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US President Barack Obama, speaking for the first time about allegations that Secret Service agents hired prostitutes, said on Sunday that "of course I'll be angry" if those accusations are proven true by an investigation.

Sci - Tech
 

New skin cancer drug ‘almost doubles survival’

Thursday - Feb 23, 2012, 11:15pm (GMT+5.5)
[+] Text [-]

Washington -  Researchers have discovered that a new drug, meant for metastatic melanoma patients nearly doubled median overall survival.

According to investigators from Vanderbilt-Ingram Cancer Center (VICC) and 12 other centres in the United States and Australia, more than half of patients who were treated with the novel drug vemurafenib, known commercially as Zelboraf, responded to treatment and experienced an impressive median overall survival of nearly 16 months.

It was far longer than the typical survival of just six to 10 months for most patients whose melanoma has spread beyond the initial tumour site.

“This study confirms what we have discovered in our earlier trials. Many of our patients are exhibiting a strong, immediate response to this drug and some are living significantly longer, with manageable side effects,” said Jeffrey Sosman, professor of Medicine at Vanderbilt University Medical Center.

“It was interesting to note that a few of the patients were treated with the drug for up to six months before showing convincing evidence of response.”

“This study shows that Zelboraf changes the natural history of the disease,” said Ribas. “These results tell us that this drug is having a very big impact, and this changes the way we treat metastatic melanoma.”

Approximately half of all patients with metastatic melanoma – the most deadly form of skin cancer – have a BRAF V600 mutation in their tumour.

Vemurafenib is an FDA-approved oral drug, which works as a kinase inhibitor of the BRAF V600 mutation.

While vemurafenib induced clinical responses in a significant number of BRAF-positive patients when it was approved last year, the initial clinical trials had not followed patients long enough to determine overall survival.

A total of 132 patients with stage IV, BRAF-positive melanoma were enrolled in the Phase II trial. All of the patients had received at least one form of systemic treatment before enrollment in the trial.

Forty-seven percent of patients had a partial response to the drug and six percent exhibited a complete response, for an overall response rate of 53 percent.

The majority of patients had at least one adverse event related to the drug, but most of these were minor.

The most common side effects were joint pain, rash, sun sensitivity, fatigue and hair loss. More than a quarter of the patients (26 percent) also developed cutaneous squamous-cell carcinomas – a less serious form of skin cancer - which were surgically removed.

A Phase III trial of this same drug confirmed significant improvement in both progression-free survival and overall survival with vemurafenib over chemotherapy in an interim analysis.

The Phase II study is the first to confirm the durability of the response.

While the clinical trials for vemurafenib have been positive to date, the great majority of patients eventually experience disease progression.

“We are trying to determine what is causing this drug resistance and are searching for new therapies that we can use, perhaps in combination with vemurafenib,” added Sosman.

The study has been published in the peer-reviewed New England Journal of Medicine.



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