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宫内吸烟暴露导致胎儿肝脏金属硫蛋白表达减少:是否与母体低锌水平有关?

Reduced hepatic metallothionein expression in first trimester fetuses in response to intrauterine smoking exposure: a consequence of low maternal zinc levels?

机构信息

Department of Biomedicine, Aarhus University, 8000 Aarhus C, Denmark.

Department of Obstetrics and Gynecology, Herning Regional Hospital, 7400 Herning, Denmark.

出版信息

Hum Reprod. 2019 Nov 1;34(11):2129-2143. doi: 10.1093/humrep/dez197.

Abstract

STUDY QUESTION

Does maternal smoking in early pregnancy affect metallothionein 1 and 2 (MT1 and MT2) mRNA and protein expression in first trimester placenta or embryonic/fetal liver?

SUMMARY ANSWER

In the first trimester, MT protein expression is seen only in liver, where smoking is associated with a significantly reduced expression.

WHAT IS KNOWN ALREADY

Zinc homeostasis is altered by smoking. Smoking induces MT in the blood of smokers properly as a result of the cadmium binding capacities of MT. In term placenta MT is present and smoking induces gene and protein expression (MT2 in particular), but the MT presence and response to smoking have never been examined in first trimester placenta or embryonic/fetal tissues.

STUDY DESIGN, SIZE, DURATION: Cross sectional study where the presence of MT mRNA and protein was examined at the time of the abortion. The material was collected with informed consent after surgical intervention and frozen immediately. For protein expression analysis, liver tissue originating from smoking exposed n = 10 and unexposed n = 12 pregnancies was used. For mRNA expression analyses, placental tissue originating from smokers n = 19 and non-smokers n = 23 and fetal liver tissue from smoking exposed n = 16 and smoking unexposed pregnancies n = 13, respectively, were used.

PARTICIPANTS/MATERIALS, SETTING, METHODS: Tissues were obtained from women who voluntarily and legally chose to terminate their pregnancy between gestational week 6 and 12. Western blot was used to determine the protein expression of MT, and real-time PCR was used to quantify the mRNA expression of MT2A and eight MT1 genes alongside the expression of key placental zinc transporters: zinc transporter protein-1 (ZNT1), Zrt-, Irt-related protein-8 and -14 (ZIP8 and ZIP14).

MAIN RESULTS AND THE ROLE OF CHANCE

A significant reduction in the protein expression of MT1/2 in liver tissue (P = 0.023) was found by western blot using antibodies detecting both MT forms. Overall, a similar tendency was observed on the mRNA level although not statistically significant. Protein expression was not present in placenta, but the mRNA regulation suggested a down regulation of MT as well. A suggested mechanism based on the known role of MT in zinc homeostasis could be that the findings reflect reduced levels of easily accessible zinc in the blood of pregnant smokers and hence a reduced MT response in smoking exposed fetal/embryonic tissues.

LIMITATIONS AND REASONS FOR CAUTION

Smoking was based on self-reports; however, our previous studies have shown high consistency regarding cotinine residues and smoking status. Passive smoking could interfere but was found mainly among smokers. The number of fetuses was limited, and other factors such as medication and alcohol might affect the findings. Information on alcohol was not consistently obtained, and we cannot exclude that it was more readily obtained from non-users. In the study, alcohol consumption was reported by a limited number (less than 1 out of 5) of women but with more smokers consuming alcohol. However, the alcohol consumption reported was typically limited to one or few times low doses. The interaction between alcohol and smoking is discussed in the paper. Notably we would have liked to measure zinc status to test our hypothesis, but maternal blood samples were not available.

WIDER IMPLICATIONS OF THE FINDINGS

Zinc deficiency-in particular severe zinc deficiency-can affect pregnancy outcome and growth. Our findings indicate that zinc homeostasis is also affected in early pregnancy of smokers, and we know from pilot studies that even among women who want to keep their babies, the zinc status is low. Our findings support that zinc supplements should be considered in particular to women who smoke.

