A pivotal role for endogenous TGF-β-activated kinase-1 in the LKB1/AMP-activated protein kinase energy-sensor pathway

Xie, Min; Zhang, Dou; Dyck, Jason R.B.; Li, Yi‐Heng; Zhang, Hui; Morishima, Masae; Mann, Douglas L.; Taffet, George E.; Baldini, Antonio; Khoury, Dirar S.; Schneider, Michael

doi:10.1073/pnas.0604708103

Cited by 322 publications

(259 citation statements)

References 49 publications

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“…14,15 Exogenous stressors and environmental changes such as osmotic stress, UV irradiation, ischemia and nutrient withdrawal activate TAK1. 13,14,16,17 Among these stimuli, the mechanism of TAK1 activation and its role in the TNFa signaling pathway has been extensively studied. Upon TNFa stimulation, adaptor molecules including TNFa receptor type-1-associated death domain protein (TRADD), TNFa receptorassociated factor 2 and 5 (TRAF2 and TRAF5), cellular inhibitor of apoptosis 1 and 2 (cIAP1/2) and RIPK1 are recruited to the receptor complex (TNF receptor 1 (TNFR1) Complex I) (Figure 1), in which RIPK1 acquires a K63-linked or linear polyubiquitin chain by E3 ligases, TRAF2/5 cIAP1/2 or linear ubiquitin chain assembly complex containing two E3 ligases HOIL-1 and HOIP.…”

Section: Tak1 Activation and Downstream Pathwaysmentioning

confidence: 99%

“…26,27 Drawing a link between TAK1 signaling and metabolism, studies have found that starvation and TRAIL induce autophagy in which TAK1 is actively involved by activating AMP-activated protein kinase and IKKs. 14,17,28,29 In summary, TAK1 responds to exogenous stress conditions through a variety of mechanisms including TNFa family Figure 1 TNFa induces cell survival, apoptosis and necroptosis. Upon TNFa stimulation, TNFR1 forms Complex I, in which RIPK1 acquires a polyubiquitin chain.…”

Section: Tak1 Activation and Downstream Pathwaysmentioning

confidence: 99%

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TAK1 control of cell death

2014

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Programmed cell death, a physiologic process for removing cells, is critically important in normal development and for elimination of damaged cells. Conversely, unattended cell death contributes to a variety of human disease pathogenesis. Thus, precise understanding of molecular mechanisms underlying control of cell death is important and relevant to public health. Recent studies emphasize that transforming growth factor-b-activated kinase 1 (TAK1) is a central regulator of cell death and is activated through a diverse set of intra-and extracellular stimuli. The physiologic importance of TAK1 and TAK1-binding proteins in cell survival and death has been demonstrated using a number of genetically engineered mice. These studies uncover an indispensable role of TAK1 and its binding proteins for maintenance of cell viability and tissue homeostasis in a variety of organs. TAK1 is known to control cell viability and inflammation through activating downstream effectors such as NF-jB and mitogen-activated protein kinases (MAPKs). It is also emerging that TAK1 regulates cell survival not solely through NF-jB but also through NF-jB-independent pathways such as oxidative stress and receptor-interacting protein kinase 1 (RIPK1) kinase activity-dependent pathway. Moreover, recent studies have identified TAK1's seemingly paradoxical role to induce programmed necrosis, also referred to as necroptosis. This review summarizes the consequences of TAK1 deficiency in different cell and tissue types from the perspective of cell death and also focuses on the mechanism by which TAK1 complex inhibits or promotes programmed cell death. This review serves to synthesize our current understanding of TAK1 in cell survival and death to identify promising directions for future research and TAK1's potential relevance to human disease pathogenesis.

