{"id":2191,"date":"2018-06-20T09:29:24","date_gmt":"2018-06-20T13:29:24","guid":{"rendered":"http:\/\/ufluidix.com\/circlesecond\/?p=2191"},"modified":"2019-10-09T14:49:13","modified_gmt":"2019-10-09T18:49:13","slug":"microfluidics-and-the-drug-discovery-pipeline","status":"publish","type":"post","link":"https:\/\/www.ufluidix.com\/circle\/microfluidics-and-the-drug-discovery-pipeline\/","title":{"rendered":"Microfluidics and the Drug Discovery Pipeline"},"content":{"rendered":"<p>From antibiotics to antihistamines, every reader has at some point benefited from the range and power of modern medicines. But the cost of drug development is a bitter pill to swallow. Did you know, on average, it takes around 12 years and over \u00a31bn to develop each new medicine<span style=\"vertical-align: super; font-size: 8pt;\"><sup><a id=\"ref1\" href=\"#fn1\">1<\/a><\/sup><\/span>?<\/p>\n<div id=\"attachment_2196\" style=\"width: 673px\" class=\"wp-caption aligncenter\"><a href=\"https:\/\/ufluidix.com\/circle\/wp-content\/uploads\/2018\/06\/Representation-of-the-drug-discovery-development-pipeline-Credit-Isobel-Steer.png\"><img loading=\"lazy\" decoding=\"async\" aria-describedby=\"caption-attachment-2196\" class=\"wp-image-2196 size-full\" src=\"https:\/\/ufluidix.com\/circle\/wp-content\/uploads\/2018\/06\/Representation-of-the-drug-discovery-development-pipeline-Credit-Isobel-Steer.png\" alt=\"Representation of the drug discovery &amp; development pipeline.Credit: Isobel Steer\" width=\"663\" height=\"391\" srcset=\"https:\/\/www.ufluidix.com\/circle\/wp-content\/uploads\/2018\/06\/Representation-of-the-drug-discovery-development-pipeline-Credit-Isobel-Steer.png 663w, https:\/\/www.ufluidix.com\/circle\/wp-content\/uploads\/2018\/06\/Representation-of-the-drug-discovery-development-pipeline-Credit-Isobel-Steer-300x177.png 300w, https:\/\/www.ufluidix.com\/circle\/wp-content\/uploads\/2018\/06\/Representation-of-the-drug-discovery-development-pipeline-Credit-Isobel-Steer-600x354.png 600w\" sizes=\"(max-width: 663px) 100vw, 663px\" \/><\/a><p id=\"caption-attachment-2196\" class=\"wp-caption-text\">Representation of the drug discovery &amp; development pipeline. Credit: Isobel Steer<\/p><\/div>\n<p>There are two ways a potential medicine can fall out of the drug development pipeline. It can simply fail to work in a human body (inefficiency), or it can cause unacceptable side effects (toxicity). Scientists want to find out which medicines are inefficient or toxic early on in the pipeline. This may be in a petri dish full of cells, or simply a vial of liquid, where the potential medicine (also called a \u2018lead\u2019) is mixed with its biological \u2018target\u2019.This test-tube stage is called in vitro (testing in live animals is called in vivo). In vitro is the first step where microfluidics comes in.<\/p>\n<h3>What is a microfluidic chip?<\/h3>\n<p><a href=\"https:\/\/ufluidix.com\/resources\/definitions\/\">Microfluidic chips<\/a> (\u2018microchips\u2019) are tiny platforms containing channel systems, designed to handle volumes of liquid smaller than a microlitre. Depending on the design, they can filter, concentrate, mix, heat, separate, and detect. There are many ways to make a microchip, but typically it requires laboratory-grade facilities and equipment. In universities, many microchips are made out of the polymer PDMS, but this is quite difficult to mass-produce. One alternative is paper microchips, as pioneered by the celebrated chemist <a href=\"http:\/\/gmwgroup.harvard.edu\/\">George Whitesides<\/a>. Another, yet to be fully explored, is 3D printed microchips.