Bowel Cancer Patients Live Longer Taking Xeloda
26/06/2008 09:05
PR Newswire
BARCELONA, Spain, June 26 /PRNewswire/ --
- Analysis Confirms That Oral Xeloda is Superior to IV 5-FU
- Not for US Media
A pre-planned multivariate analysis of the five-year follow-up data shows
that patients receiving chemotherapy after-surgery to treat colon cancer, are
more likely to live longer when taking the chemotherapy pill Xeloda
(capecitabine), compared to those receiving 5-FU/FA intravenous (IV)
chemotherapy. The study compared Xeloda to the previous gold-standard IV
chemotherapy for colon cancer, 5-FU/FA*, also known as the Mayo Clinic
regimen. The results showed that 5 years after beginning treatment, the
percentage of patients who survived was higher in the group taking Xeloda
than the group receiving IV 5-FU/FA (71.4% for Xeloda versus 68.4% in the 5
FU/FA group). Results from the study, known as the X-ACT trial, will be
presented on Saturday 28 June at the World Congress on Gastrointestinal
Cancer.
"These data leave no doubt that Xeloda is the better treatment option for
patients," said Professor Eduardo Diaz-Rubio, Chief of the Department of
Medical Oncology, San Carlos Hospital Clinic, Madrid. "The Mayo Clinic
regimen has been the standard, but now that we have long-term evidence
supporting Xeloda's superior efficacy it is time for that standard to change.
When you combine these results with results from studies of Xeloda as an
effective treatment for stomach and colorectal cancer, it is clear that
Xeloda can replace IV 5-FU in all gastrointestinal cancer chemotherapy
courses."
The Mayo Clinic regimen requires that patients visit the hospital on five
consecutive days to receive IV 5-FU/FA, whereas the chemotherapy pill Xeloda
can be taken at home and offers patients increased flexibility.
"From my perspective, I really wanted to be at work," said Andy Griffin,
a colon cancer patient. "When taking Xeloda, I was able to drive myself to
the hospital, have my checks and leave to go to work after only an hour. That
was only once a month, which is very little time spent at the hospital and
very little down time. To me that was really very good."
Results previously presented on the X-ACT study show Xeloda's superiority
over IV 5-FU/FA in several other areas:
- Xeloda is more cost-effective than IV 5-FU/FA in the Mayo
Clinic regimen.
- Xeloda causes less of the side-effects usually associated with
chemotherapy.
- Patients taking oral Xeloda spend 85% less time visiting their
doctor or hospital for treatment.
Based on the initial results of the X-ACT study, Xeloda was approved by
the European Medicines Agency (EMEA) and U.S. Food and Drug Administration
(FDA) for adjuvant (post-surgery) treatment of colon cancer in 2005. As part
of the study design, an additional analysis was planned to provide a more
precise estimate of the effect of Xeloda on patient survival, known as a Cox
analysis. This analysis showed that Xeloda was superior to IV 5-FU/FA. The
Xeloda European label (SPC) for colon cancer was updated in April 2008 to
reflect that Xeloda's superiority against bolus 5-FU/FA has been
demonstrated.
In January 2008, the EU approved Xeloda in combination with any
chemotherapy in all lines of treatment with or without Avastin for advanced
colorectal cancer.
This year will see 281,700 suffer with adjuvant colon cancer in the
majority of the developed world (UK, Spain, Italy, France, Germany, Japan,
Canada and the USA).(1)
* FA: Folinic Acid
Notes to editors:
Highlights from the X-ACT data:
- Overall Survival -- With a median follow-up of 7 years, the 5-year
overall survival rates were 71.4% (95% CI 68-74%) in the Xeloda group and
68.4% (95% CI 65-71%) in the 5-FU/FA group, corresponding to a HR of 0.86
(95% CI 0.74-1.01).
