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人房颤心房中解整合素金属蛋白酶(ADAMs)的表达改变

Altered expression of ADAMs (A Disintegrin And Metalloproteinase) in fibrillating human atria.

作者信息

Arndt Marco, Lendeckel Uwe, Röcken Christoph, Nepple Karen, Wolke Carmen, Spiess Antje, Huth Christof, Ansorge Siegfried, Klein Helmut U, Goette Andreas

机构信息

Institute of Experimental Internal Medicine, University Hospital Magdeburg, Germany.

出版信息

Circulation. 2002 Feb 12;105(6):720-5. doi: 10.1161/hc0602.103639.

DOI:10.1161/hc0602.103639
PMID:11839628
Abstract

BACKGROUND

ADAMs (A Disintegrin And Metalloproteinase) are ectoproteases that have recently been reported to be expressed in cardiac tissue. Although they are known to regulate cell-cell and cell-matrix interactions, their pathophysiological role in various cardiac diseases is unclear. The purpose of the present study was to determine whether structural remodeling of the atria during atrial fibrillation (AF) is associated with altered ADAM expression.

METHODS AND RESULTS

Atrial tissue samples of 30 patients undergoing open-heart surgery were examined. Fifteen patients had persistent AF (> or =6 months), and the remaining 15 patients had no history of AF. ADAM9, ADAM10, and ADAM15 expression was analyzed quantitatively at the mRNA and protein levels. ADAM expression was localized by immunohistochemistry. ADAM expression was correlated with amounts of integrins beta1 and beta3. The amount of ADAM10 protein more than doubled during AF (82+/-15 versus 36+/-8 U; P<0.01). Amounts of ADAM15 protein (102+/-12 versus 40+/-6 U; P<0.01) and mRNA (24.0+/-5.6 versus 10.5+/-2.5 U; P<0.05) increased significantly during AF compared with sinus rhythm. ADAM9 protein was not detected in any sample. ADAM/integrin ratios showed an increase of 4- to 6-fold (P<0.05) in patients with AF who had significantly dilated atria (4.94+/-0.6 versus 4.3+/-0.7 cm; P<0.05). ADAM/integrin ratios correlated with atrial diameter.

CONCLUSIONS

AF is associated with an increase in the expression of ADAM10 and ADAM15. Enhanced ADAM-dependent disintegrin and metalloproteinase activity may be a molecular mechanism that contributes to the dilation of fibrillating human atria.

摘要

背景

ADAMs(一种去整合素和金属蛋白酶)是一种外切蛋白酶,最近有报道称其在心脏组织中表达。尽管已知它们可调节细胞间和细胞与基质间的相互作用,但其在各种心脏疾病中的病理生理作用尚不清楚。本研究的目的是确定心房颤动(AF)期间心房的结构重塑是否与ADAM表达的改变有关。

方法与结果

对30例行心脏直视手术患者的心房组织样本进行检查。15例患者患有持续性房颤(≥6个月),其余15例患者无房颤病史。在mRNA和蛋白质水平上对ADAM9、ADAM10和ADAM15的表达进行定量分析。通过免疫组织化学对ADAM表达进行定位。ADAM表达与整合素β1和β3的量相关。在房颤期间,ADAM10蛋白的量增加了一倍多(82±15对36±8 U;P<0.01)。与窦性心律相比,房颤期间ADAM15蛋白的量(102±12对40±6 U;P<0.01)和mRNA(24.0±5.6对10.5±2.5 U;P<0.05)显著增加。在任何样本中均未检测到ADAM9蛋白。在心房明显扩张的房颤患者中(4.94±0.6对4.3±0.7 cm;P<0.05),ADAM/整合素比值增加了4至6倍(P<0.05)。ADAM/整合素比值与心房直径相关。

结论

房颤与ADAM10和ADAM15表达增加有关。增强的ADAM依赖性去整合素和金属蛋白酶活性可能是导致颤动的人心脏心房扩张的一种分子机制。

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