Downregulation of transient receptor potential cation channel, subfamily C, member 1 contributes to drug resistance and high histological grade in ovarian cancer

Liu, Xia; Zou, Jing; Su, Jie; Lü, Yi; Zhang, Jian; Li, Li; Yin, Fuqiang

doi:10.3892/ijo.2015.3254

Cited by 21 publications

(19 citation statements)

References 91 publications

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“…Possible networks of protein or gene interactions with KCNN3 included 49 gene or gene products associated with drug-resistance in OC, which further explained its association with drug resistance. These genes/gene products included 25 oncogenes ( 35 ); URI1, STAT3, SRC, RSF1, PIK3CA, NOTCH3, NINL, NFKB1, MYC, MIEN1, MET, KRAS, JUN, IKBKE, FOS, ERBB2, EGFR, DAXX, CUZD1, CLU, BCL2, BAX, AKT2, AKT1 and ACTN4 and 15 tumor suppressors ( 36 ) including BRCA1, BRCA2, CHEK2, FBXO32, MLH1, SULF1, IL24, CDKN2A, CDKN1A, TP53, TP73, PDCD4, PTEN, RASSF1 and WWOX, as well as 9 other genes, including CCL21 and SPARCL1 ( 37 ), GGNBP2 and RNASET2 ( 38 ), NEK2 ( 39 ), NEK11 ( 40 ), ALDH1A2 and ADH1B ( 41 ) and TRPC1 ( 42 ). KCNN3 directly interacted with 18 of these genes or gene products, and exhibited indirect interactions with the rest ( Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Specifically, acquisition of drug resistance in multiple myeloma is associated with the suppression of inositol 1,4,5-triphosphate receptor type 1, phospholipase C, transient receptor potential cation channel subfamily M member 7 and TRPC1 expression, and reducing the expression of TRPC1 markedly inhibits drug-induced cell death ( 51 ). It was observed that decreased expression of TRPC1 is associated with drug resistance in OC ( 42 ), and the protein interacts with KCNN3. Thus, it was concluded that low expression of KCNN3 may contribute to drug resistance via interactions with TRPC1, through inhibition of drug induced cell death.…”

Section: Discussionmentioning

confidence: 99%

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Low expression of KCNN3 may affect drug resistance in ovarian cancer

et al. 2018

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Drug resistance is a principal contributor to the poor prognosis of ovarian cancer (OC). Therefore, identifying factors that affect drug resistance in OC is critical. In the present study, 51 OC specimens from lab collections were immunohistochemically tested, public data for 489 samples from The Cancer Genome Atlas cohort and 1,656 samples from the Kaplan-Meier Plotter were downloaded, and data were retrieved from Oncomine. It was identified that the mRNA and protein expression of the potassium calcium-activated channel subfamily N member 3 (KCNN3) was markedly lower in OC tissues compared with normal tissues, and in drug-resistant OC tissues compared with sensitive OC tissues. Low KCNN3 expression consistently predicted shorter disease-free and overall survival (OS). Specifically, low KCNN3 expression predicted shorter OS in 395 patients with low expression levels of mucin-16. There was additional evidence that KCNN3 expression is mediated by microRNA-892b. Furthermore, text mining and analyses of protein and gene interactions indicated that KCNN3 affects drug resistance. To the best of the authors' knowledge, this is the first report to associate KCNN3 with poor prognosis and drug resistance in OC. The present findings indicated that KCNN3 is a potential prognostic marker and therapeutic target for OC.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Low expression of KCNN3 may affect drug resistance in ovarian cancer

et al. 2018

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“…In this analysis, in the case of two probe sets that target one gene, only the probe set with significant variability was retained. In the case of more than three probe sets that target one gene, the set exhibiting the most divergent expression was excluded and the set with significant variability was retained (12).…”

Section: Gene Expression Profilesmentioning

confidence: 99%

Cross-validation of genes potentially associated with overall survival and drug resistance in ovarian cancer

