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正常和非典型丁酰胆碱酯酶在胎盘发育、功能及功能异常中的作用

Normal and atypical butyrylcholinesterases in placental development, function, and malfunction.

作者信息

Sternfeld M, Rachmilewitz J, Loewenstein-Lichtenstein Y, Andres C, Timberg R, Ben-Ari S, Glick C, Soreq H, Zakut H

机构信息

Department of Biological Chemistry, Hebrew University of Jerusalem, Israel.

出版信息

Cell Mol Neurobiol. 1997 Jun;17(3):315-32. doi: 10.1023/a:1026394302076.

Abstract
  1. In utero exposure to poisons and drugs (e.g., anticholinesterases, cocaine) is frequently associated with spontaneous absorption and placental malfunction. The major protein interacting with these compounds is butyrylcholinesterase (BuChE), which attenuates the effects of such xenobiotics by their hydrolysis or sequestration. Therefore, we studied BuChE expression during placental development. 2. RT-PCR revealed both BuChEmRNA and acetylcholinesterase (AChE) mRNA throughout gestation. However, cytochemical staining detected primarily BuChE activity in first-trimester placenta but AChE activity in term placenta. 3. As the atypical variant of BuChE has a narrower specificity for substrates and inhibitors than the normal enzyme, we investigated its interactions with alpha-solanine and cocaine, and sought a correlation between the occurrence of this variant and placental malfunction. 4. Atypical BuChE of serum or recombinant origin presented > 10-fold weaker affinities than normal BuChE for cocaine and alpha-solanine. However, BuChE in the serum of the heterozygote and a homozygous normal were similar in their drug affinities. Therefore, heterozygous serum or placenta can protect the fetus from drug or poison exposure, unlike homozygous atypical serum or placenta. 5. Genotype analyses revealed that heterozygous carriers of atypical BuChE were threefold less frequent among 49 patients with placental malfunction than among 76 controls of the entire Israeli population. These observations exclude heterozygote carriers of atypical BuChE from being at high risk for placental malfunction under exposure to anticholinesterases.
摘要
  1. 子宫内接触毒物和药物(如抗胆碱酯酶、可卡因)常与自然吸收和胎盘功能异常有关。与这些化合物相互作用的主要蛋白质是丁酰胆碱酯酶(BuChE),它通过水解或隔离来减弱此类异源生物的作用。因此,我们研究了胎盘发育过程中BuChE的表达。2. RT-PCR显示在整个妊娠期均有BuChE mRNA和乙酰胆碱酯酶(AChE)mRNA。然而,细胞化学染色在孕早期胎盘中主要检测到BuChE活性,而在足月胎盘中检测到AChE活性。3. 由于BuChE的非典型变体对底物和抑制剂的特异性比正常酶更窄,我们研究了它与α-茄碱和可卡因的相互作用,并寻找这种变体的出现与胎盘功能异常之间的相关性。4. 血清或重组来源的非典型BuChE对可卡因和α-茄碱的亲和力比正常BuChE弱10倍以上。然而,杂合子和纯合正常个体血清中的BuChE对药物的亲和力相似。因此,与纯合非典型血清或胎盘不同,杂合子血清或胎盘可以保护胎儿免受药物或毒物暴露。5. 基因型分析显示,在49例胎盘功能异常患者中,非典型BuChE杂合子携带者的频率比整个以色列人群的76例对照者低三倍。这些观察结果排除了非典型BuChE杂合子携带者在接触抗胆碱酯酶时发生胎盘功能异常的高风险。

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