共查询到20条相似文献,搜索用时 359 毫秒
1.
目的 探讨难治性精神分裂症与细胞色素P450 2D6(CYP2D6)基因多态性的关系。方法 用聚合酶链反应-限制性片段长度多态性(PCR-RFLP)技术分析92例难治性精神分裂症患者的CYP2D6基因多态性,并以92例非难治性精神分裂症患者作为对照。结果 难治性分裂症组CYP2D6基因型C/T(OR=0.47,P=0.043)和等位基因C(OR=0.50,P=0.002)频率显著性低于非难治分裂症组,而其基因型T/T(OR=1.94,P=0.032)和等位基因T(OR=2.00,P=0.002)则显著高于非难治性分裂症组。结论 本组样本中CYP2D6C188T基因多态性与难治性精神分裂症关联,CYP2D6C188T突变可能是难治性精神分裂症发病因素之一,本组中国汉族人中22号染色体长臂(22q13.1)可能存在难治性精神分裂症易感性基因。 相似文献
2.
3.
目的探讨CYP2E1基因多态性与胃腺癌的关联,为胃癌高危人群的筛选和预防控制工作提供科学依据。方法胃腺癌患者34例及健康人对照34名,分别采用PCR-RFLP技术与多重PCR方法,检测CYP2E1基因型,观察其多态性,然后进行统计学分析。结果CYP2E1 C1/C1基因型(纯合子野生型)在胃癌组和健康人对照组中的分布频率分别是64.7和41.2,差异具有显著性(χ2=6.27;P〈0.05)。结论CYP2E1 C1/C1基因型与胃癌遗传易感性相关。 相似文献
4.
目的 研究精神分裂症患者细胞色素P450 2D6酶(CYP2D6) exonⅠC/T188基因多态性与阿立哌唑治疗效应的关系.方法 采用阳性和阴性症状量表(PANSS),治疗时需处理的副反应量表(TESS)以及锥体外系副反应量表(RSESE)对92例精神分裂症患者,分别在阿立哌唑治疗前及治疗第1、2、4、6、8周末各进行一次药物反应评定,采用聚合酶链反应技术对CYP2D6 exon ⅠC/T188基因多态性进行检测.根据其基因型将患者分为三组(C/C组30例、C/T组38例、T/T组24例),采用治疗前后PANSS减分率≥30%为标准,将92例患者分为治疗有效组和治疗无效组,比较组间药物治疗效应的差异.结果 从阿立哌唑治疗后第6周末开始,三组之间PANSS评分的差异有显著性(P<0.01);两两比较发现,C/C组PANSS分低于T/T组(P<0.01);CYP2D6 exon ⅠC/T188多态性基因型频率和等位基因频率,阿立哌唑治疗有效组与无效组之间的差异有显著性.但未发现基因型与阿立哌唑药物副反应有关.结论 中国人群精神分裂症CYP2D6 exon ⅠC/T188多态性可能是影响阿立哌唑临床疗效的遗传易感因素. 相似文献
5.
目的 :为研究CYP2C19基因在中国云南地区特色少数民族独龙族人群中的基因型及突变频率 .方法 :采用聚合酶链式反应 (PCR)与限制性内切酶片段长度多态性(RFLP)技术分析了 2 0 5例独龙族人群中的基因型 .结果 :84人为CYP2C19野生型纯合子 (wt/wt) ;98人为CYP2C19m1杂合子 (wt/m1) ;2 3人为CYP2C19m1突变纯合子 (m1/m1) .突变频率为 0 3 5 1.结果与苗族人群CYP2C19基因突变频率有显著差异 ,但与国内外其他相关报道未见显著差异中国独龙族人群中细胞色素P450 2C19基因多态性的研究(摘要)@唐莉$云南省计划生育技术科学研究所!昆明65… 相似文献
6.
