First Molecular Cytogenetic Characterization of Murine Malignant Mesothelioma Cell Line AEl7 and silico Translation to the Human Genome

Kubicova, Eva; Trifonov, Vladimir; Borovecki, Fran; Liehr, Thomas; Rincic, Martina; Kosyakova, Nadezda; Hussein, Shaymaa

izvor podataka: crosbi !

First Molecular Cytogenetic Characterization of Murine Malignant Mesothelioma Cell Line AEl7 and silico Translation to the Human Genome (CROSBI ID 274789)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Kubicova, Eva ; Trifonov, Vladimir ; Borovecki, Fran ; Liehr, Thomas ; Rincic, Martina ; Kosyakova, Nadezda ; Hussein, Shaymaa First Molecular Cytogenetic Characterization of Murine Malignant Mesothelioma Cell Line AEl7 and silico Translation to the Human Genome // Current bioinformatics, 12 (2017), 1; 11-18. doi: 10.2174/1574893611666160606164459

Podaci o odgovornosti

Autori

Kubicova, Eva ; Trifonov, Vladimir ; Borovecki, Fran ; Liehr, Thomas ; Rincic, Martina ; Kosyakova, Nadezda ; Hussein, Shaymaa

Osnovni podaci na izvornom jeziku
Osnovni podaci na ostalim jezicima

Jezik

engleski

Naslov

First Molecular Cytogenetic Characterization of Murine Malignant Mesothelioma Cell Line AEl7 and silico Translation to the Human Genome

Sažetak

Background: Mesothelial cells can be malignantly transformed e.g. due to previous asbestos exposure and form a clinically aggressive tumor called malignant mesothelioma (MM). Presently, there is extensive ongoing research in MM with the goal to identify prognostic factors and new therapeutic targets. Accordingly, well studied model systems, like cell lines, are urgently needed. Interestingly, murine MM cell lines models were established in the 1990s ; however, they were not characterized genetically in any detail, yet. Objective: Provide first genetic characterization of murine MM cell line AE17, translate into human genome and characterize the human subtype of MM AE17 is suited as a model. Method: AE17 was studied on chromosomal level by molecular cytogenetics and array comparative genomic hybridization. Results and Conclusion: AE17 did not tetraploidize yet, has a basic karyotype of 40 chromosomes with only 3 balanced inversions, one balanced translocation and five chromosomes with simple to complex rearrangements, leading in the end to partial chromosomal deletions. Besides one stemline, three additional subclones could be observed. The obtained data was, by means of bioinformatics based on silico translation of the detected imbalances and observed chromosomal breakpoints, translated to the human genome. The obtained data suggests that AE17 is a well suited cell line model for MM with (cyto)genetic changes characteristic for sarcomatoid MM form. Furthermore, genes ESR2 and BAK1 seem to be activated in one of the subclones of AE17, which also could be of interest for future studies. Overall, the present data could only be obtained through bioinformatics based on silico analyses, to cope with the microarray data and also for browser based translation of murine into human genome.

Ključne riječi

Molecular cytogenetics ; FISH-banding ; genome browsers ; databases ; in silico translation ; murine to human genome

Napomena

nije evidentirano

Jezik

nije evidentirano

Naslov

nije evidentirano

Sažetak

nije evidentirano

Ključne riječi

nije evidentirano

Napomena

nije evidentirano

Podaci o izdanju

Časopis

Current bioinformatics

Volumen (broj)

12 (1)

Godina

2017.

Stranice rada

11-18

Status objave rada

objavljeno

ISSN

1574-8936

e-ISSN

2212-392X

DOI

10.2174/1574893611666160606164459

Povezanost rada

Povezane osobe

Fran Borovečki (CroRIS ID: 3677; MBZ: 230266) (autor/i)

Martina Rinčić (CroRIS ID: 28525; MBZ: 311472) (autor/i)

Povezane ustanove

Medicinski fakultet u Zagrebu (108) (autorova ustanova)

Područje

nije evidentirano

Poveznice

doi.org

Indeksiranost

Scopus

Web of Science Core Collection, Science Citation Index Expanded (WoSCC-SCI-Exp)

Web of Science Core Collection, SCI-Exp, SSCI & A&HCI (WoSCC-SCI-Exp, SSCI, A&HCI)