Paper
Visceral fat area is an Independent Predictive Biomarker of Outcome after First-Line Bevacizumab-Based Therapy in Metastatic Colorectal Cancer
1 University Hospital, Dijon, France;
2 Georges-François Leclerc Cancer Center, Dijon, France
Correspondence to: francois ghiringhelli, Center Georges Francois LECLERC, 1 rue du professeur marion, DIJON, 21000, France; fghiringhelli{at}dijon.fnclcc.fr
Accepted 16 September 2009
Objective: Adipose tissue releases angiogenic factors that may promote tumour growth. We sought to determine whether body mass index (BMI), subcutaneous fat area (SFA), and visceral fat area (VFA) were associated with outcomes in patients given first-line bevacizumab-based treatment for metastatic colorectal cancer (MCC).
Patients: In 120 patients with MCC who received bevacizumab-based therapy (Bevacizumab Group, n=80) or chemotherapy alone (Chemotherapy Group, n=40) as first-line treatment, we used computed tomography to measure SFA and VFA. We evaluated associations linking BMI, SFA, and VFA to tumour response, time-to-progression (TTP), and overall survival (OS).
Results: Bevacizumab Group: median follow-up lasted 24 months [3-70]. BMI, SFA, and VFA values above the median (i.e. high BMI, high VFA and high SFA) were significantly associated with absence of a response. TTP was shorter in patients with high BMI (9 vs. 12 months; P=0.01) or high VFA (9 vs. 14 months; P=0.0008). High VFA was associated with shorter OS (P=0.0493). By multivariate analysis, high VFA was independently associated with response, TTP, and OS (P=0.008, P=0.005, and P=0.027, respectively).
Chemotherapy Group: median follow-up lasted 30 months [4-84]. BMI, SFA and VFA were not associated with response, TTP or OS.
In the whole population: interaction between VFA and bevacizumab administration was significant for response (P=0.005) and TTP (P=0.022), thereby confirming the results.
Conclusion: Our study provides the first evidence that high VFA independently predicts a poorer outcome in patients given first-line bevacizumab-based treatment for MCC. However, this predictive biomarker needs to be validated in a different data set.
CiteULike 
Complore 
Connotea 
Del.icio.us 
Digg 
Reddit 
Technorati What's this?
- Full Text (Rapid PDF)
-
All Versions of this Article:
gut.2009.188946v1
gut.2009.188946v2 most recent - Alert me when this article is cited
- Alert me if a correction is posted
Services
- Email this link to a friend
- Similar articles in this journal
- Similar articles in PubMed
- Add article to my folders
- Download to citation manager
Google Scholar
PubMed
Bookmark with
Register for free content
The full back archive is now available for all BMJ Journals. Institutional subscribers may access the entire archive as part of their subscription. Personal subscribers will also have access to all content when logged in. Non-subscribers who register have free access to all articles published before 2006 right back to volume 1 issue 1. Register here to access the free archive of all BMJ Journals.
Don't forget to sign up for content alerts so you keep up to date with all the articles as they are published.
