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妊娠早期类似绒毛膜癌的人绒毛膜促性腺激素(HCG)及HCG生物活性

Choriocarcinoma-like human chorionic gonadotrophin (HCG) and HCG bioactivity during the first trimester of pregnancy.

作者信息

Mock P, Kovalevskaya G, O'Connor J F, Campana A

机构信息

Department of Obstetrics and Gynaecology, University Hospital, Geneva, Switzerland.

出版信息

Hum Reprod. 2000 Oct;15(10):2209-14. doi: 10.1093/humrep/15.10.2209.

Abstract

The objective of this study was to evaluate the distribution of choriocarcinoma-like human chorionic gonadotrophin (HCG) isoforms during first trimester pregnancy and their relationship with in-vitro HCG bioactivity. This was done by means of a retrospective analysis of patients' sera with first trimester normal intrauterine and abnormal (ectopic) pregnancies. Serum samples were obtained from 38 women with an amenorrhoea of <10 weeks. From these, 19 had a normal intrauterine pregnancy (IUP) and 19 an ectopic pregnancy (EP). Total immunoreactive HCG (HCGi), free beta-HCGi and oestradiol were measured by enzyme immunoassays and bioactive HCG by the mouse Leydig cell bioassay. The alterations in HCG isoform content were measured by the combination of two immunometric assays, B152 for choriocarcinoma-like HCG and B109 for intact HCG detection and expressed as the B152/B109 ratio. Choriocarcinoma-like HCG isoforms ratio measured by B152 and B109 assays was significantly higher in the low subgroups of free beta-HCGi and gestational age (P = 0.0111 and 0.0036 respectively). Whereas bioactive to immunoreactive HCG ratios (b/i ratio) were significantly higher when free beta-HCGi concentrations were low (P = 0.0010), no correlation was found between the variation of bioactivity (b/i ratio) and the proportion of choriocarcinoma-like HCG isoforms (B159/B108). It is concluded that in first trimester pregnancies (i) the modulation of HCG in-vitro bioactivity is not related to the variation of choriocarcinoma-like HCG isoforms secretion and (ii) the amount of choriocarcinoma-like HCG isoforms secreted by the early trophoblast is predominant and may be the result of an early developmental regulation of glycosylation enzyme.

摘要

本研究的目的是评估妊娠早期绒毛膜癌样人绒毛膜促性腺激素(HCG)异构体的分布及其与体外HCG生物活性的关系。这是通过对妊娠早期宫内妊娠正常和异常(异位)妊娠患者的血清进行回顾性分析来完成的。从38名闭经<10周的女性中获取血清样本。其中,19名有正常宫内妊娠(IUP),19名有异位妊娠(EP)。通过酶免疫测定法测量总免疫反应性HCG(HCGi)、游离β-HCGi和雌二醇,通过小鼠睾丸间质细胞生物测定法测量生物活性HCG。通过两种免疫测定法的组合测量HCG异构体含量的变化,B152用于检测绒毛膜癌样HCG,B109用于检测完整HCG,并以B152/B109比值表示。通过B152和B109测定法测量的绒毛膜癌样HCG异构体比值在游离β-HCGi和孕周的低亚组中显著更高(分别为P = 0.0111和0.0036)。虽然当游离β-HCGi浓度较低时,生物活性与免疫反应性HCG比值(b/i比值)显著更高(P = 0.0010),但未发现生物活性变化(b/i比值)与绒毛膜癌样HCG异构体比例(B159/B108)之间存在相关性。得出的结论是,在妊娠早期(i)HCG体外生物活性的调节与绒毛膜癌样HCG异构体分泌的变化无关,(ii)早期滋养层分泌的绒毛膜癌样HCG异构体数量占主导,可能是糖基化酶早期发育调节的结果。

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