Uridine diphosphate glucuronosyltransferase 1A1 prevents the progression of liver injury

BACKGROUND Uridine diphosphate glucuronosyltransferase 1A1(UGT1A1)plays a crucial role in metabolizing and detoxifying endogenous and exogenous substances.However,its contribution to the progression of liver damage remains unclear.AIM To determine the role and mechanism of UGT1A1 in liver damage progression.METHODS We investigated the relationship between UGT1A1 expression and liver injury through clinical research.Additionally,the impact and mechanism of UGT1A1 on the progression of liver injury was analyzed through a mouse model study.RESULTS Patients with UGT1A1 gene mutations showed varying degrees of liver damage,while patients with acute-onchronic liver failure(ACLF)exhibited relatively reduced levels of UGT1A1 protein in the liver as compared to patients with chronic hepatitis.This suggests that low UGT1A1 levels may be associated with the progression of liver damage.In mouse models of liver injury induced by carbon tetrachloride(CCl_(4))and concanavalin A(ConA),the hepatic levels of UGT1A1 protein were found to be increased.In mice with lipopolysaccharide or liver steatosis-mediated liver-injury progression,the hepatic protein levels of UGT1A1 were decreased,which is consistent with the observations in patients with ACLF.UGT1A1 knockout exacerbated CCl_(4)-and ConA-induced liver injury,hepatocyte apoptosis and necroptosis in mice,intensified hepatocyte endoplasmic reticulum(ER)stress and oxidative stress,and disrupted lipid metabolism.CONCLUSION UGT1A1 is upregulated as a compensatory response during liver injury,and interference with this upregulation process may worsen liver injury.UGT1A1 reduces ER stress,oxidative stress,and lipid metabolism disorder,thereby mitigating hepatocyte apoptosis and necroptosis.

云南地区53例先天性高胆红素血症临床特征及UGT1A1基因多态性分析

目的探讨云南地区53例UGT1A1基因突变所致的先天性高胆红素血症(Gilbert综合征、Crigler-Najjar综合征)的临床特征及UGT1A1基因突变特点。方法选取2017年1月至2022年12月间昆明市儿童医院消化内科53例Gilbert综合征(GS组)、Crigler-NajjarⅡ型综合征(CN-2组)患儿的临床数据、UGT1A1基因突变结果,回顾性分析患儿的临床特征、实验室检查结果和基因多态性。结果少数民族患儿均在2组中发病率较高,CN-2组中女性比例比GS高。肝脏系统方面,CN-2组TBil、IDB水平较GS组更高,差异均有统计学意义(P<0.05),GS组肝脏结构正常,CN-2组有3例患者肝胆结构有异常。肝外系统方面,血液系统、糖代谢无异常,血脂、甲状腺功能代谢有异常,GS组有维生素D不足,CN-2组存在维生素A、D缺乏及维生素E水平下降。2组患儿均存在心脏结构异常,但CN-2组较GS组发病率高。在所有患者中,突变频率最高的为发生在5号外显子上的c.1456T>G(32例,60.37%),其次为c.1091C>T(14例,26.42%)、1号外显子c.211G>A(6例,11.32%)和c.1198A>C(4例,7.55%)。c.1456T>G位点突变在GS组和CN-2组的频率分别为69.23%和57.5%(9例和23例),2组间差异无统计学意义(P>0.05)。2组中,其次突变频率较高的为c.1091C>T(4例和10例),2组间差异无统计学意义(P>0.05)。UGT1A1基因单倍型1、3、4在GS组和CN-2组间的频率差异均有统计学意义(P<0.05)。UGT1A1基因的4种主要突变形式,在性别和不同民族间,差异无统计学意义(P>0.05)。结论GS组和CN-2组在肝脏系统、肝外系统的临床表现存在不同,UGT1A1基因突变频率最高的为发生在5号外显子上的c.1456T>G。

