{"id":4479,"date":"2024-11-21T10:42:54","date_gmt":"2024-11-21T10:42:54","guid":{"rendered":"https:\/\/zobio.com\/?p=4479"},"modified":"2024-11-21T11:40:55","modified_gmt":"2024-11-21T11:40:55","slug":"molecular-glues-discovery","status":"publish","type":"post","link":"https:\/\/zobio.com\/online\/blog\/molecular-glues-discovery\/","title":{"rendered":"Molecular Glues Discovery"},"content":{"rendered":"<div id=\"pl-4479\"  class=\"panel-layout\" ><div id=\"pg-4479-0\"  class=\"panel-grid panel-has-style\" ><div class=\"panel-row-style panel-row-style-for-4479-0\" ><div id=\"pgc-4479-0-0\"  class=\"panel-grid-cell\" ><div id=\"panel-4479-0-0-0\" class=\"so-panel widget widget_sow-editor panel-first-child panel-last-child\" data-index=\"0\" ><div class=\"with-icon panel-widget-style panel-widget-style-for-4479-0-0-0\" ><div\n\t\t\t\n\t\t\tclass=\"so-widget-sow-editor so-widget-sow-editor-base\"\n\t\t\t\n\t\t><h2 class=\"widget-title\">Molecular Glues Discovery<\/h2>\n<div class=\"siteorigin-widget-tinymce textwidget\">\n\t<p><i><span data-contrast=\"auto\">\u201cDid you know that many well-known molecular glues are actually fragments?\u201d<\/span><\/i><span data-ccp-props=\"{&quot;335551550&quot;:6,&quot;335551620&quot;:6}\">\u00a0<\/span><\/p>\n<p><span data-contrast=\"auto\">Molecular glues have emerged as an exciting new class of agents in drug discovery, offering a novel mechanism to modulate protein function, both as protein degraders and for other therapeutic targets [<a href=\"https:\/\/doi.org\/10.1016\/j.cell.2020.12.020\" target=\"_blank\" rel=\"noopener\">1<\/a><\/span><span data-contrast=\"auto\">]<\/span><span data-contrast=\"auto\">. Unlike traditional drugs that inhibit or block protein activity, molecular glues enhance or induce new protein-protein interactions (PPIs), allowing them to activate biological pathways rather than suppressing them. For instance, the natural compound Rapamycin has been used as an immunosuppressant for decades. It binds at the interface of mTOR and FKBP12 and increases the interaction between these two proteins [<\/span><span data-contrast=\"auto\"><a href=\"https:\/\/doi.org\/10.1126\/science.273.5272.239\" target=\"_blank\" rel=\"noopener\">2<\/a>]<\/span><span data-contrast=\"auto\">. Similarly, Paclitaxel (Taxol\u00ae) acts as an allosteric molecular glue, enhancing the binding between alpha and beta tubulin, and is widely used in breast cancer treatment [<\/span><span data-contrast=\"auto\"><a href=\"https:\/\/doi.org\/10.1006\/jmbi.2001.5077\" target=\"_blank\" rel=\"noopener\">3<\/a>]<\/span><span data-contrast=\"auto\">.\u00a0<\/span><span data-ccp-props=\"{&quot;335551550&quot;:6,&quot;335551620&quot;:6}\">\u00a0<\/span><\/p>\n<p><span data-contrast=\"auto\">Despite their potential, discovering new synthetic molecular glues has proven remarkably challenging. This is intriguing because some of the most impactful molecular glues are really small molecules. Thalidomide and Lenalidomide, which both target CRBN (cereblon) [<\/span><span data-contrast=\"auto\"><a href=\"https:\/\/doi.org\/10.1126\/science.1244851\" target=\"_blank\" rel=\"noopener\">4<\/a>]<\/span><span data-contrast=\"auto\">, are under 300 Da in molecular weight (<strong>Figure 1<\/strong>). Likewise, the plant hormone Auxin, a TIR1 glue degrader, is another example of a fragment-sized molecule with profound biological effects [<\/span><span data-contrast=\"auto\"><a href=\"https:\/\/doi.org\/10.1038\/nature05731\" target=\"_blank\" rel=\"noopener\">5<\/a>]<\/span><span data-contrast=\"auto\">. These examples underscore that molecular glues do not need to be large, complex natural products; they can be relatively simple, small molecules used in fragment-based drug design (FBDD) \u2013 provided we have the right methodologies tailored for finding them.