{"id":3121,"date":"2026-07-15T18:58:05","date_gmt":"2026-07-15T18:58:05","guid":{"rendered":"https:\/\/drsoniafawad.com\/?p=3121"},"modified":"2026-07-15T18:58:05","modified_gmt":"2026-07-15T18:58:05","slug":"blood-test-detects-often-missed-pancreatic-cancer-signals","status":"publish","type":"post","link":"https:\/\/drsoniafawad.com\/?p=3121","title":{"rendered":"Blood test detects often-missed pancreatic cancer signals"},"content":{"rendered":"<p><br \/>\n<\/p>\n<div data-component=\"ArticleContent\">\n<div class=\"article__below-title\">\n<div class=\"mobile-trust-box\">\n<div class=\"row\">\n<div class=\"col-12 col-md-5 d-xl-none\">\n<div class=\"trust-box\">\n<div class=\"trust-box-logo d-none d-md-block\">\n<img decoding=\"async\" src=\"https:\/\/www.healio.com\/~\/media\/h5\/feature\/news\/publogos\/hot.svg?la=en&amp;h=24&amp;w=141&amp;hash=2F86D471C8514C0E334E329AA799E8B4\" class=\"logo-img\" height=\"24\" alt=\"hemonc today logo\" width=\"141\"\/>\n<\/div>\n<\/div>\n<\/div>\n<div class=\"col-12 col-md-6 offset-md-1 offset-xl-0 col-xl-12\">\n<div class=\"email-alert-button-wrapper d-none\" data-component=\"EmailTopicAlert\" data-module=\"Subspecialty Email Topic Alerts Top\" data-manage-email-link=\"\/footer\/account-information\/my-account\/email-subscriptions-and-alerts#emailAlerts\">\n<hidden data-setting-item=\"d265901d-6d37-49c7-a8f6-c7bf19a02509\"\/><br \/>\n<hidden data-crm-source=\"Subspecialty Topic Alert\"\/><\/p>\n<div class=\"email-alert-button d-none\" data-topic-button=\"not-subscribed\">\n<p>\n<span data-module-track-action=\"Email Alerts TOP_Click_Healio News Article\" data-module-track-label=\"Email Alerts TOP_Healio News Article\"><br \/>\n<i class=\"fas fa-plus-circle\"\/><br \/>\nAdd topic to email alerts<br \/>\n<\/span>\n<\/p>\n<div class=\"email-alert-inner collapse ub02444111acf40afa312b65ee7e0e89b\">\n<div class=\"email-alert-dialogue\">\n<p>\nReceive an email when new articles are posted on <span data-content=\"topic-title\"\/>\n<\/p>\n<div class=\"d-none\" data-sign-up-type=\"unknown\">\nPlease provide your email address to receive an email when new articles are posted on <span data-content=\"topic-title\"\/>.<\/p>\n<\/div>\n<\/div>\n<p><button type=\"button\" class=\"btn btn-primary\" data-loading-text=\"Loading &lt;i class=\" fa=\"\" fa-spinner=\"\" fa-spin=\"\">&#8221; data-action=subscribe&gt;<br \/>\nSubscribe<br \/>\n<\/button>\n<\/div>\n<\/div>\n<div class=\"d-none\" data-topic-modal=\"failed\"> <strong>We were unable to process your request. Please try again later. If you continue to have this issue please contact <a href=\"https:\/\/www.healio.com\/news\/hematology-oncology\/20260715\/mailto:customerservice@slackinc.com\">customerservice@slackinc.com<\/a>.<\/strong> <\/p>\n<p><button data-dismiss=\"modal\" class=\"btn btn-primary btn-lg btn-block\">Back to Healio<\/button><\/p>\n<\/div>\n<\/div>\n<\/div>\n<\/div>\n<\/div>\n<\/div>\n<h2>Key takeaways:<\/h2>\n<ul>\n<li>ddPCR analysis at diagnosis and after treatment detected <i>KRAS<\/i>-mutant circulating tumor DNA more frequently than standard testing.<\/li>\n<li>The approach could allow for intervention before recurrence is clinically visible.<\/li>\n<\/ul>\n<p>A highly sensitive blood test can detect signs of pancreatic cancer that standard methods often miss, according to results of a prospective cohort study.<\/p>\n<p>Digital droplet polymerase chain reaction (ddPCR) analysis performed upon diagnosis of localized disease detected <i>KRAS<\/i>-mutant circulating tumor DNA (ctDNA) nearly four times more often than more widely used next-generation sequencing, with results strongly predicting survival.