Difference between revisions of "Telomere"

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imported>S
(Created page with "<p><span style="font-size: small">Telomeres, the protective elements at the ends of<br /> chromosomes, need to be maintained for cells to<br /> proliferate indefinitely. In many ...")
 
imported>Doyeon Kwak
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<p><span style="font-size: small">Telomeres, the protective elements at the ends of<br />
+
 
chromosomes, need to be maintained for cells to<br />
 
proliferate indefinitely. In many human cancers, the<br />
 
telomeric DNA is replenished by telomerase. However, a<br />
 
second pathway for telomere maintenance, referred to as<br />
 
the ALT pathway, has increasingly been recognized in<br />
 
human cancers. The genetic basis for activation of ALT is<br />
 
not known, but recent data have implicated a chromatin<br />
 
remodeling complex (ATRX/DAXX) and the histone variant<br />
 
H3.3 as players in the repression of ALT. We have<br />
 
examined a large panel of ALT cell lines for their genetic<br />
 
and cell biological features and found that loss of ATRX is a<br />
 
common event in the genesis of ALT lines. In addition, we<br />
 
document that ALT cell lines frequently undergo chromosomal<br />
 
changes and are impaired in their ability to detect<br />
 
and repair damage in their DNA. These hallmarks of ALT<br />
 
are expected to facilitate the detection of ALT&ndash;type tumors<br />
 
in the clinic and may lead to ALT&ndash;specific treatments.</span></p>
 

Revision as of 22:36, 9 December 2015