Ultrafine carbon particles induce apoptosis and proliferation in rat lung epithelial cells via specific signaling pathways both using EGF-R

Sydlik, Ulrich; Bierhals, Katrin; Soufi, Maria; Abel, Josef; Schins, Roel P. F.; Unfried, Klaus

doi:10.1152/ajplung.00131.2006

Cited by 81 publications

(82 citation statements)

References 22 publications

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“…The elevated background after 16 h has been described earlier (5) as induced by the starving conditions under which the cells have to be kept to identify treatmentspecific reactions. Interestingly, this time course in phosphorylation has striking similarities to the time course in ERK1/2 activation that we described in our previous studies (28).…”

Section: Activation Of Akt By Npcbsupporting

confidence: 84%

“…Nanoparticles have been shown to act as an extracellular stimulus that induces signaling dependent on the membrane receptors EGF-R and ␤ 1 -integrin (28). Because Akt activation was known to be initiated by these receptors on cell attachment, we investigated whether this signaling cascade is also triggered by nanoparticles.…”

Section: Activation Of Akt By Npcbmentioning

confidence: 99%

“…Previously, we (28) observed that treatment with two types of nanoparticles, carbon particles [nanoparticulate carbon black, (NPCB; Printex 90)] as well as silica particles (amorphous SiO 2 ), both with a median diameter of 14 nm, induced proliferation in a rat lung epithelial cell line. Investigating signaling events relevant for this specific outcome, we were able to demonstrate that the membrane receptors epidermal growth factor receptor (EGF-R) and ␤ 1 -integrin are involved in particle-induced activation of the MAPKs ERK1/2 in response to nanoparticle treatment.…”

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confidence: 99%

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Carbon nanoparticle-induced lung epithelial cell proliferation is mediated by receptor-dependent Akt activation

Unfried¹,

Sydlik²,

Bierhals³

et al. 2008

American Journal of Physiology-Lung Cellular and Molecular Phys

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Treatment of lung epithelial cells with different kinds of nano-sized particles leads to cell proliferation. Because bigger particles fail to induce this reaction, it is suggested that the special surface properties, due to the extremely small size of these kinds of materials, is the common principle responsible for this specific cell reaction. Here the activation of the protein kinase B (Akt) signaling cascade by carbon nanoparticles was investigated with regard to its relevance for proliferation. Kinetics and dose-response experiments demonstrated that Akt is specifically activated by nanoparticulate carbon particles in rat alveolar type II epithelial cells as well as in human bronchial epithelial cells. This pathway appeared to be dependent on epidermal growth factor receptor and β1-integrins. The activation of Akt by these receptors is known to be a feature of adhesion-dependent signaling. However, intracellular proteins described in this context (focal adhesion kinase pp125FAK and integrin-linked kinase) were not activated, indicating a specific signaling mechanism. Inhibitor studies demonstrate that nanoparticle-induced proliferation is mediated by phosphoinositide 3-kinases and Akt. Moreover, overexpression of mutant Akt, as well as pretreatment with an Akt inhibitor, reduced nanoparticle-specific ERK1/2 phosphorylation, which is decisive for nanoparticle-induced proliferation. With this report, we describe the activation of a pathway by carbon nanoparticles that was so far known to be triggered by ligand receptor binding or on cell adhesion to extracellular matrix proteins.

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Section: Activation Of Akt By Npcbsupporting

confidence: 84%

Section: Activation Of Akt By Npcbmentioning

confidence: 99%

mentioning

confidence: 99%

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Carbon nanoparticle-induced lung epithelial cell proliferation is mediated by receptor-dependent Akt activation

Unfried¹,

Sydlik²,

Bierhals³

et al. 2008

American Journal of Physiology-Lung Cellular and Molecular Phys

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“…31 In an earlier study, Sydlik et al could show that ultrafine carbon particles activate EGFR in lung epithelial cells subsequently leading in parallel to apoptotic events as well as proliferation. 63 While the kinase activity of EGFR was found essential for both processes, β1-integrin-mediated activation of ERK was instrumental for proliferation, whereas apoptosis was mediated by activation of cJun. In other studies, it was demonstrated, that in human bronchial epithelial cells, exposure to PM2.5 particles (i.e.…”

Section: Interaction Of Nps With Cell Membrane Receptorsmentioning

confidence: 99%

“…So far, NP toxicity was mainly described through the induction of oxidative stress, inflammation and apoptosis as cellular responses. 18 Cell death highly depends on NP concentration, duration of the exposure and the cellular system investigated and both, programmed cell death (apoptosis) as well as necrosis, were observed as an outcome 63,71 . However, ROS also play important roles as intercellular second messengers and activators of specific pathways.…”

Section: The Role Of Oxidative Stress and Ros In Np Induced Signalingmentioning

confidence: 99%

Big Signals from Small Particles: Regulation of Cell Signaling Pathways by Nanoparticles

Rauch¹,

Kölch²,

et al. 2013

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Introduction 3391 2. Medical Applications of Nanomaterials 3391 2.1. Use of Nanomaterials in Diagnostic Applications 3392 3. Interaction of Nanomaterials with Living Cells 3392 3.1. Role of Physicochemical NP Properties in the Interaction between NPs and Biological Systems 3393 3.2. NP Uptake into the Cells 3393 3.2.1. Role of Size and Shape in NP Uptake 3393 3.2.2. Role of Surface Charge and Protein Corona on NP Uptake 3395 3.3. Activation of Signal Processing Pathways by NPs 3397 3.3.1. Interaction of NPs with Cell Membrane Receptors 3397 3.3.2. Role of Oxidative Stress and ROS in NP-Induced Signaling 3398 3.3.3. NPs Induce Cell Death Pathways 3400 3.3.4. Activation of Mechanotransduction Receptors by Magnetic NPs 3400 4. Magnetic NPs and Cell Signaling 3400 4.1. Controlled Activation of Cell Surface Receptors by Magnetic NPs 3400 4.1.1. Activation of Signal Transduction Receptors by Magnetic NPs 3400 4.1.2. Activation of Mechanotransduction Receptors and Mechanosensitive Signaling Pathways by Magnetic NPs 3400 4.2. Pathway Activation by Magnetic-NP-Induced Hyperthermia 3401 4.2.1. Molecular Targets of Hyperthermia: Heat Shock Proteins and p53 3401 5. Conclusions 3402 Author Information 3402 Corresponding Author 3402 Present Address 3402 Notes 3402 Biographies 3402 Acknowledgments 3403 References 3403

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Toxicity of Inhaled Nanomaterials

Pickrell¹,

Erickson²,

Dhakal³

et al. 2009

Nanoscale Materials in Chemistry

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Ultrafine carbon particles induce apoptosis and proliferation in rat lung epithelial cells via specific signaling pathways both using EGF-R

Cited by 81 publications

References 22 publications

Carbon nanoparticle-induced lung epithelial cell proliferation is mediated by receptor-dependent Akt activation

Carbon nanoparticle-induced lung epithelial cell proliferation is mediated by receptor-dependent Akt activation

Big Signals from Small Particles: Regulation of Cell Signaling Pathways by Nanoparticles

Toxicity of Inhaled Nanomaterials

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