TELOMERES

1. Dr. José María Romero Romero TELOMERES

2. TELOMERES TELOMERES: • are specialized structures at the end of all eukaryotic chromosomes. • ensure chromosome stability and protect the ends from degradation and from fusing with other chromosomes. • contain longthy streches of non-coding tandemly repeated sequence, (TTAGGG)n, and specific proteins.

3. TELOMERES • Normal somatic cells lose telomeric repeats with ongoing cell division. • Telomere length is quite important for cells because they work as a buffer avoiding the loss of coding DNA.

4. TELOMERES • The loss of telomeric repeats triggers replicative senescense in cells. • Telomeres sequences are extraordinary highly conserved in evolution: all vertebrates have the same simple sequence repeat.

5. TELOMERES • There is an important enzyme: TELOMERASE, active only in embryonic, proliferatice cells of renewal tissues, adult male germline and cancer cells, that is the main regulator of telomere´s length. • TELOMERASE is a reverse transcriptase ( a RNA-dependent polymerase) that contains an RNA with the sequence complementary to the telomere repeat TTAGGG. RNA´s polymerase is used as the template.

6. TELOMERES • The model for telomeres is that they are the physical ends of linear eukaryotic chromosomes that contain up to 15 Kb of non-coding tandemly repeated sequence: (TTAGGG)n, and specific proteins, and an overhang of 50- 200 nucleotides in the chromosome terminus.

7. TELOMERES Model of a human telomere DNA Chromosome DNA tandem repeat - (TTAGGG)n 3’ 5’ 30-200 nt 5-15kb

8. TELOMERES T- LOOP D-LOOP 5´ 5´ TTAGGGTTAGGGTTAGGGTTA 3´ AATCCCAATCCCAA TCCCAAT 3´overhang

9. TELOMERES 3´overhang erosion This telomere structure hasn´t stability 5´ 5´ TTAGGGTT 3´ AATCCCAATCCCAA TCCCAAT 3´overhang

10. TELOMERES 3´overhang erosion 5´ 3´ Damaged chromosomes are degraded by nucleases and participate in end joining reactions that fuse two free ends. Chromosomal destabilization is linked to malignancies