目的:为研究CYP2C19基因在中国云南地区特色少数民族独龙族人群中的基因型及突变频率.方法:采用聚合酶链式反应(PCR)与限制性内切酶片段长度多态性(RFLP)技术分析了205例独龙族人群中的基因型.结果:84人为CYP2C19野生型纯合子(wt/wt);98人为CYP2C19 m1杂合子(wt/m1);23人为CYP2C19 m1突变纯合子(m1/m1).突变频率为0.351.结果与苗族人群CYP2C19基因突变频率有显著差异,但与国内外其他相关报道未见显著差异. 相似文献
7.
目的 探讨难治性精神分裂症与细胞色素P4502D6(CYP2D6)基因多态性的关系.方法 用聚合酶链反应-限制性片段长度多态性(PCR-RFLP)技术分析92例难治性精神分裂症患者的CYP2D6基因多态性,并以92例非难治性精神分裂症患者作为对照.结果 难治性分裂症组CYP2D6基因型C/T(OR=0.47,P=0.043)和等位基因C(OR=0.50,P=0.002)频率显著性低于非难治分裂症组,而其基因型T/T(OR=1.94,P=0.032)和等位基因T(OR=2.00,P=0.002)则显著高于非难治性分裂症组.结论 本组样本中CYP2D6C188T基因多态性与难治性精神分裂症关联,CYP2D6C188T突变可能是难治性精神分裂症发病因素之一,本组中国汉族人中22号染色体长臂(22q13.1)可能存在难治性精神分裂症易感性基因. 相似文献
8.
目的 探讨CYP2C19*2基因多态性与维吾尔族缺血性脑卒中患者氯吡格雷抵抗及卒中复发风险的关系.方法 检测100例维吾尔族缺血性脑卒中患者CYP2C19*2基因型,分为纯合子野生型、杂合子突变型、纯合子突变型;使用血小板聚集功能检测仪测定血小板聚集率;于氯吡格雷治疗6个月时随访所有患者的卒中复发率.结果 根据基因分型,将研究对象分为纯合子野生型组(63例)、杂合子突变型组(32例)和纯合子突变型组(5例).突变型组氯吡格雷抵抗的发生率及卒中复发率高于野生型组(P<0.05).Logistic回归分析显示:CYP2C19*2等位基因是维吾尔族缺血性脑卒中患者氯吡格雷抵抗及卒中复发的危险因素(OR=2.541,95%CI:1.052 ~6.137,P=0.038;OR =4.741,95% CI:1.273 ~7.392,P=0.045).结论 CYP2C19*2基因多态性与维吾尔族缺血性脑卒中患者氯吡格雷抵抗及卒中复发有相关性,CYP2C19*2等位基因是氯吡格雷抵抗及卒中复发的危险因素. 相似文献
9.
目的 探讨中国大连地区汉族人群细胞色素P450酶4F2(CYP4F2)rs2108622基因多态性对华法林剂量的影响,为华法林个体化用药及开发基因型检测试剂盒提供理论依据.方法 采用限制性内切酶片段长度多态性(RFLP)技术,检测196例服用华法林患者的CYP4F2 rs2108622的基因型,统计分析对华法林剂量的影响.结果 CYP4F2 rs2108622基因多态性检测结果为野生纯合子CC型99例,杂合子CT型84例,突变纯合子TT型13例;等位基因频率C 71.94%,T 28.06%.CC型患者华法林的平均稳定剂量为(3.07±1.21)mg/d,CT型为(3.66±1.33)mg/d,TT型为(3.73±1.55)mg/d,各组间华法林剂量比较,差异有统计学意义(P<0.05).结论 大连地区汉族人群中,CYP4F2 rs2108622基因多态性能明显影响华法林的稳定剂量. 相似文献
10.
