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GMJ News > Practice > Clinical Updates > New Drug Daraxonrasib Nearly Doubles Pancreatic Cancer Survival in Phase 3 Trial
Clinical UpdatesNew StudiesPracticeResearch Digest

New Drug Daraxonrasib Nearly Doubles Pancreatic Cancer Survival in Phase 3 Trial

GMJ
Last updated: 03/06/2026 21:55
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GMJ News Desk
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Medical illustration showing targeted cancer therapy attacking tumor cells
Daraxonrasib nearly doubles survival in advanced pancreatic cancer patients with KRAS G12C mutations. The breakthrough targets a previously "undruggable" protein in one of medicine's most challenging cancers. — Photo: Leeloo The First / Pexels
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🎧 Listen to this article6:05 min · 751 words · GMJ Audio
4 min read|751 words
✓ Editorially Reviewed by Prof. Giorgi Pkhakadze, MD, MPH, PhD — GMJ News Desk

🟢 Strong Evidence

Contents
    • Key takeaways
  • Targeting the “Undruggable” KRAS Mutation
  • Clinical Trial Results Show Dramatic Improvement
  • Overcoming Pancreatic Cancer’s Unique Challenges
  • Implications for Precision Oncology
    • What this means
  • Frequently asked questions
    • Who is eligible for daraxonrasib treatment?
    • How does daraxonrasib differ from traditional chemotherapy?
    • When will daraxonrasib be available to patients?

A breakthrough drug called daraxonrasib has nearly doubled survival rates for patients with advanced pancreatic cancer in a phase 3 clinical trial, representing a major advance against one of medicine’s most challenging malignancies. Around 97% of patients with advanced pancreatic cancer die within five years, according to The Conversation analysis. The drug targets the previously “undruggable” KRAS G12C mutation found in approximately 2% of pancreatic cancers.

Key takeaways

  • Daraxonrasib nearly doubled progression-free survival compared to standard chemotherapy in advanced pancreatic cancer patients
  • The drug specifically targets KRAS G12C mutations, found in 2% of pancreatic cancers but previously considered undruggable
  • Pancreatic cancer remains highly lethal with only 3% of patients surviving five years with advanced disease
97%
of patients with advanced pancreatic cancer die within five years

Targeting the “Undruggable” KRAS Mutation

Daraxonrasib represents a significant breakthrough in targeting KRAS G12C mutations, which have historically been considered undruggable by pharmaceutical researchers. The drug works by binding directly to the mutated KRAS protein, preventing it from sending growth signals that fuel tumor progression.

The KRAS family of proteins are among the most commonly mutated genes in cancer. However, developing drugs to target these proteins has proven extremely challenging due to their smooth surface structure, which lacks the binding pockets typically required for drug attachment. For more insights on targeted cancer therapies, see our Clinical Updates section.

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Clinical Trial Results Show Dramatic Improvement

In the phase 3 trial, patients receiving daraxonrasib demonstrated nearly double the progression-free survival compared to those receiving standard chemotherapy regimens. The FDA approval process for the drug is expected to accelerate given these compelling results and the urgent medical need in pancreatic cancer treatment.

Overcoming Pancreatic Cancer’s Unique Challenges

Pancreatic cancer presents unique therapeutic challenges that have made it one of the most lethal malignancies. The dense fibrous tissue surrounding pancreatic tumors creates a barrier that prevents most chemotherapy drugs from reaching cancer cells effectively, according to research from the National Cancer Institute.

Additionally, pancreatic tumors are often diagnosed at advanced stages when surgical removal is no longer possible. The World Health Organization estimates that pancreatic cancer accounts for approximately 466,000 deaths globally each year, making it the seventh leading cause of cancer mortality worldwide. Our Global Health coverage provides regular updates on cancer epidemiology trends.

Implications for Precision Oncology

The success of daraxonrasib highlights the growing importance of precision medicine approaches in oncology, where treatments are tailored to specific genetic mutations rather than tumor location. Genetic testing for KRAS mutations is becoming increasingly standard in pancreatic cancer diagnosis, enabling oncologists to identify patients who may benefit from targeted therapies.

Researchers are now investigating whether daraxonrasib could be effective in other cancer types that harbor KRAS G12C mutations, including lung and colorectal cancers. The National Institutes of Health has launched several additional studies to explore the drug’s broader applications in precision oncology.

What this means

For patients: Those with advanced pancreatic cancer should discuss genetic testing for KRAS mutations with their oncologist to determine eligibility for targeted therapies
For clinicians: Routine genetic profiling of pancreatic tumors should include KRAS mutation analysis to identify candidates for daraxonrasib treatment
For policymakers: Healthcare systems must ensure access to genetic testing and targeted therapies while managing costs of precision medicine approaches

Frequently asked questions

Who is eligible for daraxonrasib treatment?

Patients with advanced pancreatic cancer who test positive for KRAS G12C mutations may be candidates. This represents approximately 2% of all pancreatic cancer patients, requiring genetic testing for identification.

How does daraxonrasib differ from traditional chemotherapy?

Unlike broad-acting chemotherapy drugs, daraxonrasib specifically targets the KRAS G12C mutation. This precision approach typically results in fewer side effects while improving treatment effectiveness in patients with the specific genetic alteration.

When will daraxonrasib be available to patients?

The drug is currently under FDA review following successful phase 3 trials. Regulatory approval timelines typically range from 6-12 months for breakthrough therapies addressing urgent medical needs like advanced pancreatic cancer.

The development of daraxonrasib represents a paradigm shift in treating pancreatic cancer, moving from one-size-fits-all approaches to precision therapies targeting specific genetic drivers. As genetic testing becomes more routine and additional targeted therapies enter development, patients with this historically challenging diagnosis may have significantly improved treatment options and survival outcomes. The success of this KRAS inhibitor also validates years of research investment in targeting previously undruggable proteins, opening new avenues for drug development across multiple cancer types.

Source: Breakthrough drug nearly doubles survival with advanced pancreatic cancer – an oncologist explains how daraxonrasib overcame an ‘undruggable’ disease

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