Gao

Liu

et al. 2017

Oncology Reports

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Ovarian cancer is the leading cause of death among malignancies of the female reproductive system. The 5-year survival rates of ovarian cancer (OC) patients are very poor as a result of recurrent disease and emergence of drug resistance; thus, studies to find predictive markers and factors for drug resistance are ongoing. In the present study, based on the microarrays from The Cancer Genome Atlas (TCGA), and the Gene Expression Omnibus (GEO) profiles covering 1648 OC patients, 11 out of 136 genes that were found to be significantly dysregulated in OC were associated with overall survival (OS) in 489 OC patients of the TCGA cohort. Of these genes, CRISP3, LYVE1, OVGP1 and BCHE were identified as independent prognostic factors, with decreased expression of the first three genes predicting shorter OS, and decreased BCHE predicting longer OS. OVGP1, BCHE and further two genes, CKAP2 and CLDN10, were consistently and remarkably associated with OS when the number of patients increased from 489 to 1583, with increased CKAP2 and decreased CLDN10 predicted shorter OS; combining the four genes provided better predictions. Associations among the four genes with OS in subgroups of OC were further verified. Downregulation of OVGP1 was significantly associated with shorter OS in all subgroups of OC patients, including subgroups of 752 patients treated with chemotherapy regimens containing taxol, 763 with both platin and taxol, 1364 with platin, 371 patients with grade 1-2 disease, 968 with grade 3 disease, 1148 with stage III-IV disease, and 439 with TP53 mutations. In addition, CKAP2 expression was significantly associated with shorter OS in 515 OC patients who had low CA125 levels. Furthermore, comprehensive analyses that including RT-qPCR, bioinformatics analysis and clinical data revealed an association of CKAP2, BCHE, CLDN10 and OVGP1 with drug resistance in OC. The genes identified in the present study might be prognostic factors as well as potential therapeutic targets in the treatment of OC.

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“…Moreover, the altered expression profile of various members of the TRPC subfamily has been associated with chemoresistance. For instance, TRPC1 expression is significantly decreased in cisplatin-resistant (A2780 and SKOV3) and carboplatin-resistant (A2780) ovarian cancer cell lines, suggesting that the reduced expression of TRPC1 is linked to chemoresistance [169]. On the contrary, TRPC5 has increased in 5-FU-resistant colorectal cancer cells HCT-8/5-FU and LoVo/5-FU cell lines, therefore blockade of TRPC5 promotes chemosensitivity in these cells [170].…”

Section: Trpcmentioning

confidence: 99%

Exploring the Therapeutic Potential of Membrane Transport Proteins: Focus on Cancer and Chemoresistance

Almasi

Hiani

2020

Cancers

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Improving the therapeutic efficacy of conventional anticancer drugs represents the best hope for cancer treatment. However, the shortage of druggable targets and the increasing development of anticancer drug resistance remain significant problems. Recently, membrane transport proteins have emerged as novel therapeutic targets for cancer treatment. These proteins are essential for a plethora of cell functions ranging from cell homeostasis to clinical drug toxicity. Furthermore, their association with carcinogenesis and chemoresistance has opened new vistas for pharmacology-based cancer research. This review provides a comprehensive update of our current knowledge on the functional expression profile of membrane transport proteins in cancer and chemoresistant tumours that may form the basis for new cancer treatment strategies.

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Downregulation of transient receptor potential cation channel, subfamily C, member 1 contributes to drug resistance and high histological grade in ovarian cancer

Cited by 21 publications

References 91 publications

Low expression of KCNN3 may affect drug resistance in ovarian cancer

Low expression of KCNN3 may affect drug resistance in ovarian cancer

Cross-validation of genes potentially associated with overall survival and drug resistance in ovarian cancer

Exploring the Therapeutic Potential of Membrane Transport Proteins: Focus on Cancer and Chemoresistance

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