{"id":1876,"date":"2006-08-16T00:00:00","date_gmt":"2006-08-16T07:00:00","guid":{"rendered":"https:\/\/vermont.salk.edu\/news-release\/when-the-going-gets-tough-slime-molds-start-synthesizing\/"},"modified":"2015-12-03T18:14:44","modified_gmt":"2015-12-04T02:14:44","slug":"when-the-going-gets-tough-slime-molds-start-synthesizing","status":"publish","type":"disclosure","link":"https:\/\/www.salk.edu\/zh\/news-release\/when-the-going-gets-tough-slime-molds-start-synthesizing\/","title":{"rendered":"When the going gets tough, slime molds start synthesizing"},"content":{"rendered":"<p>La Jolla, CA  \u2013 In  times of plenty, the uni-cellular slime mold <em>Dictyostelium discoideum<\/em> leads a solitary life munching on bacteria  littering the forest floor. But these simple creatures can perform heroic  developmental acts: when the bacterial food supply dries up, <em>Dictyostelium<\/em> amebas band together with  their neighbors and form a multi-cellular tower designed to save the children.<\/p>\n<div class=\"imageCaption\"><img decoding=\"async\" src=\"https:\/\/www.salk.eduhttps:\/\/www.salk.edu\/wp-content\/uploads\/2015\/03\/caption_20060816b.jpg\" alt=\"Slime mold\" width=\"300\"><\/p>\n<p>When the food supply dries up, solitary  Dictyostelium discoideum cells congregate and fuse into a  spore-producing tower. A newly discovered hybrid enzyme called Steely2 (shown  in cartoon form) forges the basic structure of the chemical signal (DIF-1,  shown here as a stick model) that orchestrates this vital step in the life  cycle of Dictyostelium: the transformation of omnipotent cells into dedicated  spore or stalk cells. (Image by Mike Austin using a photo by Rob Kay.)<\/p>\n<\/div>\n<p>In a  forthcoming study in <em>Nature Chemical  Biology,<\/em> investigators at the Salk Institute for Biological Studies and the  Medical Research Council of Molecular Biology (MRC) in Cambridge, England,  use traditional and computer-based methods to show how <em>Dictyostelium<\/em> synthesizes the chemical signal called DIF-1, short  for Differentiation Inducing Factor, required for this developmental  transformation.<\/p>\n<p> The  collaboration, explains co-senior author <a href=\"\/zh\/faculty\/noel.html\/\">Joe Noel<\/a>, Ph.D, a Howard Hughes  Medical Institute investigator at Salk, &#8220;shows the power of a combined approach  involving bioinformatics, enzymology, structural biology and genetics to get at  the heart of why organisms exploit natural chemicals to survive and prosper in  challenging ecosystems.&#8221;<\/p>\n<p>When  slime molds starve, they collectively form a multicellular slug-like creature  that locomotes en masse to a warm spot. There, in response to the DIF-1 signal,  slugs literally stand up and their cells metamorphose into either a column of  stalk cells or next-generation spore cells, which perch atop the column waiting  for food supplies to be restored.<\/p>\n<p>Noel  and Michael Austin, Ph.D., a postdoctoral fellow in Noel&#8217;s lab and co-lead  author of the study, have an ongoing interest in the biosynthesis of diverse  plant and microbial polyketides by enzymes known as type III PKSs. Plants make  polyketide natural products such as flavonoids and stilbenes for use as  sunscreens, antibiotics, flower pigments and anti-oxidants. Explains Austin, &#8220;Plant  polyketides are also increasingly recognized to have significant benefits in  the human diet as health-promoting components of green tea, red wine, and  soybeans.&#8221;<\/p>\n<p>Turns  out, DIF-1 belongs to the same crowd. &#8220;While reading a review article on the  diversity of naturally occurring polyketides, we realized that the core  chemical structure of DIF-1, an important developmental signal in <em>Dictyostelium<\/em>, is similar to natural  products made by plant type III PKSs,&#8221; recalls Austin.<\/p>\n<p>At  the time, <em>Dictyostelium<\/em> was in the  midst of having its genome sequenced, and the bits and pieces of raw DNA  sequencing data were being deposited in publicly available databases. Austin recalled, &#8220;One  night I performed a bioinformatics search to look for genetic evidence that  would suggest the existence of a type III PKS in <em>Dictyostelium<\/em>.&#8221; Using various computer programs to find, assemble,  and translate <em>in silico<\/em> the relevant  raw DNA sequencing fragments first into genes then into the proteins these  genes encode, Austin  reconstructed two type III PKS-like gene sequences, and also found a surprise.<\/p>\n<p>Unexpectedly,  these deduced genetic blueprints for type III PKSs revealed each <em>Dictyostelium<\/em> type III PKS to be fused  to other enzymatically active protein domains.  