Department of Surgical Sciences, Obstetrics and Gynecology 1, University of Turin, Via Ventimiglia 1, Turin 1026, Italy.
Department of Neuroscience and Mental Health, MS Center, City of Health and Science, University Hospital of Turin, Via Cherasco 15, Turin 10126, Italy.
Mult Scler Relat Disord. 2022 Sep;65:104087. doi: 10.1016/j.msard.2022.104087. Epub 2022 Aug 1.
Multiple sclerosis does not seem to adversely affect fetal and neonatal outcomes, although some studies reported a possible reduction in mean birth weight and length, and a higher incidence of preterm delivery, mainly in relation to the exposure to disease-modifying drugs (DMDs) during pregnancy. Few data are available on intrauterine fetal growth and postnatal somatic development of newborns from mothers with multiple sclerosis compared to those from healthy women. For these reasons, we decided to investigate fetal growth, neonatal anthropometric parameters, and postnatal somatic development up to 12 months of life in offsprings from MS mothers.
This retrospective cohort study included 211 women with multiple sclerosis, and 384 healthy women paired for maternal age and parity as controls. Fetal biometric parameters (biparietal diameter, head circumference, abdominal circumference, and femur length) measured during the third trimester of pregnancy (30-34 weeks' gestation) were retrieved from the computerized database of the Department (EcoPlus*) where the results of ultrasound exams performed in the hospital are stored. Newborn measurements (weight, length and head circumference) at birth were obtained from the hospital's computerized obstetric and neonatal database (Trackare* and Remote* data base); measurements at 6 and 12 months of life were obtained from the regional database (ECWMED*) of family pediatricians of our region.
No differences between the two groups were observed for all the fetal parameters considered, expressed as centiles of growth according to gestational age (biparietal diameter: p = 0.40; head circumference: p = 0.40; abdominal circumference: p = 0.32; femur length: p = 0.32). No differences in gestational age at delivery, birthweight, and in the incidence of low birthweight and small for gestational age newborns were observed between the two groups. In the multiple sclerosis group a significantly higher incidence of caesarean section (p = 0.01) and late preterm delivery (at less than 37 weeks'gestation, p = 0.001) were registered. The trends of postnatal growth in weight (F = 0.53; p-value = 0.590) and length (F = 0.44; p-value = 0.645) were superimposable between the two groups. The trends of growth for head circumference showed a slightly, not significantly greater head circumference of infants from mothers with multiple sclerosis at 6 months of life, but the values at twelve months of life in the two groups were similar (F = 0.85; p-value = 0.427) . Moreover, the trends of postnatal increase of weight (F = 1.016; p-value = 0.331), length (F = 2.001; p-value = 0.146) and head circumference (F = 1.591; p-value = 0.212) of newborns/infants (from birth to twelve months of life) born to mothers with multiple sclerosis who breastfed, mothers who did not, and in the control group were similar.
Multiple sclerosis in pregnancy does not seem to affect fetal growth and postnatal development during the first year of the offspring life. We think that these results represent an important and reassuring information to provide the patients with during preconception counseling.
多发性硬化症似乎不会对胎儿和新生儿结局产生不利影响,尽管一些研究报告称,与健康女性相比,可能会降低胎儿的平均出生体重和身长,早产的发生率更高,主要与怀孕期间使用疾病修正药物(DMD)有关。与健康女性相比,关于多发性硬化症母亲的胎儿宫内生长和新生儿出生后体发育的数据很少。出于这些原因,我们决定研究多发性硬化症母亲的后代在子宫内的胎儿生长、新生儿人体测量参数和出生后 12 个月的体发育情况。
本回顾性队列研究纳入了 211 名多发性硬化症妇女和 384 名年龄和产次相匹配的健康妇女作为对照。从医院计算机化的数据库(EcoPlus*)中检索了妊娠晚期(30-34 周妊娠)胎儿的生物测量参数(双顶径、头围、腹围和股骨长度),该数据库存储了医院进行的超声检查结果;新生儿出生时的测量值(体重、身长和头围)从医院的计算机化产科和新生儿数据库(Trackare和 Remote数据库)中获得;6 个月和 12 个月的测量值从我们地区的家庭儿科医生的区域数据库(ECWMED*)获得。
两组之间没有观察到所有考虑的胎儿参数的差异,这些参数根据胎龄表示为生长百分位数(双顶径:p=0.40;头围:p=0.40;腹围:p=0.32;股骨长度:p=0.32)。两组之间在分娩时的胎龄、出生体重、低出生体重和小于胎龄儿的发生率方面没有差异。在多发性硬化症组中,剖宫产(p=0.01)和晚期早产(不到 37 周的分娩,p=0.001)的发生率显著更高。两组之间的体重(F=0.53;p 值=0.590)和身长(F=0.44;p 值=0.645)的生长趋势相似。头围生长趋势显示,多发性硬化症母亲的婴儿在 6 个月时的头围略大,但在 12 个月时两组的头围相似(F=0.85;p 值=0.427)。此外,母乳喂养的多发性硬化症母亲、未母乳喂养的母亲和对照组的新生儿/婴儿(从出生到 12 个月)的体重(F=1.016;p 值=0.331)、身长(F=2.001;p 值=0.146)和头围(F=1.591;p 值=0.212)的出生后增加趋势相似。
多发性硬化症在怀孕期间似乎不会影响胎儿生长和新生儿在出生后第一年的发育。我们认为,这些结果为患者提供了重要的和令人安心的信息,以帮助他们在怀孕前咨询。
