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血红素加氧酶-1在小鼠孕期的胎盘形成、螺旋动脉重塑及血压调节过程中起关键作用。

Heme oxygenase-1 is critically involved in placentation, spiral artery remodeling, and blood pressure regulation during murine pregnancy.

作者信息

Zenclussen Maria L, Linzke Nadja, Schumacher Anne, Fest Stefan, Meyer Nicole, Casalis Pablo A, Zenclussen Ana C

机构信息

Experimental Obstetrics and Gynecology, Medical Faculty, Otto-von-Guericke University Magdeburg, Magdeburg , Germany.

出版信息

Front Pharmacol. 2015 Jan 13;5:291. doi: 10.3389/fphar.2014.00291. eCollection 2014.

Abstract

The onset of pregnancy implies the appearance of a new organ, the placenta. One main function of the placenta is to supply oxygen to the fetus via hemoproteins. In this review, we highlight the importance of the enzyme heme oxygenase-1 (HO-1) for pregnancy to be established and maintained. HO-1 expression is pivotal to promote placental function and fetal development, thus determining the success of pregnancy. The deletion of the gene Hmox1 in mice leads to inadequate remodeling of spiral arteries and suboptimal placentation followed by intrauterine growth restriction (IUGR) and fetal lethality. A partial Hmox1 deletion leads to IUGR as well, with heterozygote and wild-type fetuses being born, but Hmox1 (-/-) significantly below the expected Mendelian rate. This strong phenotype is associated with diminished number of pregnancy-protective uterine natural killer (uNK) cells. Pregnant heterozygote females develop gestational hypertension. The protective HO-1 effects on placentation and fetal growth can be mimicked by the exogenous administration of carbon monoxide (CO), a product of heme catalyzed by HO-1. CO application promotes the in situ proliferation of uNK cells, restores placentation and fetal growth, while normalizing blood pressure. Similarly, HO-1 inhibition provokes hypertension in pregnant rats. The HO-1/CO axis plays a pivotal role in sustaining pregnancy and aids in the understanding of the biology of pregnancy and reveals a promising therapeutic application in the treatment of pregnancy complications.

摘要

怀孕的开始意味着一个新器官——胎盘的出现。胎盘的一个主要功能是通过血红蛋白向胎儿供应氧气。在这篇综述中,我们强调了血红素加氧酶-1(HO-1)对于怀孕的建立和维持的重要性。HO-1的表达对于促进胎盘功能和胎儿发育至关重要,从而决定了怀孕的成功与否。小鼠中Hmox1基因的缺失会导致螺旋动脉重塑不足和胎盘形成不佳,继而出现宫内生长受限(IUGR)和胎儿死亡。部分Hmox1缺失也会导致IUGR,杂合子和野生型胎儿能够出生,但Hmox1(-/-)胎儿的出生比例显著低于预期的孟德尔比率。这种强烈的表型与具有妊娠保护作用的子宫自然杀伤(uNK)细胞数量减少有关。怀孕的杂合子雌性会出现妊娠期高血压。HO-1对胎盘形成和胎儿生长的保护作用可以通过外源性给予一氧化碳(CO)来模拟,CO是HO-1催化血红素产生的产物。应用CO可促进uNK细胞的原位增殖,恢复胎盘形成和胎儿生长,同时使血压正常化。同样,抑制HO-1会在怀孕大鼠中引发高血压。HO-1/CO轴在维持妊娠中起着关键作用,有助于理解妊娠生物学,并揭示了在治疗妊娠并发症方面有前景的治疗应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bfdb/4292788/96a003ffb2e1/fphar-05-00291-g0001.jpg

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