c-Src and HSP72 interact in ATP-depleted renal epithelial cells

Wang, Y.-H.; Li, F.; Schwartz, John H.; Flint, P. J.; Borkan, Steven C.

doi:10.1152/ajpcell.2001.281.5.c1667

Cited by 20 publications

(23 citation statements)

References 59 publications

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“…Cells were depleted of ATP, by incubation in Ringer's solution containing 10 mM KCN and 5 mM deoxyglucose for 10 min as described previously (25). Zinc transport was monitored immediately following the ATP depletion using Ringer's solution containing deoxyglucose instead of glucose.…”

Section: Fig 3 Znmentioning

confidence: 99%

A Sodium Zinc Exchange Mechanism Is Mediating Extrusion of Zinc in Mammalian Cells

Ohana

Segal

Palty

et al. 2004

Journal of Biological Chemistry

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exchanger. Sodium-dependent zinc exchange, facilitating the removal of intracellular zinc, was also monitored in neurons. To our knowledge, the Na ؉ /Zn 2؉ exchanger described here is the first example of a mammalian transport mechanism capable of Na ؉ -dependent active extrusion of zinc. Such mechanism is likely to play an important role, not only in generating the transmembrane zinc gradients, but also in protecting cells from the potentially toxic effects of permeation of this ion.

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Section: Fig 3 Znmentioning

confidence: 99%

A Sodium Zinc Exchange Mechanism Is Mediating Extrusion of Zinc in Mammalian Cells

Ohana

Segal

Palty

et al. 2004

Journal of Biological Chemistry

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“…Cultured epithelial cells and animal models of injury have revealed that ATP depletion triggers an altered distribution of tight and adherens junction proteins with loss of barrier function and increased tyrosine phosphorylation (7)(8)(9). Reactive oxygen species are important mediators of injury, and H 2 O 2 stimulates TJ disruption through tyrosine kinase activation (10,11).…”

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confidence: 99%

H ₂ O ₂ activates G protein, α 12 to disrupt the junctional complex and enhance ischemia reperfusion injury

Beaudry²,

Negoro³

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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The epithelial cell tight junction separates apical and basolateral domains and is essential for barrier function. Disruption of the tight junction is a hallmark of epithelial cell damage and can lead to end organ damage including renal failure. Herein, we identify Gα12 activation by H 2 O 2 leading to tight junction disruption and demonstrate a critical role for Gα12 activation during bilateral renal ischemia/reperfusion injury. Madin–Darby canine kidney (MDCK) cells with inducible Gα12 (Gα12-MDCK) and silenced Gα12 (shGα12-MDCK) were subjected to ATP depletion/repletion and H 2 O 2 /catalase as models of tight junction disruption and recovery by monitoring transepithelial resistance. In ATP depleted cells, barrier disruption and recovery was not affected by Gα12, but reassembly was accelerated by Gα12 depletion. In contrast, silencing of Gα12 completely protected cells from H 2 O 2 -stimulated barrier disruption, a response that rapidly occurred in control cells. H 2 O 2 activated Src and Rho, and Src inhibition (by PP2), but not Rho (by Y27632), protected cells from H 2 O 2 -mediated barrier disruption. Immunofluorescent and biochemical analysis showed that H 2 O 2 led to increased tyrosine phosphorylation of numerous proteins and altered membrane localization of tight junction proteins through Gα12/Src signaling pathway. Gα12 and Src were activated in vivo during ischemia/reperfusion injury, and transgenic mice with renal tubular QLα12 (activated mutant) expression were delayed in recovery and showed more extensive injury. Conversely, Gα12 knockout mice were nearly completely protected from ischemia/reperfusion injury. Taken together, these studies reveal that ROS stimulates Gα12 to activate injury pathways and identifies a therapeutic target for ameliorating ROS mediated injury.

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“…Three Src family members (Src, Fyn, and Yes) are expressed ubiquitously in mammalian cells (56,62), and they have been shown to contribute to EGF receptor activation in several systems (45,59,61). For example, activation of Src family kinases is required for EGF receptor-mediated ERK phosphorylation in response to UV light, I/R, or H 2 O 2 (20,26,61).…”

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confidence: 99%

Heparin-binding epidermal growth factor and Src family kinases in proliferation of renal epithelial cells

Zhuang

Kinsey²,

Rasbach³

et al. 2008

American Journal of Physiology-Renal Physiology

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Our recent studies have shown that proliferation of renal proximal tubular cells (RPTC) in the absence of growth factors requires activation of the epidermal growth factor (EGF) receptor. We sought to identify the endogenous EGF receptor ligand and investigate the mechanism(s) by which RPTC proliferate in different models. RPTC expressed both pro- and cleaved forms of heparin-binding epidermal growth factor (HB-EGF) and several metalloproteinases (MMP-2, -3, -9, and ADAM10, ADAM17) that have been reported to cleave HB-EGF. Treatment of RPTC with CRM 197, an inhibitor of HB-EGF binding to the EGF receptor, or downregulation of HB-EGF with small interfering RNA inhibited RPTC proliferation following plating. Furthermore, GM6001 (pan-MMP inhibitor), tumor-necrosis factor protease inhibitor-1 (TAPI-1; MMP and ADAM17 inhibitor), and GW280264X (ADAM10 and -17 inhibitor), but not GI254023X (ADAM10 inhibitor), attenuated the proliferation after plating. Although EGF receptor activation is required for RPTC proliferation after oxidant injury, CRM197, GM6001, and TAPI-1 did not block this response. In contrast, inhibition of Src with PP1 blocked EGF receptor activation and RPTC proliferation after oxidant injury. In addition, PP1 treatment attenuated HB-EGF-enhanced RPTC proliferation. We suggest that RPTC proliferation after plating is mediated by HB-EGF produced through an autocrine/paracrine mechanism and RPTC proliferation following oxidant injury is mediated by Src without involvement of HB-EGF.

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c-Src and HSP72 interact in ATP-depleted renal epithelial cells

Cited by 20 publications

References 59 publications

A Sodium Zinc Exchange Mechanism Is Mediating Extrusion of Zinc in Mammalian Cells

A Sodium Zinc Exchange Mechanism Is Mediating Extrusion of Zinc in Mammalian Cells

H ₂ O ₂ activates G protein, α 12 to disrupt the junctional complex and enhance ischemia reperfusion injury

Heparin-binding epidermal growth factor and Src family kinases in proliferation of renal epithelial cells

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c-Src and HSP72 interact in ATP-depleted renal epithelial cells

Cited by 20 publications

References 59 publications

A Sodium Zinc Exchange Mechanism Is Mediating Extrusion of Zinc in Mammalian Cells

A Sodium Zinc Exchange Mechanism Is Mediating Extrusion of Zinc in Mammalian Cells

H 2 O 2 activates G protein, α 12 to disrupt the junctional complex and enhance ischemia reperfusion injury

Heparin-binding epidermal growth factor and Src family kinases in proliferation of renal epithelial cells

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Product

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H ₂ O ₂ activates G protein, α 12 to disrupt the junctional complex and enhance ischemia reperfusion injury