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A new study from the UT Southwestern Simmons Comprehensive Cancer Center demonstrates that antiviral drugs for hepatitis C reduce liver-related deaths by nearly 50 percent in patients with a history of liver cancer (Gastroenterology 2019;157(1):54-64).

  
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The finding builds on a December 2018 study by the same researchers who found that antiviral drugs do not increase the risk of liver cancer recurrence, as was previously feared.

 

Amit Singal, MD, Associate Professor of Internal Medicine, Medical Director of the UT Southwestern Liver Tumor Program, and Clinical Chief of Hepatology, collaborated on these studies with Caitlin Murphy, PhD, Assistant Professor of Population and Data Sciences and Internal Medicine. They are both members of the Harold C. Simmons Comprehensive Cancer Center at UT Southwestern.

 

Their studies overturn prior misconceptions that made doctors reluctant to prescribe direct-acting antivirals to treat hepatitis C in patients with a history of liver cancer. Many doctors previously believed that hepatitis C, for all its harmfulness, activates the immune system when it infects the liver, and the immune system kept liver cancer recurrence at bay.

 

But this notion appears to be false. Singal and Murphy studied nearly 800 patients from 31 medical centers across the country and found that the drugs are not only safe, they decrease death from cirrhosis and liver cancer by 46 percent.

 

"Not only are these drugs safe in this patient population, but we have now demonstrated that they are helpful," Singal noted. "Our study changes the paradigm from you could treat a patient's hepatitis C to you should treat it."

 

Carlos L. Arteaga, MD, Director of the Simmons Cancer Center, said the study's scope and impact are something that can only be produced by a National Cancer Institute-designated Comprehensive Cancer Center.

 

"Dr. Singal had more patients involved in the study than any other participating site. As an epidemiologist, Dr. Murphy brought rigor to the data that removes prior doubt on this issue," he said.

 

Murphy said previous studies compounded the misunderstandings of direct-acting antiviral therapy because they, among other things, failed to account for the timing of therapy relative to liver cancer diagnosis, did not include a comparison group, or did not properly consider clinical differences among patients.

 

The new study is a significant contribution because it clears the path to beneficial drug treatment.

 

"Hepatitis C therapy is so important because it provides a cure," Singal stated. "You take oral medications for 2 or 3 months, with minimal to no side effects, and you're done. You're cured of hepatitis C. There's less than a 1 percent chance of relapse if you're cured of hepatitis C."

 

Defeating hepatitis C is an important step because infection can otherwise lead to cirrhosis, which can increase the risk for liver cancer. Curing hepatitis C with antivirals breaks the first link in a deadly chain of events and can lead to improvement in liver function among those who have previously developed cirrhosis.

 

"Dr. Singal's and Dr. Murphy's study reports a welcome, fact-based way to oppose the adverse effects of hepatitis C infection in various demographic groups," Arteaga said. "Their findings will have a global, lifesaving impact on how hepatitis C is treated. It is particularly important to Texas because the liver cancer incidence rate in Texas is the highest in the nation."

 

Arteaga said the study is also important because liver cancer is highest among the Hispanic population in Texas, and research-based advances in reducing cancer in underserved groups are a Simmons Cancer Center priority.