<\/p>\n<figure class=\"figure article__og-image\">\n<picture><source srcset=\"https:\/\/www.healio.comhttps:\/\/www.healio.comhttps:\/\/www.healio.com\/~\/media\/slack-news\/hemonc\/misc\/infographics\/hot-infographics\/2026\/07_july\/hot0726sridalla_graphic_01.webp?w=476\" media=\"(max-width: 768px)\"><source srcset=\"https:\/\/www.healio.com\/~\/media\/slack-news\/hemonc\/misc\/infographics\/hot-infographics\/2026\/07_july\/hot0726sridalla_graphic_01.webp?w=800\" media=\"(max-width: 992px)\"><source srcset=\"https:\/\/www.healio.com\/~\/media\/slack-news\/hemonc\/misc\/infographics\/hot-infographics\/2026\/07_july\/hot0726sridalla_graphic_01.webp?w=595\" media=\"(max-width: 1200px)\"><source srcset=\"https:\/\/www.healio.comhttps:\/\/www.healio.comhttps:\/\/www.healio.com\/~\/media\/slack-news\/hemonc\/misc\/infographics\/hot-infographics\/2026\/07_july\/hot0726sridalla_graphic_01.webp?w=476\" media=\"(min-width: 1200px)\"><source srcset=\"https:\/\/www.healio.comhttps:\/\/www.healio.comhttps:\/\/www.healio.com\/~\/media\/slack-news\/hemonc\/misc\/infographics\/hot-infographics\/2026\/07_july\/hot0726sridalla_graphic_01.webp?w=476\"><img decoding=\"async\" src=\"https:\/\/www.healio.com\/~\/media\/slack-news\/hemonc\/misc\/infographics\/hot-infographics\/2026\/07_july\/hot0726sridalla_graphic_01.jpg?w=800\" alt=\"Detection of KRAS-mutant ctDNA after surgery IG\" class=\"figure-img img-fluid\" width=\"800\"\/><br \/>\n<\/source><\/source><\/source><\/source><\/source><\/picture><figcaption class=\"figure-caption\">\nData derived from Sridalla K, et al. <i>Clin Cancer Res<\/i>. 2026;doi:10.1158\/1078-0432.CCR-26-0609.<br \/>\n<\/figcaption><\/figure>\n<p>Administration of ddPCR after chemotherapy or surgery also detected traces of ctDNA with the key genetic mutation at considerably higher rates, suggesting it more effectively identifies patients with residual disease who are at greater risk for recurrence.<\/p>\n<div class=\"mug left\"><img decoding=\"async\" alt=\"Akhil Chawla, MD, FACS\" style=\" height:106px; width:80px\" src=\"https:\/\/www.healio.com\/~\/media\/slack-news\/hemonc\/mugs\/c\/chawla_akhil_2026_.jpg\"\/><\/p>\n<p><strong><b>Akhil Chawla<\/b><\/strong><\/p>\n<\/div>\n<p>\u201cThese findings provide important insights into what we are missing with next-generation sequencing \u2014 particularly after a patient has been treated,\u201d senior author <b>Akhil Chawla, M<\/b><b>D, FACS<\/b><b>,<\/b> clinical associate professor of surgery at Northwestern University Feinberg School of Medicine and complex surgical oncologist at Northwestern Medicine, told Healio. \u201cThe goal of getting more patients to cure requires a thoughtful analysis of each individual. It is an obvious hypothesis that, if a patient has a high risk for recurrence based off what we are seeing in their blood and we treat a patient earlier with a targeted treatment, that patient likely will do better.\u201d<\/p>\n<h2>Focusing on <i>KRAS<\/i><\/h2>\n<p>Only 13% of patients with pancreatic ductal adenocarcinoma (PDAC) live 5 years after diagnosis, according to American Cancer Society statistics.<\/p>\n<p>Individuals with localized disease undergo months of chemotherapy and surgery but still often develop recurrence.<\/p>\n<p>Liquid biopsies \u2014 blood tests that can be repeated over time \u2014 search for traces of DNA that cancer cells shed into the bloodstream, offering an early indication that cancer either is present or may return. However, in many cases, ctDNA levels are low and hard to detect.<\/p>\n<p> <i>RAS<\/i> mutations, found in more than 90% of <a rel=\"noopener noreferrer\" href=\"https:\/\/www.healio.com\/news\/hematology-oncology\/20250806\/major-milestone-study-validates-newonset-diabetes-as-early-pancreatic-cancer-marker\" id=\"rId12\" target=\"_blank\">pancreatic cancers<\/a>, have long been known to be a driver of disease development and progression.