Marlene McCarthy鈥檚 breast cancer has grown relentlessly over the past seven years, spreading painfully through her bones and making it impossible to walk without a cane.
Although the 73-year-old knows there鈥檚 no cure for her disease, she wants researchers to do better. It鈥檚 been years, she said, since she has found a drug that has actually helped. McCarthy said she鈥檚 frustrated that the Food and Drug Administration is approving cancer drugs without proof that they cure patients or help them live longer.
鈥淭hat simply isn鈥檛 good enough,鈥 said McCarthy, of Coventry, R.I. 鈥淚 understand [why] that could be satisfactory for some people. It isn鈥檛 to me.鈥
Pushed by patient advocates who want earlier access to medications, the颅 FDA has approved a flurry of oncology drugs in recent years, giving some people with cancer a renewed sense of hope and an array of expensive new options. A few of these drugs have been clear home runs, allowing patients with limited life expectancies to live for years.
Many more drugs, however, have offered patients only marginal benefits, with no evidence that they improve survival or quality of life, said Dr. Vinay Prasad, assistant professor of medicine at the Oregon Health and Science University, who has about the FDA鈥檚 approval process for cancer drugs.
Overall cancer survival has barely changed over the past decade. The 72 cancer therapies approved from 2002 to 2014 gave patients only 2.1 more months of life than older drugs, according to a study in
And those are the successes.
Two-thirds of cancer drugs approved in the past two years have no evidence showing that they extend survival at all, Prasad said.
The result: For every cancer patient who wins the lottery, there are many others who get little to no benefit from the latest drugs.
鈥淲e are very concerned about the push to get more drugs approved, instead of effective drugs approved,鈥 said Fran Visco, president of the National Breast Cancer Coalition, who said the last game-changing breast cancer drug, Herceptin, was approved nearly 20 years ago.
In a published in JAMA Internal Medicine, researcher Diana Zuckerman looked at 18 approved cancer drugs that didn鈥檛 help patients live longer. Only one had clear data showing that it improved patients鈥 lives, such as by relieving pain or fatigue.
Two drugs harmed quality of life. For example, thyroid cancer patients taking the most expensive drug, cabozantinib, scored worse on a scale measuring five symptoms: diarrhea, fatigue, sleep disturbance, distress, and difficulty remembering, Zuckerman said.
鈥淥ur patients need drugs that provide the greatest possible benefit, particularly when you put that in the context of cost,鈥 said Dr. Richard Schilsky, senior vice president and chief medical officer at the American Society of Clinical Oncology, which represents cancer specialists. 鈥淵ou begin to question what is the real value of a therapy when the benefit is small, the toxicity may be similar to a previous drug and the cost is much higher.鈥
Cancer drugs approved last year cost an average of $171,000 a year, according to the at New York鈥檚 Memorial Sloan Kettering Cancer Center. Although the high prices can lead patients to think they鈥檙e getting the Mercedes of cancer drugs, research shows that a medication鈥檚 price has .
鈥淲e cannot have a system where drugs that may not even work are being sold for these amazingly crazy amounts of money,鈥 said Zuckerman, president of the National Center for Health Research, a nonprofit in Washington that aims to explain research to consumers.
Recognizing the slow pace of progress, the American Society of Clinical Oncology has of extending life or controlling tumors for at least 2.5 months. The bar was set relatively low because 鈥渋t鈥檚 not very often that we come across a transformative treatment,鈥 said Dr. Sham Mailankody, an assistant attending physician and myeloma specialist at Memorial Sloan Kettering.
Yet in a study published in September in , Mailankody found that only one in five cancer drugs approved from 2014 to 2016 met those standards.
Even those slim gains, achieved during carefully controlled clinical trials, can evaporate in the real world, where patients are often older and sicker than those who participate in research studies, said Hanna Sanoff, an associate professor and section chief of the University of North Carolina School of Medicine Gastrointestinal Medical Oncology Program.
Cancer is primarily a disease of aging; 59聽percent of patients are over 65 and 30聽percent are older than 75. Yet only 33聽percent of participants in cancer trials are over age 65 and just 10聽percent are over 75, according to a
In a study published in September in Sanoff found that a drug that improved survival in liver cancer by three months offered no survival advantage among Medicare patients outside the clinical trial.
