Deletion of the ubiquitin ligase Nedd4L in lung epithelia causes cystic fibrosis-like disease

Kimura, Toshihiro; Kawabe, Hiroshi; Jiang, Chunhe; Zhang, Wenbo; Yun, Xiang; Chen, Lu; Salter, Michael W.; Brose, Nils; Lu, Wei‐Yang; Rotin, Daniela

doi:10.1073/pnas.1010334108

Cited by 97 publications

(111 citation statements)

References 40 publications

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“…Recently it was shown that ITCH knock-out mice also showed age-dependent alterations in spermatogenesis (38). NEDD4L knock-out mice died perinatally due to disrupted lung function (21,22). Therefore, it remains to clarify whether NEDD4 family ubiquitin ligases play a unique or redundant role in regulating stability of Dvl family proteins and FIGURE 6.…”

Section: Discussionmentioning

confidence: 99%

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HECT Domain-containing E3 Ubiquitin Ligase NEDD4L Negatively Regulates Wnt Signaling by Targeting Dishevelled for Proteasomal Degradation

Ding

Zhang

et al. 2013

Journal of Biological Chemistry

104

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Background: Dishevelled is a critical component of Wnt signaling; however, its stability control is not fully understood. Results: NEDD4L regulates Wnt signaling through Dishevelled2 degradation, and Wnt5a-induced NEDD4L phosphorylation by JNK1 is required for this process. Conclusion: NEDD4L modulates Wnt signaling through a negative feedback mechanism. Significance: Our findings shed light on the understanding of Dishevelled2 stability control and NEDD4L-associated diseases.

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Section: Discussionmentioning

confidence: 99%

“…By far, several proteins have been described as the substrates of NEDD4L, including ion and neurotransmitter channels, growth factor receptors, signaling intermediates, and tight junction molecules (17)(18)(19)(20). NEDD4L knock-out mice die perinatally due to impaired lung function (21,22).…”

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confidence: 99%

HECT Domain-containing E3 Ubiquitin Ligase NEDD4L Negatively Regulates Wnt Signaling by Targeting Dishevelled for Proteasomal Degradation

Ding

Zhang

et al. 2013

Journal of Biological Chemistry

104

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“…We first used the Scnn1a-Cre allele identified in our driver screen that targeted AT1 cells in the flattening stage and were thus committed to terminal differentiation. Although SCNN1A was detected in other cell types than AT1 (Borok et al, 2006;Johnson et al, 2002Johnson et al, , 2006Kimura et al, 2011), the Scnn1a-Cre allele was active in AT1 cells after E19, consistent with the perinatal upregulation of Scnn1a in the distal lung epithelium (Fig. S7D) (Chang et al, 2013), and reached a targeting efficiency (defined as the percentage of AT1 cells that were targeted) of 71% (n=153 cells) and specificity (defined as the percentage of targeted cells that were AT1 cells) of 95% (n=176 cells from three mice) (Fig.…”

Section: Developing At1 Cells Retain Cellular Plasticitymentioning

confidence: 99%

Development and plasticity of alveolar type 1 cells

et al. 2015

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Alveolar type 1 (AT1) cells cover >95% of the gas exchange surface and are extremely thin to facilitate passive gas diffusion. The development of these highly specialized cells and its coordination with the formation of the honeycomb-like alveolar structure are poorly understood. Using new marker-based stereology and single-cell imaging methods, we show that AT1 cells in the mouse lung form expansive thin cellular extensions via a non-proliferative two-step process while retaining cellular plasticity. In the flattening step, AT1 cells undergo molecular specification and remodel cell junctions while remaining connected to their epithelial neighbors. In the folding step, AT1 cells increase in size by more than 10-fold and undergo cellular morphogenesis that matches capillary and secondary septa formation, resulting in a single AT1 cell spanning multiple alveoli. Furthermore, AT1 cells are an unexpected source of VEGFA and their normal development is required for alveolar angiogenesis. Notably, a majority of AT1 cells proliferate upon ectopic SOX2 expression and undergo stage-dependent cell fate reprogramming. These results provide evidence that AT1 cells have both structural and signaling roles in alveolar maturation and can exit their terminally differentiated non-proliferative state. Our findings suggest that AT1 cells might be a new target in the pathogenesis and treatment of lung diseases associated with premature birth.

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“…The in vivo relevance of Nedd4-2 has been recently highlighted. Nedd4-2 knock-out mice die perinatally because of a failure to inflate the lungs (44,45), Nedd4-2 shows a protective regulatory role against the development of cystic fibrosis in lung (45), and it has been directly implicated in the development of peripheral neuropathic pain (46). The role of TrkA on pain has been well established for a long time in mice (47) and humans (48).…”

Section: Discussionmentioning

confidence: 99%

Ubiquitin-specific Protease 36 (USP36) Controls Neuronal Precursor Cell-expressed Developmentally Down-regulated 4-2 (Nedd4-2) Actions over the Neurotrophin Receptor TrkA and Potassium Voltage-gated Channels 7.2/3 (Kv7.2/3)

Anta

Martín-Rodriguez

Gomis-Pérez

et al. 2016

Journal of Biological Chemistry

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Ubiquitination of the TrkA neurotrophin receptor in response to NGF is critical in the regulation of TrkA activation and functions. TrkA is ubiquitinated, among other E3 ubiquitin ligases, by Nedd4-2. To understand mechanistically how TrkA ubiquitination is regulated, we performed a siRNA screening to identify deubiquitinating enzymes and found that USP36 acts as an important regulator of TrkA activation kinetics and ubiquitination. However, USP36 action on TrkA was indirect because it does not deubiquitinate TrkA. Instead, USP36 binds to Nedd4-2 and regulates the association of TrkA and Nedd4-2. In addition, depletion of USP36 increases TrkA⅐Nedd4-2 complex formation, whereas USP36 expression disrupts the complex, resulting in an enhancement or impairment of Nedd4-2-dependent TrkA ubiquitination, respectively. Moreover, USP36 depletion leads to enhanced total and surface TrkA expression that results in increased NGF-mediated TrkA activation and signaling that augments PC12 cell differentiation. USP36 actions extend beyond TrkA because the presence of USP36 interferes with Nedd4-2-dependent Kv7.2/3 channel regulation. Our results demonstrate that USP36 binds to and regulates the actions of Nedd4-2 over different substrates affecting their expression and functions.

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Deletion of the ubiquitin ligase Nedd4L in lung epithelia causes cystic fibrosis-like disease

Cited by 97 publications

References 40 publications

HECT Domain-containing E3 Ubiquitin Ligase NEDD4L Negatively Regulates Wnt Signaling by Targeting Dishevelled for Proteasomal Degradation

HECT Domain-containing E3 Ubiquitin Ligase NEDD4L Negatively Regulates Wnt Signaling by Targeting Dishevelled for Proteasomal Degradation

Development and plasticity of alveolar type 1 cells

Ubiquitin-specific Protease 36 (USP36) Controls Neuronal Precursor Cell-expressed Developmentally Down-regulated 4-2 (Nedd4-2) Actions over the Neurotrophin Receptor TrkA and Potassium Voltage-gated Channels 7.2/3 (Kv7.2/3)

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