具有XY性染色体组成的雌性小鼠会发展出严重的血管紧张素II诱导的腹主动脉瘤。
Female Mice With an XY Sex Chromosome Complement Develop Severe Angiotensin II-Induced Abdominal Aortic Aneurysms.
作者信息
Alsiraj Yasir, Thatcher Sean E, Charnigo Richard, Chen Kuey, Blalock Eric, Daugherty Alan, Cassis Lisa A
机构信息
From Department of Pharmacology and Nutritional Sciences (Y.A., S.E.T., K.C., E.B., L.A.C.), Department of Biostatistics (R.C.), Department of Physiology and Saha Cardiovascular Research Center (A.D.), University of Kentucky, Lexington, KY.
出版信息
Circulation. 2017 Jan 24;135(4):379-391. doi: 10.1161/CIRCULATIONAHA.116.023789. Epub 2016 Nov 4.
BACKGROUND
Abdominal aortic aneurysms (AAAs) are a deadly pathology with strong sexual dimorphism. Similar to humans, female mice exhibit far lower incidences of angiotensin II-induced AAAs than males. In addition to sex hormones, the X and Y sex chromosomes, and their unique complements of genes, may contribute to sexually dimorphic AAA pathology. Here, we defined the effect of female (XX) versus male (XY) sex chromosome complement on angiotensin II-induced AAA formation and rupture in phenotypically female mice.
METHODS
Female low-density lipoprotein receptor (Ldlr) deficient mice with an XX or XY sex chromosome complement were infused with angiotensin II for 28 days to induce AAAs. Abdominal aortic lumen diameters were quantified by ultrasound, whereas AAA diameters were quantified at study end point. DNA microarrays were performed on abdominal aortas. To mimic males, female mice were administered a single dose of testosterone as neonates or as adults before angiotensin II infusions.
RESULTS
Female Ldlr deficient mice with an XX and XY sex chromosome complement had similar sex organ weights and low serum testosterone concentrations. Abdominal aortas from female XY mice selectively expressed Y chromosome genes, whereas genes known to escape X inactivation were higher in XX females. The majority of aortic gene differences in XY versus XX females fell within inflammatory pathways. AAA incidences doubled and aneurysms ruptured in XY females. AAAs from XY females exhibited inflammation, and plasma interleukin-1β concentrations were increased in XY females. Moreover, aortas from XY females had augmented matrix metalloproteinase activity and increased oxidative stress. Last, testosterone exposure applied chronically, or as a single bolus at postnatal day 1, markedly worsened AAA outcomes in XY in comparison with XX adult females.
CONCLUSIONS
An XY sex chromosome complement in phenotypic females profoundly influenced aortic gene expression profiles and promoted AAA severity. When XY females were exposed to testosterone, aneurysm rupture rates were striking. Mechanisms for augmented AAA severity in XY females include increased inflammation, augmented matrix metalloproteineases, and oxidative stress. Our results demonstrate that genes on the sex chromosomes regulate aortic vascular biology and contribute to sexual dimorphism of AAAs. Sex chromosome genes may serve as novel targets for sex-specific AAA therapeutics.
背景
腹主动脉瘤(AAA)是一种具有强烈性别差异的致命性病理状态。与人类相似,雌性小鼠发生血管紧张素II诱导的腹主动脉瘤的发生率远低于雄性。除了性激素外,X和Y性染色体及其独特的基因组合可能导致腹主动脉瘤病理状态的性别差异。在此,我们确定了雌性(XX)与雄性(XY)性染色体组合对血管紧张素II诱导的表型雌性小鼠腹主动脉瘤形成和破裂的影响。
方法
对具有XX或XY性染色体组合的雌性低密度脂蛋白受体(Ldlr)缺陷小鼠输注血管紧张素II 28天以诱导腹主动脉瘤。通过超声定量腹主动脉管腔直径,而在研究终点定量腹主动脉瘤直径。对腹主动脉进行DNA微阵列分析。为模拟雄性,在血管紧张素II输注前,对雌性小鼠在新生期或成年期给予单剂量睾酮。
结果
具有XX和XY性染色体组合的雌性Ldlr缺陷小鼠具有相似的性器官重量和低血清睾酮浓度。来自雌性XY小鼠的腹主动脉选择性表达Y染色体基因,而已知逃避X染色体失活的基因在XX雌性中表达较高。XY与XX雌性之间的大多数主动脉基因差异存在于炎症途径中。XY雌性的腹主动脉瘤发生率翻倍且动脉瘤破裂。来自XY雌性的腹主动脉瘤表现出炎症,且XY雌性的血浆白细胞介素-1β浓度升高。此外,来自XY雌性的主动脉具有增强的基质金属蛋白酶活性和增加的氧化应激。最后,与XX成年雌性相比,长期给予睾酮或在出生后第1天给予单次推注睾酮,显著恶化了XY雌性的腹主动脉瘤结局。
结论
表型雌性中的XY性染色体组合深刻影响主动脉基因表达谱并促进腹主动脉瘤的严重程度。当XY雌性暴露于睾酮时,动脉瘤破裂率惊人。XY雌性中腹主动脉瘤严重程度增加的机制包括炎症增加、基质金属蛋白酶增强和氧化应激。我们的结果表明,性染色体上的基因调节主动脉血管生物学并导致腹主动脉瘤的性别差异。性染色体基因可能成为性别特异性腹主动脉瘤治疗的新靶点。
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