STUDY FUNDING/COMPETING INTEREST(S): We thank the Department of Biomedicine for providing laboratory facilities and laboratory technicians and the Lundbeck Foundation and Læge Sofus Carl Emil Friis og Hustru Olga Doris Friis Legat for financial support. The authors have no competing interests to declare.

TRIAL REGISTRATION NUMBER

N/A.

摘要

研究问题

母亲在妊娠早期吸烟是否会影响孕早期胎盘或胚胎/胎儿肝脏中金属硫蛋白 1 和 2(MT1 和 MT2)的 mRNA 和蛋白表达?

总结答案

在孕早期,仅在肝脏中观察到 MT 蛋白表达,而吸烟与 MT 表达显著降低有关。

已知情况

吸烟会改变锌的稳态。吸烟会诱导血液中的 MT,这是由于 MT 的镉结合能力。在足月胎盘中存在 MT,并且吸烟会诱导基因和蛋白表达(特别是 MT2),但在妊娠早期胎盘或胚胎/胎儿组织中从未检查过 MT 的存在和对吸烟的反应。

研究设计、规模、持续时间:在流产时检查 MT mRNA 和蛋白的存在情况。该材料是在手术干预后经知情同意收集的,并立即冷冻。为了进行蛋白表达分析,使用了 10 名暴露于吸烟的孕妇和 12 名未暴露于吸烟的孕妇的肝脏组织。为了进行 mRNA 表达分析,使用了 19 名吸烟者和 23 名非吸烟者的胎盘组织,以及 16 名暴露于吸烟的孕妇和 13 名未暴露于吸烟的孕妇的胎儿肝脏组织。

参与者/材料、设置、方法:从自愿合法选择在妊娠 6 至 12 周期间终止妊娠的妇女中获取组织。使用 Western blot 确定 MT 的蛋白表达,使用实时 PCR 定量 MT2A 和 8 个 MT1 基因以及关键胎盘锌转运蛋白的 mRNA 表达:锌转运蛋白 1(ZNT1)、Zrt-、Irt 相关蛋白-8 和 -14(ZIP8 和 ZIP14)。

主要结果和机会的作用

使用检测两种 MT 形式的抗体进行 Western blot 发现,肝脏组织中 MT1/2 的蛋白表达显著降低(P=0.023)。总体而言,尽管没有统计学意义,但在 mRNA 水平上也观察到类似的趋势。胎盘组织中未发现蛋白表达,但 mRNA 调节表明 MT 也下调。根据 MT 在锌稳态中的已知作用提出的一种机制可能是,这些发现反映了妊娠吸烟者血液中易获得锌水平降低,因此吸烟暴露的胎儿/胚胎组织中的 MT 反应降低。

局限性和谨慎的原因

吸烟是基于自我报告的;然而,我们之前的研究表明,关于可替宁残留物和吸烟状况的一致性很高。被动吸烟可能会产生干扰,但主要存在于吸烟者中。胎儿数量有限,其他因素如药物和酒精也可能影响结果。关于酒精的信息没有得到一致的获取,我们不能排除它更容易从非使用者那里获得。在研究中,报告的酒精摄入量(不到 1/5)数量有限,但吸烟者中饮酒者更多。然而,报告的酒精摄入量通常仅限于一两次低剂量。本文讨论了酒精和吸烟之间的相互作用。值得注意的是,我们本想测量锌的状态来检验我们的假设,但无法获得孕妇的血液样本。

研究结果的更广泛意义

锌缺乏症,特别是严重的锌缺乏症,会影响妊娠结局和生长。我们的研究结果表明,吸烟也会影响早期妊娠的锌稳态,我们从试点研究中知道,即使是那些想留住孩子的妇女,锌的状态也很低。我们的研究结果支持,特别是对于吸烟的妇女,应考虑补充锌。

研究资金/利益冲突:我们感谢生物医学系提供实验室设施和实验室技术人员,以及隆德基金会和 Læge Sofus Carl Emil Friis 及其夫人 Olga Doris Friis Legat 的财政支持。作者没有利益冲突。

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