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母体血清甲胎蛋白不明原因升高及随后的胎儿丢失。

Unexplained elevation in maternal serum alpha-fetoprotein and subsequent fetal loss.

作者信息

Maher J E, Davis R O, Goldenberg R L, Boots L R, DuBard M B

机构信息

Department of Obstetrics and Gynecology, University of Alabama at Birmingham.

出版信息

Obstet Gynecol. 1994 Jan;83(1):138-41.

PMID:7505911
Abstract

OBJECTIVE

To examine the frequency and timing of fetal death and its association with maternal serum alpha-fetoprotein (MSAFP) levels.

METHODS

Pregnancy outcomes were evaluated in 6927 predominantly middle-class women (83% white, 17% black) who had second-trimester MSAFP determinations performed in our laboratory. All cases of multiple gestation, preexisting fetal death, and fetal malformation were excluded.

RESULTS

The overall fetal death rate was 13 per 1000 (n = 90). Black women had a higher fetal death rate than white women (35.6 per 1000 versus 8.4 per 1000; P < .001). One hundred forty-eight women (2.1%) had an adjusted MSAFP multiples of the median (MoM) value of at least 2.5, which was not explained by multiple gestation, congenital anomaly, or preexisting fetal death. As the MSAFP increased, the fetal death rate increased (MoM less than 2.0, 11 per 1000; MoM 2-2.49, 29 per 1000; MoM 2.5 or greater, 95 per 1000; P < .001). Despite the increased risk of fetal death in the elevated MSAFP group, most fetal deaths (84%) occurred in women with levels below 2.5 MoM. Furthermore, the timing of fetal loss was significantly different between the group less than 2.5 MoM and the group at or above 2.5 MoM. Fetal death occurred at or after 26 weeks in 45% of the women with normal MSAFP, compared with only 14% of women with high MSAFP (at least 2.5 MoM) (P = .023).

CONCLUSIONS

Women with unexplained elevations in MSAFP are at increased risk for fetal loss, with most of the losses occurring in the second trimester. Because many of these fetal deaths occur at gestational ages when the neonatal survival is very low, it is unlikely that antepartum fetal surveillance aimed at early delivery would substantially increase fetal salvage.

摘要

目的

研究胎儿死亡的频率和时间及其与母血清甲胎蛋白(MSAFP)水平的关联。

方法

对在我们实验室进行孕中期MSAFP测定的6927名主要为中产阶级女性(83%为白人,17%为黑人)的妊娠结局进行评估。所有多胎妊娠、既往胎儿死亡和胎儿畸形病例均被排除。

结果

总体胎儿死亡率为每1000例中有13例(n = 90)。黑人女性的胎儿死亡率高于白人女性(每1000例中35.6例对8.4例;P <.001)。148名女性(2.1%)的校正MSAFP中位数倍数(MoM)值至少为2.5,这无法用多胎妊娠、先天性异常或既往胎儿死亡来解释。随着MSAFP升高,胎儿死亡率增加(MoM小于2.0,每1000例中有11例;MoM 2 - 2.49,每1000例中有29例;MoM 2.5或更高,每1000例中有95例;P <.001)。尽管MSAFP升高组胎儿死亡风险增加,但大多数胎儿死亡(84%)发生在MoM低于2.5的女性中。此外,MoM低于2.5组和MoM等于或高于2.5组之间胎儿丢失的时间有显著差异。MSAFP正常的女性中45%的胎儿死亡发生在26周及以后,而MSAFP高(至少2.5 MoM)的女性中只有14%(P =.023)。

结论

MSAFP不明原因升高的女性胎儿丢失风险增加,大多数丢失发生在孕中期。由于这些胎儿死亡中有许多发生在新生儿存活率非常低的孕周,旨在早期分娩的产前胎儿监测不太可能大幅提高胎儿挽救率。

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