{"id":203952,"date":"2017-07-07T01:47:16","date_gmt":"2017-07-07T05:47:16","guid":{"rendered":"http:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/researchers-explore-dna-folding-cellular-packing-with-supercomputer-simulations-phys-org\/"},"modified":"2017-07-07T01:47:16","modified_gmt":"2017-07-07T05:47:16","slug":"researchers-explore-dna-folding-cellular-packing-with-supercomputer-simulations-phys-org","status":"publish","type":"post","link":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/transhuman-news-blog\/dna\/researchers-explore-dna-folding-cellular-packing-with-supercomputer-simulations-phys-org\/","title":{"rendered":"Researchers explore DNA folding, cellular packing with supercomputer simulations &#8211; Phys.Org"},"content":{"rendered":"<p><p>July 6, 2017          Sequence-specific, twist-induced, kinked elastic    configurations, generated by molecular dynamics simulations on    supercomputers at the Texas Advanced Computing Center, help    explain how long strands of DNA can fit in small spaces.    Credit: Christopher G. Myers, B. Montgomery Pettitt, University    of Texas Medical Branch    <\/p>\n<p>      A biological mystery lies at the center of each of our cells,      namely: how one meter of DNA can be wadded up into the space      of a micron (or one millionth of a meter) within each nucleus      of our body.    <\/p>\n<p>    The nuclei of human cells are not even the most crowded    biological place that we know of. Some bactiophagesviruses    that infect and replicate within a bacteriumhave even more    concentrated DNA.  <\/p>\n<p>    \"How does it get in there?\" B. Montgomery (Monte) Pettitt, a    biochemist and professor at the University of Texas Medical    Branch, asks. \"It's a charged polymer. How does it overcome the    repulsion at its liquid crystalline density? How much order and    disorder is allowed, and how does this play a role in nucleic    acids?\"  <\/p>\n<p>    Using the Stampede and Lonestar5 supercomputers at The    University of Texas at Austin's Texas Advanced Computing Center    (TACC), Pettitt investigates how phages' DNA folds into    hyper-confined spaces.  <\/p>\n<p>    Writing in the June 2017 issue of the Journal of    Computational Chemistry, he explained how DNA may overcome    both electrostatic repulsion and its natural stiffness.  <\/p>\n<p>    The key to doing so? Kinks.  <\/p>\n<p>    The introduction of sharp twists or curves into configurations    of DNA packaged within a spherical envelope significantly    reduces the overall energies and pressures of the molecule,    according to Pettitt.  <\/p>\n<p>    He and his collaborators used a model that deforms and kinks    the DNA every 24 base pairs, which is close to the average    length that is predicted from the phage's DNA sequence. The    introduction of such persistent defects not only reduces the    total bending energy of confined DNA, but also reduces the    electrostatic component of the energy and pressure.  <\/p>\n<p>    \"We show that a broad ensemble of polymer configurations is    consistent with the structural data,\" he and collaborator    Christopher Myers, also of University of Texas Medical Branch,    wrote.  <\/p>\n<p>    Insights like these cannot be gained strictly in the lab. They    require supercomputers that serve as molecular microscopes,    charting the movement of atoms and atomic bonds at length- and    time-scales that are not feasible to study with physical    experiments alone.  <\/p>\n<p>    \"In the field of molecular biology, there's a wonderful    interplay between theory, experiment and simulation,\" Pettitt    said. \"We take parameters of experiments and see if they agree    with the simulations and theories. This becomes the scientific    method for how we now advance our hypotheses.\"  <\/p>\n<p>    Problems like the ones Pettitt is interested in cannot be    solved on a desktop computer or a typical campus cluster, but    require hundreds of computer processors working in parallel to    mimic the minute movements and physical forces of molecules in    a cell.  <\/p>\n<p>    Pettitt is able to access TACC's supercomputers in part because    of a unique program known as the Journal of    Computational Chemistry initiative, which makes TACC's    computing resources, expertise and training available to    researchers within the University of Texas Systems' 14    institutions.  <\/p>\n<p>    \"Computational research, like that of Dr. Pettitt, which seeks    to bridge our understanding of physical, chemical, and    ultimately biological phenomena, involves so many calculations    that it's only really approachable on large supercomputers like    TACC's Stampede or Lonestar5 systems,\" said Brian Beck, a life    sciences researcher at TACC.  <\/p>\n<p>    \"Having TACC supercomputing resources available is critical to    this style of research,\" Pettitt said.  <\/p>\n<p>    FINDING THE ORDER IN DISORDERED PROTEINS  <\/p>\n<p>    Another phenomenon that has long interested Pettitt is the    behavior of Intrinsically Disordered Proteins (IDPs) and    intrinsically disordered domains, where parts of a protein have    a disordered shape.  <\/p>\n<p>    Unlike crystals or the highly-packed DNA in viruses, which have    distinct, rigid shapes, IDPs \"fold up into a gooey mess,\"    according to Pettitt. And yet they're critical for all forms of    life.  <\/p>\n<p>    It is believed that in eukaryotes (organisms whose cells have    complex substructures like nuclei), roughly 30 percent of    proteins have an intrinsically disordered domain. More than 60    percent of proteins involved in cell signaling (molecular    processes that take signals from outside the cell or across    cells that tell the cell what behaviors to turn on and off in    response) have disordered domains. Similarly, 80 percent of    cancer-related signaling proteins have IDP regions - making    them important molecules to understand.  <\/p>\n<p>    Among the IDPs Pettitt and his group are studying are nuclear    transcription factors. These molecules control the expression    of genes and have a signaling domain that is rich in the    flexible amino acid, glycine.  <\/p>\n<p>    The folding of the nuclear transcription factor signaling    domain is not brought about by hydrogen bonding and hydrophobic    effects, like most protein molecules, according to Pettitt.    Rather, when the longer molecules find too many glycines in a    space, they go beyond their solubility and start associating    with each other in unusual ways.  <\/p>\n<p>    \"It's like adding too much sugar in your tea,\" Pettitt    explains. \"It won't get any sweeter. The sugar must fall out of    solution and find a partner - precipitating into a lump.\"  <\/p>\n<p>    Writing in Protein    Science in 2015, he described molecular simulations    performed on Stampede that helped to explain how and why IDPs    collapse into globule-like structures.  <\/p>\n<p>    The simulations calculated the forces from carbonyl (CO)    dipole-dipole interactionsattractions between the positive end    of one polar molecule and the negative end of another polar    molecule. He determined that these interactions are more    important in the collapse and aggregation of long strands of    glycine than the formation of H-bonds.  <\/p>\n<p>    \"Given that the backbone is a feature of all proteins, CO    interactions may also play a role in proteins of nontrivial    sequence where structure is eventually determined by interior    packing and the stabilizing effects of H-bonds and CO-CO    interactions,\" he concluded.  <\/p>\n<p>    The research was enabled by an allocation of compute time on    Stampede through the Extreme Science and Engineering Discovery    Environment (XSEDE) which is supported by the National Science    Foundation.  <\/p>\n<p>    Pettitt, a long-time champion of supercomputing, doesn't only    use TACC resources himself. He encourages other scholars,    including his colleagues at the Sealy Center for Structural    Biology and Molecular Biophysics, to use supercomputers as    well.  <\/p>\n<p>    \"Advanced computing is important for data analysis and data    refinement from experiments, X-ray and electron microscopy, and    informatics,\" he says. \"All of these problems have big data    processing issues that can be addressed using advanced    computing.\"  <\/p>\n<p>    When it comes to uncovering the mysteries of biology on the    tiniest scales, nothing quite beats a giant supercomputer.  <\/p>\n<p>     Explore further:    Rosetta    online server that includes everyone  <\/p>\n<p>    More information: Christopher G. Myers et al, Phage-like    packing structures with mean field sequence dependence,    Journal of Computational Chemistry (2017). DOI: 10.1002\/jcc.24727<\/p>\n<p>        Our bodies are made of biomolecules like proteins, nucleic        acids, fats and sugars. 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Read more    <\/p>\n<p><!-- Auto Generated --><\/p>\n<p>The rest is here:<br \/>\n<a target=\"_blank\" href=\"https:\/\/phys.org\/news\/2017-07-explore-dna-cellular-supercomputer-simulations.html\" title=\"Researchers explore DNA folding, cellular packing with supercomputer simulations - Phys.Org\">Researchers explore DNA folding, cellular packing with supercomputer simulations - Phys.Org<\/a><\/p>\n","protected":false},"excerpt":{"rendered":"<p> July 6, 2017 Sequence-specific, twist-induced, kinked elastic configurations, generated by molecular dynamics simulations on supercomputers at the Texas Advanced Computing Center, help explain how long strands of DNA can fit in small spaces. Credit: Christopher G. Myers, B.  <a href=\"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/transhuman-news-blog\/dna\/researchers-explore-dna-folding-cellular-packing-with-supercomputer-simulations-phys-org\/\">Continue reading <span class=\"meta-nav\">&rarr;<\/span><\/a><\/p>\n","protected":false},"author":4,"featured_media":0,"comment_status":"closed","ping_status":"closed","sticky":false,"template":"","format":"standard","meta":{"footnotes":""},"categories":[26],"tags":[],"class_list":["post-203952","post","type-post","status-publish","format-standard","hentry","category-dna"],"_links":{"self":[{"href":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/wp-json\/wp\/v2\/posts\/203952"}],"collection":[{"href":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/wp-json\/wp\/v2\/posts"}],"about":[{"href":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/wp-json\/wp\/v2\/types\/post"}],"author":[{"embeddable":true,"href":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/wp-json\/wp\/v2\/users\/4"}],"replies":[{"embeddable":true,"href":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/wp-json\/wp\/v2\/comments?post=203952"}],"version-history":[{"count":0,"href":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/wp-json\/wp\/v2\/posts\/203952\/revisions"}],"wp:attachment":[{"href":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/wp-json\/wp\/v2\/media?parent=203952"}],"wp:term":[{"taxonomy":"category","embeddable":true,"href":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/wp-json\/wp\/v2\/categories?post=203952"},{"taxonomy":"post_tag","embeddable":true,"href":"https:\/\/www.euvolution.com\/prometheism-transhumanism-posthumanism\/wp-json\/wp\/v2\/tags?post=203952"}],"curies":[{"name":"wp","href":"https:\/\/api.w.org\/{rel}","templated":true}]}}