{"id":1908,"date":"2007-02-14T00:00:00","date_gmt":"2007-02-14T08:00:00","guid":{"rendered":"https:\/\/vermont.salk.edu\/news-release\/dna-ends-common-tool-different-job\/"},"modified":"2007-02-14T00:00:00","modified_gmt":"2007-02-14T08:00:00","slug":"dna-ends-common-tool-different-job","status":"publish","type":"disclosure","link":"https:\/\/www.salk.edu\/zh\/news-release\/dna-ends-common-tool-different-job\/","title":{"rendered":"DNA ends: common tool, different job"},"content":{"rendered":"<p>La Jolla, CA \u2013 Every time a cell repairs or replicates its DNA, the  resulting single strand is wrapped up by a dedicated protein complex. In  eukaryotes or organisms whose cells have a nucleus, this job is handled by a  tripartite complex called replication protein A (RPA). Researchers at the Salk  Institute for Biological Studies have now unearthed a novel RPA-like complex  that specifically homes in on the short single-stranded DNA &#8220;tail&#8221; end of yeast  chromosomes.<\/p>\n<p>Their findings, reported in the online edition of <em>Nature Structural &#038; Molecular Biology<\/em>,  will help scientists to better understand the dynamics that keep chromosomes  ends, called telomeres, intact. <\/p>\n<p>&#8220;Identification of  this new RPA-like complex, which is targeted to a specific region of the  genome, suggests that multiple RPA-like complexes have evolved, each making  individual contributions to genomic stability,&#8221; says the study&#8217;s lead author <a href=\"\/zh\/faculty\/lundblad.html\/\">Vicki Lundblad<\/a>, Ph.D., a professor in the Molecular Cell Biology Laboratory at  the Salk Institute.<\/p>\n<p>With each round of cell division, telomeres  \u2013  long  stretches of repetitive DNA  \u2013  erode a little bit further. Some have likened  this progressive shortening to a genetic biological clock that winds down over  time. In fact, when telomeres reach a &#8220;critical length,&#8221; the cell can  no longer multiply  \u2013  a characteristic sign of cellular senescence. <\/p>\n<p>In certain cells, such as our germ cells or baker&#8217;s yeast  cells, which need to divide indefinitely, an enzyme called telomerase elongates  telomeres to compensate for the continual attrition at chromosome ends. At the  same time, telomerase activity is the main mechanism by which human tumor cells  achieve immortal growth.<\/p>\n<p>In addition, the natural ends of chromosomes could  potentially look like broken strands of DNA that a cell&#8217;s repair machinery is  designed to fix. This has been a long-standing puzzle, because mending  chromosome ends as though they were double-strand breaks would result in either  unregulated degradation or end-to-end fusions. Such repair events are lethal  for the genome, and in certain settings, can promote the development of cancer.<\/p>\n<p>About 10 years ago, Lundblad discovered that Cdc13, a  protein that binds single-stranded telomeric DNA, plays a central role at the  telomeres of baker&#8217;s yeast. But the function of two Cdc13-associated proteins,  Stn1 and Ten1, remained unclear.<\/p>\n<p>When members of the Lundblad laboratory searched the  Protein Data Bank for relatives of Stn1, they dug up Rpa2, the middle subunit  of the RPA complex. In particular, Stn1 and Rpa2 share similarities in a region  known as oligonucleotide\/oligosaccharide-binding fold or OB-fold, a protein  fold that is commonly used to recognize and bind to either DNA or RNA. <\/p>\n<p>Based on these findings, Lundblad and her colleagues  developed a model, which predicts that Cdc13, Stn1 and Ten1 come together at  the very end of chromosomes to form a telomere-dedicated RPA-like complex they dubbed the t-RPA complex.<\/p>\n<p>Graduate student and first author Hua Gao tested this  model, using detailed biochemical experiments which revealed that Stn1 and Ten1  behave just like their counterparts in the conventional RPA complex. However,  Stn1 and Ten1 have the same predilection for single-stranded telomeric DNA as  Cdc13, thereby helping to ensure that this complex only targets chromosome tips. <\/p>\n<p>According to Lundblad, this finding raises important  questions about the potential biological parallels between the conventional RPA  complex and the newly discovered t-RPA complex. <\/p>\n<p>&#8220;Whereas the conventional RPA complex acts elsewhere in  the genome to raise a red flag to attract the attention of the repair  machinery,&#8221; says Lundblad<em>, <\/em>&#8220;curiously,  the t-RPA complex performs the exact opposite function at chromosome ends,  ensuring that these tips do not become targets for DNA repair.&#8221;<\/p>\n<p>Lundblad&#8217;s group is currently working on elucidating  what distinguishes the activities of these two RPA complexes from each other. Researchers  who also contributed to this work include postdoctoral researcher Rachel B.  Cervantes, Ph.D., and graduate students Edward K. Mandell and Joel. H. Otero. <\/p>\n<p>The Salk Institute for  Biological Studies in La Jolla,   California, is an independent  nonprofit organization dedicated to fundamental discoveries in the life  sciences, the improvement of human health and the training of future generations  of researchers. Jonas Salk, M.D., whose polio vaccine all but eradicated the  crippling disease poliomyelitis in 1955, opened the Institute in 1965 with a  gift of land from the City of San    Diego and the financial support of the March of Dimes.<\/p>","protected":false},"featured_media":0,"template":"","faculty":[98],"disease-research":[],"class_list":["post-1908","disclosure","type-disclosure","status-publish","hentry","faculty-vicki-lundblad"],"acf":[],"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v27.3 - https:\/\/yoast.com\/product\/yoast-seo-wordpress\/ -->\n<title>DNA ends: common tool, different job - Salk Institute for Biological Studies<\/title>\n<meta name=\"robots\" content=\"index, follow, max-snippet:-1, max-image-preview:large, max-video-preview:-1\" \/>\n<link rel=\"canonical\" href=\"https:\/\/www.salk.edu\/zh\/news-release\/dna-ends-common-tool-different-job\/\" \/>\n<meta property=\"og:locale\" content=\"zh_CN\" \/>\n<meta property=\"og:type\" content=\"article\" \/>\n<meta property=\"og:title\" content=\"DNA ends: common tool, different job - Salk Institute for Biological Studies\" \/>\n<meta property=\"og:description\" content=\"La Jolla, CA \u2013 Every time a cell repairs or replicates its DNA, the resulting single strand is wrapped up by a dedicated protein complex. 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