<\/p>\n<p>Commercially available assays that use <a rel=\"noopener noreferrer\" href=\"https:\/\/www.healio.com\/news\/hematology-oncology\/20260421\/glass-half-full-nextgeneration-sequencing-for-advanced-cancer-lags-but-rates-improving\" id=\"rId13\" target=\"_blank\">next-generation sequencing<\/a> or digital PCR methods for cancer detection, <a rel=\"noopener noreferrer\" href=\"https:\/\/www.healio.com\/news\/hematology-oncology\/20260626\/streamlined-biomarker-testing-processes-needed-to-ensure-patients-receive-optimal-care\" id=\"rId14\" target=\"_blank\">tumor profiling<\/a> and therapy selection provide valuable insights, but market forces have driven the technology toward broad panels. In contrast, ddPCR \u2014 which often costs less and yields results quicker \u2014 analyzes one set of genes at a time.<\/p>\n<p>Studies that Chawla\u2019s group conducted a few years ago using next-generation sequencing panels confirmed <i>KRAS<\/i> to be the most prognostic mutation in pancreatic cancer.<\/p>\n<p>In their current study, the researchers leveraged that insight to evaluate a ddPCR assay that targets the three most common mutations in the <i>KRAS<\/i> gene \u2014 G12D, G12V and G12R \u2014 with about a thousand times more sensitivity than more commonly used broader testing approaches.<\/p>\n<p>The analysis included 106 patients with localized PDAC who were undergoing neoadjuvant chemotherapy across multiple Northwestern Medicine sites as part of a larger clinical trial.<\/p>\n<p>Investigators collected blood samples at multiple time points \u2014 at diagnosis, after chemotherapy and after surgery \u2014 and performed ddPCR and next-generation sequencing on all samples to assess for <i>KRAS<\/i>-mutant ctDNA.<\/p>\n<h2>A \u2018hidden group\u2019<\/h2>\n<p>At diagnosis, ddPCR detected <i>KRAS<\/i>-mutant ctDNA in nearly four times as many patients as next-generation sequencing (64.9% vs. 17.2%).<\/p>\n<p>The ddPCR test continued to detect residual cancer more effectively after treatment, identifying <i>KRAS<\/i>-mutant DNA in 12 times as many patients after chemotherapy (60% vs. 5%) and six times more patients after surgery (56% vs. 9%).<\/p>\n<p>\u201cAll of these time points are informative but the diagnosis time point has been shown in our studies to be most prognostic, indicating how a patient will do with subsequent neoadjuvant chemotherapy and surgery,\u201d Chawla said. \u201cThis suggests if they have a <i>KRAS <\/i>mutation at high levels early in their disease course, they may already have more resistant disease or potentially be a more basal-like subtype. These are the patients who recur early and have worse survival.\u201d<\/p>\n<p>Detection of <i>KRAS<\/i>-mutant ctDNA appeared predictive for outcomes.<\/p>\n<p>Patients who tested negative on both ddPCR and next-generation sequencing survived a median 40.7 months after diagnosis. <\/p>\n<p>A previously \u201chidden group\u201d of high-risk patients \u2014 those whose cancer had been missed by standard next-generation sequencing but detected by ddPCR \u2014 survived a median 26.9 months, Chawla said.<\/p>\n<p>Those who tested positive on both tests survived a median 10.9 months (<i>P<\/i> &lt; .001 for comparison).<\/p>\n<p>The high sensitivity of ddPCR allows it to do more than show \u201cpresence or absence\u201d of ctDNA by offering valuable insights into tumor mutational burden, Chawla said.<\/p>\n<h2>A fundamental change<\/h2>\n<p>Earlier this spring, results from the randomized phase 3 RASolute 302 trial showed the oral pan-RAS inhibitor <a rel=\"noopener noreferrer\" href=\"https:\/\/www.healio.com\/news\/hematology-oncology\/20260619\/transformational-daraxonrasib-data-signal-new-era-in-pancreatic-cancer\" id=\"rId15\" target=\"_blank\">daraxonrasib (RMC-6236, Revolution Medicines)<\/a> doubled survival \u2014 from 6.7 months to 13.2 months \u2014 compared with standard chemotherapy among patients with previously treated metastatic PDAC.