MET Expression and Cancer Stem Cell Networks Impact Outcome in High-Grade Serous Ovarian Cancer

Bååth, Maria; Jönsson, Jenny-Maria; Westbom-Fremer, Sofia; Fuente, Laura Martín de la; Tran, Lena; Malander, Susanne; Kannisto, Päivi; Måsbäck, Anna; Honeth, Gabriella; Hedenfalk, Ingrid

doi:10.3390/genes12050742

Cited by 8 publications

(6 citation statements)

References 42 publications

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“…The potential utilization of crizotinib, a c-MET inhibitor, is relevant to the finding that in 7-27% of OC cases, c-MET was overexpressed. Its activation was found related to poor prognosis in patients with high-grade serous ovarian cancer (HGSOC) [67]. In addition, our results corroborate previous finding showing synergistic activity of crizotinib and platinum compounds in animal models of OC [68,69].…”

Section: Discussionsupporting

confidence: 90%

Secreted soluble factors from tumor-activated mesenchymal stromal cells confer platinum chemoresistance to ovarian cancer cells

Carmi

Adawi

Khamaisi

et al. 2023

Preprint

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Ovarian cancer ranks as the second most common type of gynecological malignancy, has poor survival rates, and is frequently diagnosed at an advanced stage. Platinum-based chemotherapy, such as carboplatin, represents the standard-of-care for OC. However, toxicity and acquired resistance to therapy have proven challenging in the treatment of patients, most of who will experience relapse, mainly due to chemoresistance. Chemoresistance, a principal obstacle to durable response in OC patients, is attributed to alterations within the cancer cells, and can also be mediated by the tumor microenvironment (TME). In this study, we report that conditioned medium (CM) derived from murine and human stromal cells, MS-5 and HS-5 respectively, and tumor-activated HS-5, was active in conferring platinum chemoresistance to OC cells. Moreover, CM derived from differentiated murine pre-adipocyte (3T3-L1), but not undifferentiated pre-adipocyte cells, confers platinum chemoresistance to OC cells. Interestingly, CM derived from tumor-activated HS-5 was more effective in conferring chemoresistance than was CM derived from HS-5 cells. Various OC cells exhibit variable sensitivity to CM activity. Moreover, exposure of OC to CM affected ERK phosphorylation in a non-consistent pattern and in a cell-specific manner, and does not correlate with platinum chemoresistance. Exploring CM content revealed the enrichment of a number of soluble factors in the tumor-activated HS-5, such as soluble uPAR (SuPAR), IL-6, and hepatocyte growth factor (HGF). FDA-approved JAK inhibitors were mildly effective in restoring platinum sensitivity in two of the three OC cell lines in the presence of CM. Exposure to increasing concentrations of HGF resulted in increased proliferation and reduced platinum sensitivity. Crizotinib, an ALK and c-MET inhibitor, in combination with platinum, blocked the ability of HGF to promote platinum resistance and restore platinum sensitivity to OC cells. Finally, exposure to 2-hydroxyestardiol (2HE2) was effective in restoring platinum sensitivity to OC cells exposed to CM.

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Section: Discussionsupporting

confidence: 90%

Secreted soluble factors from tumor-activated mesenchymal stromal cells confer platinum chemoresistance to ovarian cancer cells

Carmi

Adawi

Khamaisi

et al. 2023

Preprint

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“…ATM haploinsufficiency is the feature that make cells overexpressing MET susceptible to the combined treatment even at low doses of the small molecule METi. Data shown here confirm that MET expression and activation are not sufficient to make MET overexpressing cells, such as ovarian cancer cells, susceptible to METi or to the combined treatment, in line with the report that no synergistic effects of the combined treatment with PARPi and METi were found in cell lines with BRCA1 or BRCA2 deficiency [ 40 ]. This agrees also with the recent report that increased MET protein expression was found in primary cultures of PARPi resistant high-grade serous ovarian carcinomas [ 41 ].…”

Section: Discussionsupporting

confidence: 89%

Cancer Cells Haploinsufficient for ATM Are Sensitized to PARP Inhibitors by MET Inhibition

D'Ambrosio

Erriquez

Capellero

et al. 2022

IJMS

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The MET oncogene encodes a tyrosine kinase (TK) receptor. Its activation protects cells from death but also stimulates DNA damage response by triggering excess replicative stress. Transcriptomic classification of cancer cell lines based on MET expression showed that response to the PARP inhibitor (PARPi) olaparib is poorer in MET overexpressing cell lines. Accordingly, a high MET expressing lung carcinoma cell line was sensitized to PARPi by MET TK inhibition. This was not linked solely to MET overexpression: other MET overexpressing cell lines were biochemically but not functionally responsive to combined inhibition. Moreover, exogenously induced MET overexpression was unable to induce resistance to PARPi. The MET overexpressing cell line, responsive to the combined PARP and MET inhibition, carried a heterozygous mutation of the ATM gene and showed an attenuated response of ATM to PARPi. Among the downstream targets of ATM activation, NuMA was phosphorylated only in response to the combined PARP and MET inhibition. Given the role played by NuMA in mitosis, data show that the latter is affected by MET and PARP inhibition in cells with haploinsufficient ATM. This is important as ATM heterozygous mutation is frequently found in human cancer and in lung carcinomas in particular.

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“…Overexpression of c-MET was reported in 7–27 % of OC patients. Its activation was linked to a poor prognosis in individuals with high-grade serous ovarian cancer (HGSOC) [50] , lung, breast, stomach, and head and neck cancers. Treatment with crizotinib increased apoptosis and reduced cell proliferation in OC cell carcinomas with elevated levels of c-MET.…”

Section: Discussionmentioning

confidence: 99%

Ovarian cancer ascites confers platinum chemoresistance to ovarian cancer cells

Carmi,

Agbarya,

Khamaisi

et al. 2024

Translational Oncology

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MET Expression and Cancer Stem Cell Networks Impact Outcome in High-Grade Serous Ovarian Cancer

Cited by 8 publications

References 42 publications

Secreted soluble factors from tumor-activated mesenchymal stromal cells confer platinum chemoresistance to ovarian cancer cells

Secreted soluble factors from tumor-activated mesenchymal stromal cells confer platinum chemoresistance to ovarian cancer cells

Cancer Cells Haploinsufficient for ATM Are Sensitized to PARP Inhibitors by MET Inhibition

Ovarian cancer ascites confers platinum chemoresistance to ovarian cancer cells

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