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出生时的拯救:胎盘成熟缺陷与晚期胎儿死亡

Rescue by birth: defective placental maturation and late fetal mortality.

作者信息

Stallmach T, Hebisch G, Meier K, Dudenhausen J W, Vogel M

机构信息

Pediatric Pathology, Department of Pathology, University Hospital, Zurich, Switzerland.

出版信息

Obstet Gynecol. 2001 Apr;97(4):505-9. doi: 10.1016/s0029-7844(00)01208-4.

DOI:10.1016/s0029-7844(00)01208-4
PMID:11275018
Abstract

OBJECTIVE

To estimate the incidence and lethality of placental maturation defect, and to determine the impact of the pattern of placental dysfunction on the risk of recurrent stillbirth or maternal disease in later life.

METHODS

Questionnaire and archival analysis of fetal deaths from placental dysfunction at 32-42 weeks (1975-1995 in Zurich), classified as chronic (parenchyma loss) or acute (maturation defect of the terminal chorionic villi). Population survey of 17,415 consecutive unselected singleton placentas (1994-1998 in Berlin).

RESULTS

Of the 71 stillbirths, 34 were due to parenchyma loss and 37 to maturation defect. Parenchyma loss predominated in the first pregnancy (73.5% compared with 43.2%; P <.05). The risks of recurrent stillbirth and subsequent childlessness did not differ between the two groups. Eleven percent of mothers whose placenta had maturation defect had diabetes in the index pregnancy; none of the other women in the group developed diabetes over the 5-20-year observation period. In the population survey, incidence of maturation defect was 5.7%, and was associated with fetal death in 2.3% of cases. Normal placentas were associated with fetal death in 0.033%.

CONCLUSION

Placental maturation defect can be a cause of fetal hypoxia. Although the risk of stillbirth is 70-fold that of a normal placenta, few affected fetuses actually die. The risk of recurrent stillbirth is tenfold above baseline and occurs mostly after 35 weeks' gestation.

摘要

目的

评估胎盘成熟缺陷的发生率和致死率,并确定胎盘功能障碍模式对晚期复发性死产风险或母体疾病的影响。

方法

对苏黎世32 - 42周因胎盘功能障碍导致的胎儿死亡进行问卷调查和档案分析(1975 - 1995年),分为慢性(实质丧失)或急性(终末绒毛成熟缺陷)。对柏林连续17415例未经选择的单胎胎盘进行人群调查(1994 - 1998年)。

结果

在71例死产中,34例是由于实质丧失,37例是由于成熟缺陷。实质丧失在初产妇中占主导(73.5%,而成熟缺陷组为43.2%;P < 0.05)。两组复发性死产和随后不育的风险没有差异。胎盘有成熟缺陷的母亲中,11%在本次妊娠时患有糖尿病;在5 - 20年的观察期内,该组其他女性均未患糖尿病。在人群调查中,成熟缺陷的发生率为5.7%,其中2.3%的病例与胎儿死亡有关。正常胎盘与胎儿死亡的关联率为0.033%。

结论

胎盘成熟缺陷可能是胎儿缺氧的一个原因。虽然死产风险是正常胎盘的70倍,但实际死亡的受影响胎儿很少。复发性死产的风险比基线高10倍,大多发生在妊娠35周后。

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