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线粒体转运体 ATP 结合盒线粒体红系是缺血/再灌注后心脏恢复所必需的新基因。

Mitochondrial transporter ATP binding cassette mitochondrial erythroid is a novel gene required for cardiac recovery after ischemia/reperfusion.

机构信息

Department of Medicine, Obesity and Diabetes Research Centers, Boston University School of Medicine, 650 Albany St, Room 804, Boston, MA 02118, USA.

出版信息

Circulation. 2011 Aug 16;124(7):806-13. doi: 10.1161/CIRCULATIONAHA.110.003418. Epub 2011 Jul 25.

DOI:10.1161/CIRCULATIONAHA.110.003418
PMID:21788586
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4491919/
Abstract

BACKGROUND

Oxidative stress and mitochondrial dysfunction are central mediators of cardiac dysfunction after ischemia/reperfusion. ATP binding cassette mitochondrial erythroid (ABC-me; ABCB10; mABC2) is a mitochondrial transporter highly induced during erythroid differentiation and predominantly expressed in bone marrow, liver, and heart. Until now, ABC-me function in heart was unknown. Several lines of evidence demonstrate that the yeast ortholog of ABC-me protects against increased oxidative stress. Therefore, ABC-me is a potential modulator of the outcome of ischemia/reperfusion in the heart.

METHODS AND RESULTS

Mice harboring 1 functional allele of ABC-me (ABC-me(+/-)) were generated by replacing ABC-me exons 2 and 3 with a neomycin resistance cassette. Cardiac function was assessed with Langendorff perfusion and echocardiography. Under basal conditions, ABC-me(+/-) mice had normal heart structure, hemodynamic function, mitochondrial respiration, and oxidative status. However, after ischemia/reperfusion, the recovery of hemodynamic function was reduced by 50% in ABC-me(+/-) hearts as a result of impairments in both systolic and diastolic function. This reduction was associated with impaired mitochondrial bioenergetic function and with oxidative damage to both mitochondrial lipids and sarcoplasmic reticulum calcium ATPase after reperfusion. Treatment of ABC-me(+/-) hearts with the superoxide dismutase/catalase mimetic EUK-207 prevented oxidative damage to mitochondria and sarcoplasmic reticulum calcium ATPase and restored mitochondrial and cardiac function to wild-type levels after reperfusion.

CONCLUSIONS

Inactivation of 1 allele of ABC-me increases the susceptibility to oxidative stress induced by ischemia/reperfusion, leading to increased oxidative damage to mitochondria and sarcoplasmic reticulum calcium ATPase and to impaired functional recovery. Thus, ABC-me is a novel gene that determines the ability to tolerate cardiac ischemia/reperfusion.

摘要

背景

氧化应激和线粒体功能障碍是缺血/再灌注后心脏功能障碍的核心介质。ATP 结合盒线粒体红系(ABC-me;ABCB10;mABC2)是一种在红细胞分化过程中高度诱导的线粒体转运蛋白,主要在骨髓、肝脏和心脏中表达。到目前为止,ABC-me 在心脏中的功能尚不清楚。有几条证据表明,ABC-me 的酵母直系同源物可防止氧化应激增加。因此,ABC-me 是心脏缺血/再灌注结局的潜在调节剂。

方法和结果

通过用新霉素抗性盒替换 ABC-me 的外显子 2 和 3,生成了携带 1 个功能性 ABC-me 等位基因(ABC-me(+/-))的小鼠。通过 Langendorff 灌注和超声心动图评估心脏功能。在基础条件下,ABC-me(+/-) 小鼠的心脏结构、血液动力学功能、线粒体呼吸和氧化状态正常。然而,在缺血/再灌注后,由于收缩和舒张功能均受损,ABC-me(+/-) 心脏的血液动力学功能恢复减少了 50%。这种减少与线粒体生物能功能受损以及再灌注后线粒体脂质和肌浆网钙 ATP 酶的氧化损伤有关。在用超氧化物歧化酶/过氧化氢酶模拟物 EUK-207 处理 ABC-me(+/-) 心脏后,可防止线粒体和肌浆网钙 ATP 酶的氧化损伤,并在再灌注后将线粒体和心脏功能恢复到野生型水平。

结论

ABC-me 的 1 个等位基因失活会增加缺血/再灌注引起的氧化应激易感性,导致线粒体和肌浆网钙 ATP 酶的氧化损伤增加,并导致功能恢复受损。因此,ABC-me 是决定心脏耐受缺血/再灌注能力的新基因。

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