Literature DB >> 25227893

Differential cellular responses induced by dorsomorphin and LDN-193189 in chemotherapy-sensitive and chemotherapy-resistant human epithelial ovarian cancer cells.

Jennifer L Ali1, Brittany J Lagasse, Ainsley J Minuk, Allison J Love, Amani I Moraya, Linda Lam, Gilbert Arthur, Spencer B Gibson, Ludivine Coudière Morrison, Tamra E Werbowetski-Ogilvie, Yangxin Fu, Mark W Nachtigal.   

Abstract

Inherent or acquired drug resistance is a major contributor to epithelial ovarian cancer (EOC) mortality. Novel drugs or drug combinations that produce EOC cell death or resensitize drug resistant cells to standard chemotherapy may improve patient treatment. After conducting drug tolerability studies for the multikinase inhibitors dorsomorphin (DM) and it is structural analogue LDN-193189 (LDN), these drugs were tested in a mouse intraperitoneal xenograft model of EOC. DM significantly increased survival, whereas LDN showed a trend toward increased survival. In vitro experiments using cisplatin (CP)-resistant EOC cell lines, A2780-cp or SKOV3, we determined that pretreatment or cotreatment with DM or LDN resensitized cells to the killing effect of CP or carboplatin (CB). DM was capable of blocking EOC cell cycle and migration, whereas LDN produced a less pronounced effect on cell cycle and no effect on migration. Subsequent analyses using primary human EOC cell samples or additional established EOC cells lines showed that DM or LDN induced a dose-dependent autophagic or cell death response, respectively. DM induced a characteristic morphological change with the appearance of numerous LC3B-containing acidic vacuoles and an increase in LC3BII levels. This was coincident with a decrease in cell growth and the altered cell cycle consistent with DM-induced cytostasis. By contrast, LDN produced a caspase 3-independent, reactive oxygen species-dependent cell death. Overall, DM and LDN possess drug characteristics suitable for adjuvant agents used to treat chemotherapy-sensitive and -resistant EOC.
© 2014 UICC.

Entities:  

Keywords:  autophagy; dorsomorphin analogues; drug resistance; epithelial ovarian cancer; mouse xenograft; reactive oxygen species

Mesh:

Substances:

Year:  2014        PMID: 25227893     DOI: 10.1002/ijc.29220

Source DB:  PubMed          Journal:  Int J Cancer        ISSN: 0020-7136            Impact factor:   7.396


  18 in total

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Review 6.  Autophagy as an emerging therapy target for ovarian carcinoma.

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Review 7.  Structural basis for the potent and selective binding of LDN-212854 to the BMP receptor kinase ALK2.

Authors:  Eleanor Williams; Alex N Bullock
Journal:  Bone       Date:  2017-09-12       Impact factor: 4.398

8.  BMP4 Upregulation Is Associated with Acquired Drug Resistance and Fatty Acid Metabolism in EGFR-Mutant Non-Small-Cell Lung Cancer Cells.

Authors:  Duc-Hiep Bach; Thi-Thu-Trang Luu; Donghwa Kim; Yong Jin An; Sunghyouk Park; Hyen Joo Park; Sang Kook Lee
Journal:  Mol Ther Nucleic Acids       Date:  2018-08-04       Impact factor: 8.886

Review 9.  BMP signaling and its paradoxical effects in tumorigenesis and dissemination.

Authors:  Lijie Zhang; Yingnan Ye; Xinxin Long; Pei Xiao; Xiubao Ren; Jinpu Yu
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10.  Kallikrein-related peptidases 4, 5, 6 and 7 regulate tumour-associated factors in serous ovarian cancer.

Authors:  Ping Wang; Viktor Magdolen; Christof Seidl; Julia Dorn; Enken Drecoll; Matthias Kotzsch; Feng Yang; Manfred Schmitt; Oliver Schilling; Anja Rockstroh; Judith Ann Clements; Daniela Loessner
Journal:  Br J Cancer       Date:  2018-10-05       Impact factor: 7.640

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