<\/p>\n<p>The investigational agent, which can be used under an <a rel=\"noopener noreferrer\" href=\"https:\/\/www.healio.com\/news\/hematology-oncology\/20260505\/expanded-access-to-daraxonrasib-signals-dawn-of-a-new-era-in-pancreatic-cancer-treatment\" id=\"rId16\" target=\"_blank\">FDA-authorized expanded access protocol<\/a> and is expected to receive agency approval later this year, also improved several other outcomes, including doubling time to deterioration of pain and quality of life.<\/p>\n<p>The findings, which culminate a three-decade commitment to overcome what many in the field had considered an undruggable driver mutation, may lay the foundation for additional therapies or combinations that could lead to longer or deeper responses.<\/p>\n<p>This will make the ability to use a high-sensitivity ddPCR test that tracks the same mutation even more valuable, Chawla said.<\/p>\n<p>In fact, it may \u201cfundamentally change\u201d how high-risk patients are identified and microscopic disease is monitored, he said, increasing the likelihood that clinicians can intervene before recurrence is clinically visible.<\/p>\n<p>\u201cThis remains a very challenging disease to treat, but it is an exciting time for pancreatic cancer,\u201d Chawla said. \u201cHopefully improvements in technology can be leveraged with the advances that have been made scientifically to help us further improve outcomes. Biomarker-directed therapy will be crucial to ensure we are using appropriate treatments earlier to optimize outcomes. If a patient is tolerating daraxonrasib, how long do we continue to treat them? What happens when they develop resistance? These are open-ended questions, and we need high-sensitivity biomarkers to answer them.\u201d<\/p>\n<p>The findings from the ddPCR analysis must be validated in larger, multicenter cohorts before the approach can be broadly adopted, Chawla said.<\/p>\n<p>Plasma banks available through larger multi-institutional trials could represent an opportunity to validate the early data.<\/p>\n<p>Investigators also are looking to partner with commercial entities interested in better understanding how <i>KRAS<\/i>-targeting treatments work with this biomarker, Chawla said.<\/p>\n<p>Use of the ddPCR approach so far has focused on distinguishing \u201cdetection vs. lack of detection,\u201d Chawla said. However, he noted it could potentially be used more like \u201ca continuous variable\u201d in conjunction with other biomarkers such as CA 19-9, a protein in the blood that helps clinicians monitor efficacy of pancreatic cancer treatment.<\/p>\n<p>More work also is necessary to determine if ddPCR should complement rather than replace next-generation sequencing.<\/p>\n<p>\u201cOur publication shows we are missing a lot just by doing next-generation sequencing, but next-generation sequencing does have a capability that ddPCR does not,\u201d Chawla said. \u201cThe ability to look at a large panel of genes could help us better understand whether co-occurrence of certain genes \u2014 such as <i>KRAS<\/i> and <i>TP53<\/i> \u2014 has an impact on phenotype or may harbor additional resistance.\u201d<\/p>\n<h2>For more information:<\/h2>\n<p> <b>Akhil Chawla<\/b><b>, MD, FACS,<\/b> can be reached at akhil.chawla@northwestern.edu.