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Featured researches published by Jérôme Carayol.


European Journal of Human Genetics | 2007

Estimating cancer risk in HNPCC by the GRL method

Flora Alarcon; Christine Lasset; Jérôme Carayol; Valérie Bonadona; Hervé Perdry; Françoise Desseigne; Qing Wang; Catherine Bonaïti-Pellié

Hereditary nonpolyposis colorectal cancer (HNPCC) is an autosomal dominant syndrome caused by germline mutations of the mismatch repair (MMR) genes. Only a few studies have taken into account the selection of families tested for these mutations in estimating colorectal cancer (CRC) risk in carriers. They found much lower estimates of CRC risks than previous ones, but these estimates lacked precision despite the large number of families. The aim of this study was to evaluate the efficiency of the ‘genotype restricted likelihood’ (GRL) method that provides unbiased estimates of risks whatever the ascertainment process of families, and to estimate CRC and endometrial cancer risk for carriers of the MMR genes. Efficiency of the GRL method was evaluated using simulations. Risks were estimated from a sample of 36 families diagnosed with HNPCC and carrying a mutation of MSH2 or MLH1, ascertained through a cancer family clinic in Lyon (France). The efficiency of the GRL method was found to be strongly dependent on the proportion of family members tested. By age 70 years, CRC risk was estimated at 47% (95% confidence interval: 12–98%) for men and 33% (95% confidence interval: 24–54%) for women. The endometrial cancer risk was only 14% (confidence interval: 6–20%). As methods allowing for the selection of families lack efficiency, large-scale family studies should be undertaken and data should be pooled to provide reliable and precise estimates of risks for an optimal familial management.


BMC Cancer | 2006

Genetic polymorphisms of MMP1, MMP3 and MMP7 gene promoter and risk of colorectal adenoma

Astrid Lièvre; Jacqueline Milet; Jérôme Carayol; Delphine Le Corre; Chantal Milan; Alexandre Pariente; Bernard Nalet; Jacques Lafon; Jean Faivre; Claire Bonithon-Kopp; Sylviane Olschwang; Catherine Bonaïti-Pellié; Pierre Laurent-Puig

BackgroundMatrix metalloproteinases (MMP) have been shown to play a role in colorectal cancer (CRC). More recently, MMP1, MMP3 and MMP7 functional gene promoter polymorphisms have been found to be associated with CRC occurrence and prognosis. To document the role of MMP polymorphisms in the early step of colorectal carcinogenesis, we investigated their association with colorectal adenoma risk in a case-control study comprising 295 patients with large adenomas (LA), 302 patients with small adenomas (SA) and 568 polyp-free (PF) controls.MethodsPatients were genotyped using automated fragment analysis for MMP1 -1607 ins/del G and MMP3 -1612 ins/delA (MMP3.1) polymorphisms and allelic discrimination assay for MMP3 -709 A/G (MMP3.2) and MMP7 -181 A/G polymorphisms. Association between MMP genotypes and colorectal adenomas was first tested for each polymorphism separately and then for combined genotypes using the combination test. Adjustment on relevant variables and estimation of odds ratios were performed using unconditional logistic regression.ResultsNo association was observed between the polymorphisms and LA when compared to PF or SA. When comparing SA to PF controls, analysis revealed a significant association between MMP3 -1612 ins/delA polymorphism and SA with an increased risk associated with the 6A/6A genotype (OR = 1.67, 95%CI: 1.20–2.34). Using the combination test, the best association was found for MMP3.1-MMP1 (p = 0.001) with an OR of 1.88 (95%CI: 1.08–3.28) for the combined genotype 2G/2G-6A/6A estimated by logistic regression.ConclusionThese data show a relation between MMP1 -1607 ins/del G and MMP3 -1612 ins/delA combined polymorphisms and risk of SA, suggesting their potential role in the early steps of colorectal carcinogenesis.


Genetic Epidemiology | 2004

Estimating penetrance from family data using a retrospective likelihood when ascertainment depends on genotype and age of onset.

Jérôme Carayol; Catherine Bonaïti-Pellié


/data/revues/03998320/0026SUP5/74/ | 2008

Iconography : Les formes familiales de cancers du côlon, PAF, HNPCC et les autres

Pierre Laurent-Puig; Jérôme Carayol; Frank Zinzindouhoue; Paul-Henri Cugnenc


Revue D Epidemiologie Et De Sante Publique | 2006

B1-3 - Estimation du risque de cancer associé aux gènes BRCA : étude GENECAN

S. Hassid; Catherine Noguès; Jérôme Carayol; Flora Alarcon; M. Labbé; A. Rezvani; Dominique Stoppa-Lyonnet; Pascaline Berthet; Jean-Pierre Fricker; Nadine Andrieu; Catherine Bonaïti-Pellié


3èmes Assises de Génétique Humaine et Médicale | 2006

Estimation du risque de cancer associé aux gènes BRCA : étude GENECAN

Sophie Hassid; Catherine Noguès; Jérôme Carayol; Flora Alarcon; Martine Labbé; Ali Rezvani; Dominique Stoppa-Lyonnet; Pascaline Berthet; Jean-Pierre Fricker; Nadine Andrieu; Catherine Bonaïti-Pellié


Revue D Epidemiologie Et De Sante Publique | 2004

E1-1 Estimation des risques associs une mutation des gnes MLH1 ou MSH2 dans le syndrome de prdi

Valérie Bonadona; Jérôme Carayol; Christine Lasset; Catherine Bonaïti-Pellié


Revue D Epidemiologie Et De Sante Publique | 2004

E1-1 Estimation des risques associés à une mutation des gènes MLH1 ou MSH2 dans le syndrome de prédisposition héréditaire au cancer du côlon non polyposique

Valérie Bonadona; Jérôme Carayol; Christine Lasset; Catherine Bonaïti-Pellié


Gastroenterologie Clinique Et Biologique | 2002

Les formes familiales de cancers du côlon, PAF, HNPCC et les autres

Pierre Laurent-Puig; Jérôme Carayol; Frank Zinzindouhoue; Paul-Henri Cugnenc


Gastroenterologie Clinique Et Biologique | 2002

[Familial forms of colon cancer, familial adenomatous polyposis, hereditary non-polyposis colorectal cancers].

Pierre Laurent-Puig; Jérôme Carayol; Frank Zinzindouhoue; Paul-Henri Cugnenc

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Delphine Le Corre

Paris Descartes University

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Jean Faivre

University of Burgundy

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Martine Labbé

Université libre de Bruxelles

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