Publication | Open Access
Telomere-Associated Protein TIN2 Is Essential for Early Embryonic Development through a Telomerase-Independent Pathway
84
Citations
20
References
2004
Year
GeneticsGenomic MechanismEpigeneticsTelomere LengthTelomerase-independent PathwayGenome InstabilityTelomere Length RegulationEmbryonic DevelopmentGene ExpressionCell BiologyTranscription RegulationCell LineageDevelopmental BiologyTin2 Mutant MiceEarly Embryonic DevelopmentGene RegulationTelomere-associated Protein Tin2Cellular SenescenceCell Fate DeterminationMedicine
TIN2 is a negative regulator of telomere elongation that interacts with telomeric DNA repeat binding factor 1 (TRF1) and affects telomere length by a telomerase-dependent mechanism. Here we show that inactivation of the mouse TRF1-interacting protein 2 (TIN2) gene results in early embryonic lethality. We further observed that the embryonic lethality of TIN2 mutant mice was not affected by inactivation of the telomerase reverse transcriptase gene, indicating that embryonic lethality is not the result of telomerase-dependent changes in telomere length or function. Our findings suggest that TIN2 has a role independent of telomere length regulation that is essential for embryonic development and cell viability.
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