Exercise changed cancer from something doctors treat to something patients help heal
Daraxonrasib nearly doubled survival in metastatic pancreatic cancer patients, extending median survival from 6.7 to 13.2 months with fewer severe side effects. Drug-conjugated antibodies (ADCs) are advancing across ovarian, bladder, prostate, breast and lung cancers, representing a major emerging treatment trend.
- Daraxonrasib doubled median survival in metastatic pancreatic cancer: 6.7 to 13.2 months
- Only 3% of metastatic pancreatic cancer patients survive five years
- Exercise reduced colon cancer recurrence by 28% and death risk by 37%
- Antibody-drug conjugates advancing in ovarian, bladder, prostate, breast, and lung cancers
- RAS mutations found in pancreatic, lung, colorectal, and bile duct cancers
ASCO 2026 conference reveals major advances in cancer treatment, including a drug that doubles pancreatic cancer survival and demonstrates lifestyle changes significantly reduce recurrence risk across multiple cancer types.
In late May, oncologists gathered in Chicago for their annual meeting, and the news they shared suggested the landscape of cancer treatment is shifting in ways both molecular and mundane. A new drug for pancreatic cancer nearly doubled how long patients survive. Antibody-drug conjugates—compounds that deliver chemotherapy directly to tumor cells—are advancing across five different cancer types. And perhaps most striking: people who exercise after colon cancer treatment cut their risk of the disease returning by more than a quarter.
The pancreatic cancer finding arrived with particular weight. Only three percent of people diagnosed with metastatic pancreatic cancer live five years. The disease remains among the cruelest solid tumors. A study called RASolute-302, which tracked five hundred patients who had already tried other treatments, tested a drug named daraxonrasib. The results were stark: median survival jumped from 6.7 months to 13.2 months. The drug reduced the risk of death by sixty percent. Patients also experienced less severe side effects, took longer to report worsening pain, and maintained their quality of life longer than those on conventional chemotherapy.
The significance extends beyond pancreatic cancer alone. Daraxonrasib targets mutations in the RAS gene family—KRAS, NRAS, and HRAS—which act as master switches for cell growth and division. When these genes mutate, they get stuck in the "on" position, flooding cells with signals to multiply. These mutations appear in pancreatic, lung, colorectal, and bile duct cancers. A treatment that works against RAS mutations in one cancer type might work in others. The drug opens a door to a whole class of therapies targeting this fundamental molecular pathway.
Elsewhere at the conference, researchers presented evidence that existing drugs are moving into earlier stages of disease. In prostate cancer, a study called Proteus involved more than two thousand men with high-risk tumors still confined to the prostate but likely to spread or return. Adding apalutamida to hormone therapy before surgery increased the rate at which tumors were completely eliminated by more than tenfold. Another trial, Talapro-3, combined talazoparibe with standard hormone therapy in men whose cancers carried mutations in DNA repair genes like BRCA1 and BRCA2. After three years, seventy-seven percent of those receiving the combination remained disease-free, compared to fifty-six percent on hormone therapy alone.
The emerging star of the conference was a class of drugs called antibody-drug conjugates, or ADCs. These compounds attach a cancer-killing drug to an antibody that recognizes proteins on tumor cell surfaces, essentially guiding the medicine directly to its target. Oren Smaletz, an oncologist at Einstein Hospital in São Paulo who attended the meeting, described ADCs as likely to dominate the next several years. They are advancing in ovarian, bladder, prostate, breast, and lung cancers. Researchers are also refining these drugs to maintain their power while reducing side effects.
Lung cancer illustrates what targeted therapy can accomplish. For patients whose tumors carry actionable genetic changes, these treatments have extended the time before disease progresses, lengthened overall survival, and improved quality of life for tens of thousands of people. Gregory Durm, an oncologist at Indiana University, noted that in some cases, metastatic lung cancer has been transformed from a death sentence into a manageable chronic condition—not curable, but livable. Yet access remains the central problem. Cost keeps these treatments out of reach for many patients, even in wealthy countries.
Perhaps the most resonant finding concerned what happens after treatment ends. A study called Challenge examined colon cancer patients who completed surgery and chemotherapy, then enrolled in a structured exercise program. Those who exercised regularly cut their risk of cancer returning or a new cancer developing by twenty-eight percent. Their risk of death fell by thirty-seven percent. Five-year disease-free survival reached eighty percent in the exercise group versus seventy-four percent in those who received only general advice about healthy living. Overall five-year survival was ninety percent versus eighty-three percent.
These results are reshaping how oncologists counsel patients after treatment. For years, doctors recommended exercise, healthy eating, and weight control as general wellness measures. Now evidence is accumulating that these practices directly influence whether cancer comes back. Smaletz reflected on the shift: oncology is moving from faith-based recommendations to data-driven ones. The implication is profound. The fight against cancer is no longer confined to the clinic. It extends into the patient's daily life—into the hours spent moving, eating, resting. Treatment and living have become inseparable.
Notable Quotes
This will probably be one of the main trends in the coming years. We're seeing ADCs advance in ovarian, bladder, prostate, breast and lung cancer.— Oren Smaletz, oncologist at Einstein Hospital
In some cases, these treatments have transformed metastatic lung cancer into a treatable chronic condition, though still not curable.— Gregory Durm, oncologist at Indiana University
The Hearth Conversation Another angle on the story
Why does a drug that works on pancreatic cancer matter if it only extends survival by six months?
Because three percent of these patients were alive five years ago. Six months doubled is twelve months. Some of those people will reach a year, maybe longer. And the drug opens a path to treating RAS mutations across many cancers, not just pancreas.
So the real story isn't pancreatic cancer—it's RAS?
Partly. But pancreatic cancer is the story because it's where the breakthrough happened first. It's the proof that targeting RAS works in humans, not just in labs.
What's an antibody-drug conjugate, really?
A guided missile. You attach a poison to a homing device. The homing device finds cancer cells. The poison kills them. Normal cells mostly get left alone.
And that's new?
The concept isn't. But they're getting better at it—more accurate, fewer side effects. It's like the difference between carpet bombing and precision strikes.
The exercise study seems almost too simple. People exercise, cancer doesn't come back as often?
It's not magic. Exercise changes metabolism, reduces inflammation, strengthens immunity. But yes, the data shows it works. The surprise is how much it works—twenty-eight percent reduction in recurrence.
So doctors were wrong to not emphasize this before?
Not wrong. They didn't have the evidence. Now they do. It changes what "treatment" means. It's not just what happens in the hospital anymore.