The Canonical Notch Signaling Pathway: Structural and Biochemical Insights into Shape, Sugar, and Force

Kovall, Rhett A.; Gebelein, Brian; Sprinzak, David; Kopan, Raphael

doi:10.1016/j.devcel.2017.04.001

Cited by 318 publications

(304 citation statements)

References 105 publications

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“…A number of direct CSL target genes commonly upregulated by its silencing in HKCs and SCC13 cells could be involved in the In Drosophila, it has long been known that the role of Su(H) (CSL homologue) as mediator of NOTCH activation cannot explain the different phenotypes resulting from loss of either gene (14)(15)(16). Increasing evidence indicates that, also in mammalian systems, CSL and NOTCH play only partially overlapping functions.…”

Section: Discussionmentioning

confidence: 99%

“…While functioning as an essential mediator of Notch activation, CSL is endowed with intrinsic transcription-repressive function and can be converted by other cofactors, besides NOTCH, into an activator (15,16). Evidence from various genetic models indicates that abrogation of CSL function can have consequences beyond suppression of Notch signaling, while conversely, NOTCH activation may involve other mediators besides CSL (15,16). In skin, the more pronounced phenotype of mice with keratinocyte-specific deletion of NOTCH1 and NOTCH2 genes versus CSL suggests that NOTCH has a broader function than CSL (17).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Notch-effector CSL promotes squamous cell carcinoma by repressing histone demethylase KDM6B

Labban¹,

Jo²,

Ostano³

et al. 2018

Journal of Clinical Investigation

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Notch-effector CSL promotes squamous cell carcinoma by repressing histone demethylase KDM6B

Labban¹,

Jo²,

Ostano³

et al. 2018

Journal of Clinical Investigation

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“…Notch proteins are single-pass transmembrane receptors for cell surface ligands of the Delta/Serrate/Lag2 (DSL) superfamily (reviewed in Kovall et al, 2017). DSL ligands induce extracellular cleavage of the juxtamembrane “Negative Regulatory Region” (NRR) of Notch.…”

Section: Introductionmentioning

confidence: 99%

“…“Pulling” models posit that Epsin is required after DSL ligands bind Notch, to allow endocytosis of Dl to exert force on the NRR exposing the S2 site for cleavage. Diverse experiments have been taken as evidence for or against these models (Weinmaster and Fischer, 2011; Musse et al, 2012; Kovall et al, 2017). However, this evidence has been more circumstantial than compelling.…”

Section: Introductionmentioning

confidence: 99%

Epsin-Dependent Ligand Endocytosis Activates Notch by Force

Langridge

Struhl

2017

Cell

118

126

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Summary DSL ligands activate Notch by inducing cleavage and shedding of the receptor ectodomain—an event that requires ligand to be endocytosed in signal-sending cells by the adaptor protein Epsin. Two classes of explanation for this unusual requirement are: (i) recycling models, in which ligand must be endocytosed to be modified or repositioned before it binds Notch, and (ii) pulling models, in which ligand must be endocytosed after it binds Notch to exert force that exposes an otherwise buried cleavage site. We demonstrate in vivo that ligands that cannot enter the Epsin pathway nevertheless bind Notch but fail to activate the receptor because they cannot exert sufficient force. This argues against recycling models and in favor of pulling models. Our results also suggest that once ligand binds receptor, activation depends on a competition between Epsin-mediated ligand endocytosis, which induces cleavage, and transendocytosis of ligand by receptor, which aborts the incipient signal.

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“…Notch signaling is a highly conserved cell-to-cell communication pathway mediated by Notch ligand-receptor interactions between adjacent cells (Figure 3a) (124). Four Notch receptors (Notch1-4) and five Notch ligands of the Jagged ( Jag) and Delta-like (Dll) families ( Jag1 (117,119,120,122,125,126).…”

Section: Overview Of Notch Signalingmentioning

confidence: 99%

New Insights into Graft-Versus-Host Disease and Graft Rejection

Perkey

Maillard

2018

Annu. Rev. Pathol. Mech. Dis.

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Allogeneic transplantation of foreign organs or tissues has lifesaving potential, but can lead to serious complications. After solid organ transplantation, immune-mediated rejection mandates the use of prolonged global immunosuppression and limits the life span of transplanted allografts. After bone marrow transplantation, donor-derived immune cells can trigger life-threatening graft-versus-host disease. T cells are central mediators of alloimmune complications and the target of most existing therapeutic interventions. We review recent progress in identifying multiple cell types in addition to T cells and new molecular pathways that regulate pathogenic alloreactivity. Key discoveries include the cellular subsets that function as potential sources of alloantigens, the cross talk of innate lymphoid cells with damaged epithelia and with the recipient microbiome, the impact of the alarmin interleukin-33 on alloreactivity, and the role of Notch ligands expressed by fibroblastic stromal cells in alloimmunity. While refining our understanding of transplantation immunobiology, these findings identify new therapeutic targets and new areas of investigation.

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The Canonical Notch Signaling Pathway: Structural and Biochemical Insights into Shape, Sugar, and Force

Cited by 318 publications

References 105 publications

Notch-effector CSL promotes squamous cell carcinoma by repressing histone demethylase KDM6B

Notch-effector CSL promotes squamous cell carcinoma by repressing histone demethylase KDM6B

Epsin-Dependent Ligand Endocytosis Activates Notch by Force

New Insights into Graft-Versus-Host Disease and Graft Rejection

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