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首页> 外文期刊>The journal of maternal-fetal & neonatal medicine >Clues to apoptosis pathway involvement in hemolysis, elevated liver enzyme, and low platelet (HELLP) syndrome and intrauterine growth restriction (IUGR)
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Clues to apoptosis pathway involvement in hemolysis, elevated liver enzyme, and low platelet (HELLP) syndrome and intrauterine growth restriction (IUGR)

机译:凋亡途径参与溶血,肝酶升高,低血小板(HELLP)综合征和子宫内生长受限(IUGR)的线索

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Objective: The neurotrophin family comprises molecules involved in growth, differentiation, survival, regeneration, normal functions of the neuronal system, and in angiogenesis. We have investigated the expression pattern of neurotrophic signaling molecules in pregnancies complicated by elevated liver enzyme, and low platelet (HELLP) syndrome and intrauterine growth restriction (IUGR). Methods: Placentas from normal and pathological pregnancies were collected. Macroarray analysis was performed and the data were confirmed by real-time PCR. Results: Real-time PCR analyses (pathological vs. normal pregnancies) confirmed a significant down-regulation for IL-6, STAT3 alpha, STAT3 beta, and Bcl-2. The expression of Mcl-1 isoform 1 (long) was significantly increased. Conclusions: We suggest that decreased expression of IL-6 could mean that abnormalities in the immunological system function involve inflammatory cytokines other than IL-6 in examined pathological pregnancies. The STAT3 alpha and STAT3 beta down-regulation lead to a marked reduction of cellular transcriptional activity. Decreased expression of IL-6 is associated with a down-regulation of Bcl-2 but not of Mcl-1 isoform 1, suggesting that these two antiapoptotic proteins may function independently and that Mcl-1 may have a distinct role in controlling apoptotic pathway.
机译:目的:神经营养蛋白家族包含与神经元系统的生长,分化,存活,再生,正常功能以及血管生成有关的分子。我们研究了妊娠期间神经营养信号分子在肝酶升高,低血小板(HELLP)综合征和子宫内生长受限(IUGR)的表达模式。方法:收集正常妊娠和病理妊娠的胎盘。进行大阵列分析,并通过实时PCR确认数据。结果:实时PCR分析(病理妊娠与正常妊娠)证实IL-6,STAT3α,STAT3β和Bcl-2明显下调。 Mcl-1同工型1(长)的表达明显增加。结论:我们认为IL-6表达降低可能意味着免疫系统功能异常涉及所检查的病理妊娠中IL-6以外的炎性细胞因子。 STAT3 alpha和STAT3 beta下调导致细胞转录活性明显降低。 IL-6的表达减少与Bcl-2的下调有关,而与Mcl-1的亚型1无关,这表明这两种抗凋亡蛋白可能独立发挥作用,而Mcl-1可能在控制凋亡途径中具有独特的作用。

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