Activating Mutations of
            <i>NOTCH1</i>
            in Human T Cell Acute Lymphoblastic Leukemia

Weng, Andrew P.; Ferrando, Adolfo A.; Lee, Woojoong; Morris, John P.; Silverman, Lewis B.; Sanchez-Irizarry, Cheryll; Blacklow, Stephen C.; Look, A. Thomas; Aster, Jon C.

doi:10.1126/science.1102160

Cited by 2,496 publications

(2,730 citation statements)

References 23 publications

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“…In our study, although we noted that the Notch 2 locus (1p13-11) in Mary-X was moderately amplified on array comparative genomic hybridization, the Notch 3 locus was not amplified. It had also been demonstrated that mutations within Notch receptors can activate signaling in the absence of a ligand (Sanchez-Irizarry et al, 2004;Weng et al, 2004;Gordon et al, 2007). However, we did not find these gain-of-function mutations in Notch 3 in Mary-X.…”

Section: Notch 3 Dependency Of Ibc Embolus Y Xiao Et Alcontrasting

confidence: 76%

The lymphovascular embolus of inflammatory breast cancer exhibits a Notch 3 addiction

Xiao

Zou

et al. 2010

Oncogene

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Section: Notch 3 Dependency Of Ibc Embolus Y Xiao Et Alcontrasting

confidence: 76%

The lymphovascular embolus of inflammatory breast cancer exhibits a Notch 3 addiction

Xiao

Zou

et al. 2010

Oncogene

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“…This is in contrast to the NOTCH1 alteration pattern revealed in hematopoietic malignancies, where Notch is known as tumor suppressor 4, 89. The majority of these mutations include missense mutations in the NRR domain and nonsense/frame‐shift ones in the PEST domain (Fig.…”

Section: A Complete View Of Notch1 Mutations Across Sccsmentioning

confidence: 88%

Does Notch play a tumor suppressor role across diverse squamous cell carcinomas?

et al. 2016

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The role of Notch pathway in tumorigenesis is highly variable. It can be tumor suppressive or pro‐oncogenic, typically depending on the cellular context. Squamous cell carcinoma (SCC) is a cancer of the squamous cell, which can occur in diverse human tissues. SCCs are one of the most frequent human malignancies for which the pathologic mechanisms remain elusive. Recent genomic analysis of diverse SCCs identified marked levels of mutations in NOTCH1, implicating Notch signaling pathways in the pathogenesis of SCCs. In this review, evidences highlighting NOTCH's role in different types of SCCs are summarized. Moreover, based on accumulating structural information of the NOTCH receptor, the functional consequences of NOTCH1 gene mutations identified from diverse SCCs are analyzed, emphasizing loss of function of Notch in these cancers. Finally, we discuss the convergent view on an intriguing possibility that Notch may function as tumor suppressor in SCCs across different tissues. These mechanistic insights into Notch signaling pathways will help to guide the research of SCCs and development of therapeutic strategies for these cancers.

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“…In support of this, many studies in mice have subsequently revealed that expression of constitutive-active Notch proteins leads to potent and specific induction of T-ALL [158]. Aster and colleagues searched for specific Notch1 mutations in T-ALLs that do not harbor the t(7;9) translocation and identified two hotspot regions in the Notch1 gene: the heterodimerization and the PEST-domain [159]. Mutations in the heterodimerization domain enhance S3 cleavage of Notch and cause, via augmented NICD production, a significant increase in Notch signaling.…”

Section: Notch and Leukemiamentioning

confidence: 97%

“…Genetic and biochemical data suggest that loss of the PEST-domain enhance NICD protein stability, reviewed in [160]. Synergistic heterodimerization and PEST domain mutants are found together in cis in 10 -20 % of human T-ALLs [159] and low copy number amplification of Notch1 has also been reported [161]. Notch mutations appear to collaborate with a diverse collection of other proteins dysregulated in T-ALL.…”

Section: Notch and Leukemiamentioning

confidence: 99%

The Notch signaling pathway: Transcriptional regulation at Notch target genes

Borggrefe

Oswald

2009

Cell. Mol. Life Sci.

584

499

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. The Notch gene encodes a transmembrane receptor that gave the name to the evolutionary highly conserved Notch signaling cascade. It plays a pivotal role in the regulation of many fundamental cellular processes such as proliferation, stem cell maintenance and differentiation during embryonic and adult development. After specific ligand binding, the intracellular part of the Notch receptor is cleaved off and translocates to the nucleus, where it binds to the transcription factor RBP-J. In the absence of activated Notch, RBP-J represses Notch target genes by recruiting a corepressor complex. Here, we review Notch signaling with a focus on gene regulatory events at Notch target genes. This is of utmost importance to understand Notch signaling since certain RBP-J associated cofactors and particular epigenetic marks determine the specificity of Notch target gene expression in different cell types. We subsequently summarize the current knowledge about Notch target genes and the physiological significance of Notch signaling in development and cancer.

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Activating Mutations of NOTCH1 in Human T Cell Acute Lymphoblastic Leukemia

Cited by 2,496 publications

References 23 publications

The lymphovascular embolus of inflammatory breast cancer exhibits a Notch 3 addiction

The lymphovascular embolus of inflammatory breast cancer exhibits a Notch 3 addiction

Does Notch play a tumor suppressor role across diverse squamous cell carcinomas?

The Notch signaling pathway: Transcriptional regulation at Notch target genes

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