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Early identification of the risk for free radical-related diseases in preterm newborns
Authors:Serafina Perrone  Simona Negro  Barbara Marzocchi  Francesca Iacoponi  Giuseppe Buonocore
Institution:a Department of Pediatrics, Obstetrics and Reproductive Medicine, Division of Neonatology, University of Siena, Italy
b Department of Biomedical Sciences, Biology Section Institute of General Biology, University of Siena, Italy
Abstract:

Background

Despite recent advances in preterm newborns healthcare, perinatal pathologies and disabilities are increasing. Oxidative stress (OS) is determinant for the onset of an unbalance between free radicals (FRs) production and antioxidant systems which plays a key role in pathogenesis of pathologies such as retinopathy of prematurity (ROP), bronchopulmonary dysplasia (BPD), necrotizing enterocolitis (NEC), intraventricular hemorrhage (IVH), grouped as ‘free radical-related diseases’ (FRD).

Aim

This study tests the hypothesis that OS markers levels in cord blood may predict the onset of FRD pathologies.

Patients and methods

168 preterm newborns of GA: 24-32 weeks (28.09 ± 1.99); and BW: 470-2480 gr (1358.11 ± 454.09) were consecutively recruited. Markers of potential OS risk (non-protein bound iron, NPBI; basal superoxide anion, BSA; under stimulation superoxide anion, USSA) and markers of OS-related damage (total hydroperoxides, TH; advanced oxidation protein products, AOPP) were assessed in cord blood. Associations between FRD onset and OS markers were checked through inferential analysis (univariate logistic regression).

Results

The development of FRD was significantly associated to high cord blood levels of TH, AOPP and NPBI (respectively p = 0.000, OR = 1.025, 95%CI = 1.013-1.038; p = 0.014, OR = 1.092, 95%CI = 1.018-1.172; p = 0.007, OR = 1.26995%CI = 1.066-1.511).

Conclusions

Elevated levels of TH, AOPP and, above all, NPBI, in cord blood are associated with increased risk for FRD. OS markers allow the early identification of infants at risk for FRD because of perinatal oxidant exposure. This can be useful in devising strategies to prevent or ameliorate perinatal outcome.
Keywords:FRD  Free Radicals Disease  FRs  free radicals  OS  oxidative stress  BPD  bronchopulmonary dysplasia  RP  retinopathy of prematurity  NEC  necrotizing enterocolitis  PDA  patent ductus arteriosus  PVL  periventricular leukomalacia  IVH  intraventricular haemorrhage  PHH  post-haemorrhagic hydrocephalus  TH  total hydroperoxides  AOPP  advanced oxidation protein products  NPBI  non-protein bound iron  BSA  basal superoxide anion  USSA  under stimulation superoxide anion  GA  gestational age  BW  birth weight
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