| Literature DB >> 25366565 |
Jolijn W Groeneweg1,2, Rosemary Foster3,4,5, Whitfield B Growdon6,7,8, René H M Verheijen9, Bo R Rueda10,11,12.
Abstract
Ovarian cancer is the most lethal of all gynecologic malignancies because women commonly present with advanced stage disease and develop chemotherapy refractory tumors. While cytoreductive surgery followed by platinum based chemotherapy are initially effective, ovarian tumors have a high propensity to recur highlighting the distinct need for novel therapeutics to improve outcomes for affected women. The Notch signaling pathway plays an established role in embryologic development and deregulation of this signaling cascade has been linked to many cancers. Recent genomic profiling of serous ovarian carcinoma revealed that Notch pathway alterations are among the most prevalent detected genomic changes. A growing body of scientific literature has confirmed heightened Notch signaling activity in ovarian carcinoma, and has utilized in vitro and in vivo models to suggest that targeting this pathway with gamma secretase inhibitors (GSIs) leads to anti-tumor effects. While it is currently unknown if Notch pathway inhibition can offer clinical benefit to women with ovarian cancer, several GSIs are currently in phase I and II trials across many disease sites including ovary. This review will provide background on Notch pathway function and will focus on the pre-clinical literature that links altered Notch signaling to ovarian cancer progression.Entities:
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Year: 2014 PMID: 25366565 PMCID: PMC4228063 DOI: 10.1186/s13048-014-0095-1
Source DB: PubMed Journal: J Ovarian Res ISSN: 1757-2215 Impact factor: 4.234
Figure 1The Notch signaling cascade is activated by cell-cell interaction.
Ongoing phase I and phase II trials of therapies targeting the Notch pathway
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| MK-0752 | γ-secretase | NCT01098344 | 60 | Oral | Unresectable pancreatic cancer | Combination with gemcitabine |
| RO4929097 | γ-secretase | NCT01071564 | 46 | Oral | Unresectable breast cancer | Combination with vismodegib |
| RO4929097 | γ-secretase | NCT01238133 | 14 | Oral | Neoadjuvant breast cancer | Combination with carboplatin and paclitaxel |
| RO4929097 | γ-secretase | NCT01122901 | 60 | Oral | Glioblastoma | Monotherapy |
| RO4929097 | γ-secretase | NCT01151449 | 30 | Oral | Breast cancer | Monotherapy |
| NCT01120275 | 24 | Melanoma | ||||
| NCT01232829 | 21 | Pancraetic cancer | ||||
| RO4929097 | γ-secretase | NCT01119599 | 34 | Oral | Glioblastoma | Combination with radiation therapy and temozolomide |
| RO4929097 | γ-secretase | NCT01193881 | 39 | Oral | Lung cancer | Combination with erlotinib |
| RO4929097 | γ-secretase | NCT01158274 | 30 | Oral | Refractory solid tumors | Combination with capecitabine |
| RO4929097 | γ-secretase | NCT01141569 | 5 | Oral | Renal cell cancer | Monotherapy |
| RO4929097 | γ-secretase | NCT01189240 | 13 | Oral | Glioblastoma | Combination with bevacizumab |
| RO4929097 | γ-secretase | NCT01200810 | 78 | Oral | Refractory prostate cancer | Combination with bicalutamide |
| RO4929097 | γ-secretase | NCT01175343 | 37 | Oral | Refractory ovarian, fallopian tube or peritoneal cancer | Monotherapy |
| BMS-906024 | γ-secretase | NCT01653470 | 95 | IV | Advanced/metastatic solid tumors | Combination with weekly paclitaxel; 5-FU and irinotecan; carboplatin and paclitaxel |
| BMS-906024 | γ-secretase | NCT01292655 | 110 | IV | Advanced/metastatic solid tumors | Monotherapy |
| BMS-906024 | γ-secretase | NCT01363817 | 42 | IV | T-cell leukemia or lymphoma | Monotherapy |
| BMS-986115 | γ-secretase | NCT01986218 | 40 | Oral | Advanced/metastatic solid tumors | Monotherapy |
| PF-03084014 | γ-secretase | NCT01981551 | 17 | Oral | Desmoid tumors | Monoterapy |
Completed phase I and phase II trials of therapies targeting Notch pathway
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| MK-0752 | γ-secretase | NCT00106145 [ | 103 | Oral | Solid tumors | Monotherapy | 1 (1) | 0 (0) | 10 (10) |
| MK-0752 | γ-secretase | NCT00645333 [ | 30 | Oral | Breast cancer | Combination with docetaxel | 0 (0) | 11 (42) | 9 (34) |
| MK-0752 | γ-secretase | NCT00572182 [ | 23 | Oral | Refractory Pediatric CNS cancer | Monotherapy | 0 (0) | 0 (0) | 2 (9) |
| RO4929097 | γ-secretase | NCT01198184 [ | 17 | Oral | Solid tumors | Combination with temsirolimus | 0 (0) | 0 (0) | 11 (73) |
| RO4929097 | γ-secretase | NCT01145456 [ | 18 | Oral | Solid tumors | Combination with gemcitabine | 0 (0) | 1 (6) | 4 (22) |
| RO4929097 | γ-secretase | NCT01131234 [ | 20 | Oral | Solid Tumors | Combination with cediranib | 0 (0) | 1 (5) | 11 (55) |
| RO4929097 | γ-secretase | NCT01116687 [ | 33 | Oral | Metastatic colorectal cancer | Monotherapy | 0 (0) | 0 (0) | 6 (18) |
| RO4929097 | γ-secretase | NCT01232829 [ | 12 | Oral | Refractory pancreatic cancer | Monotherapy | 0 (0) | 0 (0) | 3 (25) |