烟草UGT92A1基因的全基因组鉴定和表达分析

为探究尿苷二磷酸(uridine diphosphate,UDP)-依赖性糖基转移酶(UGT)在烟叶适应环境中的作用,以拟南芥UGT92A1基因为参考,对烟草、番茄、马铃薯的UGT92A1基因进行全基因组鉴定,随后对鉴定到的候选基因进行蛋白理化性质、系统进化、染色体定位、基因结构的分析。此外,通过顺式作用元件分析,以及对云烟87、韭菜坪2号这2个烟草品种的UGT92A1基因在达依、可乐、铁匠这3个烟叶产区的基因表达差异分析,预测烟草UGT92A1基因家族的关键基因成员。结果显示,从烟草、番茄、马铃薯中分别鉴定到9、2、7个同源基因,系统发育树将其按亲缘关系分为3组;基因结构分析显示,4个物种中19个UGT92A1基因都具有UDPGT结构域,但结构域的结构和长度差异较大;顺式作用元件分析显示,烟草UGT92A1基因启动子区域含有大量光响应元件,此外还包含低温响应、缺氧诱导、干旱、创伤反应等非生物胁迫相关元件;转录组测序结果表明,NtUGT92A1-2、NtUGT92A1-7、NtUGT92A1-8这3个基因的表达量相对较高,且其表达均显著受烟叶产区的影响。综上,本研究在烟草中共鉴定到9个UGT92A1基因,其中NtUGT92A1-2、NtUGT92A1-7、NtUGT92A1-8这3个基因可能是烟草适应不同环境的关键基因,后续可进行深入研究。

结直肠癌患者UGT1A1基因多态性与伊立替康不良反应的相关性研究进展

结直肠癌(CRC)是消化系统中常见的恶性肿瘤,其发病率和死亡率在全球恶性肿瘤中均位列前位。FOLFRIL方案即以伊立替康(CPT-11)为基础的联合化疗方案是晚期结直肠癌患者的标准一线治疗方案,但伊立替康治疗常伴有明显的不良反应,也正是因为这样才导致没有得到大范围的临床应用。通过进一步了解后得到出现这一现象的主要原因在于伊立替康存在活性产物7-乙基10-羟基喜树碱(SN-38)。在人体内,SN-38被尿苷二磷酸葡萄糖醛酸转移酶(UGTs)催化形成其无活性代谢物葡萄糖醛酸苷(SN-38G),通过肾脏和肠道排出体外,以达到解毒的目的。目前已经有相关研究证实UGT1A1基因多态性与伊立替康化疗毒性有关,存在UGT1A1基因突变的患者,其UGTs酶活性减弱,导致SN-38代谢延迟,在患者体内蓄积引发不良反应,影响患者生活质量,更有可能导致抗癌治疗中断和临床死亡。因此在接受伊立替康治疗的患者中,将UGT1A1基因型视为毒性预测因子,并实施个体化治疗策略,避开相关风险,是临床亟待解决的问题。本文将对晚期结直肠癌患者UGT1A1基因多态性与伊立替康不良反应之间的关系进行研究,对国内外文献进行综述。

Postoperative jaundice related to UGT1A1 and ABCB11 gene mutations:A case report and literature review

BACKGROUND Patients with obstructive jaundice caused by intrahepatic bile duct stones can be effectively managed by surgery.However,some patients may develop postope-rative complications,liver failure,and other life-threatening situations.Here,we report a patient with mutations in the uridine 5’-diphospho-glucuronosyltrans-ferase 1A1(UGT1A1)and bile salt export pump(adenosine triphosphate-binding cassette subfamily B member 11,ABCB11)genes who presented multiple intrahe-patic bile duct stones and cholestasis,and the jaundice of the patient increased after partial hepatectomy.CASE SUMMARY A 52-year-old male patient admitted to the hospital on October 23,2021,with a progressive exacerbation of jaundice,was found to have multiple intrahepatic bile duct stones with the diagnoses of obstructive jaundice and acute cholecystitis.Subsequently,the patient underwent left hepatectomy with biliary exploration,stone extraction,T-tube drainage,and cholecystectomy without developing any intraoperative complications.The patient had a dark urine color with worsening jaundice postoperatively and did not respond well to plasma exchange and other symptomatic and supportive treatments.Since the progressive increase in postoperative bilirubin could not be clinically explained with any potential reason,including,if not at all,viral infection,cholangitis,autoimmune liver disease,and other causes,the patient underwent whole-exon screening for any genetic diseases,which surprisingly identified UGT1A1 and ABCB11 gene mutations related to glucuronidation of indirect bilirubin as well as bile acid transport in hepatocytes,respectively.Thus,we hypothesized that postoperative refractory cholestasis might result from UGT1A1 and ABCB11 gene mutations and further recommended liver transplantation to the patient,who eventually declined it and died from liver failure six months later.CONCLUSION Surgery may aggravate cholestasis in patients with multiple intrahepatic bile duct stones and cholestasis associated with UGT1A1 and ABCB11 gene mutations.A liver transplant may be the best option if active medical treatment fails.

