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正常妊娠、宫内生长受限妊娠及子痫前期妊娠的人胎盘和脐带中的一氧化氮合酶

Nitric oxide synthase in human placenta and umbilical cord from normal, intrauterine growth-retarded and pre-eclamptic pregnancies.

作者信息

Rutherford R A, McCarthy A, Sullivan M H, Elder M G, Polak J M, Wharton J

机构信息

Department of Histochemistry, Royal Postgraduate Medical School, Hammersmith Hospital, London.

出版信息

Br J Pharmacol. 1995 Dec;116(8):3099-109. doi: 10.1111/j.1476-5381.1995.tb15111.x.

Abstract
  1. It has been suggested that a deficiency of nitric oxide (NO) may explain many of the pathophysiological features of pre-eclampsia (PE) and intra-uterine (foetal) growth retardation (IUGR). To elucidate further the role of NO in the pathophysiology of pregnancy we have determined the relative amount and activity of NO synthase (NOS) in first trimester and normal-term placental tissues, as well as in the placenta and umbilical cord in pregnancies complicated by PE and IUGR, using NG-nitro-L-[2,3,4,5(-3)H]-arginine ([3H]-L-NOARG) binding, quantitative in vitro autoradiography, [3H]-arginine to [3H]-citrulline conversion and Western blotting. 2. Specific, high affinity (KD = 38 nM) [3H]-L-NOARG binding was demonstrated in the villous trophoblast of normal-term placentae. Binding was calcium-independent, stereoselective and exhibited a rank order of inhibition by NOS inhibitors and substrate (L-NOARG > or = L-NMMA > or = 7-NI > L-NAME > L-Arg > or = L-NIO > ADMA). 3. [3H]-L-NOARG binding density and NOS activity were both significantly greater in placental tissues from first trimester and PE or IUGR complicated pregnancies compared to normal-term placentae. 4. Western blotting, using an endothelial NOS peptide antiserum, demonstrated a approximately 140 KDa protein band in placental extracts and indicated that the amount of immunoreactive material was significantly greater in first trimester compared to normal-term placentae. 5. Specific [3H]-L-NOARG binding was also localized to the endothelial lining of umbilical arteries and veins, binding density being greater in the artery than the vein. [3H]-L-NOARG binding to the umbilical artery endothelium was significantly lower in PE and IUGR complicated pregnancies compared to normal-term controls. 6. The role of trophoblast-derived NO in human placental pathophysiology remains to be established, but differences in the amount of placental [3H]-L-NOARG binding, NOS activity and immunoreactive material indicate that expression of NOS in the villous trophoblast falls during pregnancy. Conversely, the apparent reduction in NOS in the umbilical artery endothelium in PE and IUGR complicated pregnancies may be indicative of endothelial dysfunction.
摘要
  1. 有人提出,一氧化氮(NO)缺乏可能解释先兆子痫(PE)和宫内(胎儿)生长受限(IUGR)的许多病理生理特征。为了进一步阐明NO在妊娠病理生理学中的作用,我们使用NG-硝基-L-[2,3,4,5(-3)H]-精氨酸([3H]-L-NOARG)结合、定量体外放射自显影、[3H]-精氨酸到[3H]-瓜氨酸的转化以及蛋白质免疫印迹法,测定了孕早期和足月胎盘组织中,以及患有PE和IUGR的妊娠胎盘和脐带中一氧化氮合酶(NOS)的相对含量和活性。2. 在足月胎盘的绒毛滋养层中证实了特异性、高亲和力(KD = 38 nM)的[3H]-L-NOARG结合。结合不依赖钙,具有立体选择性,并且NOS抑制剂和底物对其抑制作用呈现出一定的顺序(L-NOARG ≥ L-NMMA ≥ 7-NI > L-NAME > L-Arg ≥ L-NIO > ADMA)。3. 与足月胎盘相比,孕早期以及患有PE或IUGR的妊娠胎盘组织中的[3H]-L-NOARG结合密度和NOS活性均显著更高。4. 使用内皮型NOS肽抗血清进行蛋白质免疫印迹分析,在胎盘提取物中显示出一条约140 kDa的蛋白条带,并且表明与足月胎盘相比,孕早期免疫反应性物质的量显著更多。5. 特异性[3H]-L-NOARG结合也定位于脐动脉和静脉的内皮,动脉中的结合密度高于静脉。与足月对照组相比,患有PE和IUGR的妊娠中,[3H]-L-NOARG与脐动脉内皮的结合显著降低。6. 滋养层来源的NO在人类胎盘病理生理学中的作用仍有待确定,但胎盘[3H]-L-NOARG结合量、NOS活性和免疫反应性物质的差异表明,绒毛滋养层中NOS的表达在孕期下降。相反,患有PE和IUGR的妊娠中脐动脉内皮中NOS的明显减少可能表明存在内皮功能障碍。

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