Department of Surgery, University of Tennessee Graduate School of Medicine, Knoxville, Tennessee.
Department of Surgery, University of Tennessee Graduate School of Medicine, Knoxville, Tennessee.
J Surg Res. 2014 Jul;190(1):319-27. doi: 10.1016/j.jss.2014.03.017. Epub 2014 Mar 12.
Androgen deficiency (AD) is associated with increased risk of atherosclerosis, cardiovascular, and peripheral arterial disease. Although the biochemical and molecular mechanisms underlying this risk remain unclear, higher testosterone (TST) levels correlate to significant immunoprotective molecular and cellular responses. Our group has previously demonstrated that female sex hormones influence vascular pathogenesis via inflammatory-modulated matrix metalloproteinase (MMP) regulation. Here we investigated the role of AD and androgen replacement therapy in the modulation of these hormonally responsive pathways that could be playing a role in the development of vascular pathogenesis.
Aged orchiectomized male rats underwent TST supplementation per controlled release pellet implantation (0-150 mg). Young and aged intact groups served as controls. Serum was collected at 0-4 wk and analyzed by enzyme-linked immunosorbent assays, qualitative cytokine screening, and quantitative multiplex analyses. Human aortic smooth muscle cells were treated with 4,5α-dihydrotestosterone (DHT; 0-3000 nM) before or after interleukin 1β (IL-1β; 5 ng/mL) stimulation. Quantitative polymerase chain reaction and in-gel zymography was used to assay the effect on MMP expression and activity.
Subphysiological, physiological, and supraphysiological levels of TST were achieved with 0.5, 2.5, and 35 mg TST pellet implants in vivo, respectively. Inflammatory arrays indicated that interleukin cytokines, specifically IL-2, IL-6, IL-10, IL-12, and IL-13, were elevated at subphysiological level of TST, whereas TST supplementation decreased interleukins. Supraphysiological TST resulted in a significant increase in MMP-9 and tissue inhibitor of metalloproteinase-1 (TIMP-1) in vivo. Pretreatment with IL-1β slightly increased membrane type 1-MMP (MT1-MMP) and MMP-2 expression at low to mid-level DHT exposure in vitro, although these trends were not statistically significant.
Here we demonstrate AD is a proinflammatory modulator and indicate that MMP-independent mechanisms may play a role downstream of AD-induced inflammatory signaling in dysfunctional vascular remodeling. Future in vivo studies will examine AD and TST supplementation in acute inflammatory response to vascular injury and in MMP-modulated vascular disease.
雄激素缺乏(AD)与动脉粥样硬化、心血管和外周动脉疾病的风险增加有关。尽管这种风险的生化和分子机制尚不清楚,但较高的睾丸酮(TST)水平与显著的免疫保护分子和细胞反应相关。我们的小组先前已经证明,女性性激素通过炎症调节的基质金属蛋白酶(MMP)调节来影响血管发病机制。在这里,我们研究了 AD 和雄激素替代疗法在调节这些激素反应途径中的作用,这些途径可能在血管发病机制的发展中发挥作用。
年老的去势雄性大鼠通过控制释放微球植入(0-150mg)进行 TST 补充。年轻和年老的完整组作为对照。在 0-4 周时收集血清,通过酶联免疫吸附试验、定性细胞因子筛选和定量多重分析进行分析。用人主动脉平滑肌细胞在白细胞介素 1β(IL-1β;5ng/mL)刺激之前或之后用 4,5α-二氢睾丸酮(DHT;0-3000nM)处理。定量聚合酶链反应和凝胶内酶谱法用于测定对 MMP 表达和活性的影响。
在体内,分别用 0.5、2.5 和 35mg TST 微球植入物实现了亚生理、生理和超生理水平的 TST。炎症分析表明,白细胞介素细胞因子,特别是 IL-2、IL-6、IL-10、IL-12 和 IL-13,在 TST 的亚生理水平升高,而 TST 补充降低了白细胞介素。超生理水平的 TST 导致 MMP-9 和组织金属蛋白酶抑制剂-1(TIMP-1)在体内的显著增加。在体外,IL-1β 预处理在低至中水平的 DHT 暴露下略微增加了膜型 1-MMP(MT1-MMP)和 MMP-2 的表达,但这些趋势在统计学上并不显著。
在这里,我们证明 AD 是一种促炎调节剂,并表明 MMP 非依赖性机制可能在 AD 诱导的炎症信号下游在功能失调的血管重塑中发挥作用。未来的体内研究将检查 AD 和 TST 补充在血管损伤后的急性炎症反应中和 MMP 调节的血管疾病中的作用。