<\/p>\n<div class=\"article__content--footer\">\n<div class=\"publisher-logo\">\n<span>Published by:<\/span><br \/>\n<img decoding=\"async\" src=\"https:\/\/www.healio.com\/~\/media\/h5\/feature\/news\/publogos\/hot.svg?la=en&amp;h=24&amp;w=141&amp;hash=2F86D471C8514C0E334E329AA799E8B4\" class=\"logo-img\" height=\"24\" alt=\"hemonc today logo\" width=\"141\"\/>\n<\/div>\n<div class=\"healio-ai-component-inline\" data-no-ads=\"true\" data-module-track-category=\"Healio AI\" data-module-track-action=\"Click\" data-module-track-label=\"Access Healio Ai from component - News_AI Component - In-Content (all devices)\">\n<div class=\"healio-ai-content\">\n<img decoding=\"async\" src=\"https:\/\/m3.healio.com\/~\/media\/images\/healio-ai\/healio-ai_logo.svg\" alt=\"Healio AI\" class=\"healio-ai-logo\"\/><\/p>\n<p><strong>Ask a clinical question<\/strong> and tap into <strong>Healio AI&#8217;s knowledge<\/strong> base.<\/p>\n<ul>\n<li>PubMed, enrolling\/recruiting trials, guidelines<\/li>\n<li>Clinical Guidance, Healio CME, FDA news<\/li>\n<li>Healio&#8217;s exclusive daily news coverage of clinical data<\/li>\n<\/ul>\n<p><button class=\"healio-ai-button\" onclick=\"window.location.href=\" https:=\"\">Learn more<\/button>\n<\/div>\n<\/div>\n<div class=\"email-alert-button-wrapper d-none\" data-component=\"EmailTopicAlert\" data-module=\"Subspecialty Email Topic Alerts Top\" data-manage-email-link=\"\/footer\/account-information\/my-account\/email-subscriptions-and-alerts#emailAlerts\">\n<hidden data-setting-item=\"d265901d-6d37-49c7-a8f6-c7bf19a02509\"\/><br \/>\n<hidden data-crm-source=\"Subspecialty Topic Alert\"\/><\/p>\n<div class=\"email-alert-button d-none\" data-topic-button=\"not-subscribed\">\n<p>\n<span data-module-track-action=\"Email Alerts TOP_Click_Healio News Article\" data-module-track-label=\"Email Alerts TOP_Healio News Article\"><br \/>\n<i class=\"fas fa-plus-circle\"\/><br \/>\nAdd topic to email alerts<br \/>\n<\/span>\n<\/p>\n<div class=\"email-alert-inner collapse ub02444111acf40afa312b65ee7e0e89b\">\n<div class=\"email-alert-dialogue\">\n<p>\nReceive an email when new articles are posted on <span data-content=\"topic-title\"\/>\n<\/p>\n<div class=\"d-none\" data-sign-up-type=\"unknown\">\nPlease provide your email address to receive an email when new articles are posted on <span data-content=\"topic-title\"\/>.<\/p>\n<\/div>\n<\/div>\n<p><button type=\"button\" class=\"btn btn-primary\" data-loading-text=\"Loading &lt;i class=\" fa=\"\" fa-spinner=\"\" fa-spin=\"\">&#8221; data-action=subscribe&gt;<br \/>\nSubscribe<br \/>\n<\/button>\n<\/div>\n<\/div>\n<div class=\"d-none\" data-topic-modal=\"failed\"> <strong>We were unable to process your request. Please try again later. If you continue to have this issue please contact <a href=\"https:\/\/www.healio.com\/news\/hematology-oncology\/20260715\/mailto:customerservice@slackinc.com\">customerservice@slackinc.com<\/a>.<\/strong> <\/p>\n<p><button data-dismiss=\"modal\" class=\"btn btn-primary btn-lg btn-block\">Back to Healio<\/button><\/p>\n<\/div>\n<\/div>\n<\/div>\n<\/div>\n<p><br \/>\n<br \/><a href=\"https:\/\/www.healio.com\/news\/hematology-oncology\/20260715\/sensitive-blood-test-detects-pancreatic-cancer-signs-often-missed-by-standard-methods\">Source link <\/a><\/p>\n","protected":false},"excerpt":{"rendered":"<p>Add topic to email alerts Receive an email when new articles are posted on Please provide your email address to receive an email when new articles are posted on . &#8221; data-action=subscribe&gt; Subscribe We were unable to process your request. Please try again later. If you continue to have this issue please contact customerservice@slackinc.com. Back to Healio Key takeaways: ddPCR analysis at diagnosis and after treatment detected KRAS-mutant circulating tumor DNA more frequently than standard testing. The approach could allow for intervention before recurrence is clinically visible. A highly sensitive blood test can detect signs of pancreatic cancer that standard methods often miss, according to results of a prospective cohort study. Digital droplet polymerase chain