<\/p>\n<h3>Microchip advantages<\/h3>\n<p>Initially, microchips were designed in order to increase efficiency and reduce waste by using smaller reaction volumes. Furthermore, their low cost and ease of automation make them attractive commercially. However, it was quickly realized that miniaturization can expand the capability of existing bioassays, as well as chemical synthesis technology. Scaling down the size will dramatically alter the surface to volume ratio, and molecular diffusion. The result? You can do more reactions, faster. This high-throughput technology is one of the holy grails for medicine discovery.<\/p>\n<h3>Microchips for medicine synthesis<\/h3>\n<p>The number of potentially medicinal molecules is estimated to be of the order of 10<sup>63<\/sup>\u2013 a.k.a. one vigintillion<span style=\"vertical-align: super; font-size: 8pt;\"><sup><a id=\"ref2\" href=\"#fn2\">2<\/a><\/sup><\/span>. Synthesizing and screening candidate molecules using macroscale methods is time-consuming and expensive. Microfluidics can offer significant improvements. One example is where researchers used a micro-reactor to synthesize a dipeptide with high yield in 20 minutes, a huge improvement on the previous 24hr, 50% yield macro-reactor<span style=\"vertical-align: super; font-size: 8pt;\"><sup><a id=\"ref3\" href=\"#fn3\">3<\/a><\/sup><\/span>.<\/p>\n<h3>Microchips for screening medicines in vitro<\/h3>\n<p>Not only can microchips be used to synthesize potential medicine molecules; but also to test how these chemical molecules bind to biological targets. For example, a high-throughput microfluidic platform was developed to test the binding of transcription factors to DNA, successfully predicting in vivo functionality<span style=\"vertical-align: super; font-size: 8pt;\"><sup><a id=\"ref4\" href=\"#fn4\">4<\/a><\/sup><\/span>. In another interesting example, herbal medicines (a multi-billion dollar market) were tested as antidepressants on electrode microchips<span style=\"vertical-align: super; font-size: 8pt;\"><sup><a id=\"ref5\" href=\"#fn5\">5<\/a><\/sup><\/span>.<\/p>\n<p>An innovative combination of both synthesis and screening was developed earlier this year, which synthesized metal complexes and then tested how they bound to folded DNA structures called telomeres<span style=\"vertical-align: super; font-size: 8pt;\"><sup><a id=\"ref6\" href=\"#fn6\">6<\/a><\/sup><\/span>. The entire process was carried out on a single microfluidic platform.<\/p>\n<h3>Microchips for testing medicines on cells<\/h3>\n<p>Testing compounds on live cells is a key step in the drug discovery pipeline, but this requires physiological conditions that are as close to the living body as possible. With microfluidics, you can manipulate cells or volumes of cellular size; and you can look at huge numbers simultaneously. For example, PDMS microchips have been used to study antibiotics passing through bacterial membranes<span style=\"vertical-align: super; font-size: 8pt;\"><sup><a id=\"ref7\" href=\"#fn7\">7<\/a><\/sup><\/span>.