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Association of Fas/Apo1 gene promoter (-670 A/G) polymorphism in Tunisian patients with IBD 被引量:3
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作者 Walid Ben Aleya imen sfar +9 位作者 Leila Mouelhi Houda Aouadi Mouna Makhlouf Salwa Ayed-Jendoubi Samira Matri Azza Filali Taoufik Najjar Taeib Ben Abdallah Khaled Ayed Yousr Gorgi 《World Journal of Gastroenterology》 SCIE CAS CSCD 2009年第29期3643-3648,共6页
AIM: To detect a possible association between the polymorphism of the (-670 A/G) Fas/Apo1 gene promoter and susceptibility to Crohn's disease (CD) and ulcerative colitis (UC) in the Tunisian population. METHODS: T... AIM: To detect a possible association between the polymorphism of the (-670 A/G) Fas/Apo1 gene promoter and susceptibility to Crohn's disease (CD) and ulcerative colitis (UC) in the Tunisian population. METHODS: The (-670 A/G) Fas polymorphism was analyzed in 105 patients with CD, 59 patients with UC, and 100 controls using the polymerase chain reaction restriction fragment length polymorphism method. RESULTS: Significantly lower frequencies of the Fas -670 A allele and A/A homozygous individuals were observed in CD and UC patients when compared with controls. Analysis of (-670 A/G) Fas polymorphism with respect to sex in CD and UC showed a significant difference in A/A genotypes between female patients and controls (P corrected = 0.004 in CD patients and P corrected = 0.02 in UC patients, respectively). Analysis also showed a statistically significant association between genotype AA of the (-670 A/G) polymorphism and the ileum localization of the lesions (P corrected = 0.048) and between genotype GG and the colon localization (Pcorrected = 0.009). The analysis ofinflammatory bowel disease patients according to clinical behavior revealed no difference. CONCLUSION: Fas-670 polymorphism was associated with the development of CD and UC in the Tunisian population. 展开更多
关键词 溃疡性结肠炎 多态性分析 基因启动子 突尼斯 患者 限制性片段长度多态性 FAS 协会
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Cytokine and apoptosis gene polymorphisms influence the outcome of hepatitis C virus infection 被引量:4
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作者 Leila Ksiaa Cheikhrouhou imen sfar +5 位作者 Hajer Aounallah-Skhiri Houda Aouadi Salwa Jendoubi-Ayed Taieb Ben Abdallah Khaled Ayed Yousr Lakhoua-Gorgi 《Hepatobiliary & Pancreatic Diseases International》 SCIE CAS 2011年第3期280-288,共9页
BACKGROUND:Hepatitis C virus (HCV) infection is thought to be chronic and the factors leading to viral clearance or persistence are poorly understood.This study was undertaken to investigate the possibility of a signi... BACKGROUND:Hepatitis C virus (HCV) infection is thought to be chronic and the factors leading to viral clearance or persistence are poorly understood.This study was undertaken to investigate the possibility of a significant relationship between the spontaneous clearance or the persistence of hepatitis C virus (HCV) infection and cytokine and apoptosis gene polymorphisms in Tunisian patients on hemodialysis.METHODS:Polymorphisms of the genes IL-1 (-889 IL-1α,-511 and +3954 IL-1β,IL-1Ra),IL-18 (-137 and-607),IL-12 (-1188) and Apo1/Fas (-670) were determined by PCR-RFLP,PCR-SSP and PCR-VNTR in 100 healthy blood donors and 100 patients infected with HCV and undergoing hemodialysis.The patients were classified into two groups:G1 consisted of 76 active chronic hepatitis patients (positive for HCV RNA) and G2 consisted of 24 hemodialysed patients who spontaneously eliminated the virus (negative for HCV RNA).RESULTS:The frequency of genotype association [-137GC/-607CA] IL-18 was higher in G2 (41.7%) than in G1 (15.8%) (P=0.008;OR=0.26;95% CI,0.10-0.73).We also found a higher frequency of the AA genotype of the Apo1/Fas gene in G2 (41.6%) than in G1 (17.5%) (P=0.026;OR=3.49;95% CI,1.13-10.69).Adjustment for known covariate factors (age,gender and genotype) confirmed these univariate findings and revealed that the genotype association GC-CA of the (-137 and-607) IL-18 gene and the AA genotype of the Apo1/Fas gene were associated with the clearance of HCV (P=0.041 and 0.017,respectively).CONCLUSION:The two genotypes GC-CA of the (-137 and-607) IL-18 polymorphism and the AA genotype of the Apo1/Fas gene influence the outcome of HCV infection in Tunisian patients on hemodialysis. 展开更多
