That’s a nice two-fer
Massachusetts General Hospital
A new study led by investigators from Mass General Cancer Center, a founding member of the Mass General Brigham healthcare system, reveals that statins -- commonly used cholesterol-lowering drugs -- may block a particular pathway involved in the development of cancer that results from chronic inflammation. The findings are published in Nature Communications.
"Chronic inflammation is a major cause
of cancer worldwide," said senior author Shawn Demehri, MD, PhD, a
principal investigator at the Center for Cancer Immunology and Cutaneous
Biology Research Center of Massachusetts General Hospital and an associate
professor of Dermatology at Harvard Medical School.
"We investigated the mechanism by which environmental toxins drive the initiation of cancer-prone chronic inflammation in the skin and pancreas," says Demehri, who is also theBob and Rita Davis Family MGH Research Scholar 2023-2028.
"Furthermore, we examined safe and
effective therapies to block this pathway in order to suppress chronic
inflammation and its cancer aftermath."
Demehri and his colleagues' study relied on cell lines, animal models, human tissue samples and epidemiological data. The group's cell-based experiments demonstrated that environmental toxins (such as exposure to allergens and chemical irritants) activate two connected signaling pathways called the TLR3/4 and TBK1-IRF3 pathways.
This activation leads to the production of
the interleukin-33 (IL-33) protein, which stimulates inflammation in the skin
and pancreas that can contribute to the development of cancer.
When they screened a library of U.S. Food
and Drug Administration-approved drugs, the researchers found that a statin,
pitavastatin, effectively suppresses IL-33 expression by blocking the
activation of the TBK1-IRF3 signaling pathway.
In mice, pitavastatin suppressed
environmentally-induced inflammation in the skin and the pancreas and prevented
the development of inflammation-related pancreatic cancers.
In human pancreas tissue samples, IL-33 was
over-expressed in samples from patients with chronic pancreatitis
(inflammation) and pancreatic cancer compared with normal pancreatic tissue.
Also, in analyses of electronic health records data on more than 200 million
people across North America and Europe, use of pitavastatin was linked to a
significantly reduced risk of chronic pancreatitis and pancreatic cancer.
The findings demonstrate that blocking
IL-33 production with pitavastatin may be a safe and effective preventive
strategy to suppress chronic inflammation and the subsequent development of
certain cancers.
"Next, we aim to further examine the impact of statins in preventing cancer development in chronic inflammation in liver and gastrointestinal tract and to identify other novel, therapeutic approaches to suppress cancer-prone chronic inflammation" said Demehri.