<\/span><span data-ccp-props=\"{&quot;335551550&quot;:6,&quot;335551620&quot;:6}\">\u00a0<\/span><\/p>\n<p style=\"text-align: center;\"><span data-ccp-props=\"{&quot;335551550&quot;:6,&quot;335551620&quot;:6,&quot;335559739&quot;:0}\"> <img decoding=\"async\" class=\"alignnone wp-image-4489\" src=\"https:\/\/zobio.com\/online\/online\/wp-content\/uploads\/2024\/11\/Glues-2-300x157.png\" alt=\"\" width=\"864\" height=\"452\" srcset=\"https:\/\/zobio.com\/online\/wp-content\/uploads\/2024\/11\/Glues-2-300x157.png 300w, https:\/\/zobio.com\/online\/wp-content\/uploads\/2024\/11\/Glues-2-1024x535.png 1024w, https:\/\/zobio.com\/online\/wp-content\/uploads\/2024\/11\/Glues-2-768x401.png 768w, https:\/\/zobio.com\/online\/wp-content\/uploads\/2024\/11\/Glues-2.png 1200w\" sizes=\"(max-width: 864px) 100vw, 864px\" \/><\/span><\/p>\n<p><b><span data-contrast=\"auto\"><em>Figure 1: <\/em><\/span><\/b><em>Examples of well-known molecular glues.<\/em><em> Natural products like Rapamycin and Paclitaxel are widely recognized as molecular glue. However, many small molecules less than 300 Da have profound biological effects, highlighting the diversity of molecular glues and the potential for small molecules as cooperative binders. (PDB: 1FAP[<a href=\"https:\/\/doi.org\/10.1126\/science.273.5272.239\" target=\"_blank\" rel=\"noopener\">2<\/a>], 1JFF[<a href=\"https:\/\/doi.org\/10.1006\/jmbi.2001.5077\" target=\"_blank\" rel=\"noopener\">3<\/a>], 5FQD[<a href=\"https:\/\/doi.org\/10.1038\/nature16979\" target=\"_blank\" rel=\"noopener\">6<\/a>], 2P1Q[<a href=\"https:\/\/doi.org\/10.1038\/nature05731\" target=\"_blank\" rel=\"noopener\">5<\/a>])<\/em><\/p>\n<p><span data-contrast=\"auto\">The main challenge in discovering new molecular glues is that the dynamics go beyond a simple 1:1 binding model. Unlike 1:1 binding events, molecular glues facilitate three-body interactions, where two proteins and the glue form a complex and all components can interact with each other. In this context cooperativity or enhancement of the binding affinity plays a crucial role [<\/span><span data-contrast=\"auto\"><a href=\"https:\/\/doi.org\/10.1021\/ja311795d\" target=\"_blank\" rel=\"noopener\">7<\/a>]<\/span><span data-contrast=\"auto\">. The main idea in our approach is to prioritize cooperativity first in the search for new glues and then focus on raw binding affinity. Potent molecular glues exhibit high cooperativity, basically the amount of gluing potential, requiring some intrinsic affinity for at least one of the targets to observe this cooperativity [<\/span><span data-contrast=\"auto\"><a href=\"https:\/\/doi.org\/10.1039\/C8SC05242E\" target=\"_blank\" rel=\"noopener\">8<\/a>]<\/span><span data-contrast=\"auto\">. This functions as a \u201cdouble filter,\u201d where hits need both high cooperativity and sufficient initial affinity. Promising glue-like molecules may be overlooked due to a lack of sensitivity. Since there are decades of experience in medicinal chemistry in optimizing binding affinity, it makes sense to screen for cooperativity and select for that first, and start with hits that have high cooperativity.\u00a0<\/span><span data-ccp-props=\"{&quot;335551550&quot;:6,&quot;335551620&quot;:6}\">\u00a0<\/span><\/p>\n<p style=\"text-align: center;\"><img decoding=\"async\" class=\"alignnone wp-image-4487\" src=\"https:\/\/zobio.com\/online\/online\/wp-content\/uploads\/2024\/11\/Glues-1-1-300x157.png\" alt=\"\" width=\"713\" height=\"373\" srcset=\"https:\/\/zobio.com\/online\/wp-content\/uploads\/2024\/11\/Glues-1-1-300x157.png 300w, https:\/\/zobio.com\/online\/wp-content\/uploads\/2024\/11\/Glues-1-1-1024x535.png 1024w, https:\/\/zobio.com\/online\/wp-content\/uploads\/2024\/11\/Glues-1-1-768x401.png 