胃肠道血管状况中血管生成因子的共同变化:一项初步研究。

Atiyekeogbebe R Douglas, Grainne Holleran, Sinead M Smith, Deirdre McNamara
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引用次数: 3

摘要

背景:新生血管在各种不同病因和表现的胃肠道疾病中是常见的;通常影响60岁以上的成年人。由疾病特异性因子调节的共享血管生成因子可能是一个共同点,并代表新的诊断和治疗靶点。到目前为止,对几种与复发性出血和贫血相关的胃肠道血管疾病的血管生成因子的评估尚未见报道。目的:评价几种肠道血管疾病患者血清血管生成因子水平。方法:在Tallaght大学医院对经内镜证实的小肠血管发育不全(SBA)、门脉高压性胃病(PHG)、胃胃窦血管扩张(GAVE)和无出血、无贫血对照患者进行病例对照研究。采用酶联免疫吸附法测定知情同意后2根血清管血液中血管生成素1 (ang1)、ang2和血管内皮生长因子(VEGF)的浓度。计算各组间Ang-1、Ang-2的相对表达量及Ang-1/2比值。采用t检验进行统计学分析,P值< 0.05为显著性。结果:迄今为止共检测了44个样本:SBA 10个,PHG 11个,give 8个,对照15个。平均年龄60岁(20-85岁),男性20岁(45%)。对照组明显更年轻(49岁vs 66岁,P = 0.0005)。两组间VEGF水平差异无统计学意义(P = 0.6)。SBA、PHG和give Ang-1水平相似且显著低于对照组(P = 0.0002, 95%CI: 241 ~ 701)。与对照组相比,PHG组和give组Ang-2水平在统计学上较高(P = 0.01, 95%CI: 77.8 ~ 668),因此Ang-1/2比值也较对照组低。SBA组Ang-2水平高于对照组,但无统计学意义。年龄和血红蛋白水平在不同疾病组之间是相似的,都不能解释这种差异。此外,所有患者的中位ang1 / ang2比值均显著低于对照组,分别为8 vs 28, P = 0.001, 95%CI: -27.55 ~ -7.12。结论:我们的新初步研究表明,在几种胃肠道血管疾病中,Ang-1和Ang-2水平发生了共同的改变。血管疾病患者与对照组相比,Ang-1/Ang-2比值的差异提示疾病特异性调节。
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Shared changes in angiogenic factors across gastrointestinal vascular conditions: A pilot study.

Background: Neovascularisation is common to a variety of gastrointestinal (GI) disorders with differing aetiologies and presentations; usually affecting adults above 60 years. Shared angiogenic factors modulated by disease specific elements could be a common denominator and represent novel diagnostic and therapeutic targets. As yet, assessment of angiogenic factors across several GI vascular disorders associated with recurrent bleeding and anaemia has not been reported.

Aim: To assess serum levels of angiogenic factors in several intestinal vascular disorders.

Methods: A case control study was performed in Tallaght University Hospital in patients with endoscopically proven small bowel angiodysplasia (SBA), portal hypertensive gastropathy (PHG), gastric antral vascular ectasia (GAVE) and non-bleeding, non-anaemic controls. Using enzyme-linked immunosorbent assay, concentrations of Angiopoietin 1 (Ang-1), Ang-2 and vascular endothelial growth factor (VEGF) were measured from 2 serum tubes of blood following informed consent. The relative expression of Ang-1 and Ang-2 and Ang-1/2 ratio was calculated and compared between groups. Statistical analysis was applied using a t-test, and a P value of < 0.05 was considered significant.

Results: To date 44 samples were tested: 10 SBA, 11 PHG, 8 GAVE and 15 controls. Mean age 60 (range 20-85) years and 20 (45%) were males. Controls were significantly younger (49 years vs 66 years, P = 0.0005). There was no difference in VEGF levels between the groups (P = 0.6). SBA, PHG and GAVE Ang-1 levels were similar and were significantly lower than controls, (P = 0.0002, 95%CI: 241 to 701). Ang-2 levels were statistically higher in PHG and GAVE groups compared to controls (P = 0.01, 95%CI: 77.8 to 668) and as a result, also had a lower Ang-1/2 ratios compared to controls. While SBA Ang-2 levels were higher than controls, this did not reach statistical significance. Neither age nor haemoglobin level, which was similar between disease groups, could explain the difference. In addition, the median Ang-1/Ang-2 ratio for all patients was found to be significantly lower compared to controls, 8 vs 28 respectively, P = 0.001, 95%CI: -27.55 to -7.12.

Conclusion: Our novel pilot study suggests common alterations in Ang-1 and Ang-2 levels across several GI vascular disorders. Differences in Ang-1/Ang-2 ratios among vascular disorders compared to controls suggest disease-specific modulation.

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