Advanced glycation end products accumulate in vascular smooth muscle and modify vascular but not ventricular properties in elderly hypertensive canines.

Shapiro BP; Owan TE; Mohammed SF; Meyer DM; Mills LD; Schalkwijk CG; Redfield MM

首页> 外文期刊>Circulation: An Official Journal of the American Heart Association >Advanced glycation end products accumulate in vascular smooth muscle and modify vascular but not ventricular properties in elderly hypertensive canines.

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Advanced glycation end products accumulate in vascular smooth muscle and modify vascular but not ventricular properties in elderly hypertensive canines.

机译：晚期糖基化终末产物在血管平滑肌中积累，并改变老年高血压犬的血管特性，但不能改变其心室特性。

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BACKGROUND: Advanced glycation end products (AGEs) are believed to increase left ventricular (LV) and vascular stiffness, in part via cross-linking proteins. We determined whether and where AGEs were increased in elderly hypertensive nondiabetic dogs and whether an AGE cross-link breaker (ALT-711) improved vascular or ventricular function. METHODS AND RESULTS: Elderly dogs with experimental hypertension (old hypertensives [OH]) were randomized to receive ALT-711 (OH+ALT group; n=11; 1 mg/kg PO) or not (OH group; n=11) for 8 weeks. Conscious blood pressure measurements (weekly), echocardiography (week 8), and anesthetized study (week 8) with LV pressure-volume analysis and aortic pressure-dimension and pressure-flow assessment over a range of preloads and afterloads were performed. In LV and aorta from OH, OH+ALT, and young normal dogs, AGE content (immunohistochemistry and Western analysis for N(epsilon)-(carboxymethyl)lysine [CML]) was assessed. Aortic CML content was markedly increased in OH and OH+ALT dogs compared with young normal dogs. CML was localized to aortic and aortic vasa vasorum smooth muscle but not to collagen or elastin. CML was essentially undetectable in young normal, OH, or OH+ALT myocardium but was visible in large vessels in the LV. ALT-711 therapy was associated with lower blood pressure and pulse pressure, decreased systemic vascular resistance, increased aortic distensibility and arterial compliance, and, notably, significant aortic dilatation. Neither LV systolic nor diastolic function was different in OH+ALT versus OH dogs. CONCLUSIONS: In elderly hypertensive canines, AGE accumulation and AGE cross-link breaker effects were confined to the vasculature without evidence of myocardial accumulation or effects. The lack of AGE accumulation in collagen-rich areas suggests that the striking vascular effects may be mediated by mechanisms other than collagen cross-linking.

机译：背景：晚期糖基化终产物（AGEs）被认为会部分通过交联蛋白增加左心室（LV）和血管僵硬。我们确定了老年高血压非糖尿病犬的AGEs是否升高以及在何处升高，以及AGE交联剂（ALT-711）是否改善了血管或心室功能。方法和结果：实验性高血压的老年犬（老年高血压[OH]）随机接受ALT-711（OH + ALT组; n = 11; 1 mg / kg PO）或不接受ALT-711（OH组; n = 11） 8个星期。进行了意识的血压测量（每周一次），超声心动图检查（第8周）和麻醉研究（第8周），并在一系列预紧力和后紧力的基础上进行了LV压力容量分析以及主动脉压力尺寸和压力流量评估。在OH，OH + ALT和年轻正常犬的LV和主动脉中，评估了AGE含量（免疫组化和N（ε）-（羧甲基）赖氨酸[CML]的Western分析）。与年轻的正常犬相比，OH和OH + ALT犬的主动脉CML含量明显增加。 CML定位于主动脉和主动脉血管平滑肌，但不定位于胶原蛋白或弹性蛋白。在年轻的正常人，OH或OH + ALT心肌中，CML基本上不可检测，但在LV的大血管中可见。 ALT-711治疗与降低血压和脉压，降低全身血管阻力，增加主动脉扩张性和动脉顺应性以及显着的主动脉扩张有关。 OH + ALT与OH狗的LV收缩功能和舒张功能均没有差异。结论：在老年高血压犬中，AGE积累和AGE交联破坏作用仅限于脉管系统，而没有心肌积累或作用的证据。胶原蛋白丰富区域缺乏AGE积累表明，血管新生效应可能是由胶原蛋白交联以外的机制介导的。