reaction (ddPCR) analysis performed upon diagnosis of localized disease detected KRAS-mutant circulating tumor DNA (ctDNA) nearly four times more often than more widely used next-generation sequencing, with results strongly predicting survival. Data derived from Sridalla K, et al. Clin Cancer Res. 2026;doi:10.1158\/1078-0432.CCR-26-0609. Administration of ddPCR after chemotherapy or surgery also detected traces of ctDNA with the key genetic mutation at considerably higher rates, suggesting it more effectively identifies patients with residual disease who are at greater risk for recurrence. Akhil Chawla \u201cThese findings provide important insights into what we are missing with next-generation sequencing \u2014 particularly after a patient has been treated,\u201d senior author Akhil Chawla, MD, FACS, clinical associate professor of surgery at Northwestern University Feinberg School of Medicine and complex surgical oncologist at Northwestern Medicine, told Healio. \u201cThe goal of getting more patients to cure requires a thoughtful analysis of each individual. It is an obvious hypothesis that, if a patient has a high risk for recurrence based off what we are seeing in their blood and we treat a patient earlier with a targeted treatment, that patient likely will do better.\u201d Focusing on KRAS Only 13% of patients with pancreatic ductal adenocarcinoma (PDAC) live 5 years after diagnosis, according to American Cancer Society statistics. Individuals with localized disease undergo months of chemotherapy and surgery but still often develop recurrence. Liquid biopsies \u2014 blood tests that can be repeated over time \u2014 search for traces of DNA that cancer cells shed into the bloodstream, offering an early indication that cancer either is present or may return. However, in many cases, ctDNA levels are low and hard to detect. RAS mutations, found in more than 90% of pancreatic cancers, have long been known to be a driver of disease development and progression. Commercially available assays that use next-generation sequencing or digital PCR methods for cancer detection, tumor profiling and therapy selection provide valuable insights, but market forces have driven the technology toward broad panels. In contrast, ddPCR \u2014 which often costs less and yields results quicker \u2014 analyzes one set of genes at a time. Studies that Chawla\u2019s group conducted a few years ago using next-generation sequencing panels confirmed KRAS to be the most prognostic mutation in pancreatic cancer. In their current study, the researchers leveraged that insight to evaluate a ddPCR assay that targets the three most common mutations in the KRAS gene \u2014 G12D, G12V and G12R \u2014 with about a thousand times more sensitivity than more commonly used broader testing approaches. The analysis included 106 patients with localized PDAC who were undergoing neoadjuvant chemotherapy across multiple Northwestern Medicine sites as part of a larger clinical trial. Investigators collected blood samples at multiple time points \u2014 at diagnosis, after chemotherapy and after surgery \u2014 and performed ddPCR and next-generation sequencing on all samples to assess for KRAS-mutant ctDNA. A \u2018hidden group\u2019 At diagnosis, ddPCR detected KRAS-mutant ctDNA in nearly four times as many patients as next-generation sequencing (64.9% vs. 17.2%). The ddPCR test continued to detect residual cancer more effectively after treatment, identifying KRAS-mutant DNA in 12 times as many patients after chemotherapy (60% vs. 5%) and six times more patients after surgery (56% vs. 9%). \u201cAll of these time points are informative but the diagnosis time point has been shown in our studies to be most prognostic, indicating how a patient will do with subsequent neoadjuvant chemotherapy and surgery,\u201d Chawla said. \u201cThis suggests if they have a KRAS mutation at high levels early in their disease course, they may already have more resistant disease or potentially be a more basal-like subtype. These are the patients who recur early and have worse survival.