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细胞因子在预防和治疗新生儿败血症中的基本原理及潜在应用

Rationale and potential use of cytokines in the prevention and treatment of neonatal sepsis.

作者信息

Goldman S, Ellis R, Dhar V, Cairo M S

机构信息

Children's Hospital of North Texas, Dallas, USA.

出版信息

Clin Perinatol. 1998 Sep;25(3):699-710.

PMID:9779342
Abstract

Despite advances in the use of newer antimicrobials and aggressive supportive care, sepsis and its sequalae remain a major source of morbidity and mortality in the neonate. The VLBW neonate is especially at high risk. We and others have demonstrated that neonatal MNC are deficient in their production of G-CSF and GM-CSF, which, in part, may explain the neonates propensity to develop neutropenia during times of sepsis. G-CSF and GM-CSF have been shown to both enhance neonatal neutrophil superoxide production in vitro and to increase circulating neutrophil numbers through expansion of the NSP in the BM in neonatal rats and humans. G-CSF is protective (if given with or before antibiotics) during experimental GBS in the neonatal rat and appears to be well tolerated (both short term and 2 years after its use) in the human neonate. In a phase II randomized pilot multicenter study, GM-CSF prophylaxis in the VLBW neonate was well tolerated during 4 weeks of administration and was noted to have significantly reduced the incidence of nosocomial infections. Future efficacy and safety studies in more neonates need to be completed and assessed before the routine pharmacologic use of G-CSF or GM-CSF is recommended to prevent and treat neonatal sepsis.

摘要

尽管在使用新型抗菌药物和积极的支持性治疗方面取得了进展,但败血症及其后遗症仍然是新生儿发病和死亡的主要原因。极低出生体重儿尤其高危。我们和其他人已经证明,新生儿单核细胞产生粒细胞集落刺激因子(G-CSF)和粒细胞-巨噬细胞集落刺激因子(GM-CSF)的能力不足,这在一定程度上可能解释了新生儿在败血症期间易发生中性粒细胞减少的倾向。G-CSF和GM-CSF已被证明在体外可增强新生儿中性粒细胞超氧化物的产生,并通过在新生大鼠和人类中扩大骨髓中的中性粒细胞干细胞池来增加循环中性粒细胞数量。在新生大鼠实验性B族链球菌感染期间,G-CSF(如果与抗生素同时使用或在抗生素之前使用)具有保护作用,并且在人类新生儿中似乎耐受性良好(使用后短期和2年)。在一项II期随机试点多中心研究中,极低出生体重儿在4周的GM-CSF预防给药期间耐受性良好,并且注意到医院感染的发生率显著降低。在推荐常规使用G-CSF或GM-CSF预防和治疗新生儿败血症之前,需要完成并评估更多新生儿的未来疗效和安全性研究。

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