关键词 hepatitis C virus spontaneous clearance cytokine gene polymorphisms Apo1/Fas gene polymorphisms
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Natural evolution of hepatitis C virus infection in hemodialysis Tunisian patients and CTLA-4 SNP's 被引量:2
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作者 Leila Ksiaa Cheikhrouhou Yousr Lakhoua-Gorgi +5 位作者 imen sfar Salwa Jendoubi-Ayed Houda Aouadi Mouna Makhlouf Khaled Ayed Taieb Ben Abdallah 《World Journal of Gastroenterology》 SCIE CAS 2015年第35期10150-10158,共9页
AIM: To analyze the polymorphisms of CTLA-4 gene involved in the response against hepatitis C virus(HCV) infection.METHODS: We recruited 500 hemodialysed patients from several hemodialysis centers, all HCV-antibody po... AIM: To analyze the polymorphisms of CTLA-4 gene involved in the response against hepatitis C virus(HCV) infection.METHODS: We recruited 500 hemodialysed patients from several hemodialysis centers, all HCV-antibody positive, spread over different regions of Tunisia, as part of a national survey in 2008 conducted in the laboratory of immunology at the Charles Nicolle hospital Tunisia, classified into two groups G1(PCR+) and G2(PCR-) according to the presence or absence of viral RNA. Of these patients, 307 were followed prospectively on a viral molecular level over a period from 2002 to 2008, divided into two groups based on the persistence and viral clearance. PCR-RFLP was performed for the analysis of SNPs(+49) A/G and(+6230) G/A CTLA-4 for these 500 patients and 358 healthy controls.RESULTS: Analysis of clinical and virological charac-teristics of our cohort suggests a nosocomial infection in our hemodialysed patients with transfusion history as a primary risk factor and a predominance of genotype 1b. The haplotype analysis revealed an increase of frequencies of GG(+49)/(CT60) CTLA-4 in the entire patients group compared to controls(P = 0.0036 and OR = 1.42; 95%CI: 1.12-1.79, respectively). This haplotype is therefore associated with susceptibility to HCV infection. CONCLUSION: Our study suggests a possible role of CTLA-4 polymorphisms in the outcome of HCV infection in the Tunisian hemodialysed population. 展开更多
关键词 HEPATITIS C VIRUS HEMODIALYSIS NATURAL evolution C
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Lymphoid tyrosine phosphatase R620W variant and inflammatory bowel disease in Tunisia 被引量:1
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作者 imen sfar Walid Ben Aleya +9 位作者 Leila Mouelhi Houda Aouadi Thouraya Ben Rhomdhane Mouna Makhlouf Salwa Ayed-Jendoubi Houda Gargaoui Taoufik Najjar Taieb Ben Abdallah Khaled Ayed Yousr Gorgi 《World Journal of Gastroenterology》 SCIE CAS CSCD 2010年第4期479-483,共5页
AIM:To assess the possible association between PTPN22(R620W) gene polymorphism and inflammatory bowel disease(IBD).METHODS:One hundred and sixty-four patients with IBD 105 Crohn's disease(CD) and 59 ulcerative col... AIM:To assess the possible association between PTPN22(R620W) gene polymorphism and inflammatory bowel disease(IBD).METHODS:One hundred and sixty-four patients with IBD 105 Crohn's disease(CD) and 59 ulcerative colitis(UC) and 100 healthy controls were recruited.Genotyping of the PTPN22 gene 1858C→T polymorphism was performed by restriction fragment length polymorphism-polymerase chain reaction with Rsa Ⅰ digestion.RESULTS:The genotypic and allelic frequencies of(R620W) PTPN22 gene polymorphism reveal a significant association of the PTPN22 620-W allele with IBD,compared to the healthy control group(OR:17.81,95% CI:4.18-21.86,P = 0.00001).Nevertheless,nodifference in this polymorphism was found between CD and UC patients.No significant association was found between the frequencies of genotypes of the PTPN22 gene with either the clinical features such as sex,age,age at disease onset,and extent of colitis,or the production of serological markers(anti-Saccharomyces cerevisiae antibody in CD and perinuclear anti-neutrophil cytoplasmic antibody in UC).CONCLUSION:These observations confirm the association of IBD susceptibility with the PTPN22 1858T(620-W) allele in Tunisian patients. 展开更多
关键词 Inflammatory bowel disease PTPN22 Genetic polymorphism Genetic susceptibility
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Direction of Arrival Estimation of RF Signals Using Five-Port Technology and High Resolution Method 被引量:1
