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double-blind study to clai-ify whether magnesium supplementation has an influence on these variables. The following null hypotheses were stated: magnesium supplementation has no effect on: (i) pre-eclampsia; (ii) preterm labour (and consequently gestational age at delivery) and (iii) fetal growth.
Cnrrcspondcncc: Dr Ludwig SpStling. UnivcrsitiitsFraucnklinik Bochum, Maricnhospital. Hdkcskampring 40. D 4690 Hcrnc 1, FKCi
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each visit patients were questioned on regular intake, number of tablets and side-effects of medication. Classification of diagnoses and therapies used the coding system of the Munich Perinatal Study (Selbmann et al. 1980).
Statistical analysis
l h e Wilcoxon and Mann-Whitney U-tests werc used to compare the central trends. Categorical variables were analysed by thc x? tcst. The results were considered significant at the 5% level. Assessment always used two-tailed tests. Values are given as medians and the 5th and 95th centiles. For various reasons, such as refusal to take further tablets, delivery in other hospitals or abortion. some data were not available for analyFis. Reference values for the 10th centilc of birthweight were taken from Largo ei al. (1980).
Results
Of the 568 women entered into the study, 278 were treated with magnesium and 2913 received the placebo. Age, parity and gravidity were similar in the two groups. There was no diffcrence with regard to the birthweight of children born before the start of this study o r the duration of previous pregnancies (Table 1). Based on the clinical history of the patients, the risk of abnormal pregnancy was cornparable in the two groups. The daily rate of tablet consumption was comparable in the two groups. However, the total number of tablets ingested was much higher in the group receiving magnesium, because of the longer length of gestation in that group (Table 2). The frequency of complaints attributed to the tablets uras low and comparable in the two groups. In the magnesium group one woman complained of diarrhoea, four of nausea. six of vomiting a n d six of heartburn; in the placeho group two complained of diarrhoea, one of nausea, 10 of vomiting, six of heartburn and one of fullness. Five women in the magnesium group and three wornen in the control group had a miscarriage. Median maternal weight increase was 11 kg in both groups and there were no statistically significant differences in maximum systolic and
diastolic blood pressures or in oedema between the two groups (Table 2). In the niagnesium group 44 women were hospitalized for 533 days. In the placebo group 65 women spent 887 days in hospital. Of the indications for admission to hospital, haemorrhage during pregnancy. incompetent cervix and preterm labour were more frequent in the placebo group, the difference w tatistically significant, The average duration of each admission to hospital was similar in the two groups and so were the number of miscarriages (Table 3). The median gestation was significantly longer in the women treated with magnesium, although the difference between the medians was not more than 1 day. This difference was particularly notable when the pretcrm deliveries (< 37 weeks) are compared (Table 4). There were no differences between the groups in the duration of the first stage of labour. Although the second stage of labour was longer and operative delivery more frequent in the magncsiumtreated group than in the placebo group, these differences were not statistically significant (Table 4). Differences between the two groups in respect of placental weight. infant weight and length, frequency of low Apgar scores (C7) and low birthweight are qhown in Table 5. These differences reflect the decreased frequency of preterm delivery associated with magnesium supplementation but they d o not reach statistical significancc. Therc were no differences between the groups in infant head circumference or in neonatal acid base values. Significantly fewer infants in the group receiving magnesium were admitted to the neonatal intensive care unit. The biggest differences were found in the admission rates for pretcrm birth and asphyxia (Table 5 ) . There was one perinatal death in the magnesium group. The mother was a 40-year-old diabetic in her first pregnancy. She was hospitalized twice, i n early pregnancy because of haemorrhage and hyperemesis gravidarum and again in later pregnancy because of the diabetes and preterm labour. A growth-retarded fetus was born at 33 week, gestation by forceps after severe fetal bradycardia and died immediately after delivery because it proved impossible to oxygenate the infant sufficiently. In the subsidiary analysis we excluded all those women who did not fulfil the protocol of medication as prescribed. After these exclusions, 217 women remained in the niagnesiuni
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L . Spatling
R,
G. Spii,iifling
Magncsiuni group
(11
Placcbo group
( n =390)
=27X)
Centile Variable Age (years) Parity tiravidity* Birthweight of 1st child (g) Duration of 1st prcgnancy (weeks) 5th
20.3
Ocntile 95th
37.9 3 5 3915 42
50th
28.2 2 2 3250 40
5th 19.5
1
50th
38.0 2 2 3280 40
95th
34.6 3 5 4020 42
1 1
2500 37
1 2200 36
Table 2. Clinical details of women trcated with magnesium o r placebo during pregnancy
Magnesium group Centile Variable Number of tabletsiday Duration of medication (days) Total number of tablets Weight gain (kg) Maximum blood pressure (mmHg) Systolic Diastolic No. with oedema (subjective) 5th
