Targeting the Notch1 and mTOR pathways in a mouse T-ALL model

Cullion, Kathleen; Draheim, Kyle; Hermance, Nicole; Tammam, Jennifer; Sharma, Vishva Mitra; Ware, Christopher; Nikov, George N.; Krishnamoorthy, Veena; Majumder, Pradip K.; Kelliher, Michelle A.

doi:10.1182/blood-2008-02-136762

Cited by 132 publications

(132 citation statements)

References 50 publications

(83 reference statements)

Supporting

Mentioning

125

Contrasting

Order By: Relevance

“…Of note, Cullion et al observed murine Tal1 leukemias lacking Pten also to remain sensitive to GSI treatment. 43 These findings raise the question as to what complement of secondary genetic alterations can indeed relieve T-cell leukemias of their addiction to Notch signaling. It was proposed recently that FBW7 mutation may contribute to GSI resistance by reducing c-Myc protein turnover.…”

Section: Discussionmentioning

confidence: 99%

“…Although early clinical studies have identified goblet cell hyperplasia-associated secretory diarrhea as a doselimiting toxicity, both intermittent dosing strategies 43,48 and coadministration of glucocorticoids 49 may help to ameliorate these gastrointestinal side effects yet allow a therapeutic window to be achieved. We observed GSI resistance to occur in only a small fraction of primary human samples (2/13 assayed; 15%), and we and others 43 have encountered GSI resistance only infrequently in murine leukemias. With respect to the human samples, it is worth noting that all of the primary samples reported here were collected from patients at initial diagnosis.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Acute T-cell leukemias remain dependent on Notch signaling despite PTEN and INK4A/ARF loss

Medyouf

Gao

Armstrong

et al. 2010

Blood

View full text Add to dashboard Cite

NOTCH1 is activated by mutation in more than 50% of human T-cell acute lymphoblastic leukemias (T-ALLs) and inhibition of Notch signaling causes cell-cycle/ growth arrest, providing rationale for NOTCH1 as a therapeutic target. The tumor suppressor phosphatase and tensin homolog (PTEN) is also mutated or lost in up to 20% of cases. It was recently observed among human T-ALL cell lines that PTEN loss correlated with resistance to Notch inhibition, raising concern that patients with PTEN-negative disease may fail Notch inhibitor therapy. As these studies were limited to established cell lines, we addressed this issue using a genetically defined mouse retroviral transduction/bone marrow transplantation model and observed primary murine leukemias to remain dependent on NOTCH1 signaling despite Pten loss, with or without additional deletion of p16 Ink4a /p19 Arf IntroductionThe 4 mammalian Notch genes (NOTCH1-4) encode a family of highly conserved type I transmembrane receptors that are normally activated by ligands of the Delta/Serrate/Lag-2 family expressed on the surface of neighboring cells. Once activated by ligand, the Notch receptors undergo proteolytic cleavage first by a disintegrin and metalloprotease, then by a ␥-secretase, which releases the intracellular domain (ICN) from the plasma membrane to translocate to the nucleus to stimulate transcription of downstream target genes in complex with the DNA-binding factor CBF1(RBPJ)/ suppressor of hairless/Lag-1 and coactivators of the Mastermind family. Although regulated NOTCH1 signaling is important for normal T-cell development, 1 it is frequently activated by mutation in the human cancer T-cell acute lymphoblastic leukemia (T-ALL). 2 The potent oncogenicity of activated NOTCH1 has been demonstrated in murine bone marrow transduction/transplantation models and several transgenic mouse lines. 3 Activating NOTCH1 mutations occur in more than 50% of primary human T-ALLs and cluster in the heterodimerization (HD) and C-terminal proline-, glutamic acid-, serine-, and threonine-rich (PEST) domains. 4 HD mutations result in weakened association or complete dissociation of the receptor subunits, and thus lead to heightened/constitutive activation of the receptor. 5 PEST domain mutations often generate premature stop codons that delete the PEST degron, and thus enhance signaling by reducing turnover/ prolonging half-life of activated ICN. 6 When present together, the HD and PEST mutations occur in cis, and stimulate signaling in a synergistic fashion. 4 Interestingly, a similar overall frequency of Notch1 mutations (mostly PEST, but some HD) has been observed in various mouse models of T-ALL, underscoring the importance of Notch1 signaling in T-cell leukemogenesis. In addition, both human and murine T-ALL cells bearing NOTCH1 mutations are frequently sensitive to treatment with inhibitors of Notch signaling including ␥-secretase inhibitors (GSIs) that induce G1 cell-cycle/ growth arrest and in some cases apoptosis. 4,7-10 Based on these findings, GSIs and other inhi...

show abstract

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Acute T-cell leukemias remain dependent on Notch signaling despite PTEN and INK4A/ARF loss

Medyouf

Gao

Armstrong

et al. 2010

Blood

View full text Add to dashboard Cite

show abstract

“…[131,132,[134][135][136][137][138][139][140] Our work and the work of others suggest that rapalogs may have the highest degree of activity against ALL types with the worst prognosis, including pre-T, adult, BCR-ABL and Ikaros mutant. [29,135,141,142] Supporting this are recent data demonstrating that early engraftment of pre-B-ALL in immune-deficient mice is associated with the activation of the mTOR pathway and a very high risk of relapse. [143] Experience with chemotherapy for decades, as well as more recent experience with targeted therapies demonstrates that no single agent is likely to be curative.…”