McCarthy, who reviews breast cancer research for the Department of Defense, said she was twice turned down for clinical trials because of her age. When researching experimental therapies, 鈥淚鈥檇 get excited by something that seemed promising, only to be told I was too old to join the trial, because the cutoff age was 70,鈥 she said.
McCarthy works on a computer as her husband, Joe, looks on. McCarthy, a mother of four, was first diagnosed with breast cancer at 44. Seven years ago, the disease returned in her bones, a condition that is not curable. (Katye Brier for KHN)
Lowering聽The Bar
FDA officials said there are good reasons why many promising cancer drugs lack evidence of improved survival.
Because some cancers grow slowly, it can take many years for a study to show whether a new drug helps people live longer, said Dr. Richard Pazdur, director of the FDA鈥檚 Oncology Center of Excellence. While individual drugs may only modestly improve survival, 鈥渨hen used sequentially or in combination, they can transform a disease,鈥 Pazdur said.
The design of some cancer trials also can make it hard to tell if drugs help patients live longer. That鈥檚 because many trials now allow patients in the control group the opportunity to 鈥渃ross over鈥 to get the drug being studied, if preliminary data suggests it could聽help them, Pazdur said. While such crossover benefits people in the study, who are facing a life-threatening disease, it can lead to inconclusive findings.
Lastly, Pazdur said that overall survival rates also don鈥檛 reflect the fact that some drugs, such as targeted therapies for lung cancer, allow a subset of patients to do extremely well, surviving for years instead of months.
The number of patients with advanced melanoma who survive five years after diagnosis has increased from 5 percent before the advent of immune therapies to 30 percent to 40 percent today, said Dr. Steven O鈥橠ay, director of immuno-oncology and clinical research at the John Wayne Cancer Institute at Providence Saint John鈥檚 Health Center in Santa Monica, Calif. Immune therapies work by stimulating a patient鈥檚 natural immune system to combat cancer cells.
鈥淭here is a lot of excitement about these [immunotherapy] drugs, and for good reason,鈥 Schilsky said. 鈥淭here鈥檚 no diminishing the progress that鈥檚 been made.鈥
The FDA wants to give patients the chance to benefit as soon as possible, rather than waiting for definitive proof of improved survival, Pazdur said. In some cases, the FDA requires pharmaceutical companies to perform long-term studies after drugs are approved, to measure whether drugs live up to their early promise.
But many of these studies never provide an answer, Zuckerman said. Once a drug is approved and is available to anyone, patients have no incentive to participate in a clinical trial. So studies can end with no clear conclusion.
In a , Prasad looked at 36 drugs approved without proven survival advantages. More than four years later, only five had evidence of improved survival.
Otis Brawley, chief medical officer at the American Cancer Society, said he鈥檚 concerned that the FDA is lowering its standards.
鈥淲e鈥檙e getting less rigorous scientifically because we want to get these drugs out to people faster,鈥 Brawley said.
Unless the FDA requires companies to provide survival data before approving a drug, 鈥渨e may never have answers,鈥 Zuckerman said. 鈥淲e will have all of these expensive drugs on the market and we will never have the information we need about how well they work or even how safe they are.鈥
President Donald Trump has vowed to cut regulations at the FDA and recently told pharmaceutical industry leaders that he wants to further speed up the drug approval process.
Helpful Or Harmful?
Cancer patients, who are making decisions at a time of intense stress, don鈥檛 always understand the full risks and benefits of therapy, Brawley said. Studies suggest that both and drugs鈥 benefits, but underestimate their risks and side effects.
A study of 2,944 people in found that 39 percent mistakenly believed the FDA only approves 鈥渆xtremely effective鈥 drugs, while 25 percent mistakenly believed the agency only approves treatments without serious side effects.
