天。结论:典型和非典型的SCAR表现在这个以PWH为主的易感南非队列中都有体现。SJS/TEN是最常见的表型,复方新诺明是最常见的致病药物。这一数据强调需要在不同的非洲人群中收集前瞻性数据,以进行有效的SCAR表型和药物因果评估。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Spectrum of offending drugs and cutaneous adverse drug reactions requiring hospitalisation in a tertiary South African hospital in TB/HIV endemic setting.

Introduction: Cutaneous immune-mediated adverse drug reactions are more prevalent in people with human immunodeficiency virus (PWH). Severe cutaneous adverse drug reactions (SCAR) are a life-threatening subset of cutaneous adverse drug reactions (CADRs) and a significant public health issue in settings endemic for human immunodeficiency virus and tuberculosis. However, limited data are available on CADR requiring hospitalisation in African settings. The aim of this study is to describe the epidemiology, offending drugs and outcomes of CADRs requiring admission to a South African tertiary dermatology service.

Methods: Retrospective folder review was conducted on all CADRs requiring hospitalisation at Nelson Mandela Academic Hospital in Mthatha, Eastern Cape, South Africa between 30 July 2015 and 15 December 2022. This data was compared to prospective inclusion of CADR admissions between 03 March 2021 and 09 April 2024 as part of the Immune-Mediated Adverse Drug Reactions (IMARI) Registry and Biorepository and AFRISCAR consortium. Where possible, phenotype and drug causality assessment was performed through RegiSCAR, or Naranjo and/or ALDEN scoring respectively.

Results: CADR admissions included 122 cases: 89 and 33 in the retrospective and prospective cohorts respectively. The commonest SCAR phenotype was Stevens-Johnson syndrome/toxic epidermal necrolysis (SJS/TEN) at 59.8% (73/122), although other validated SCAR phenotypes included drug reaction with eosinophilia and systemic symptoms (DRESS), acute generalized exanthematous pustulosis (AGEP) and generalized fixed bullous drug eruption (GBFDE). Cutaneous presentations included typical and atypical SCAR features against a background Fitzpatrick skin tones of type IV and above. Amongst the retrospective cohort 16.9% (15/89) of phenotypes were unclassifiable due to lack of photographs. The overall median (IQR) age was 38 (25-50) years, 50.8% (62/122) were male and 60.7% (74/122) were PWH [median (IQR) CD4T-cell count of 267 (76-470) cells/mm3]. The commonest offending drugs included cotrimoxazole in 24.6% (30/122); and anti-retroviral therapy (ART) in 13.9% (17/122). No offending drug could be identified in 24.7% (22/89) of the retrospective cohort. The median (IQR) length of hospital stay for validated SCAR was 13 (8-21) days for the retrospective cohort and 19 (13-28) days for the prospective cohort (p = 0.03). The median (IQR) length of hospital stay for non-SCAR was 9 (5-13) days for the retrospective cohort and 11 (9-16) days for the prospective cohort.

Conclusion: Typical and atypical presentations of SCAR were represented in this vulnerable South African cohort of predominantly PWH. SJS/TEN was the commonest phenotype, and cotrimoxazole the most frequent offending drug. This data emphasises the need for prospective data collection across a diverse African population for valid SCAR phenotyping and drug causality assessment.

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