May is Skin Cancer Awareness Month
According to Marcus Cook, professor and chair of the Department of Molecular Biosciences and co-corresponding author of the study, recent research indicates there may be a more effective way to treat melanoma by using ascorbic acid (vitamin C) to increase DNA damage in cancer cells, causing them to die.
The multidisciplinary research team found that melanoma cells had more DNA damage and lower antioxidant defenses than normal skin cells. When treated with hydrogen peroxide and vitamin C, melanoma cells had more DNA damage and higher rates of cell death, while normal cells were protected. Additionally, the results showed that vitamin C increased the effectiveness of elesclomol, an existing melanoma treatment.
Cook, who also leads the oxidative stress group, said the effects of vitamin C on DNA and skin cells have been studied for many years, which led to the current research.
“We have been studying the effects of antioxidants since the late 1990s and have been fascinated by vitamin C’s ability to act as a pro-oxidant (causing DNA damage) and antioxidant (preventing DNA damage) and its apparent ability to help regulate DNA repair. This, combined with our long-standing interest in skin biology/solar UV radiation, also dating back to the 1990s, led to this research.”
“Our results show that melanoma cells have higher levels of DNA damage than keratinocytes (the main cells found in the epidermis), and that this damage is proportional to the amount of melanin in the melanocytes – the more melanin, the greater the damage,” explains Cook. “This was also seen in cells that had not been exposed to sun, suggesting that melanin in the cells may be damaging to melanoma cells.”
“Our studies have revealed that the levels of potentially harmful reactive substances are proportional to the amount of melanin, while the levels of protective antioxidants are inversely proportional. With all this in mind, we have discovered that we can exploit this situation to selectively kill melanoma cells,” he said.
Cook acknowledges that further clinical studies and trials will help bolster these findings and move us forward toward incorporating ascorbic acid as an adjunct to treatment.
“Ascorbic acid is already well studied and known to be well tolerated, so if it acts like elesclomol to induce DNA damage, I think clinicians could add ascorbic acid to existing treatments to augment existing approaches,” he said. “The biomarkers of oxidative stress that we use in our lab in my oxidative stress group are particularly well suited to clinical studies, so we’re looking forward to using them in clinical trials.”
In vivo Once patient biomonitoring (of whole living cell organisms) and clinical studies begin.”
