2017
DOI: 10.1016/j.cmet.2017.09.023
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Abrogating Mitochondrial Dynamics in Mouse Hearts Accelerates Mitochondrial Senescence

Abstract: Summary Mitochondrial fusion and fission are critical to heart health; genetically interrupting either is rapidly lethal. To understand whether it is loss of, or the imbalance between, fusion and fission that underlies observed cardiac phenotypes, we engineered mice in which Mfn-mediated fusion and Drp1-mediated fission could be concomitantly abolished. Compared to fusion-defective Mfn1/Mfn2 cardiac knockout or fission-defective Drp1 cardiac knockout mice, Mfn1/Mfn2/Drp1 cardiac triple knockout mice survived l… Show more

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Cited by 252 publications
(203 citation statements)
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“…Indeed, studies indicate suppression of mitophagy with prolonged cardiac stress, such as pressure overload, which can be rescued by stimulating autophagosome formation with Tat-Beclin-1 transduction (196) or enhancing AMPK2α-mediated PINK1 phorphorylation (225). Molecular players that mediate mitochondrial dynamics, namely mitofusins (MFN1 and MFN2) that mediate mitochondrial fusion; and Drp1, that mediates mitochondrial fission, play a critical role in maintaining mitochondrial quality control and regulating mitophagy in the heart (201, 203). Mitochondrial fission via Drp-1 was shown to be essential for basal mitophagy and heterozygous disruption of Drp1 in cardiac myocytes was sufficient to induce cardiomyopathic dysfunction with fasting (91), indicating a critical need for mitophagy under nutrient deprivation conditions (55).…”
Section: Lysosomes As Regulators Of Cardiac Homeostasis and The Fastimentioning
confidence: 99%
“…Indeed, studies indicate suppression of mitophagy with prolonged cardiac stress, such as pressure overload, which can be rescued by stimulating autophagosome formation with Tat-Beclin-1 transduction (196) or enhancing AMPK2α-mediated PINK1 phorphorylation (225). Molecular players that mediate mitochondrial dynamics, namely mitofusins (MFN1 and MFN2) that mediate mitochondrial fusion; and Drp1, that mediates mitochondrial fission, play a critical role in maintaining mitochondrial quality control and regulating mitophagy in the heart (201, 203). Mitochondrial fission via Drp-1 was shown to be essential for basal mitophagy and heterozygous disruption of Drp1 in cardiac myocytes was sufficient to induce cardiomyopathic dysfunction with fasting (91), indicating a critical need for mitophagy under nutrient deprivation conditions (55).…”
Section: Lysosomes As Regulators Of Cardiac Homeostasis and The Fastimentioning
confidence: 99%
“…21,[25][26][27] Therefore, mitochondria represent a potential therapeutic target. 16 In most clinical pathology, excessive mitochondrial fragmentation is observed, which is mediated by either profusion factor mfn2 deficiency or profission factor Drp1 hyperactivation, thus Mfn2 activation or Drp1 inhibition arising as a potential therapeutic target for mitochondrial dynamics emendation. 28 Mitochondrial fusion and fission play a critical role in mitochondria functional quality control, in which dysfunctional mitochondrial will be ultimately eliminated by autophagy and replaced by mitochondrial biogenesis for 3,29 Recent data indicate that perturbation between mitochondrial fusion or fission is more deleterious than the simultaneous abrogation of both processes.…”
Section: Discussionmentioning
confidence: 99%
“…35 Indeed, Drp1 deletion increased the mitochondrial calcium uptake through upregulating MCU and MICU1 expression. 16,17,41 Additionally, Mfn1 expression can protect the heart against ischemia-reperfusion injury. 36,37 Mfn 2 and Drp1 have other functional roles in addition to fission and fusion.…”
Section: Discussionmentioning
confidence: 99%
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