3 53
50th
6
95th
6 217 1302 18 135
50th
6
95th
6 224 1344 19 136 87
Significance
NS <041 <041
266 5
107 61
NS
NS NS
NS NS NS NS
85
+ ++ +++
79 15 1 95
Table 3. Indications for hospitalization during pregnancy in women trcatcd with magnesium o r placebo
Variable Number of admissions to hospital ( n ) Number of women hospitalized ( n ) Time spent in hospital (days) Total length Mcdian lengthipatient Indications coded ( n ) Haemorrhage Threatened miscarriage Incompetent cervix Preterm labour Premature membrane rupture Urinary tract infection Diabetes Pre-eclampsia Twin prcgnancy Fetal growth retardation Not encoded Miscarriage
Magnesium group
48 44 533 7.5 4 3 8 12 1 4 1 2 1
Placebo group
80
Significance
65
887
7.0
17 2 17 26 1 2 0 2 2 3 8 3
N S
<041
NS <045
<045
NS NS NS
N S
NS
0 12 5
NS
NS
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Magnesium group Centile Variable Gestational age at delivery (weeksldays) Delivery before 37 weeks (17) Length of 1st stage (h) Length of 2nd stage (rnin) Operative delivery ( n ) 5th 3713 50th 95th
4116
95th
41th
Significance
2 5
4010 7 6 19 70
13 100
2 5
15 90
<0.05 NS NS NS NS
Magnesium group Centile Variable Placental weight (g) Birthweight (g) No. < 2500g No. < 1500g No. < 10th centile Incant length (cm) Head circumlerence (cm) Unihilical blood pH Artery Vein No. with Apgar score Q7 at 1 min at 5 min at 10 rnin Adrnittcd to intensive care ( n ) Indications coded (17) Preterm birth Growth retardation Prolonged asphyxia Observation Respiratory insufficiency Rh-incompatibility Jaundice Malformation facc abdomen multiple Metabolic d i s e a x Fits after delivery Not encoded Perinatal death 5th
400 2.530
Placebo group Centile 95th 800 4270 5th 390 2280 50th
570 3300 19 6 33 49 34 7.28 7.35 47 8 5 36*
95th
800
4120
46 32
7.17 7.23
53 37 ?.37 7.44
45 32
53 37
7.36 744
7.17 7.24
12 3 1 20
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Table 6. Comparison between magnesium and placebo groups afier exclusion o l patients who did not take their tablets regularly* Magnesium group (n=217) Centile Variable* Rirthweight ( 9 ) No. <2500g No. <15t!Ug Infant length (cm) Head circumference (cm) No. with 10-min Apgar scorc S7 No. of womcn hospitalized No. with ocdcma grade+ 5th 2610 50th 3340 6 0 50 35 0 26 42 95th 4285 Placebo group (n=220) Centile 5th 2245
50th
3300 18 6 49 34
95th 4110
Significance
<0.05
<om
<O-05 <045 4.05 <0.05 <0.01 4.05
46 33
53 37
44.5 31
53 36.5
5 48 63
* Only the variables with better significance than in the main analysis are listed.
group and 220 in the placebo group. Some of the differences that only reflected a trend in the main study became statistically significant and some of the differences that werc already significant in the main study were confirmed at a higher level of significance (Table 6).
Discussion
nant women may be compensated by magnesium replacement. More than 300 enzymatic reactions depend on magnesium (Giinther 1981).The results of this study suggest that magnesium supplementation during pregnancy may have important benefits.
Acknowledgments
We found no evidence of a protective effect of magnesium supplementation on thc frcqucncy of pre-eclampsia and to be able to address this question the study groups would have had to have been considerably bigger. Similarly, the observation that a very early start of magensium supplementation is associated with a decreased rate of early miscarriage (Kiss ef al. 1981) could not b e assessed because insufficient numbers of women joined the study early enough and there were no statistically significant differences in the frequency of miscarriage between the groups. In spite of a relatively small difference of only 1 day between the median lengths of gestation, this difference is significant at the 5% level. This is due to fewer preterm deliveries in the magnesium group, an observation which confirms our second hypothesis. Although this difference was reflected in a reduction in thc frequency of low birthweight, there was no evidence that magnesium supplementation had any effect on fetal growth as such. Nevertheless magnesium supplementation was associated with a significant reduction in maternal and fetal morbidity both before and after delivery. It seems reasonable to suppose that the specific magnesium depletion in preg-
We are grateful to Falk Fallenstein, Research Unit, Department of Obstetrics and Gynaecology, University of Bochum. Maricnhospital Herne foi his help in statistical evaluation. We thank Verla-Pharm,Tutring (FGK), for preparing adequate placebo and supplying us with Mg-aspartate-HCI (Magnesiocard).
References
Conradt, A . , Wcidinger, H. & Algayer, H. (1983) O n the role of magnesium in fetal hypolrophy. pregnancy induced hypertension and pre-eclampsia. Mag Bull 6, 68-76 I ~ u m o n t . M. (1965) Traitement des douleur uterM. incs gravidique par le lactate de magncsium. Lyon Med 213, 1571-1582. Giinther, 1.(1981) Biochcmistry and pathobiochcmistry of magnesium. Mug Bull 3, 91-101. Kiss, V . . Balasz, M., Morvay, F., Varenka. Z., Szekely, A . & Szucs, M. (1981) Elfect of maternal magnesium supply on spontaneous abortion and premature birth and o n intraiitcrinc foetal development: experimental epidemiological study. Mag Bull 3, 73-79. Largo, R. H . . Willi, R., Duc, G . , Fariconi, A . & Prader, A . (1980) Evaluation o f perinatal growth. Helv Paediatr Actu 35, 439-436.
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