アジスロマイシンと未熟児の慢性肺疾患の予防(Azithromycin and preventing chronic lung disease in premature babies)

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2024-04-26 カーディフ大学

カーディフ大学による研究で、早産児の慢性肺疾患の発症を予防するためのアジスロマイシンの早期使用が効果的でないことが明らかになりました。この研究は、アジスロマイシンが早産児の慢性肺疾患の発症率を減少させるかどうかを確かめるための最大規模の臨床試験であり、796人の早産児を対象にイギリス全土の28の新生児集中治療室で行われました。しかし、アジスロマイシンの長期的な効果と安全性については、さらに評価が必要です。

<関連情報>

未熟児慢性肺疾患予防のためのアジスロマイシン療法(AZTEC):多施設共同二重盲検無作為化プラセボ対照試験 Azithromycin therapy for prevention of chronic lung disease of prematurity (AZTEC): a multicentre, double-blind, randomised, placebo-controlled trial

John Lowe, PhD;David Gillespie, PhD;Ali Aboklaish, PhD;Tin Man Mandy Lau, BSc;Claudia Consoli, PhD;Malavika Babu, MSc;et al.
The Lancet Respiratory Medicine  Published:April 25, 2024
DOI:https://doi.org/10.1016/S2213-2600(24)00079-1

アジスロマイシンと未熟児の慢性肺疾患の予防(Azithromycin and preventing chronic lung disease in premature babies)

Summary

Background
Systematic reviews have reported conflicting evidence on whether macrolide antibiotics reduce rates of chronic lung disease of prematurity (CLD) in at-risk preterm infants born at less than 30 weeks’ gestation, including in those colonised with pulmonary Ureaplasma spp. Since an adequately powered trial has been lacking, we aimed to assess if the macrolide azithromycin improved survival without the development of physiologically defined moderate or severe CLD in preterm infants.

Methods
AZTEC was a multicentre, double-blind, randomised, placebo-controlled trial conducted in 28 tertiary neonatal intensive care units in the UK. Infants were eligible if they were born at less than 30 weeks’ gestation and had received at least 2 h of either non-invasive (continuous positive airway pressure or humidified high flow nasal cannula therapy) or invasive respiratory support (via endotracheal tube) within 72 h of birth. Eligible infants were randomly allocated in a 1:1 ratio using random permuted blocks of four to receive either intravenous azithromycin at 20 mg/kg per day for 3 days followed by 10 mg/kg for 7 days, or to placebo. Allocation was stratified by centre and gestational age at birth (<28 weeks vs ≥28 weeks). Azithromycin and placebo vials were encased in tamper-evident custom cardboard cartons to ensure masking for clinicians, parents, and the research team. The primary outcome was survival without development of physiologically defined moderate or severe CLD at 36 weeks’ postmenstrual age. Outcomes and safety were analysed on an intention-to-treat basis (all randomly allocated infants, regardless of any post-randomisation events). The study was registered with ISRCRN (11650227) and is closed.

Findings
Infants were recruited between Oct 9, 2019, and March 22, 2022. 799 (53·1%) of 1505 eligible infants underwent random allocation; three infants were withdrawn, including consent to use their data, leaving 796 infants for analysis. Survival without moderate or severe CLD occurred in 166 (42%) of 394 infants in the intervention group and 179 (45%) of 402 in the placebo group (three-level adjusted OR [aOR] 0·84, 95% CI 0·55–1·29, p=0·43). Pulmonary Ureaplasma spp colonisation did not influence treatment effect. Overall, seven serious adverse events were reported for the azithromycin group (five graded as severe, two as moderate), and six serious adverse events were reported in the placebo group (two severe, two moderate, and two mild), as assessed by the local principal investigators.

Interpretation
Since prophylactic use of azithromycin did not improve survival without development of physiologically-defined CLD, regardless of Ureaplasma spp colonisation, it cannot be recommended in clinical practice.

Funding
UK National Institute for Health and Care Research.

医療・健康
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