Cell Immortalization: In Vivo Molecular Bases and In Vitro Techniques for Obtention

Author:

de Bardet Javier Curi1,Cardentey Celeste Ramírez2,González Belkis López3ORCID,Patrone Deanira4,Mulet Idania Lores5,Siniscalco Dario4ORCID,Robinson-Agramonte María de los Angeles6

Affiliation:

1. Department of Neurobiology, International Center for Neurological Restoration, Havana 11300, Cuba

2. Department of Virology, Tropical Medicine Institute Pedro Kouri, Havana 11400, Cuba

3. Department of Allergy, Calixto Garcia General University Hospital, Havana 10400, Cuba

4. Department of Experimental Medicine, Division of Molecular Biology, Biotechnology and Histology, University of Campania, 80138 Naples, Italy

5. Ramon Gonzalez Coro Hospital, Havana 10400, Cuba

6. Department of Immunochemical, International Center for Neurological Restoration, Havana 11300, Cuba

Abstract

Somatic human cells can divide a finite number of times, a phenomenon known as the Hayflick limit. It is based on the progressive erosion of the telomeric ends each time the cell completes a replicative cycle. Given this problem, researchers need cell lines that do not enter the senescence phase after a certain number of divisions. In this way, more lasting studies can be carried out over time and avoid the tedious work involved in performing cell passes to fresh media. However, some cells have a high replicative potential, such as embryonic stem cells and cancer cells. To accomplish this, these cells express the enzyme telomerase or activate the mechanisms of alternative telomere elongation, which favors the maintenance of the length of their stable telomeres. Researchers have been able to develop cell immortalization technology by studying the cellular and molecular bases of both mechanisms and the genes involved in the control of the cell cycle. Through it, cells with infinite replicative capacity are obtained. To obtain them, viral oncogenes/oncoproteins, myc genes, ectopic expression of telomerase, and the manipulation of genes that regulate the cell cycle, such as p53 and Rb, have been used.

Publisher

MDPI AG

Subject

Applied Microbiology and Biotechnology,Biomedical Engineering,Biochemistry,Bioengineering,Biotechnology

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