768w, https:\/\/zobio.com\/online\/wp-content\/uploads\/2024\/11\/Glues-1-1.png 1200w\" sizes=\"(max-width: 713px) 100vw, 713px\" \/><\/p>\n<p><b><span data-contrast=\"auto\"><em>Figure 2: <\/em><\/span><\/b><em>Cascade of biophysical techniques optimized for molecular glue discovery. <\/em><em>New Molecular glues can actually be found using the same biophysical methods as traditional hits. It only requires a slight adjustment in assay setup and data interpretation. By focusing on cooperativity first, a robust pipeline is formed combining SPR, NMR and X-ray crystallography. The combination of immobilized and in solution techniques, provide a robust workflow in profiling new molecular glues.\u00a0\u00a0<\/em><\/p>\n<p><span data-contrast=\"auto\">At ZoBio, we employ a cascade of biophysical techniques (<strong>Figure 2<\/strong>), such as <strong>S<\/strong>urface <strong>P<\/strong>lasmon <strong>R<\/strong>esonance (SPR) and <strong>NMR<\/strong>, in a format we call <a href=\"https:\/\/www.eurekaselect.com\/article\/30417\" target=\"_blank\" rel=\"noopener\">TINS,<\/a><\/span><span data-contrast=\"auto\">\u00a0to identify new molecular glues. These assays, that are widely used, are highly sensitive and have been optimized to specifically detect cooperative binding. Our process typically begins with a special SPR assay designed for screening cooperativity, followed by assessment of affinity and ligand-observed NMR for confirmation in solution. 2D-titrations (cooperativity assays) are performed for further, more detailed profiling and ultimately structural biology information is obtained via a combination of X-ray crystallography, NMR, or cryo-<strong>EM<\/strong> for binary and ternary structures leading then to structure-based drug design. With some small alterations, finding new molecular glues is not so different from finding traditional leads.\u00a0 <\/span><span data-ccp-props=\"{&quot;335551550&quot;:6,&quot;335551620&quot;:6}\">\u00a0<\/span><\/p>\n<\/div>\n<\/div><\/div><\/div><\/div><\/div><\/div><\/div>","protected":false},"excerpt":{"rendered":"<p>Molecular glues have emerged as an exciting new class of agents in drug discovery, offering a novel mechanism to modulate protein function, both as protein degraders and for other therapeutic targets. Unlike traditional drugs that inhibit or block protein activity, molecular glues enhance or induce new protein-protein interactions (PPIs), allowing them to activate biological pathways rather than suppressing them. For instance, the natural compound Rapamycin has been used as an immunosuppressant for decades. It binds at the interface of mTOR and FKBP12 and increases the interaction between these two proteins&#8230;  <\/p>\n","protected":false},"author":3,"featured_media":0,"comment_status":"closed","ping_status":"closed","sticky":false,"template":"","format":"standard","meta":{"gpsa_enabled":false,"gpsa_required_form_ids":[],"gpsa_require_unique_form_submission":false,"gpsa_access_behavior":"show_message","gpsa_form_redirect_path":"","gpsa_requires_access_message":"","gpsa_access":[],"gpsa_content_loading_message":"","footnotes":""},"categories":[13],"tags":[8],"class_list":["post-4479","post","type-post","status-publish","format-standard","hentry","category-blog","tag-zobio"],"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v27.1.1 - https:\/\/yoast.com\/product\/yoast-seo-wordpress\/ -->\n<title>Molecular Glues Discovery - ZoBio - Drug Discovery Technology<\/title>\n<meta name=\"description\" content=\"It is well known, and accepted, that it is essential to have \u201chigh quality\u201d protein at the outset of a target based, small molecule drug discovery campaign. 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