Researchers recommend ‘caution’ when using the chemotherapy busulfan in patients with Gilbert’s syndrome
By Susan Keown, Staff Writer, Fred Hutch News Service, Fred Hutchinson Cancer Research Center
Research published Thursday shows that a common genetic disorder ― one that many people don’t even know they have ― is linked to a more than twofold increase in death rates among patients treated with a particular cancer drug.
Scientists estimate that between 3 percent and 10 percent of people worldwide have Gilbert’s syndrome, which alters the way the liver processes one of the byproducts that results from the body’s recycling of dead red blood cells. Gilbert’s typically causes no ill effects; in fact, it’s even been linked to long life and good health in the general population.
This study found, however, that what typically seems to be a Dr. Jekyll turns into a Mr. Hyde for patients who receive a chemotherapy drug called busulfan, which is commonly used as part of a chemotherapy regimen prior to bone marrow transplantation. Bone marrow transplantation is a standard therapy for people with serious blood disorders like advanced leukemia.
The research overturns decades of conventional wisdom in the transplant field about the importance of Gilbert’s [“zhil-BARE’s”] syndrome, said Dr. George McDonald, a lead researcher on the study.
“In the medical textbooks, it’s always said to be totally benign, nothing bad ever happens,” said McDonald, a clinical researcher at Fred Hutchinson Cancer Research Center. This study’s results “came out the total opposite of what I expected.”
This study is just the latest example of how variations in metabolism from patient to patient can have huge impacts on the toxicity or effectiveness of a drug treatment, McDonald said.
“People are born with certain hair color, certain skin color, certain eye color — and certain metabolizing enzymes. You can tell people’s hair color … But you can’t tell what their enzymes are,” he said. “Right now, we assume every human being is going to metabolize drugs in the exact same way. But we know that that’s not true.”
McDonald’s hope is that this study, an analysis of 20 years of data on several thousand patients who were transplanted at via the Fred Hutch/University of Washington Cancer Consortium, will swiftly be validated and implemented to save lives.
“Like all science, it needs to be replicated,” McDonald said. “If it’s replicated with the same dimensions of risk, it’s something that should be universally applied in practice.”
A surprising and mysterious result
Gilbert’s syndrome typically has no outward signs unless a person is under particular physical stress, when they can develop mild jaundice, tiredness or abdominal pain. It’s detected via a blood test that measures levels of bilirubin, the blood-cell-breakdown byproduct whose processing is affected by the genetic disorder. McDonald estimates that about half of people with Gilbert’s are unaware of it; most people have no reason to be.
This isn’t the first study to show that Gilbert’s syndrome can affect how a drug is processed, or metabolized, by the body. Over the last couple of decades, reports have come out about patients with Gilbert’s syndrome who’ve experienced toxic side effects after taking certain drugs that are metabolized by the same enzymes affected by the syndrome.
These reports began to make McDonald wonder about the chemotherapy drugs that patients receive to prepare their bodies for transplantation.
“I’m a big believer in what’s called evidence-based medicine,” McDonald said on a recent day in his office at Fred Hutch in Seattle, behind a desk thoroughly covered in scientific papers.
McDonald was in the middle of moving offices, and a giant canvas mail cart alongside his desk was two-thirds full with outdated textbooks, now destined for the trash, that he collected over his career, which has spanned more than four decades.
For many of those years, McDonald was one of just a handful of people whose research was focused on gastrointestinal and liver complications of transplantation.
With this study, McDonald said, “I just wanted to see if the advice we’d been giving to patients for 40 years really had a factual basis when it came to people getting very high-dose chemotherapy.”
He felt confident. All available evidence on these drugs indicated that they were not processed by the metabolic mechanisms affected by Gilbert’s syndrome. If anything, McDonald reasoned, patients with Gilbert’s syndrome would experience fewer toxic side effects from these chemotherapy drugs than everyone else: Because of Gilbert’s effects on bilirubin-processing enzymes, these people have a higher blood concentration than normal of the preprocessed form of bilirubin ― which just so happens to be an antioxidant, a substance that protects cells from damage. (This antioxidant effect, researchers suspect, could be the reason why people with Gilbert’s tend to live longer and have lower rates of cardiovascular and lung disease than the rest of us.)
To find the answer to his question, McDonald and colleagues turned to a massive database dubbed Gateway, a compendium of medical data from patients treated by Fred Hutch and its consortium partners over 30 years. (The patients had all previously consented for their information to be used anonymously in research.)
Statistician Dr. Ted Gooley of Fred Hutch crunched the numbers from almost 3,500 transplant patients seen between 1991 and 2011, including more than 200 patients the researchers identified as having Gilbert’s syndrome based on records of their blood test results.
What came out of their analysis is rare in science, McDonald said ― a result that is dramatically different from what the researchers expected going into the study. In the first 200 days after transplant, patients with Gilbert’s syndrome who also received busulfan prior to transplant were more than twice as likely to die of any cause than all other patients, and they were nearly three times as likely to die of a cause not related to disease relapse. Gilbert’s seemed to have no effect on the outcomes when any other type of chemotherapy was used.