Even doctors think 鈥渨e are better than I actually think we are,鈥 Brawley said. 鈥淭he thought that these drugs could be harmful is foreign to them.鈥
Patients 鈥渟ee the survival benefit, and of course these are scared, desperate people trying to get themselves any chance they can get,鈥 said Dr. Ellyn Lee, who guides patients about cancer treatments as director of Seattle’s Swedish Palliative Care Services. 鈥淗owever, the survival benefit is not often realized, or it鈥檚 three months of misery due to side effects and bankruptcy at the end. Is that really fair?鈥
One of the biggest recent changes at the FDA is that more drugs are being approved based on 鈥減rogression-free survival鈥 鈥 medical jargon for the amount of time that patients live while their tumors are under control.
Because small changes in tumor size aren鈥檛 always clearly visible on scans, doctors consider tumors to be under control as long as they don鈥檛 grow more than 20 percent, Brawley said.
Doctors always hope that a drug that delays tumor growth will help patients live longer. But in a Prasad found that most statistical analyses have found the link between progression-free survival and overall survival to be very weak.
Measures such as progression-free survival 鈥渁re just a guess as to whether or not the drug actually works,鈥 Brawley said. 鈥淭he problem with approving a drug based on a progression-free survival is that you don鈥檛 know if the drug is actually doing anything positive for the patient.鈥
Brawley said he鈥檚 concerned that patients could be harmed by oncology drugs whose long-term side effects are unknown.
The drug Avastin, which was approved for breast cancer in 2008, without evidence that it improved survival, three years later, after studies showed it did not help people live longer. The FDA concluded that life-threatening side effects, which included heart attacks, bleeding and high blood pressure, outweighed the drug鈥檚 benefits.
鈥淭here are all these drugs that we used for a long, long time, but we ended up taking them off the market because we finally realized they were harmful,鈥 Brawley said. 鈥淲e are setting ourselves up for that again.鈥
鈥淏reast cancer doesn鈥檛 seem to have a road map to cure,” said Marlene McCarthy. “It鈥檚 just a damn sneaky disease.” (Katye Brier for KHN)
McCarthy has been disappointed in the new cancer therapies she鈥檚 tried. The last drug that kept her tumors from growing was letrozole, which was approved in 1997. It kept McCarthy鈥檚 tumors under control for three years.
In 2015, after her tumors began growing again, McCarthy began a new breast cancer drug, called The FDA approved Ibrance because it improved progression-free survival by 10 months when combined with a standard hormonal therapy. Four months after McCarthy began the drug, however, scans found new bone tumors.
A spokeswoman for Pfizer, Sally Beatty, noted that Ibrance鈥檚 proven benefits have improved since then. In a , women taking the Ibrance combination lived 24.8 months with limited tumor growth, compared to 14.5 months for women who took the hormonal therapy alone.
McCarthy opted not to try another breast cancer drug, Afinitor, after doctors warned her that it posed too many risks. The in 2012 because it limited tumor growth for four months longer than placebo.
鈥淭hat鈥檚 nothing to be excited about,鈥 said McCarthy, who has four children and four grandchildren. 鈥淚 want to live more than four months.鈥
But keeping tumors in check can be a huge help to patients, said Pazdur, who notes that there are many ways for drugs to help patients, even without extending life. Shrinking a bone tumor, for example, can relieve pain. Shrinking a lung tumor can make it easier for someone to breathe.
鈥淢ost patients are pleased if they go to the doctor and the doctor says, 鈥榊our scan says everything is stable. There are no new lesions,鈥欌 Schilsky said. 鈥淚鈥檝e given that result to patients many times over the years and they are all happy about it. Are they as happy as they would be if the tumor were gone? Of course not. But being free from progression and otherwise feeling OK is not such a bad outcome.鈥
As someone with incurable cancer, McCarthy remains frustrated with the pace of progress. Scientists, she said, aren鈥檛 asking the right questions.
McCarthy said she wants researchers to focus on prevention of cancer, and to learn why breast cancers like hers can remain dormant for years before suddenly reactivating. Her cancer, which was first diagnosed when she was 44, disappeared for two decades before reappearing in her bones.
鈥淭he status quo isn鈥檛 good enough,鈥 said McCarthy. 鈥淚 want us to have a breast cancer vaccine to prevent my granddaughter from getting cancer. I鈥檒l be working for that with my dying breath.鈥
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