CYP2D6基因G4268C单核苷酸多态性与肺癌遗传易感性 总被引:1,自引:0,他引:1
目的:研究CYP2D6(cytochromes P450 2D6)基因G4268C单核苷酸多态性与肺癌遗传易感性的关系.方法:应用病例-对照研究及聚合酶链反应-限制性片段长度多态性分析(PCR-RFLP)方法检测肺癌患者和按性别、年龄频数匹配的正常对照各118例的CYP2D6基因G4268C多态性,并应用Logistic回归分析各基因型与肺癌发病危险的关系.结果:肺癌组和对照组人群发生G4268→C的频率可高达69.49%和75.00%;非C4268/C(即G4268/G G4268/C)基因型与肺癌风险升高相关,经年龄、性别、吸烟情况调整OR=1.80(95%CI=1.06~3.06),尤其在腺癌中OR=2.95(95%CI=1.39~6.23);对吸烟情况进行分层分析并经年龄、性别调整后发现,不吸烟者及轻度吸烟者中携带非C4268/C基因型的个体患肺癌的风险显著增高,其OR值分别为2.12(95%CI=1.03~4.36)和3.75(95%CI=1.15~12.22).结论:CYP2D6 C4268/C基因型可能是肺腺癌的遗传保护因素,并可降低不吸烟者、轻度吸烟者患肺癌的危险度. 相似文献
11.
12.
Coffee, CYP1A2 genotype, and risk of myocardial infarction 总被引:8,自引:0,他引:8
Context The association between coffee intake and risk of myocardial infarction (MI) remains controversial. Coffee is a major source of caffeine, which is metabolized by the polymorphic cytochrome P450 1A2 (CYP1A2) enzyme. Individuals who are homozygous for the CYP1A2*1A allele are "rapid" caffeine metabolizers, whereas carriers of the variant CYP1A2*1F are "slow" caffeine metabolizers. Objective To determine whether CYP1A2 genotype modifies the association between coffee consumption and risk of acute nonfatal MI. Design, Setting, and Participants Cases (n = 2014) with a first acute nonfatal MI and population-based controls (n = 2014) living in Costa Rica between 1994 and 2004, matched for age, sex, and area of residence, were genotyped by restriction fragment–length polymorphism polymerase chain reaction. A food frequency questionnaire was used to assess the intake of caffeinated coffee. Main Outcome Measure Relative risk of nonfatal MI associated with coffee intake, calculated using unconditional logistic regression. Results Fifty-five percent of cases (n = 1114) and 54% of controls (n = 1082) were carriers of the slow *1F allele. For carriers of the slow *1F allele, the multivariate-adjusted odds ratios (ORs) and 95% confidence intervals (CIs) of nonfatal MI associated with consuming less than 1, 1, 2 to 3, and 4 or more cups of coffee per day were 1.00 (reference), 0.99 (0.69-1.44), 1.36 (1.01-1.83), and 1.64 (1.14-2.34), respectively. Corresponding ORs (95% CIs) for individuals with the rapid *1A/*1A genotype were 1.00, 0.75 (0.51-1.12), 0.78 (0.56-1.09), and 0.99 (0.66-1.48) (P = .04 for gene x coffee interaction). For individuals younger than the median age of 59 years, the ORs (95% CIs) associated with consuming less than 1, 1, 2 to 3, or 4 or more cups of coffee per day were 1.00, 1.24 (0.71-2.18), 1.67 (1.08-2.60), and 2.33 (1.39-3.89), respectively, among carriers of the *1F allele. The corresponding ORs (95% CIs) for those with the *1A/*1A genotype were 1.00, 0.48 (0.26-0.87), 0.57 (0.35-0.95), and 0.83 (0.46-1.51). Conclusion Intake of coffee was associated with an increased risk of nonfatal MI only among individuals with slow caffeine metabolism, suggesting that caffeine plays a role in this association. 相似文献
13.
