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首页> 外文期刊>Journal of Infectious Diseases >Prevention and Treatment of Influenza in High‐Risk Groups: Children, Pregnant Women, Immunocompromised Hosts, and Nursing Home Residents
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Prevention and Treatment of Influenza in High‐Risk Groups: Children, Pregnant Women, Immunocompromised Hosts, and Nursing Home Residents

机译:预防和治疗高危人群的流感:儿童,孕妇,免疫功能低下的宿主和疗养院居民

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penta [cl11.4]>The pediatric population experiences preventable hospitalizations and serves as a reservoir for influenza and its transmission to other children as well as adults. As a consequence, the Advisory Committee on Immunization Practices has recommended initiating influenza immunization of children as young as 6 months of age through 23 months of age and, recently, up to 5 years of age. However, immunization of older children has not yet become a priority of the US Public Health Service. As a consequence, the importance of antiviral agents, particularly neuraminidase (NA) inhibitors, cannot be overemphasized. From an epidemiological perspective, influenza resulted in higher childhood mortality than did Bordetella pertussis infection in 2003–2004. During that season, 153 children died of influenza, and two‐thirds were <5 years of age. Importantly, nearly 50% of these children were previously healthy, with no underlying illness. Currently, 2 NA inhibitors are approved for the treatment of influenza in children. Zanamivir is approved for children >7 years of age, and oseltamivir is approved for children >1 year of age. Arguably, the younger children are at particular risk for influenza complications and hospitalization. In placebo‐controlled studies in children >1 year of age, oseltamivir therapy accelerated resolution of clinical illness and defervescence and decreased both the incidence of otitis media and the concomitant use of antibiotics. However, oseltamivir is not currently approved for children <1 year of age. Three clinical toxicology studies identified neurotoxicity in newborn rats administered this medication. In these preclinical toxicology studies, the dose of oseltamivir exceeded that which would be used in humans. In addition, the metabolism of oseltamivir is different in rats than in humans. A key component of influenza therapy is the possibility for development of resistance. Although in studies performed in North America, resistance was not a frequent event, it has been documented in Japanese children treated with this medication; the adequacy of the dose used has been questioned. Children represent only one unique study population among others. Individuals who are at increased risk for influenza infection include the elderly, the immunocompromised, and pregnant women. Collectively, antiviral medications must be evaluated in populations in which they have not yet been assessed. The development of additional antiviral drugs is an important recommendation for the future, so that antiviral resistance can be circumvented. Similarly, availability of drugs for children <1 year of age is mandatory.
机译:penta [cl11.4]>儿科人群可预防的住院治疗并充当流行性感冒的储存库,并传染给其他儿童和成人。因此,免疫实践咨询委员会建议对年龄在6个月至23个月之间,最近到5岁以下的儿童进行流感免疫。但是,对较大的孩子进行免疫尚未成为美国公共卫生服务的重点。因此,不能过分强调抗病毒剂,尤其是神经氨酸酶(NA)抑制剂的重要性。从流行病学的角度来看,2003年至2004年,流感导致的儿童死亡率高于百日咳博德特氏菌感染。在那个季节,有153名儿童死于流感,三分之二的人年龄小于5岁。重要的是,这些孩子中近50%以前是健康的,没有潜在的疾病。目前,有2种NA抑制剂被批准用于治疗儿童流感。扎那米韦被批准用于7岁以上的儿童,奥司他韦被批准用于1岁以上的儿童。可以说,年幼的孩子特别容易患流感并发症和住院。在对1岁以上儿童进行的安慰剂对照研究中,奥司他韦疗法可加快临床疾病和退热的速度,并降低中耳炎的发生率和同时使用抗生素。但是,奥司他韦目前不被批准用于1岁以下的儿童。三项临床毒理学研究确定了使用这种药物的新生大鼠的神经毒性。在这些临床前毒理学研究中,奥司他韦的剂量超过了人类的剂量。另外,奥司他韦在大鼠中的代谢与在人中不同。流感疗法的关键组成部分是可能产生耐药性。尽管在北美进行的研究中,耐药性不是一个经常发生的事件,但在使用这种药物治疗的日本儿童中已有记载。所用剂量是否足够受到质疑。儿童仅代表一个独特的研究人群。流感感染风险增加的个体包括老人,免疫力低下和孕妇。总的来说,必须在尚未评估抗病毒药物的人群中评估抗病毒药物。开发其他抗病毒药物是未来的重要建议,因此可以避免抗病毒耐药性。同样,必须为小于1岁的儿童提供药物。

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