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首页> 外文期刊>Drug safety: An international journal of medical toxicology and drug experience >A risk-benefit assessment of drugs used for neonatal chronic lung disease.
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A risk-benefit assessment of drugs used for neonatal chronic lung disease.

机译:新生儿慢性肺部疾病药物的风险收益评估。

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Improvements in neonatal intensive care have resulted in more extremely low birthweight babies surviving who are at risk of developing chronic lung disease. The preterm lung is vulnerable as it is both structurally immature and deficient in surfactant and antioxidant defences. Mechanical ventilation and high inspired oxygen concentrations are often necessary for preterm babies to survive but they can cause pulmonary inflammation which leads to lung damage. Abnormal healing in the presence of ongoing inflammation leads to airways remodelling which can result in protracted respiratory problems in these babies. A commonly used definition for chronic lung disease is the requirement for supplemental oxygen beyond 36 weeks' postconception. Many drugs that are commonly used for chronic lung disease have not been subjected to proper randomised controlled trials but are widely used on the basis of small studies showing short term benefits. They can be broadly divided into 2 groups. First, there are preventative drugs that are administered early to reduce oxygen toxicity and pulmonary inflammation. Secondly, there are those administered in established chronic lung disease, designed to reduce respiratory morbidity. Pulmonary inflammation in the neonate is reduced by systemic corticosteroids. Corticosteroid therapy within the first 2 weeks of life enables earlier extubation of preterm babies with subsequent reduced chronic lung disease and improved neonatal survival when given between 7 and 14 days. However, there is an increased risk of gastrointestinal haemorrhage, metabolic derangement, ventricular hypertrophy and potential effects on long term growth and brain development. Diuretics and inhaled bronchodilators improve pulmonary compliance and reduce oxygen requirements in established chronic lung disease but probably have little effect in reducing the incidence. In babies with established chronic lung disease, home oxygen therapy enables earlier discharge and prophylaxis against respiratory syncytial virus can reduce morbidity from bronchiolitis. All of the above therapies have adverse effects that need to be considered before initiating treatment. Recently, new drugs have become available which may be beneficial. These include inhaled nitric oxide for reduction of ventilation-perfusion mismatching, recombinant human superoxide dismutase for protection against oxidative stress and alpha-1 proteinase inhibitor which may reduce airways remodelling. At present these therapies are undergoing clinical trials. Exogenous surfactant is beneficial in respiratory distress syndrome and may reduce the risk of chronic lung disease but there have been no randomised controlled trials of its use in established chronic lung disease. Drugs which have been tried unsuccessfully include erythromycin, ambroxol and mast cell stabilisers.
机译:新生儿重症监护病房的改善已导致有可能患上慢性肺病的极低出生体重的婴儿幸存下来。早产肺是脆弱的,因为它在结构上既不成熟,又缺乏表面活性剂和抗氧化剂的防御。机械通风和高浓度的氧气通常是早产婴儿生存所必需的,但它们会引起肺部炎症,从而导致肺部损害。在持续发炎的情况下异常愈合会导致气道重塑,这可能导致这些婴儿长期呼吸困难。慢性肺疾病的一个常用定义是在怀孕后36周后需要补充氧气。许多常用于慢性肺部疾病的药物尚未经过适当的随机对照试验,但在显示短期获益的小型研究的基础上被广泛使用。它们可以大致分为2组。首先,有些预防药物要尽早服用,以减少氧气中毒和肺部炎症。其次,有些是在已建立的慢性肺部疾病中给药的,旨在减少呼吸道疾病。全身性皮质类固醇激素可减轻新生儿的肺部炎症。在出生后的前两周内应用皮质类固醇激素疗法可以使早产儿早早拔管,随后在7至14天之间给予治疗,从而可以减少慢性肺部疾病并改善新生儿存活率。但是,胃肠道出血,代谢紊乱,心室肥大以及对长期生长和大脑发育的潜在影响的风险增加。利尿剂和吸入性支气管扩张剂可改善已确诊的慢性肺部疾病的肺顺应性并降低氧气需求,但对降低发病率的作用可能很小。在患有慢性肺病的婴儿中,家庭吸氧疗法可以使出院更早,预防呼吸道合胞病毒可以降低毛细支气管炎的发病率。上述所有疗法均具有不良反应,需要在开始治疗之前进行考虑。近来,新药物已经上市,这可能是有益的。这些措施包括用于减少通气-灌注不匹配的吸入一氧化氮,用于抵抗氧化应激的重组人超氧化物歧化酶和可减少气道重塑的α-1蛋白酶抑制剂。目前,这些疗法正在临床试验中。外源性表面活性剂对呼吸窘迫综合征有益,并且可以降低慢性肺部疾病的风险,但是尚无关于将其用于已确定的慢性肺部疾病的随机对照试验。尝试不成功的药物包括红霉素,氨溴索和肥大细胞稳定剂。

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