Effects of prenatal exposure to dexamethasone on early complications and survival outcome in the newborns with very and extremely low birth weight

doi:10.16150/j.1671-2870.2021.01.009

Abstract

Abstract:

Objective: To explore the effect of prenatal exposure to dexamethasone on early postnatal complications and survival outcomes in the newborns with very low and extremely low birth weight. Methods: The information of 355 infants born in the Obstetrics Department of the Lianyungang Hospital Affiliated to Xuzhou Medical University from Ja-nuary 1, 2012 to July 31, 2020 was collected and used to do a retrospective analysis. The newborns were transferred directly to the Department of Neonatal in the same hospital because of birth weight ≤1 500 g. The infants with very low(birth weight greater than 1 000 g and less than 1 500 g) and extremely low birth weight(birth weight<1 000 g） were divi-ded into the exposed and unexposed groups according to whether their mothers received or did not receive standard dexamethasone therapy before giving birth, and the survival outcomes and incidence of early complications were compared between the two groups. Based on the general data of 298 living premature infants, a univariate analysis and binary logistic regression were performed to analyzethe risk factors of earlycomplications. Results: In 326 infants with very low birth weight,the mortality rate of the exposed group was lower than that of the unexposed group (8.1% vs. 19.1%) ( χ²=6.774, P=0.009). The clinical data between the exposed and unexposed groups including gender, birth weight, gestational age, Apgar score, fetal number, delivery method, hospital stay, oxygen therapy time didn′t show statistically different (P>0.05). In addition, the early postnatal complications including the incidence of jaundice, neonatal anemia, neonatal pneumonia, necrotizing enterocolitis, patent ductus arteriosus and intraventricular hemorrhage were similar between the exposed and unexposed groups (P>0.05). The incidences of RDS (respiratory distress syndrome) and broncho-pulmonary dysplasia in the exposed group were lower than those in the unexposed group (24.5% vs. 37.9%, 19.6% vs. 31.0%, P<0.05), and prenatal use of dexamethasone was a protective factor for occurrences of RDS. However, the incidences of neonatal hypoglycemia, neonatal sepsis, and retinopathy of prematurity in the exposed group were higher than those in the unexposed group (P<0.05) in the infants with very low weight. The prenatal use of dexamethasone was an independent risk factor for occurrences of early complications mentioned above (OR values were 4.332, 2.813, 4.888, and 95%CI were 2.443-7.681, 1.316-6.014, 1.609-14.849, respectively).There was no statistical difference in the perinatal complication of pregnant women between the exposed group and the unexposed group (P>0.05). For extremely low birth weight infant,there was no significant difference in survival outcomes, general neonatal information, early postnatal complications, and maternal complications between exposed and unexposed groups. Conclusions: Prenatal use of dexamethasone has no effect on survival outcomes and early complications in the infants with extremely low birth weight. It could improve survival rate and prognosis in the infants with very low birth weight by reducing the occurrences of postnatal RDS and broncho-pulmonary dysplasias, while it may increase the incidences of retinopathy of prematurity, neonatal hypoglycemia and neonatal sepsis in them.

Key words: Dexamethasone, Very low birth weight, Extremely low birth weight, Complication

CLC Number:

R722

SHEN Lu, YIN Qigai. Effects of prenatal exposure to dexamethasone on early complications and survival outcome in the newborns with very and extremely low birth weight[J]. Journal of Diagnostics Concepts & Practice, 2021, 20(01): 60-65.

Figures/Tables 5

References 21

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结局	超低体重早产儿(n=29)		极低体重早产儿(n=326)
结局	暴露组 (n=12)	未暴露组 (n=17)	暴露组 (n=111)	未暴露组 (n=215)
存活	10	12	102(91.9%)	174(80.9%)
死亡	2	5	9(8.1%)	41(19.1%)
χ²值		-^a)		6.774
P值		0.665		0.009

项目	超低体重早产儿(n=22)				极低体重早产儿( n=276)
项目	暴露组(n=10)	未暴露组(n=12)	t或z或χ²值	P值	暴露组(n=102)	未暴露组(n=174)	t或z或χ²值	P值
住院时间(d)	66±26	48±19	t=-1.902	0.075	36(27~48)	38(29~47)	z=0.589	0.556
氧疗时间(d)	42±33	35±20	t=-0.598	0.559	6(3~19)	7(2~17)	z=-0.107	0.915
出生时体重(g)	900(763~968)	900(890~978)	z=-0.497	0.619	1 365±156	1 369±149	t=-0.210	0.834
出生时胎龄(周)	29(27~29)	29(28~29)	z=-0.100	0.920	31(29~32)	30(29~32)	z=-0.370	0.711
1 min Apgar评分（分）	6(4~8)	7(2~8)	z=-0.034	0.973	8(7~8)	8(7~8)	z=-0.642	0.521
5 min Apgar评分（分）	8(6~8)	8(4~8)	z=-0.137	0.891	9(8~9)	9(8~9)	z=-0.132	0.895
男性	5	3	-^a)	0.378	58	89	χ²=0.843	0.358
单胎	5	8	-^a)	0.666	79	136	χ²=0.019	0.891
剖宫产分娩	4	6	-^a)	0.691	57	79	χ²=2.826	0.093

并发症	超低体重早产儿^a)(n=22)		P值	极低体重早产儿(n=276)		χ²值	P值
并发症	暴露组(n=10)	未暴露组(n=12)	P值	暴露组(n=102)	未暴露组(n=174)	χ²值	P值
新生儿低血糖	3	2	0.624	49	32	27.261	<0.001
新生儿黄疸	6	6	0.691	47	82	0.028	0.866
新生儿贫血	10	9	0.221	49	93	0.753	0.385
新生儿肺炎	8	9	0.323	46	72	0.363	0.547
新生儿败血症	3	1	0.293	20	17	5.361	0.021
RDS	7	9	1.000	25	66	5.241	0.021
BPD	7	6	0.415	20	54	4.279	0.039
坏死性小肠结肠炎	1	0	0.455	9	8	1.987	0.159
动脉导管未闭	2	0	0.481	7	10	0.138	0.710
脑室内出血	2	3	1.000	12	23	0.123	0.726
ROP	3	0	0.078	11	6	5.987	0.014

并发症	超低体重早产儿^a)(n=22)		P值	极低体重早产儿(n=276)		χ²值	P值
并发症	暴露组(n=10)	未暴露组(n=12)	P值	暴露组(n=102)	未暴露组(n=174)	χ²值	P值
妊娠糖尿病	1	0	0.455	3	6	<0.001	1.000
妊娠高血压	4	6	0.691	36	49	1.535	0.215
前置胎盘	0	1	1.000	1	5	0.376	0.540
胎膜早破	2	0	0.195	22	45	0.645	0.422
胎盘早剥	0	1	1.000	3	11	1.526	0.217

影响因素	β	标准误差	Wald	OR值	95%CI	P值
影响因素	β	标准误差	Wald	OR值	下限~上限	P值
RDS	-0.680	0.337	4.075	0.507	0.262~0.980	0.044
BPD	-0.415	0.356	1.358	0.661	0.329~1.327	0.244
ROP	1.587	0.567	7.834	4.888	1.609~14.849	0.005
新生儿低血糖	1.466	0.292	25.176	4.332	2.443~7.681	<0.001
新生儿败血症	1.034	0.388	7.119	2.813	1.316~6.014	0.008