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己糖激酶-线粒体相互作用在成年和新生心肌细胞中差异调节葡萄糖代谢。

Hexokinase-mitochondrial interactions regulate glucose metabolism differentially in adult and neonatal cardiac myocytes.

机构信息

UCLA Cardiovascular Research Laboratory, 2 Department of Medicine (Cardiology), and 3 Department of Physiology, David Geffen School of Medicine at UCLA, Los Angeles, CA 90095.

出版信息

J Gen Physiol. 2013 Oct;142(4):425-36. doi: 10.1085/jgp.201310968.

Abstract

In mammalian tumor cell lines, localization of hexokinase (HK) isoforms to the cytoplasm or mitochondria has been shown to control their anabolic (glycogen synthesis) and catabolic (glycolysis) activities. In this study, we examined whether HK isoform differences could explain the markedly different metabolic profiles between normal adult and neonatal cardiac tissue. We used a set of novel genetically encoded optical imaging tools to track, in real-time in isolated adult (ARVM) and neonatal (NRVM) rat ventricular myocytes, the subcellular distributions of HKI and HKII, and the functional consequences on glucose utilization. We show that HKII, the predominant isoform in ARVM, dynamically translocates from mitochondria and cytoplasm in response to removal of extracellular glucose or addition of iodoacetate (IAA). In contrast, HKI, the predominant isoform in NRVM, is only bound to mitochondria and is not displaced by the above interventions. In ARVM, overexpression of HKI, but not HKII, increased glycolytic activity. In neonatal rat ventricular myocytes (NVRM), knockdown of HKI, but not HKII, decreased glycolytic activity. In conclusion, differential interactions of HKI and HKII with mitochondria underlie the different metabolic profiles of ARVM and NRVM, accounting for the markedly increased glycolytic activity of NRVM.

摘要

在哺乳动物肿瘤细胞系中,己糖激酶(HK)同工型定位于细胞质或线粒体已被证明可以控制其合成代谢(糖原合成)和分解代谢(糖酵解)活性。在这项研究中,我们研究了 HK 同工型差异是否可以解释正常成年和新生儿心脏组织之间明显不同的代谢特征。我们使用了一组新型的遗传编码光学成像工具,实时跟踪分离的成年(ARVM)和新生(NRVM)大鼠心室肌细胞中 HK I 和 HK II 的亚细胞分布,以及对葡萄糖利用的功能后果。我们表明,HK II 是 ARVM 中的主要同工型,会响应于去除细胞外葡萄糖或添加碘乙酸(IAA)而从线粒体和细胞质中动态移位。相比之下,HK I 是 NRVM 中的主要同工型,仅与线粒体结合,并且不会被上述干预措施置换。在 ARVM 中,过表达 HKI 而不是 HKII 会增加糖酵解活性。在新生大鼠心室肌细胞(NVRM)中,敲低 HKI 而不是 HKII 会降低糖酵解活性。总之,HK I 和 HK II 与线粒体的不同相互作用是 ARVM 和 NRVM 不同代谢特征的基础,解释了 NRVM 明显增加的糖酵解活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2044/3787771/d710c5cc644c/JGP_201310968_Fig1.jpg

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