<\/p>\n<p>A microchip has also been developed to administer repeat, tiny doses of bradykinin(an inflammatory mediator) to neuronal cells<span style=\"vertical-align: super; font-size: 8pt;\"><sup><a id=\"ref8\" href=\"#fn8\">8<\/a><\/sup><\/span>. This mimics a biological synapse \u2013 on a chip. Indeed, a growing number of studies are using microfluidic platforms to monitor the long-term effects of drugs on cells, effectively building artificial blood vessels, nerves, and muscles. In the future, such devices have the potential to replace animal testing<span style=\"vertical-align: super; font-size: 8pt;\"><sup><a id=\"ref9\" href=\"#fn9\">9<\/a><\/sup><\/span>. Such work blurs the lines between the scientific terms \u2018in vitro\u2019, and \u2018in vivo\u2019.<\/p>\n<h3>The future<\/h3>\n<p>In the early stages of the drug delivery pipeline, such as chemical synthesis, screening of molecules, and preclinical testing of drugs in living cells, microfluidic platforms clearly offer a not-so-small improvement on existing technologies. However, ask any microfluidics researcher (myself included!) and they will tell you that various limitations must first be overcome. These include standardizing materials and geometry of the microfluidic channels, as well as studying long-term microchip performance. Mass-production of microchips also needs to take off in order to help the next generation of industrial medical researchers in their mission to shorten and streamline the drug development pipeline.<\/p>\n<hr \/>\n<p><sup id=\"fn1\">1. <a href=\"http:\/\/www.abpi.org.uk\/what-we-do\/research-medical-and-innovation\/our-work-to-deliver-the-medicines-of-tomorrow\">http:\/\/www.abpi.org.uk\/what-we-do\/research-medical-and-innovation\/our-work-to-deliver-the-medicines-of-tomorrow<\/a><br \/>\n<\/sup><br \/>\n<sup id=\"fn2\">2. Bohacek RS, McMartin C, Guida WC. The art and practice of structure\u2010based drug design: A molecular modeling perspective. Medicinal research reviews. 1996 Jan 1;16(1):3-50.<br \/>\n<\/sup><br \/>\n<sup id=\"fn3\">3. Watts P, Wiles C, Haswell SJ, Pombo-Villar E, Styring P. The synthesis of peptides using micro reactors. InMicroreaction Technology 2001 (pp. 508-517). Springer, Berlin, Heidelberg.<br \/>\n<\/sup><br \/>\n<sup id=\"fn4\">4. Maerkl SJ, Quake SR. A systems approach to measuring the binding energy landscapes of transcription factors. Science. 2007 Jan 12;315(5809):233-7.<br \/>\n<\/sup><br \/>\n<sup id=\"fn5\">5. Gramowski A, J\u00fcgelt K, St\u00fcwe S, Schulze R, McGregor GP, Wartenberg\u2010Demand A, Loock J, Schr\u00f6der O, Weiss DG. Functional screening of traditional antidepressants with primary cortical neuronal networks grown on multielectrodeneurochips. European Journal of Neuroscience. 2006 Jul 1;24(2):455-65.<br \/>\n<\/sup><br \/>\n<sup id=\"fn6\">6. Rakers V, Cadinu P, Edel JB, Vilar R. Development of microfluidic platforms for the synthesis of metal complexes and evaluation of their DNA affinity using online FRET melting assays. Chemical Science. 2018;9(14):3459-69.<br \/>\n<\/sup><br \/>\n<sup id=\"fn7\">7. Cama J, Bajaj H, Pagliara S, Maier T, Braun Y, Winterhalter M, Keyser UF. Quantification of fluoroquinolone uptake through the outer membrane channel OmpF of Escherichia coli. Journal of the American Chemical Society. 2015 Oct 27;137(43):13836-43.