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Book
Year: 2012 Publisher: Bruxelles: UCL,
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Pancreatic cancer remains a disease hard to treat, with an incidence of 37 000 cases in the United States and 96.000 in Europe. Life expectancy at diagnosis does not extend beyond six months, partly due to the absence of screening. Several studies nevertheless revealed the presence of somatic mutations at the level of the oncogene KRAS, p53, p16, and SMAD 4 tumour suppressor genes. The SPARC protein is overexpressed in this cancer and involve in the metastatic path. These genetic alterations can lead to the target molecules development. Major risk factors are diabetes, obesity, smoking and family history. Several molecules have been developed. Since 1997, gemcitabine has become the Tirst line treatment as it performs better than 5-fluorouracil. But since then, other trials have shown some results. The randomized trials led by Conroy and his team that compares Folfirinox to gemcitabine, a combination of irinotecan, oxaliplatin, 5-FU and folinic acid showed real benefits. The median overall survival is 11.1 months for Folfirinox and 6.8 months for gemcitabine (HR. 0.57; 95% CI; 0, 37-0, 57; p < 0.001). The response rate is statistically significant and is 31.6% versus 9.4%, The percentage of hematological . side effects such as neutropenia is higher in the Folfirinox group (45.7%) than in the gemcitabine Group (2 1.0%). The Folfirinox might become a standard for metastatic pancreatic cancer patients with a good performance status and respecting at the same time the criteria for inclusion in the study. Le cancer du pancreas derneure une maladie difficile a soigner avec une incidence de 37 000 cas aux Etats-Unis et 96 000 en Europe en 2008. L’espérance de vie au moment du diagnostic ne s’étend pas au-delà de six mois. Cela s’explique entre autres par l’absence de dépistage. Plusieurs etudes ont pourtant révélé la presence de mutations somatiques au niveau de l’oncogène KRAS, des genes suppresseurs de tumeur p53, p16 et SMAD 4. La protéine SPARC est surexprimée dans ce cancer et impliquée dans le chemin métastatique. Ces alterations génétiques peuvent mener au développement de molecules cibies. Les facteurs de risque les plus marques sont le diabète, l’obésité, le tabac et les antécédents familiaux. Plusieurs molecules ont été développees. Depuis 1997, Ia gemcitabine est devenue le traitement de premiere intention suite a sa supériorité au 5 -fluorouracile. Mais depuis, d’autres essais ont montré des résultats. L’étude randomisée fflenée par Conroy et son équipe qui compare la gemcitabine au Folfirinox, une combinaison d’irinotécan, d’oxaliplatine, de 5- FU et d’acide folinique a montré de reels bénéfices. La survie médiane globale est de 11,1 mois pour le Folfirinox et de 6,8 mois pour la gemcitabine (HR 0,57; IC 95%; 0,37-0,57; p
Book
ISBN: 8178955482 Year: 2012 Publisher: [Place of publication not identified] Transworld Research Network
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Connective Tissue Cells --- Carcinoma --- Endocrine Gland Neoplasms --- Digestive System Neoplasms --- Pancreatic Diseases --- Cell Physiological Phenomena --- Phenomena and Processes --- Digestive System Diseases --- Neoplasms by Site --- Neoplasms, Glandular and Epithelial --- Cells --- Endocrine System Diseases --- Diseases --- Neoplasms by Histologic Type --- Anatomy --- Neoplasms --- Pancreatic Neoplasms --- Adenocarcinoma --- Tumor Microenvironment --- Stromal Cells
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