首页> 外文期刊>Diabetic medicine: A journal of the British Diabetic Association >Complications impaired endothelial progenitor cell function in Type 2 diabetic patients with or without critical leg ischaemia: implication for impaired neovascularization in diabetes.
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Complications impaired endothelial progenitor cell function in Type 2 diabetic patients with or without critical leg ischaemia: implication for impaired neovascularization in diabetes.

机译:并发症会损害2型糖尿病伴或不伴有严重腿部缺血的2型糖尿病患者的内皮祖细胞功能:对糖尿病患者新血管形成的影响。

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AIMS: This study tested the hypothesis that migratory function of endothelial progenitor cells (EPCs) is impaired in Type 2 diabetic patients with or without critical leg ischaemia. METHODS: Seventy-four patients were classified into four groups: Type 2 diabetic (n = 21) and non-diabetic patients (n = 10) with critical leg ischaemia and Type 2 diabetic patients without lower extremity vascular disease (n = 30) and healthy subjects (n = 13). The number and functional activity of circulating and cultured EPCs were determined. RESULTS: The migratory function of cultured EPCs was significantly impaired in diabetic patients without (median, 48, interquartile range, 46, 49 count/view/well) and with (median, 51, interquartile range, 46, 60 count/view/well) critical leg ischaemia and non-diabetic patients with critical leg ischaemia (median, 49, interquartile range, 47, 55 count/view/well) compared with healthy subjects (median, 63, interquartile range, 57, 65 count/view/well) (P < 0.0001). The number of circulating EPCs was lower in Type 2 diabetic patients without lower extremity vascular disease (median, 3500, interquartile range, 1600, 6600/10(6) cytometric events) than Type 2 diabetic patients with critical leg ischaemia (median, 5300, interquartile range, 2400, 11,100/10(6) cytometric events), non-diabetic patients with critical leg ischaemia (median, 5550, interquartile range, 2000, 32,100/10(6) cytometric events) and healthy subjects (median, 5400, interquartile range, 2700, 8700/10(6) cytometric events) (P = 0.413). CONCLUSIONS: The migratory function of EPCs is impaired in patients with Type 2 diabetes, even in those without critical leg ischaemia. These findings present an important new insight into the pathogenesis of impaired neovascularization and critical limb ischaemia in diabetic patients and provide avenues of future clinical study.
机译:目的:本研究检验了以下假设:在患有或不患有严重腿部缺血的2型糖尿病患者中,内皮祖细胞(EPC)的迁移功能受到损害。方法:将74例患者分为四组:2型糖尿病伴严重下肢缺血的非糖尿病患者(n = 10)和无下肢血管疾病的2型糖尿病患者(n = 30),以及健康受试者(n = 13)。确定了循环和培养的EPC的数量和功能活性。结果:在无(中位数,48,四分位间距,46,49计数/视图/孔)和有(中位数,51,四分位间距,46,60计数/视图/孔)的糖尿病患者中,培养的EPC的迁移功能显着受损。 )严重腿部缺血和非糖尿病性严重腿部缺血的患者(中位数49,四分位间距47,55计数/视图/孔)与健康受试者(中位数63,四分位间距57,65计数/视图/孔) )(P <0.0001)。没有下肢血管疾病的2型糖尿病患者的循环EPC数量(中位数3500,四分位间距1600、6600 / 10(6)细胞计数事件)低于伴有严重下肢缺血的2型糖尿病患者(中位数5300,四分位数间距,2400、11,100 / 10(6)细胞计数事件),非糖尿病性重症肢体缺血患者(中位数5550,四分位数范围,2000、32,100 / 10(6)细胞计数事件)和健康受试者(中位数5400,四分位间距,2700、8700 / 10(6)细胞计数事件)(P = 0.413)。结论:EPCs的迁移功能在2型糖尿病患者中受损,即使在没有严重腿部缺血的患者中也是如此。这些发现为糖尿病患者新血管形成受损和肢体关键缺血的发病机理提供了重要的新见解,并为将来的临床研究提供了途径。

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