{"id":1911,"date":"2006-12-07T00:00:00","date_gmt":"2006-12-07T08:00:00","guid":{"rendered":"https:\/\/vermont.salk.edu\/news-release\/detailed-3-d-image-catches-a-key-regulator-of-neural-stem-cell-differentiation-in-action\/"},"modified":"2006-12-07T00:00:00","modified_gmt":"2006-12-07T08:00:00","slug":"detailed-3-d-image-catches-a-key-regulator-of-neural-stem-cell-differentiation-in-action","status":"publish","type":"disclosure","link":"https:\/\/www.salk.edu\/de\/news-release\/detailed-3-d-image-catches-a-key-regulator-of-neural-stem-cell-differentiation-in-action\/","title":{"rendered":"Detailed 3-D image  catches a key regulator of neural stem cell differentiation in action"},"content":{"rendered":"<p>La Jolla, CA  \u2013 Researchers at the Salk Institute for Biological Studies in  collaboration with scientists at the University of California, San Diego (UCSD)  took a high resolution &#8220;action shot&#8221; of a protein switch that plays a crucial  role in the development of the nervous system. Their findings, published in the  Dec. 8 issue of the journal <em>Molecular  Cell<\/em>, provide a template for the design of small molecule inhibitors to  control that switch, a protein called Scp1, at will.<\/p>\n<p>&#8220;Scp1 is an important brake that regulates the transition  from neuronal precursor to mature neuron,&#8221; explains senior author <a href=\"\/de\/faculty\/noel.html\/\">Joseph Noel<\/a>,  Ph.D, a Howard Hughes Medical Institute investigator at Salk. &#8220;Loosening the  brake with an inhibitor would allow us to influence the timing of neuronal  differentiation,&#8221; he adds. <\/p>\n<p>A finely tuned network of molecular &#8220;on&#8221; and &#8220;off&#8221; switches  orchestrates the differentiation of embryonic stem cells into different tissue  types. Being able to manipulate individual switches would allow scientists to  nudge embryonic stem cells into becoming specific cell types, a plus for both  basic research and potential therapies.<\/p>\n<p>&#8220;At the moment, the differentiation of stem cells into  neurons in a Petri dish is a little bit like a black box and not very  efficient,&#8221; explains co-author <a href=\"\/de\/faculty\/pfaff.html\/\">Samuel Pfaff<\/a>, Ph.D., a professor in the Salk&#8217;s  Gene Expression Laboratory, who together with co-author Gordon Gill, Ph.D., of  the Departments of Medicine and Cellular and Molecular Medicine at UCSD, found that  Scp1 silences neuron-specific genes in non-neuronal cells last year. &#8220;Having a  specific inhibitor would give us a lot of insight into the development of the  fetal nervous system and would allow us to chemically push embryonic stem cells  to acquire a neuronal fate in an informed way,&#8221; adds Pfaff.<\/p>\n<p>Scp1 belongs to group of proteins called small  carboxyl-terminal phosphatases (SCPs) that are expressed in almost all tissues  of the body. When active, Scp1 prevents the enzyme RNA polymerase II from  reading and switching on neuronal genes in tissues where they shouldn&#8217;t be  expressed, such as skin, muscle and liver. In the nervous system Scp1 is  switched off, enabling RNA polymerase II to efficiently transcribe information encoded  by neuronal genes and driving the maturation of neural stem cells into  specialized neurons. <\/p>\n<p>&#8220;Scp1 is an interesting twist on how genes can be regulated  during development,&#8221; says Pfaff. &#8220;In the past there has been a lot of emphasis  on chromatin modifications and physical access to genes, but Scp1 regulates the  activity of the enzyme that transcribes genes directly,&#8221; he adds.<\/p>\n<p>Scp1 is not the only protein that directly influences the  activity of RNA polymerase II. A constantly fluctuating brigade of enzymatic  foot soldiers regulates RNA polymerase II&#8217;s activity by chemically modifying the  long cord-like tail that hangs from its globular structure, like a chain on a  light fixture. <\/p>\n<p>Enzymes called kinases turn the &#8220;light&#8221; on by adding small  phosphate chemical groups \u2013 giving RNA polymerase the go-ahead to transcribe  genes \u2013 while removal of those phosphates by phosphatases like Scp1 turns out  the light, effectively stopping RNA polymerase in its tracks.<\/p>\n<p>Noel and postdoctoral fellow Yan Zhang, Ph.D, analyzed the  crystal structure of Scp1 and RNA polymerase together and obtained a  3-dimensional image showing how Scp1 hangs onto the seven amino acid residues  reiterated in the polymerase tail. &#8220;We captured Scp1 bound to a single seven  amino-acid long repeat containing specific phosphates,&#8221; explains Zhang, the  paper&#8217;s first author. &#8220;It turns out that only three amino acids are important  for Scp1&#8217;s ability to know how to remove phosphates from RNA polymerase.&#8221; <\/p>\n<p>She adds that knowing how enzymes like Scp1 precisely  recognize that seven amino acid stretch is exactly the kind of  &#8220;unambiguous information relevant for the design of a chemical inhibitor  by a process known as structure-based drug design.&#8221;<\/p>\n<p>Capitalizing on information gleaned from their structural  studies, Noel&#8217;s lab has already started that structure-based program. &#8220;We have  designed the first generation of inhibitors and now it is a matter of  chemically synthesizing them, testing them in test tubes and cells, and imaging  them bound to Scp1 in 3D,&#8221; says Noel. This will set the stage for the rational  fine-tuning of their efficacy using an established process Noel likens to  molecular dentistry, because his group is striving to shape inhibitory  molecules to fit the groove in Scp1 much the same way that a dentist molds a  filling to fit the cavity in a patient&#8217;s tooth. <\/p>\n<p>Researchers who contributed to the work include Nicolas  Genoud, Ph.D., in the Gene Expression Laboratory at the Salk Institute, Jack E.  Dixon, Ph.D., and Youngjun Kim, Ph.D., in the Departments of Pharmacology and  Cellular and Molecular Medicine at UCSD, and Jianmin Gao, Ph.D., and Jeffery W.  Kelly, Ph.D., at the Skaggs Institute for Chemical Biology of The Scripps  Research Institute, La Jolla. <\/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":[102,106],"disease-research":[],"class_list":["post-1911","disclosure","type-disclosure","status-publish","hentry","faculty-joseph-noel","faculty-samuel-pfaff"],"acf":[],"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v27.3 - https:\/\/yoast.com\/product\/yoast-seo-wordpress\/ -->\n<title>Detailed 3-D image catches a key regulator of neural stem cell differentiation in action - 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\/de\/news-release\/detailed-3-d-image-catches-a-key-regulator-of-neural-stem-cell-differentiation-in-action\/\" \/>\n<meta property=\"og:locale\" content=\"de_DE\" \/>\n<meta property=\"og:type\" content=\"article\" \/>\n<meta property=\"og:title\" content=\"Detailed 3-D image catches a key regulator of neural stem cell differentiation in action - Salk Institute for Biological Studies\" \/>\n<meta property=\"og:description\" content=\"La Jolla, CA \u2013 Researchers at the Salk Institute for Biological Studies in collaboration with scientists at the University of California, San Diego (UCSD) took a high resolution &#8220;action shot&#8221; of a protein switch that plays a crucial role in the development of the nervous system. 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