BACKGROUND AND AIMS: Complications associated with Crohn's disease (CD) are common and influence treatment decisions and outcomes. Appropriate early treatment may offer a therapeutic advantage to patients. The aim of our study was to indentify predictive factors for occurrence of complications at the time of CD diagnosis. METHODS: The study population consisted of 269 CD patients treated during a ten year period. Risk factors compared between complicated and non-complicated disease included phenotypical characteristics, disease classification and the presence of NOD2/CARD15 mutations and single nucleotide polymorphisms in selected autophagy and phagosome genes. RESULTS: Complete data was obtained for 146 patients with an average follow up of 12years. Sixty five patients (44%) developed a complication during follow up. The only independent risk factors associated with developing a complication were smoking and male gender. There was no association between developing complications and the presence of selected SNPs (P=0.07 for Tyrosine residue on both alleles in NCF4 SNP rs4821544 and P=0.06 for a Guanine residue on both alleles in ATG16L SNP rs2241880). Multivariate analysis using a backwards logistic regression model left only male gender as an independent statistically significant association with complicated disease (OR 2.6017, 95% CI: 1.17 to 5.75). The median time to developing a complication was 4years, and the most common complication was the need for surgical intervention (54%). CONCLUSIONS: In the present study, a risk factor for developing CD complication was male gender. Further studies are warranted to assess additional risk factors and how such findings should affect therapy.
BACKGROUND AND AIMS: Complications associated with Crohn's disease (CD) are common and influence treatment decisions and outcomes. Appropriate early treatment may offer a therapeutic advantage to patients. The aim of our study was to indentify predictive factors for occurrence of complications at the time of CD diagnosis. METHODS: The study population consisted of 269 CDpatients treated during a ten year period. Risk factors compared between complicated and non-complicated disease included phenotypical characteristics, disease classification and the presence of NOD2/CARD15 mutations and single nucleotide polymorphisms in selected autophagy and phagosome genes. RESULTS: Complete data was obtained for 146 patients with an average follow up of 12years. Sixty five patients (44%) developed a complication during follow up. The only independent risk factors associated with developing a complication were smoking and male gender. There was no association between developing complications and the presence of selected SNPs (P=0.07 for Tyrosine residue on both alleles in NCF4 SNP rs4821544 and P=0.06 for a Guanine residue on both alleles in ATG16L SNP rs2241880). Multivariate analysis using a backwards logistic regression model left only male gender as an independent statistically significant association with complicated disease (OR 2.6017, 95% CI: 1.17 to 5.75). The median time to developing a complication was 4years, and the most common complication was the need for surgical intervention (54%). CONCLUSIONS: In the present study, a risk factor for developing CD complication was male gender. Further studies are warranted to assess additional risk factors and how such findings should affect therapy.
Authors: Jean-Francois Turcotte; Karen Wong; Stephanie J Mah; Levinus A Dieleman; Dina Kao; Karen Kroeker; Brian Claggett; John R Saltzman; Eytan Wine; Richard N Fedorak; Julia J Liu Journal: Clin Transl Gastroenterol Date: 2012-07-26 Impact factor: 4.488
Authors: Leonid Belyayev; Jason Hawksworth; Khalid Khan; Stuart Kaufman; Sukanya Subramanian; Alexander Kroemer; Katrina Loh; Raffaele Girlanda; Thomas M Fishbein; Cal S Matsumoto Journal: Transplant Direct Date: 2020-05-21
Authors: Jee Hye Kwon; Jong Pil Im; Byong Duk Ye; Jae Hee Cheon; Hyun Joo Jang; Kang Moon Lee; You Sun Kim; Sang Wook Kim; Young Ho Kim; Geun Am Song; Dong Soo Han; Won Ho Kim; Joo Sung Kim Journal: Gut Liver Date: 2016-07-15 Impact factor: 4.519