Effect of St John's wort on drug metabolism by induction of cytochrome P450 3A4 enzyme 总被引:8,自引:0,他引:8
Context St John's wort is a popular herbal product used to treat depression but it has been implicated in drug interactions. Objective To assess the potential of St John's wort administration to alter the activity of the cytochrome P450 (CYP) enzymes extensively involved in drug metabolism. Design, Setting, and Participants Open-label crossover study with fixed treatment order conducted March 2002 to February 2003 in a US general clinical research center involving 12 healthy volunteers (6 men and 6 women) aged 22 to 38 years before and after 14 days of administration of St John's wort. Intervention Participants were given probe drugs (30 mg of dextromethorphan and 2 mg of alprazolam) to establish baseline CYP 3A4 and CYP 2D6 activity. After a minimum 7-day washout period, participants began taking one 300-mg tablet 3 times per day. After 14 days of St John's wort administration, participants were given the probe drugs along with 1 St John's wort tablet to establish postadministration CYP activity; the St John's wort dosing regimen was continued for 48 hours. Main Outcome Measures Changes in plasma pharmacokinetics of alprazolam as a probe for CYP 3A4 activity and the ratio of dextromethorphan to its metabolite, dextrorphan, in urine as a probe for CYP 2D6 activity. Results A 2-fold decrease in the area under the curve for alprazolam plasma concentration vs time (P<.001) and a 2-fold increase in alprazolam clearance (P<.001) were observed following St John's wort administration. Alprazolam elimination half-life was shortened from a mean (SD) of 12.4 (3.9) hours to 6.0 (2.4) hours (P<.001). The mean (SD) urinary ratio of dextromethorphan to its metabolite was 0.006 (0.010) at baseline and 0.014 (0.025) after St John's wort administration (P = .26). Conclusions A 14-day course of St John's wort administration significantly induced the activity of CYP 3A4 as measured by changes in alprazolam pharmacokinetics. This suggests that long-term administration of St John's wort may result in diminished clinical effectiveness or increased dosage requirements for all CYP 3A4 substrates, which represent at least 50% of all marketed medications. 相似文献
14.
Zhang Xiaoxing Yan Lirong Wang Dongxue Li Yan Han Lulu Tian Lei Liu Hong Li Yishi 《中华医学杂志(英文版)》2014,127(14):2571-2577
Background Whether two clopidogrel pretreatment strategies prior to elective percutaneous coronary intervention (PCI): a 300 mg loading dose (LD) in clopidogrel naive patients and a 75 mg maintenance dose (MD) once daily in patients on chronic clopidogrel therapy play the same role in the platelet inhibition in Chinese with different CYP2C19 genotypes remains unknown. We aim to evaluate the impact on platelet inhibition by clopidogrel pretreatment strategy and its interaction effect with CYP2C19 genotype. Methods Chinese patients undergoing PCI (n=840) were assigned to 2x2 groups in the trial according to different clopidogrel pretreatment strategies (470 patients in LD, 370 patients in MD) and CYP2C19 genotypes (494 carriers of any CYP2C19 *2 or *3 loss-of-function allele, 346 non-carriers). The primary outcome was platelet aggregation (PA) as measured by the 10 umol/L adenosine diphosphate induced light transmission aggregation. Results Compared with MD group, LD strategy showed a significantly higher PA-((59.22+11.67)% vs. (52.83±12.17)%, P 〈0.01), similar PA difference was observed in CYP2C19 loss-of-function carriers compared with non-carriers ((59.41±10.91)% vs. (52.10±12.90)%, P 〈0.01). LD patients in either the CYP2C19 loss-of-function allele carrier or non- carrier group showed a significantly higher PA compared with MD group ((61.50±10.61)% vs. (56.84±10.74)%, P 〈0.01; (56.06±12.34)% vs. (46.88±11.78)%, P 〈0.01, respectively). A quantitative interaction effect was observed between clopidogrel pretreatment strategy and CYP2C19 genotype (P=0.001). Conclusion The 300 mg LD strategy results in a decreased effect on platelet inhibition compared with the 75 mg MD in Chinese patients receiving clopidogrel prior to PCI, especially in the CYP2C19 *2 or *3 loss-of-function allele non-carriers. (ClinicalTrials.gov number NCT01710436) Chin tided J 2014;127 (14): 2571-2577 相似文献
15.