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《Circulation: An Official Journal of the American Heart Association 》 |2008年第10期| 共9页
作者
Shapiro BP; Owan TE; Mohammed SF; Meyer DM; Mills LD; Schalkwijk CG; Redfield MM;
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正文语种 eng
中图分类心脏、血管（循环系）疾病 ;
关键词
Aging; Animals; Aorta; Collagen; Dogs; Drug Evaluation; Preclinical; Elastin; 衰老; 动物; 主动脉; 胶原; 狗; 弹性蛋白; 糖基化终产物; 高级; 高血压; 赖氨酸;

机译：Aging;Animals;Aorta;Collagen;Dogs;Drug Evaluation;Preclinical;Elastin;衰老;动物;主动脉;胶原;狗;弹性蛋白;糖基化终产物;高级;高血压;赖氨酸;

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专利

1. Advanced glycation end products accumulate in vascular smooth muscle and modify vascular but not ventricular properties in elderly hypertensive canines. [J] . Shapiro BP, Owan TE, Mohammed SF, Circulation: An Official Journal of the American Heart Association . 2008 ,第10期

机译：晚期糖基化终末产物在血管平滑肌中积累，并改变老年高血压犬的血管特性，但不能改变其心室特性。
2. Possible involvement of altered RGD sequence in reduced adhesive and spreading activities of advanced glycation end product-modified fibronectin to vascular smooth muscle cells. [J] . Sakata N, Sasatomi Y, Meng J, Connective tissue research . 2000 ,第3期

机译：RGD序列的改变可能参与了晚期糖基化终产物修饰的纤连蛋白在血管平滑肌细胞中的减少的黏附和扩散活性。
3. Advanced Glycation End-Products Induce Apoptosis of Vascular Smooth Muscle Cells: A Mechanism for Vascular Calcification [J] . Sayo Koike, Shozo Yano, Sayuri Tanaka, International Journal of Molecular Sciences . 2016 ,第9期

机译：先进的糖化终产物诱导血管平滑肌细胞凋亡：血管钙化的机制
4. RAGE engagement and vascular cell derangement by short chain sugar-derived advanced glycation end products [C] . Hideto Yonekura, Yasuhiko Yamamoto, Shigeru Sakurai, International Symposium on the Maillard Reaction . 2002

机译：短链糖衍生的先进糖糖末端产品的愤怒接合和血管细胞紊乱
5. The Synergistic Action of Chronic Ethanol and Reactive Oxygen Species on Insulin Signaling in Hypertensive Vascular Smooth Muscle Cells. [D] . Williams, Sparkle D. 2014

机译：慢性乙醇和活性氧对高血压血管平滑肌细胞中胰岛素信号的协同作用。
6. Advanced Glycation End-products Accumulate in Vascular Smooth Muscle and Modify Vascular but not Ventricular Properties in Elderly Hypertensive Canines [O] . Brian P. Shapiro, Theophilus E. Owan, Selma F. Mohammed, -1

机译：晚期糖基化终末产物在血管平滑肌中积累并改变了老年高血压犬的血管性质但未改变其心室性质
7. Letter by Hartog et al Regarding Article, "Advanced Glycation End Products Accumulate in Vascular Smooth Muscle and Modify Vascular but Not Ventricular Properties in Elderly Hypertensive Canines" [O] . Hartog, Jasper W. L., Willemsen, Suzan, Voors, Adriaan A. 2009

机译：Hartog等人关于文章“老年糖基化终末产物在血管平滑肌中积累并改变血管性而不是心室性的信件”

Advanced glycation end products accumulate in vascular smooth muscle and modify vascular but not ventricular properties in elderly hypertensive canines.

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