Section: Acute Lymphoblastic Leukemiamentioning

confidence: 90%

“…Encouraging results have been found in preclinical studies combining rapalogs with inhibitors of Notch signaling, Jak/stat and the proteasome. [141,147,148] Based on the large amount of preclinical data supporting their use, rapalogs are being investigated in clinical trials in patients with ALL. Two adult patients with ALL have been treated in early-phase trials using single-agent rapalogs.…”

Section: Acute Lymphoblastic Leukemiamentioning

confidence: 99%

Targeting the PI3K/AKT/mTOR Signaling Axis in Children with Hematologic Malignancies

et al. 2012

View full text Add to dashboard Cite

The phosphatidylinositiol 3-kinase (PI3K), AKT, mammalian target of rapamycin (mTOR) signaling pathway (PI3K/AKT/mTOR) is frequently dysregulated in disorders of cell growth and survival, including a number of pediatric hematologic malignancies. The pathway can be abnormally activated in childhood acute lymphoblastic leukemia (ALL), acute myelogenous leukemia (AML), and chronic myelogenous leukemia (CML), as well as in some pediatric lymphomas and lymphoproliferative disorders. Most commonly, this abnormal activation occurs as a consequence of constitutive activation of AKT, providing a compelling rationale to target this pathway in many of these conditions. A variety of agents, beginning with the rapamycin analogue (rapalog) sirolimus, have been used successfully to target this pathway in a number of pediatric hematologic malignancies. Rapalogs demonstrate significant preclinical activity against ALL, which has led to a number of clinical trials. Moreover, rapalogs can synergize with a number of conventional cytotoxic agents and overcome pathways of chemotherapeutic resistance for drugs commonly used in ALL treatment, including methotrexate and corticosteroids. Based on preclinical data, rapalogs are also being studied in AML, CML, and non-Hodgkin's lymphoma. Recently, significant progress has been made using rapalogs to treat pre-malignant lymphoproliferative disorders, including the autoimmune lymphoproliferative syndrome (ALPS); complete remissions in children with otherwise therapy-resistant disease have been seen.Rapalogs only block one component of the pathway (mTORC1), and newer agents are under preclinical and clinical development that can target different and often multiple protein kinases in the PI3K/AKT/mTOR pathway. Most of these agents have been tolerated in early-phase clinical trials. A number of PI3K inhibitors are under investigation. Of note, most of these also target other protein kinases. Newer agents are under development that target both mTORC1 and mTORC2, mTORC1 and PI3K, and the triad of PI3K, mTORC1, and mTORC2. Preclinical data suggest these dual-and multi-kinase inhibitors are more potent than rapalogs against many of the aforementioned hematologic malignancies. Two classes of AKT inhibitors are under development, the alkyl-lysophospholipids (APLs) and small molecule AKT inhibitors. Both classes have agents currently in clinical trials. A number of drugs are in development that target other components of the pathway, including eukaryotic translation initiation factor (eIF) 4E (eIF4E) and phosphoinositide-dependent protein kinase 1 (PDK1). Finally, a number of other key signaling pathways interact with PI3K/AKT/mTOR, including Notch, MNK, Syk, MAPK, and aurora kinase. These alternative pathways are being targeted alone and in combination with PI3K/AKT/mTOR inhibitors with promising preclinical results in pediatric hematologic malignancies. This review provides a comprehensive overview of the abnormalities in the PI3K/AKT/mTOR signaling pathway in pediatric hematologic malignanc...

show abstract

“…The effect of MRK-003 on sphere-and colony-formation by mammary epithelial cell and tumor cell populations To determine whether Notch pathway activity was required for the survival or self-renewal of tumorsphereand mammosphere-forming cells, we used MRK-003, an orally active inhibitor of g-secretase, which is required for the proteolytic processing of Notch receptors (Fan et al, 2006;Konishi et al, 2007;Lewis et al, 2007;Cullion et al, 2009;Rao et al, 2009). We performed quantitative sphere-and colony-forming assays, which can be used to approximate the frequency of mammary epithelial stem and progenitor cells in heterogeneous cell populations (Reynolds and Weiss, 1992;Dontu et al, 2003).…”

Section: Differential Expression Of Notch Pathway-related Genesmentioning

confidence: 99%

Gamma-secretase inhibitors target tumor-initiating cells in a mouse model of ERBB2 breast cancer

et al. 2011

View full text Add to dashboard Cite

Targeting the Notch1 and mTOR pathways in a mouse T-ALL model

Cited by 132 publications

References 50 publications

Acute T-cell leukemias remain dependent on Notch signaling despite PTEN and INK4A/ARF loss

Acute T-cell leukemias remain dependent on Notch signaling despite PTEN and INK4A/ARF loss

Targeting the PI3K/AKT/mTOR Signaling Axis in Children with Hematologic Malignancies

Gamma-secretase inhibitors target tumor-initiating cells in a mouse model of ERBB2 breast cancer

Contact Info

Product

Resources

About