目的 :探讨代谢酶CYP1B1基因CYP1B1*2 142 C/G,CYP1B1*2 355 G/T,CYP1B1*3 4326 C/G多态性与北方地区汉族人群喉癌易感性的关系。方法:采用病例-对照研究的方法,运用多重聚合酶链反应方法(Multi-PCR)及基质辅助激光解析-飞行时间质谱分析技术(MALDI-TOF MS)对200例北方地区汉族人群喉癌患者和200例健康对照组外周血DNA中CYP1B1*2 142 C/G、355 G/T,CYP1B1*3 4326 C/G基因进行多态性研究,并分析上述基因位点之间及基因和烟酒的联合作用与喉癌发生风险的关联强度。结果:携带CYP1B1*2 355 G/T突变型基因型的病例组患病风险高于对照组(OR=2.281,95%CI: 1.142~3.516,P<0.001),携带CYP1B1*3 4326 C/G突变型基因型的病例组患病风险低于对照组(OR=0.571,95%CI: 0.370~0.882,P=0.011)。C142T355C4326单倍体型具有协同效应,显著增加喉癌风险(Adjusted OR=3.180,95%CI:1.760~5.746,P<0.001)。在非吸烟及吸烟者中携带CYP1B1*2 355 G/T突变型等位基因的危险度OR分别为2.080(95%CI: 0.742~5.830)、6.322(95%CI: 2.541~15.725,P<0.001)。结论:CYP1B1基因的多态性与喉癌患病风险密切相关。CYP1B1*2 355 G/T突变型基因是喉癌的风险基因,CYP1B1*3 4326 C/G突变型基因是喉癌的保护基因。CYP1B1*2 142 C/G基因多态性与喉癌易感性无相关性。基因与基因之间具有协同作用,风险基因越多患癌风险越大。烟酒与基因之间无相互协同效应。 相似文献
16.
TANG Xiao-fang ZHANG Jia-hui WANG Jing HAN Ya-ling XU Bo QIAO Shu-bin WU Yong-jian 《中华医学杂志(英文版)》2013,126(6):1069-1075
Background The CYP2C19 G681A single polymorphism has been proven to affect clopidogrel responsiveness.However,the effect of coexisting polymorphisms of other genes has not yet been reported in the Chin... 相似文献
17.
目的 探讨CYP2D6*10等位基因C188T和G4268C位点单核苷酸多态性与肺癌遗传易感性的关系.方法 采用PCR-RFLP法检测118例肺癌患者和按性别、年龄频数匹配的118名正常对照者CYP2D6基因C188T和G4268C位点的单核苷酸多态性,Logistic回归分析各基因型与肺癌发病危险的关系以及基因多态与吸烟在肺癌发生中的联合作用.结果 非T188/T(C188/C C188/T)基因型和非CA268/C(G4268/G G4268/C)基因型与肺癌均有中等强度关联.按照吸烟情况进行分层分析后发现,不吸烟者、轻度吸烟者中携带非T188/T基因型或非CA268/C基因型的个体患肺癌风险增高.但是CYP2D6非T188/T基因型或非CA268/C基因型与吸烟在肺癌的发生中均不存在交互作用,CYP2D6C188T、G4268C两位点之间也不存在交互作用.结论 T188/T和C4268/C基因型在不吸烟者和轻度吸烟者中可能作为保护因素而降低肺癌易感性. 相似文献
18.