\u201d Detection of KRAS-mutant ctDNA appeared predictive for outcomes. Patients who tested negative on both ddPCR and next-generation sequencing survived a median 40.7 months after diagnosis. A previously \u201chidden group\u201d of high-risk patients \u2014 those whose cancer had been missed by standard next-generation sequencing but detected by ddPCR \u2014 survived a median 26.9 months, Chawla said. Those who tested positive on both tests survived a median 10.9 months (P &lt; .001 for comparison). The high sensitivity of ddPCR allows it to do more than show \u201cpresence or absence\u201d of ctDNA by offering valuable insights into tumor mutational burden, Chawla said. A fundamental change Earlier this spring, results from the randomized phase 3 RASolute 302 trial showed the oral pan-RAS inhibitor daraxonrasib (RMC-6236, Revolution Medicines) doubled survival \u2014 from 6.7 months to 13.2 months \u2014 compared with standard chemotherapy among patients with previously treated metastatic PDAC. The investigational agent, which can be used under an FDA-authorized expanded access protocol and is expected to receive agency approval later this year, also improved several other outcomes, including doubling time to deterioration of pain and quality of life. The findings, which culminate a three-decade commitment to overcome what many in the field had considered an undruggable driver mutation, may lay the foundation for additional therapies or combinations that could lead to longer or deeper responses. This will make the ability to use a high-sensitivity ddPCR test that tracks the same mutation even more valuable, Chawla said. In fact, it may \u201cfundamentally change\u201d how high-risk patients are identified and microscopic disease is monitored, he said, increasing the likelihood that clinicians can intervene before recurrence is clinically visible. \u201cThis remains a very challenging disease to<\/p>\n","protected":false},"author":1,"featured_media":3122,"comment_status":"open","ping_status":"open","sticky":false,"template":"","format":"standard","meta":{"footnotes":""},"categories":[1],"tags":[],"class_list":["post-3121","post","type-post","status-publish","format-standard","has-post-thumbnail","hentry","category-uncategorized"],"_links":{"self":[{"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=\/wp\/v2\/posts\/3121","targetHints":{"allow":["GET"]}}],"collection":[{"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=\/wp\/v2\/posts"}],"about":[{"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=\/wp\/v2\/types\/post"}],"author":[{"embeddable":true,"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=\/wp\/v2\/users\/1"}],"replies":[{"embeddable":true,"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=%2Fwp%2Fv2%2Fcomments&post=3121"}],"version-history":[{"count":0,"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=\/wp\/v2\/posts\/3121\/revisions"}],"wp:featuredmedia":[{"embeddable":true,"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=\/wp\/v2\/media\/3122"}],"wp:attachment":[{"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=%2Fwp%2Fv2%2Fmedia&parent=3121"}],"wp:term":[{"taxonomy":"category","embeddable":true,"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=%2Fwp%2Fv2%2Fcategories&post=3121"},{"taxonomy":"post_tag","embeddable":true,"href":"https:\/\/drsoniafawad.com\/index.php?rest_route=%2Fwp%2Fv2%2Ftags&post=3121"}],"curies":[{"name":"wp","href":"https:\/\/api.w.org\/{rel}","templated":true}]}}