This never seen before hybrid arrangement works like a very efficient  bucket brigade that synthesizes polyketide molecules in slime mold cells. <\/p>\n<p>&#8220;Nature  has paved the way to exploit this novel domain arrangement to bioengineer more  efficient ways of making modified polyketides for human uses,&#8221; said Austin. <\/p>\n<p>Moving  to the bench, Austin and Noel lab manager Marianne Bowman isolated <em>Dictyostelium<\/em> DNA encoding the type III  PKS domains and not only determined their structure, which indeed resembled a  plant PKS, but also showed that one of them, called Steely2, made the chemical  scaffold of DIF-1 in a test tube. All that was left was to prove was that slime  molds themselves used the newly discovered enzyme to make DIF-1.<\/p>\n<p>For  that Noel and Austin  turned to co-senior author Robert Kay, Ph.D., a <em>Dictyostelium<\/em> cellular differentiation expert and groupleader at  the MRC. &#8220;We wrote a paper and sent a version to Rob Kay and said, &#8216;You  don&#8217;t know us, but here&#8217;s what we do. Biochemically we have identified the  machinery that makes the essential precursor for the bioactive DIF-1 molecule.&#8217;  &#8220;<\/p>\n<p>Kay replied that he and co-lead author Tamao Saito, PhD., a  scientist on sabbatical in his lab, had also focused on these unusual type III  PKS genes following the recently completed final assembly and annotation of the  entire <em>Dictyostelium<\/em> genome, which  was carried out by a worldwide collaboration of many scientists, including the  Kay group. <\/p>\n<p>Working  independently, Saito and Kay had deleted the <em>Dictyostelium<\/em> gene for Steely2. Not only could the resulting  &#8220;deficient&#8221; slime molds not make DIF-1 but they couldn&#8217;t construct  the rescue tower, which was exactly the biological corroboration that the Noel  lab wanted to hear. The  two labs pooled data and now publish their work as one, very complete story  while continuing to collaborate on the chemical diversity found in this  fascinating organism that crawls around on the forest floor.<\/p>\n<p>Says  Noel, who is a professor in the Jack H. Skirball Center for Chemical Biology  and Proteomics at Salk, &#8220;This is a wonderful example of where egos get  pushed aside about who did what and instead, as a scientific community, groups  come together to address a fundamental question in biology. In the process, we  collectively discovered an efficient chemical factory in<em> Dicytostelium<\/em> cells that informs us about how to modify similar  systems used in other organisms to produce important medicines from nature.&#8221;<\/p>\n<p>For Noel the problem is to understand biocomplexity at a  level traditionally ignored &#8211; the plethora of natural chemicals found  throughout nature. Organisms use chemicals as a means of interacting with their  surroundings and mankind has exploited this fact to discover the vast majority  of pharmaceuticals used to treat disease today. &#8220;The major fundamental question  in our case is why do organisms make chemicals, what role do these molecules  play in nature and how does the cellular machinery used to make them evolve  over millions of years to provide new ways for the host organisms to survive  and prosper. Understanding the diversity of natural chemicals and the machinery  that produces them gives us a window to look back in time and understand how  organisms evolve at the molecular level.&#8221;<\/p>\n<p>Also  contributing to the study were Steven Haydock, MD, who worked with Kay, Atsushi  Kato, who along with Saito is now at Hokkaido  University in Sapporo, Japan,  and Bradley Moore, PhD., at Scripps Institute of Oceanography,<\/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],"disease-research":[],"class_list":["post-1876","disclosure","type-disclosure","status-publish","hentry","faculty-joseph-noel"],"acf":[],"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v27.3 - https:\/\/yoast.com\/product\/yoast-seo-wordpress\/ -->\n<title>When the going gets tough, slime molds start synthesizing - 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\/when-the-going-gets-tough-slime-molds-start-synthesizing\/\" \/>\n<meta property=\"og:locale\" content=\"zh_CN\" \/>\n<meta property=\"og:type\" content=\"article\" \/>\n<meta property=\"og:title\" content=\"When the going gets tough, slime molds start synthesizing - Salk Institute for Biological Studies\" \/>\n<meta property=\"og:description\" content=\"La Jolla, CA \u2013 In times of plenty, the uni-cellular slime mold Dictyostelium discoideum leads a solitary life munching on bacteria littering the forest floor. 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