- Disease-free Survival (DFS) -- At a median follow-up of 3.8 years, DFS
in the Xeloda group was at least equivalent to 5-FU/FA (intent-to-treat
analysis, P
- Relapse-free Survival (RFS) -- Xeloda improved RFS (hazard ratio, 0.86;
95% confidence interval, 0.74 to 0.99; P=0.0407) and was associated with
significantly fewer adverse events than 5-FU/FA (P
About the X-ACT Study:
The goal of the X-ACT trial (Xeloda in Adjuvant Colon Cancer Therapy) was
to evaluate the safety and efficacy of Xeloda (capecitabine), a targeted oral
chemotherapy, versus the old global standard of care, bolus intravenous
5-FU/FA (also known as the Mayo Clinic regimen), in patients who recently
have had colon cancer surgery (adjuvant therapy).
The X-ACT trial randomly assigned 1987 patients with resected stage III
colon cancer to oral capecitabine (n=1004) or bolus 5-FU/FA (Mayo Clinic
regimen; n=983) over 24 weeks. The primary efficacy endpoint was at least
equivalence in disease-free survival (DFS); other efficacy endpoints included
relapse-free survival (RFS) and overall survival.
Results presented at WCGI:
Abstract Number: 316.00
Session XVIII: Adjuvant therapy for colon cancer
June 28 2008, 15:00 - 16:20
Updated 5-year efficacy data from X-ACT trial of capecitabine vs. 5-FU/LV
in stage III colon cancer and preliminary analysis of relationship between
hand-foot syndrome and efficacy
About Xeloda (capecitabine)
Xeloda is a highly effective targeted oral chemotherapy offering patients
a survival advantage when taken on its own or in combination with other
anticancer drugs. Xeloda uniquely activates the cancer-killing agent 5-FU
(5-fluorouracil) directly inside the cancer cells so avoiding damage to
healthy cells. Xeloda tablets can be taken by patients in their own home,
reducing the number of hospital visits.
Licensed in more than 100 countries worldwide, Xeloda has over ten years
proven clinical experience providing an effective and flexible treatment
option to over 1.5 million people with cancer. Xeloda is currently approved
in:
- Adjuvant Colon Cancer
- Monotherapy (US & EU) - 2005
- Monotherapy (Japan) - 2007
- Metastatic Colorectal Cancer
- Monotherapy 1st line (US & EU) - 2001
- In combination with any chemotherapy in all lines of treatment with or
without Avastin (EU) - 2008
- Advanced Gastric Cancer
- 1st line treatment (South Korea) - 2002
- In combination with platinum-based chemotherapy 1st line (EU) - 2007
- Metastatic Breast Cancer
- Monotherapy 1st line in patients with tumours resistant to other
chemotherapy drugs such as paclitaxel and anthracyclines - (US) 1998
and (EU) 2002
- In combination with docetaxel in patients whose disease has progressed
following iv chemotherapy with anthracyclines - (US) 2001 and (EU) 2002
- In patients with inoperable or recurrent breast cancer - (Japan) 2003
- Metastatic Pancreatic Cancer
- In combination with gemcitabine 1st line (South Korea) - 2006
About Roche
Headquartered in Basel, Switzerland, Roche is one of the world's leading
research-focused healthcare groups in the fields of pharmaceuticals and
diagnostics. Additional information is available on the Internet at
http://www.roche.com.
Further information available:
- Colorectal cancer fact sheet
- Xeloda fact sheet
- Roche: http://www.roche.com
- Broadcast quality B-roll including doctor, caregiver and patient
interviews is available for download via www.thenewsmarket.com
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(1) GLOBOCAN - Cancer Incidence, Mortality and Prevalence Worldwide
For further information please contact: Julia Pipe, International Communications Manager - Xeloda, F.Hoffmann-La Roche, Mob: +41-79-263-9715, Email: julia.pipe@roche.com; Aba Edwards-Idun, OgilvyHealthPR, Mob : +44-7790-038579, Email : aba.edwards-idun@ohpr.com
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