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Section: Tak1 Activation and Downstream Pathwaysmentioning

confidence: 99%

Section: Tak1 Activation and Downstream Pathwaysmentioning

confidence: 99%

TAK1 control of cell death

2014

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“…AMPK activation was originally proposed to be dependent on Thr172 phosphorylation via action of upstream kinases including LKB1, 43,44 calmodulin-dependent protein kinase kinase II␤, 45 and Tak1. 46 However, Xie et al 47 suggested that LKB1 actually acts downstream of Tak1 in mouse fibroblasts. Because TGF-␤1 seems to be crucial in AMPK-dependent p38MAPK activation and because it is part of the FAK/Tak1/JNK pathway crucial for myofibroblast activation, 35 we chose to analyze Tak1 activation in aged fibroblasts treated with TGF-␤1 and AICAR.…”

Section: Rescue Of Defective Function Requires Ampk Activationmentioning

confidence: 99%

Defective Myofibroblast Formation from Mesenchymal Stem Cells in the Aging Murine Heart

Cieslik

Trial

Entman

2011

The American Journal of Pathology

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Cardiac fibroblasts are the most prevalent cell type in the heart. These cells exert a critical role in regulating normal myocardial function and in the adverse myocardial remodeling that occurs after myocardial infarction (MI). 1 Irreversible cardiomyocyte damage owing to cessation of oxygen supply during MI leads to necrosis, which stimulates inflammatory reactions that trigger reparative pathways and activate cells to form a scar. Cytokines released by inflammatory infiltrating leukocytes promote endogenous mesenchymal stem cell (MSC) proliferation and migration toward the infarct site, followed by differentiation into fibroblasts that deposit scar-forming collagen. The fibroblasts mature into myofibroblasts, expressing scar-contracting ␣-smooth muscle actin (␣-SMA). 2 Resident fibroblasts also become activated and participate in this process. After several weeks, a mature scar is formed, and most of the myofibroblasts undergo apoptosis. [3][4][5] We have previously established in a model of mouse MI that, compared with young animals, aged mice demonstrate greater infarct expansion and less effective myocardial repair. 6 Defective scar formation arises from a decreased number of myofibroblasts and diminished collagen deposition in the infarct, which results in a structurally unstable scar formed by loose connective tissue. 7 Evidence indicates that multipotent cells can be generated in vitro from several adult organs including the heart. 8 Tissue-resident progenitor cells of mesenchymal origin can differentiate into myogenic, adipocytic, chondrocytic, osteoblastic, and fibroblastic lineages. 9 -11 The potential of those stem cells to differentiate decreases

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“…1 To date, three AMPKKs have been identified in the heart, the tumor suppressor kinase LKB1, a calmodulindependent protein kinase kinase, and a TGF-b-activated kinase-1. 26 Although LKB1 and TGF-b-activated kinase-1 are highly expressed in heart, calmodulin-dependent protein kinase kinase is expressed only at low levels. 27 To date, the role of either of these AMPKKs in the control of AMPK phosphorylation and activation has not been clearly defined.…”

Section: Ampk Activation During Ischemia/reperfusionmentioning

confidence: 99%

“…Recent evidence in endothelial cells suggests that PKC-z phosphorylates LKB1 at Ser428, resulting in an increased association of LKB1 with AMPK and consequent AMPK Thr172 phosphorylation by LKB1. 26 Whether a similar pathway exists in the heart has yet to be determined.…”

Section: Ampk Activation During Ischemia/reperfusionmentioning

confidence: 99%

AMP-activated protein kinase control of energy metabolism in the ischemic heart

Lopaschuk

2008

Int J Obes

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Myocardial ischemia produces an energy-deficient state in heart muscle, which if not corrected can lead to cardiomyocyte death. AMP-activated protein kinase (AMPK) is a key kinase that can increase energy production in the ischemic heart. During ischemia a rapid activation of AMPK occurs, resulting in an activation of both myocardial glucose uptake and glycolysis, as well as an increase in fatty acid oxidation. This activation of AMPK has the potential to increase energy production, thereby protecting the heart during ischemic stress. However, at clinically relevant high levels of fatty acids, ischemia-induced activation of AMPK also stimulates fatty acid oxidation during and following ischemia. This can contribute to ischemic injury secondary to an inhibition of glucose oxidation, which results in a decrease in cardiac efficiency. As a result, AMPK activation has the potential to be either beneficial or harmful in the ischemic heart.

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A pivotal role for endogenous TGF-β-activated kinase-1 in the LKB1/AMP-activated protein kinase energy-sensor pathway

Cited by 322 publications

References 49 publications

TAK1 control of cell death

TAK1 control of cell death

Defective Myofibroblast Formation from Mesenchymal Stem Cells in the Aging Murine Heart

AMP-activated protein kinase control of energy metabolism in the ischemic heart

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