<br \/>\n<\/sup><br \/>\n<sup id=\"fn8\">8. Peterman MC, Noolandi J, Blumenkranz MS, Fishman HA. Localized chemical release from an artificial synapse chip. Proceedings of the National Academy of Sciences of the United States of America.<br \/>\n2004 Jul 6;101(27):9951-4.<br \/>\n<\/sup><br \/>\n<sup id=\"fn9\">9. Sin A, Chin KC, Jamil MF, Kostov Y, Rao G, Shuler ML. The design and fabrication of three\u2010chamber microscale cell culture analog devices with integrated dissolved oxygen sensors. Biotechnology progress. 2004 Jan 1;20(1):338-45.<br \/>\n<\/sup><\/p>\n<p><em><strong>Enjoyed this article? Don\u2019t forget to share.<\/strong><\/em><\/p>\n<div class=\"sharing-default-minimal\"><div class=\"nectar-social default\" data-position=\"left\" data-color-override=\"only_when_needed\"><div class=\"nectar-social-inner\"><a href=\"#\" class=\"nectar-love\" id=\"nectar-love-2191\" title=\"Love this\"> <i class=\"icon-salient-heart-2\"><\/i><span class=\"love-text\">Love<\/span><span class=\"total_loves\"><span class=\"nectar-love-count\">0<\/span><\/span><\/a><a class='facebook-share nectar-sharing' href='#' title='Share this'>  <i class='fa fa-facebook'><\/i> <span class='social-text'>Share<\/span> <\/a><a class='twitter-share nectar-sharing' href='#' title='Tweet this'> <i class='fa fa-twitter'><\/i> <span class='social-text'>Tweet<\/span> <\/a><a class='linkedin-share nectar-sharing' href='#' title='Share this'> <i class='fa fa-linkedin'><\/i> <span class='social-text'>Share<\/span> <\/a><\/div><\/div><\/div>\n<p>&nbsp;<\/p>\n<style>#rt-team-container-255102461 .single-team-area .overlay a.detail-popup, \n\t\t\t\t\t\t#rt-team-container-255102461 .contact-info ul li i{color:#0367bf;}#rt-team-container-255102461 .single-team-area .skill-prog .fill,.tlp-team #rt-team-container-255102461 .tlp-content, \n\t\t\t\t\t\t.tlp-tooltip + .tooltip > .tooltip-inner,\n\t\t\t\t\t\t#rt-team-container-255102461 .layout1 .tlp-content,\n\t\t\t\t\t\t#rt-team-container-255102461 .layout11 .single-team-area .tlp-title,\n\t\t\t\t\t\t#rt-team-container-255102461 .carousel7 .single-team-area .team-name,\n\t\t\t\t\t\t#rt-team-container-255102461 .layout14 .rt-grid-item .tlp-overlay, \n\t\t\t\t\t\t#rt-team-container-255102461 .carousel8 .rt-grid-item .tlp-overlay,\n\t\t\t\t\t\t#rt-team-container-255102461 .isotope6 .single-team-area h3 .team-name,\n\t\t\t\t\t\t#rt-team-container-255102461 .carousel8 .rt-grid-item .tlp-overlay .social-icons:before,\n\t\t\t\t\t\t#rt-team-container-255102461 .layout14 .rt-grid-item .tlp-overlay .social-icons:before,\n\t\t\t\t\t\t#rt-team-container-255102461 .skill-prog .fill,\n\t\t\t\t\t\t#rt-team-container-255102461 .special-selected-top-wrap .ttp-label,\n\t\t\t\t\t\t.tlp-team .layout6 .tlp-info-block{background:#0367bf;}.tooltip.top .tooltip-arrow{border-top-color:#0367bf;}#rt-team-container-255102461 layout6 .tlp-right-arrow:after{border-color: transparent#0367bf;}#rt-team-container-255102461 layout6 .tlp-left-arrow:after{border-color:#0367bf transparent transparent;}.md-content, .md-content > .tlp-md-content-holder .tlp-md-content,\n\t\t\t\t\t\t#rt-team-container-255102461 .layout12 .single-team-area h3 .team-name,\n\t\t\t\t\t\t#rt-team-container-255102461 .isotope6 .single-team-area h3 .team-name,\n\t\t\t\t\t\t.rt-team-container .layout12 .single-team-area h3 .team-name,\n\t\t\t\t\t\t.rt-team-container .isotope6 .single-team-area h3 .team-name {background:#0367bf;}#rt-team-container-255102461 .special-selected-top-wrap .img:after{background:rgba(3,103,191,0.2)}#rt-team-container-255102461 h3,\n\t\t\t\t\t\t\t#rt-team-container-255102461 h3 a,\n\t\t\t\t\t\t\t#rt-team-container-255102461 .overlay h3 a,\n\t\t\t\t\t\t\t#rt-team-container-255102461 .single-team-area .tlp-content h3 a{ color:#333333;font-size:25px;font-weight:bold; }#rt-team-container-255102461 h3:hover,\n\t\t\t\t\t\t\t#rt-team-container-255102461 h3 a:hover,\n\t\t\t\t\t\t\t#rt-team-container-255102461 .overlay h3 a:hover,\n\t\t\t\t\t\t\t#rt-team-container-255102461 .single-team-area .tlp-content h3 a:hover{ color: #333333; }#rt-team-container-255102461 .short-bio p,#rt-team-container-255102461 .short-bio p a,\n\t\t\t\t\t\t#rt-team-container-255102461 .overlay .short-bio p, #rt-team-container-255102461 .overlay .short-bio p a{font-weight:normal;}#rt-team-container-255102461 .overlay .social-icons a,\n\t\t\t\t\t\t#rt-team-container-255102461 .tlp-social,\n\t\t\t\t\t\t#rt-team-container-255102461 .social-icons a{ color:#1e73be; }<\/style><div class='rt-container-fluid rt-team-container ' id='rt-team-container-255102461'  data-layout='layout3' data-desktop-col='1'  data-tab-col='1'  data-mobile-col='1' data-sc-id='2190''><div data-title='Loading ...' class='rt-row rt-content-loader layout3 ttp-even ttp-pre-loader'><div class='rt-col-md-12 rt-col-sm-12 rt-col-xs-12 even-grid-item rt-grid-item round-img' data-id='2181'><div class=\"single-team-area\"><figure><img class='img-responsive rt-profile-img' src='https:\/\/www.ufluidix.com\/circle\/wp-content\/uploads\/2018\/06\/Isobel-Steer_authorphoto-150x150.png' alt='Isobel Steer'\/><\/figure><div class='tlp-content2'><h3><span class=\"team-name\">Isobel Steer<\/span><\/h3><div class=\"short-bio\"><p>Isobel Steer is a Ph.D. researcher in the Bioengineering and Chemistry Departments of Imperial College London, working to develop optical microfluidic devices. She also writes for BioNews and tweets as <a href=\"https:\/\/twitter.com\/isosteer\">@isosteer<\/a>. \r\n<\/p><\/div><\/div><div class=\"social-icons\"><a href='https:\/\/www.linkedin.com\/in\/isobel-steer-28403388\/' title='linkedin' target='_blank'><i class='fa fa-linkedin'><\/i><\/a><a href='https:\/\/twitter.com\/isosteer' title='twitter' target='_blank'><i class='fa fa-twitter'><\/i><\/a><\/div><\/div><\/div><div class=\"rt-loading-overlay\"><\/div><div class=\"rt-loading rt-ball-clip-rotate\"><div><\/div><\/div><\/div><\/div>\n","protected":false},"excerpt":{"rendered":"<p>Isobel Steer is a Ph.D. researcher in the Bioengineering and Chemistry Departments of Imperial College London, working to develop optical microfluidic devices. She also writes for BioNews and tweets as&#8230;<\/p>\n","protected":false},"author":1,"featured_media":2192,"comment_status":"closed","ping_status":"open","sticky":false,"template":"","format":"standard","meta":{"footnotes":""},"categories":[107],"tags":[106,77],"class_list":{"0":"post-2191","1":"post","2":"type-post","3":"status-publish","4":"format-standard","5":"has-post-thumbnail","7":"category-isobel-steer","8":"tag-drug-discovery","9":"tag-microfluidics"},"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v23.4 - https:\/\/yoast.com\/wordpress\/plugins\/seo\/ -->\n<title>Microfluidics and the Drug Discovery Pipeline - The MicroFluidic Circle<\/title>\n<meta name=\"description\" content=\"From antibiotics to antihistamines, every reader has at some point benefited from the range and power of modern medicines.