目的 建立CYP1A2基因-3860G >A、-3113G >A、-2467delT、-739T >G、-163C >A、2321G >C、5347C >T等7个SNP位点的检测方法,探讨7个SNP位点在华北地区人群中的分布。方法 选取健康受试者,提取全血样本DNA,以Primer Premier 5软件自设计引物及探针,采用扩增阻滞突变系统(ARMS)结合TaqMan探针技术(ARMS-TaqMan法)建立CYP1A2基因7个SNP位点基因分型方法。结果 -3860G >A、-3113G >A、-2467delT、-739T >G、-163C >A、2321G >C、5347C >T7个SNP位点的突变等位基因频率分别为0.292、0.078、0.524、0.078、0.657、0.148、0.127。结论 成功建立7个SNP位点的ARMS-TaqMan基因分型方法,该方法具有准确、操作简单、高通量等优势。 相似文献
19.
目的:探讨代谢酶CYP1B1基因CYP1B1*2142C/G,CYP1B1*2355G/T,CYP1B1*34326C/G多态性与北方地区汉族人群喉癌易感性的关系。方法:采用病例-对照研究的方法,运用多重聚合酶链反应方法(Multi—PCR)及基质辅助激光解析-飞行时间质谱分析技术(MALDI—TOFMS)对200例北方地区汉族人群喉癌患者和200例健康对照组外周血DNA中CYP1B1*2142c/G、355G/T,CYP1B1*34326c/G基因进行多态性研究,并分析上述基因位点之间及基因和烟酒的联合作用与喉癌发生风险的关联强度。结果:携带CYP1B1*2355G/T突变型基因型的病例组惠病风险高于对照组(0R=2.281,95%CI:1.142~3.516,P〈0.001),携带CYP1B1*34326c/c突变型基因型的病例组患病风险低于对照组(0R=0.571,95%CI:0.370~0.882,P=-0.011)。C142T355C4326单倍体型具有协同效应,显著增加喉癌风险(AdjustedOR=3.180,95%CI:1.760~5.746,P〈0.001)。在非吸烟及吸烟者中携带CYP1B1*2355G/T突变型等位基因的危险度OR分另U为2.080(95%CI:0.742—5.830)、6.322(95%CI:2.541~15.725,尸〈0.001)。结论:CYP1B1基因的多态性与喉癌患病风险密切相关。CYP1B1*2355G/T突变型基因是喉癌的风险基因,CYP1B1*34326C/G突变型基因是喉癌的保护基因。CYP1B1*2142c/G基因多态性与喉癌易感性无相关性。基因与基因之间具有协同作用,风险基因越多惠癌风险越大。烟酒与基因之间无相互协同效应。 相似文献
20.
目的 分析武汉地区消化系统疾病患者CYP2C19 基因的多态性。方法 选取2016 年1 月—
2017 年12 月于湖北省武汉市第三医院行CYP2C19 基因多态性检测的无血缘关系汉族消化系统疾病患者314
例。采用实时荧光定量聚合酶链反应检测质子泵抑制剂代谢相关酶CYP2C19 基因型,根据基因型判断代谢表
型,并分析性别、年龄及消化系统疾病临床分型与CYP2C19 基因多态性的相关性。结果 该研究共检测到8
种基因型:CYP2C19 *1*17、*1*1、*1*2、*1*3、*2*17、*3*17、*2*2 及*2*3 ;4 种代谢表型:超快代谢型
为0.96%,快代谢型型为36.94%,中间代谢型型为45.54%,慢代谢型型为16.56%。不同年龄、性别及消化系统
疾病临床分型患者CYP2C19 基因型比较,差异无统计学意义(P >0.05);不同性别、消化系统疾病临床分型
患者代谢表型比较,差异无统计学意义(P >0.05);不同年龄患者代谢表型比较,差异有统计学意义(P <0.05)。
结论 武汉地区消化系统疾病患者CYP2C19 基因具有多态性,其等位基因频率和代谢表型分布情况与亚洲
人群接近,与欧洲等其他国家人群存在明显差异。 相似文献