Literature DB >> 26885453

Evaluation of 9-cis retinoic acid and mitotane as antitumoral agents in an adrenocortical xenograft model.

Zoltán Nagy1, Kornélia Baghy2, Éva Hunyadi-Gulyás3, Tamás Micsik2, Gábor Nyírő4, Gergely Rácz2, Henriett Butz4, Pál Perge1, Ilona Kovalszky2, Katalin F Medzihradszky3, Károly Rácz5, Attila Patócs6, Peter Igaz1.   

Abstract

The available drug treatment options for adrenocortical carcinoma (ACC) are limited. In our previous studies, the in vitro activity of 9-cis retinoic acid (9-cisRA) on adrenocortical NCI-H295R cells was shown along with its antitumoral effects in a small pilot xenograft study. Our aim was to dissect the antitumoral effects of 9-cisRA on ACC in a large-scale xenograft study involving mitotane, 9-cisRA and their combination. 43 male SCID mice inoculated with NCI-H295R cells were treated in four groups (i. control, ii. 9-cisRA, iii. mitotane, iv. 9-cisRA + mitotane) for 28 days. Tumor size follow-up, histological and immunohistochemical (Ki-67) analysis, tissue gene expression microarray, quantitative real-time-PCR for the validation of microarray results and to detect circulating microRNAs were performed. Protein expression was studied by proteomics and Western-blot validation. Only mitotane alone and the combination of 9-cisRA and mitotane resulted in significant tumor size reduction. The Ki-67 index was significantly reduced in both 9-cisRA and 9-cisRA+mitotane groups. Only modest changes at the mRNA level were found: the 9-cisRA-induced overexpression of apolipoprotein A4 and down-regulation of phosphodiesterase 4A was validated. The expression of circulating hsa-miR-483-5p was significantly reduced in the combined treatment group. The SET protein was validated as being significantly down-regulated in the combined mitotane+9-cisRA group. 9-cisRA might be a helpful additive agent in the treatment of ACC in combination with mitotane. Circulating hsa-miR-483-5p could be utilized for monitoring the treatment efficacy in ACC patients, and the treatment-induced reduction in protein SET expression might raise its relevance in ACC biology.

Entities:  

Keywords:  9-cis retinoic acid; Adrenocortical cancer; SET protein; circulating microRNA; mitotane; xenograft

Year:  2015        PMID: 26885453      PMCID: PMC4731638     

Source DB:  PubMed          Journal:  Am J Cancer Res        ISSN: 2156-6976            Impact factor:   6.166


  65 in total

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Journal:  Oncogene       Date:  2012-04-23       Impact factor: 9.867

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Authors:  P Igaz; Z Tömböl; P M Szabó; I Likó; K Rácz
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2.  Optimal Design for Informative Protocols in Xenograft Tumor Growth Inhibition Experiments in Mice.

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3.  Network-guided modeling allows tumor-type independent prediction of sensitivity to all-trans-retinoic acid.

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Journal:  Am J Cancer Res       Date:  2016-09-01       Impact factor: 6.166

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8.  Establishment of a mouse xenograft model of metastatic adrenocortical carcinoma.

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  9 in total

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