\" \/>\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.ufluidix.com\/circle\/microfluidics-and-the-drug-discovery-pipeline\/\" \/>\n<meta property=\"og:locale\" content=\"en_US\" \/>\n<meta property=\"og:type\" content=\"article\" \/>\n<meta property=\"og:title\" content=\"Microfluidics and the Drug Discovery Pipeline\" \/>\n<meta property=\"og:description\" content=\"From antibiotics to antihistamines, every reader has at some point benefited from the range and power of modern medicines. But the cost of drug development is a bitter pill to swallow. Did you know, on average, it takes around 12 years and over \u00a31 bn to develop each new medicine1?\" \/>\n<meta property=\"og:url\" content=\"https:\/\/www.ufluidix.com\/circle\/microfluidics-and-the-drug-discovery-pipeline\/\" \/>\n<meta property=\"og:site_name\" content=\"The MicroFluidic Circle\" \/>\n<meta property=\"article:published_time\" content=\"2018-06-20T13:29:24+00:00\" \/>\n<meta property=\"article:modified_time\" content=\"2019-10-09T18:49:13+00:00\" \/>\n<meta property=\"og:image\" content=\"https:\/\/www.ufluidix.com\/circle\/wp-content\/uploads\/2019\/07\/microfluidic-circle.png\" \/>\n\t<meta property=\"og:image:width\" content=\"1920\" \/>\n\t<meta property=\"og:image:height\" content=\"1000\" \/>\n\t<meta property=\"og:image:type\" content=\"image\/png\" \/>\n<meta name=\"author\" content=\"admin\" \/>\n<meta name=\"twitter:card\" content=\"summary_large_image\" \/>\n<meta name=\"twitter:label1\" content=\"Written by\" \/>\n\t<meta name=\"twitter:data1\" content=\"admin\" \/>\n\t<meta name=\"twitter:label2\" content=\"Est. reading time\" \/>\n\t<meta name=\"twitter:data2\" content=\"5 minutes\" \/>\n<script type=\"application\/ld+json\" class=\"yoast-schema-graph\">{\"@context\":\"https:\/\/schema.org\",\"@graph\":[{\"@type\":\"Article\",\"@id\":\"https:\/\/www.ufluidix.com\/circle\/microfluidics-and-the-drug-discovery-pipeline\/#article\",\"isPartOf\":{\"@id\":\"https:\/\/www.ufluidix.com\/circle\/microfluidics-and-the-drug-discovery-pipeline\/\"},\"author\":{\"name\":\"admin\",\"@id\":\"https:\/\/www.ufluidix.com\/circle\/#\/schema\/person\/c9f8fca6595d5bc96ae9fd78b89752b2\"},\"headline\":\"Microfluidics and the Drug Discovery Pipeline\",\"datePublished\":\"2018-06-20T13:29:24+00:00\",\"dateModified\":\"2019-10-09T18:49:13+00:00\",\"mainEntityOfPage\":{\"@id\":\"https:\/\/www.ufluidix.com\/circle\/microfluidics-and-the-drug-discovery-pipeline\/\"},\"wordCount\":1055,\"publisher\":{\"@id\":\"https:\/\/www.ufluidix.com\/circle\/#organization\"},\"image\":{\"@id\":\"https:\/\/www.ufluidix.com\/circle\/microfluidics-and-the-drug-discovery-pipeline\/#primaryimage\"},\"thumbnailUrl\":\"https:\/\/www.ufluidix.com\/circle\/wp-content\/uploads\/2018\/06\/top_image_660_220.png\",\"keywords\":[\"drug discovery\",\"microfluidics\"],\"articleSection\":[\"Isobel Steer\"],\"inLanguage\":\"en-US\"},{\"@type\":\"WebPage\",\"@id\":\"https:\/\/www.ufluidix.com\/circle\/microfluidics-and-the-drug-discovery-pipeline\/\",\"url\":\"https:\/\/www.ufluidix.com\/circle\/microfluidics-and-the-drug-discovery-pipeline\/\",\"name\":\"Microfluidics and the Drug Discovery Pipeline - 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