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作者 imen sfar Lotfi Osman +1 位作者 Ferid Harabi Ali Gharsallah 《通讯和计算机(中英文版)》 2012年第9期1051-1056,共6页
关键词 DOA估计 RF信号 高清晰度 技术 解调器 到达方向 射频信号 天线阵列
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Wideband Demodulator Based on Five-Port Correlator for Channel Sounding Applications
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作者 imen sfar Lotfi Osman Ali Gharsallah 《Journal of Electromagnetic Analysis and Applications》 2013年第2期79-84,共6页
We present in this paper a wideband RF demodulator using a five-port correlator and a power detector for channel sounding applications. The demodulator has been fabricated using microstrip components. The correlator r... We present in this paper a wideband RF demodulator using a five-port correlator and a power detector for channel sounding applications. The demodulator has been fabricated using microstrip components. The correlator receives from the five-port qualities that allow it to be low-cost and less sensitive to the phase and amplitude imbalances. A calibration procedure is proposed to find the complex envelope of the RF signal applied at the input of the five-port correlator. Simulation with Advanced Design System software and measurement results have been conducted to demonstrate its capabilities as a RF signal demodulator operating in a wideband around 2.4 GHz frequency. 展开更多
关键词 Calibration Procedure Channel Sounder Diode Power Detector Five-Port CORRELATOR
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The Monitoring Interest of BK Virus Load in Renal Allograft Tunisian Recipients: Prospective Study
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作者 Yousr Gorgi Mohamed M. Bacha +11 位作者 imen sfar A. Ben Mohamed Hajer Aounallah-Skhiri Tarak Dhaouadi Rafika Bardi N. Skouri Ezzeddine Abderrahim M. Makhlouf T.Ben Romdhane S. Jendoubi-Ayed K. Ayed Taieb Ben Abdallah 《Open Journal of Organ Transplant Surgery》 2012年第4期56-61,共6页
BK virus (BKV) may cause nephropathy in renal transplant recipients receiving immunosuppressive therapy, resulting in renal dysfunction and, possibly graft loss. However, the positive and negative predictive values of... BK virus (BKV) may cause nephropathy in renal transplant recipients receiving immunosuppressive therapy, resulting in renal dysfunction and, possibly graft loss. However, the positive and negative predictive values of BK viral load are still controversial. In this prospective, single-center study, BKV DNA was measured 1, 3 and 6 months after transplantation. The viral load in urine and plasma was quantified with the real-time Q-PCR (Argen kit) in 73 renal allograft recipients Three of them showed acute rejection. To determine the cutoff value of viral load, 60 sera samples of healthy blood donors, matched for age and sex, were tested. The mean plasmatic viral load one month post-transplantation was statistically higher in renal transplant recipients (17.23 copies/ml) compared to that in controls (2 copies/ml) (p: 0.06). This difference of the distribution of viremia values is more evident in the third and sixth month (p: 0.002 and 0.010 respectively). Furthermore, analysis of the kinetic of viral load revealed an average rise of viremia at 3 months (1589.14 copies/ml) followed by its decrease at 6 months (249.75 copies/ml). However, the difference was not statistically significant. The same is true for the distribution of values of viruria and in all cases the average viral load was statistically higher in urine than in plasma. In addition, this study did not shown significant relationsheep between viremia/viruria and the occurrence of acute rejection, the renal function deterioration, the source of allograft or immunosuppressive therapy protocol. If the results of this study demonstrate the importance of the replication of BKV in renal transplant patients from the first month compared to that in immunocompetent subjects, the screening of the DNA of this virus does not appear to have a prognostic value in the occurrence of acute rejection. However, the plasma and urine monitoring of BKV load beyond 6 months , not appear to exclude the relationsheep between these two biomarkers and the occurrence of chronic graft dysfunction. 展开更多
关键词 BK Virus Renal Transplantation URINE and Plasma VIRAL LOAD ALLOGRAFT Dysfunction
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