{"id":1884,"date":"2006-06-27T00:00:00","date_gmt":"2006-06-27T07:00:00","guid":{"rendered":"https:\/\/vermont.salk.edu\/news-release\/finding-a-cellular-neverland-how-stem-cells-stay-childlike\/"},"modified":"2006-06-27T00:00:00","modified_gmt":"2006-06-27T07:00:00","slug":"finding-a-cellular-neverland-how-stem-cells-stay-childlike","status":"publish","type":"disclosure","link":"https:\/\/www.salk.edu\/es\/news-release\/finding-a-cellular-neverland-how-stem-cells-stay-childlike\/","title":{"rendered":"Finding a cellular Neverland: How stem cells stay childlike"},"content":{"rendered":"<p>La Jolla, CA  \u2013 Despite their celebrated &#8220;immortality,&#8221; the capacity of  embryonic stem (ES) cells for endless division has its limits. After a very  extended childhood spent dividing in a culture dish, even stem cells tend to  grow up and assume adult roles as workaday nerve, muscle, or blood cells, never  to return to their youthful state.<\/p>\n<p>How some ES cells succeed in recapturing lost cellular  innocence and start anew once they begin maturing is described in a forthcoming  study in <em>Proceedings of the National  Academy of Sciences<\/em>, authored by a team of scientists from the Salk  Institute for Biological Studies. <\/p>\n<p>The team, headed by professor <a href=\"\/es\/faculty\/belmonte.html\/\">Juan Carlos Ispiz\u00faa Belmonte<\/a>,  Ph.D., of the Gene Expression Laboratory and including professor <a href=\"\/es\/faculty\/gage.html\/\">Fred Gage<\/a>,  Ph.D., of the Laboratory of Genetics, demonstrates how a DNA-binding protein  called Nanog coaxes mouse ES cells trying to differentiate into muscle cells  back into an immature state. Nanog is named for the legendary Celtic land Tir  nan Og where people remained forever young<\/p>\n<p>&#8220;Embryonic stem cells represent enormous hope for treating  otherwise incurable diseases,&#8221; says Belmonte. &#8220;But before we can design  therapeutic strategies or introduce these cells into patients, we must learn  how to differentiate them into specific cell types and how to tame their  formidable proliferating ability,&#8221; he explains.<\/p>\n<p>Nanog is a critical factor required for what cell biologists  call &#8220;stemness,&#8221; which is defined by two qualities: the ability of ES cells to  divide or &#8220;self-renew&#8221; and their plasticity in assuming the identity of almost  any cell type, which is also known as &#8220;pluripotency.&#8221; <\/p>\n<p>In a study published earlier this year, the same Belmonte  and Gage lab team demonstrated that a few ES cells in a culture dish tended to  lose stemness and evolve into muscle cell precursors, most likely goaded by a  muscle differentiation factor known as BMP. But when those maturing cells were  forced to produce Nanog, they reverted to their na\u00efve state and regained  pluripotency. <\/p>\n<p>Atsushi Suzuki, PhD., a former postdoctoral fellow in the  Belmonte lab, was the lead author of both that and the present study. &#8220;It was exciting  because nobody knew that \u2018reverse differentiation&#8217; occurred in ES cell  cultures,&#8221; he said referring to the first report. &#8220;And nobody knew how Nanog  maintains an undifferentiated ES cell population.&#8221; <\/p>\n<p>Their current study explains how. When BMP turns ES cells  into muscle it activates a protein called Smad1, a DNA-binding protein that, in  opposition to Nanog, switches on genes responsible for muscle cell fate. Smad1  can only do this when assisted by generic factors known as co-activators, which  stimulate gene expression. <\/p>\n<p>The team found that in ES cells attempting to differentiate  prematurely, Nanog actually binds to Smad1 protein and interferes with its  ability to recruit those obligatory coactivators, thereby rendering Smad1  powerless to initiate muscle gene expression. With Smad1 out of the game and  Nanog in full control, cells revert to their forever-young state. <\/p>\n<p>&#8220;We found that in suitable conditions, differentiated cells are  still capable of producing stem cells as descendants,&#8221; says Suzuki. &#8220;The molecular mechanisms that we identified  here might be used to regenerate stem cells from differentiated cells.&#8221; <\/p>\n<p>Identifying  the Nanog\/Smad1 feedback loop indeed has significant implications for  regenerative medicine. Animals like salamanders readily regenerate severed  limbs as adults, but mammals cannot. In fact, mammals have a limited repertoire  of tissues they can regenerate, and some essential ones, such as nerves and  cardiac muscle, are not on that list.<\/p>\n<p>For  human tissue regeneration to become a viable therapy for conditions like  neurodegeneration or diabetes, clinicians will likely need to artificially  manipulate factors that return adult brain or pancreatic cells to a cellular  &#8220;Tir Nan Og&#8221; to restore adult cell types. &#8220;Our findings open the possibility of  de-differentiating cells in our body so that they can replace diseased cells,&#8221;  says Belmonte.<\/p>\n<p>Suzuki,  possibly inspired by his new job as a research scientist at the Research Unit for Organ  Regeneration in Kobe, Japan, explains it this way: &#8220;Just  as humans can start over in life, differentiated cells can also take on other  fates following the generation of undifferentiated stem cells.&#8221;<\/p>\n<p>Other  contributors to the study include Yasuhiko Kawakami, PhD., Masanobu Morita,  PhD., and Concepci\u00f3n Rodr\u00edguez-Esteban, PhD., all currently in the Belmonte  lab; and former Belmonte lab members, \u00c1ngel Raya, PhD., now at the Center for Regenerative Medicine of Barcelona, and Takaaki Matsui, PhD., now at the Nara Institute of Science and Technology in Japan. Also contributing was Kinichi  Nakashima, PhD., also at the Nara Institute of  Science and Technology and a former visiting  scientist in the Gage lab.<\/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":[85,76],"disease-research":[],"class_list":["post-1884","disclosure","type-disclosure","status-publish","hentry","faculty-juan-carlos-izpisua-belmonte","faculty-rusty-gage"],"acf":[],"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v27.3 - https:\/\/yoast.com\/product\/yoast-seo-wordpress\/ -->\n<title>Finding a cellular Neverland: How stem cells stay childlike - 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\/es\/news-release\/finding-a-cellular-neverland-how-stem-cells-stay-childlike\/\" \/>\n<meta property=\"og:locale\" content=\"es_MX\" \/>\n<meta property=\"og:type\" content=\"article\" \/>\n<meta property=\"og:title\" content=\"Finding a cellular Neverland: How stem cells stay childlike - Salk Institute for Biological Studies\" \/>\n<meta property=\"og:description\" content=\"La Jolla, CA \u2013 Despite their celebrated &#8220;immortality,&#8221; the capacity of embryonic stem (ES) cells for endless division has its limits. 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