Several reports have shown that the ectopic expression of the human telomerase catalytic subunit gene (hTERT) leads to an indefinite extension of the life span of human fibroblasts cultured in vitro without the appearance of cancer-associated changes. We infected two fibroblast strains derived from centenarian individuals with an hTERT containing retrovirus and isolated transduced massive populations (cen2tel and cen3tel). In both populations, hTERT expression reconstituted telomerase activity and extended the life span. In cen2tel, a net telomere lengthening was observed while, in cen3tel, telomeres stabilized at a length lower than that detected in senescent parental cells. Interestingly, both cen2tel and cen3tel cells developed chromosome anomalies, numerical first and structural thereafter. Moreover, cen3tel cells acquired the ability to grow in the absence of solid support, a typical feature of transformed cells. The results we present here highlight an unexpected possible outcome of cellular immortalization driven by telomerase reactivation, and indicate that, in some cases, an artificial extension of cellular replicative capacity can increase the probability of occurrence of genomic alterations, which can lead to cellular transformation.

Karyotype instability and anchorage-independent growth in telomerase-immortalized fibroblasts from two centenarian individuals

REBUZZINI, PAOLA;GIULOTTO, ELENA;
2003-01-01

Abstract

Several reports have shown that the ectopic expression of the human telomerase catalytic subunit gene (hTERT) leads to an indefinite extension of the life span of human fibroblasts cultured in vitro without the appearance of cancer-associated changes. We infected two fibroblast strains derived from centenarian individuals with an hTERT containing retrovirus and isolated transduced massive populations (cen2tel and cen3tel). In both populations, hTERT expression reconstituted telomerase activity and extended the life span. In cen2tel, a net telomere lengthening was observed while, in cen3tel, telomeres stabilized at a length lower than that detected in senescent parental cells. Interestingly, both cen2tel and cen3tel cells developed chromosome anomalies, numerical first and structural thereafter. Moreover, cen3tel cells acquired the ability to grow in the absence of solid support, a typical feature of transformed cells. The results we present here highlight an unexpected possible outcome of cellular immortalization driven by telomerase reactivation, and indicate that, in some cases, an artificial extension of cellular replicative capacity can increase the probability of occurrence of genomic alterations, which can lead to cellular transformation.
2003
The Biology category includes resources that individually cover a broad range of topics in the biological sciences. Resources covering specific areas in biology, such as general microbiology, protozoology, parasitology, biometrics, biological education, heredity, and evolutionary biology are also placed in this category.
Sì, ma tipo non specificato
Inglese
Internazionale
STAMPA
308
4
914
921
TELOMERES; TELOMERASE; CELLULAR IMMORTALIZATION; ANCHORAGE-INDEPENDENT GROWTH; CELLULAR TRANSFORMATION; KARYOTYPE INSTABILITY; CENTENARIANS
10
info:eu-repo/semantics/article
262
Mondello, C.; Chiesa, M.; Rebuzzini, Paola; Zongaro, S.; Verri, A.; Colombo, T.; Giulotto, Elena; D'Incalci, M.; Franceschi, C.; Nuzzo, F.
1 Contributo su Rivista::1.1 Articolo in rivista
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11571/106137
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