Gilbert综合征与UGT1A1基因突变的研究进展

Gilbert综合征(Gilbert syndrome, GS)是一种以反复、轻度高间接胆红素血症为特征的常染色体隐性遗传病,尿苷二磷酸葡糖醛酸基转移酶1A1 (uridine diphosphate glucuronosyl transferase 1A1, UGT1A1)基因突变所导致UGT1A1酶的活性降低是Gilbert综合征的主要发病机制。GS诊断主要依据临床表现及实验室检查,在排除溶血及其他肝脏疾病后进行UGT1A1基因检测确诊。UGT1A1的基因突变是确定不明来源的高胆红素血症病因的重要步骤,分子诊断避免了肝穿刺等侵袭性的诊断方法,在疾病早期即可建立正确的治疗程序。除肝脏疾病外,GS患者中UGT1A1基因突变还参与其他多系统疾病的发病及相关药物代谢过程。本文对GS诊治及UGT1A1基因突变与GS关系研究进展进行综述。

真核表达肝药酶UGT1A9可溶重组蛋白方法探索

UDP-葡萄糖醛酸基转移酶(UGTs)是人体重要的肝脏药物代谢酶,其底物选择性、催化机制等研究因难以获得可溶性全酶而受到限制.本研究以制备UGT1A9可溶重组蛋白为研究目标,通过筛选重组蛋白表达体系、融合标签种类及linker长度,优化重组蛋白表达纯化条件和方法,实现了重组UGT1A9的大量制备.HEK293F细胞分泌表达的His8-MBP-NSAS-UGT1A9(氨基酸25-466)重组蛋白经Ni-TED亲和纯化介质从培养基上清液中分离,洗脱产物经SDS-PAGE、Western blot及MS检测鉴定为目的蛋白,通过Bradford法测得重组蛋白最终产量为2 mg/L,纯度达到95%以上.本研究建立了一种人源药物代谢酶UGT1A9的可溶重组蛋白表达纯化方法,为UGT1A9及UGTs同工酶的药物代谢、催化机制及结构解析研究奠定基础.

UGT1A1基因突变与多例延迟晚发特异性黄疸探索研究

目的 探索研究UGT1A1基因突变与多例延迟晚发特异性黄疸的关系。方法 选取我院2022年2月1日至2023年3月1日期间临床诊断70例迁延性黄疸新生儿为观察组,65例无黄疸新生儿为对照组,采用PCR法检测Gly71Arg位点突变类型,对比两组间等位基因频率差异。结果 两组新生儿基因型分布存在差异(χ^(2)检验,P<0.05),其中突变型观察组占比48.57%(34例)显著高于对照组占比24.62%(16例)(χ^(2)检验,P<0.05);等位基因频率比较中观察组Arg基因频率(29.29%)显著高于对照组(13.85%)(χ^(2)检验,P<0.05);Gilbert综合征发病风险观察组42例(60.00%)显著高于对照组12例(18.46%)(χ^(2)检验,P<0.05);72h后观察组总胆红素均值396.37±79.15μmol/L显著高于对照组总胆红素均值305.21±41.34μmol/L(χ^(2)检验,P<0.05)。结论 UGT1A1基因Gly71Arg点突变及多态性与新生儿延迟晚发特异性黄疸有极为紧密的关联,同时由基因突变引发的Gilbert综合征也会增加新生儿迁延性黄疸的发病风险,故UGT1A1基因多态性研究具有极高的临床价值,对疾病病因寻找,早期预防、早期治疗、早期干预显得非常重要。

Link between colorectal cancer and polymorphisms in the uridine-diphosphoglucuronosyltransferase 1A7and 1A1 genes

AIM: To investigate the relationship between single nucleotide polymorphisms in the uridine-diphosphoglucurono-syltransferase (UGT) UGT1A7 and UGT1A1 genes and patients suffering from colorectal cancer (CRC). METHODS: A case-control study was designed in order to investigate the genotypes of the UGT1A7 and UGT1A1 genes, which were identified by the polymerase chain reaction-restriction fragment length polymorphism (RFLP) method, for 268 CRC patients and 441 healthy controls. RESULTS: The results of simple logistical regressions revealed odds ratios (ORs) of 1.97 (P<0.001),1.91 (P<0.001),and 2.03 (P<0.001) for patients who carried the UGT1A7*1/*3 genotype,UGT1A7*3 allele,and variant-211 UGT1A1 allele.The interaction of UGT1A7*3 allele and variant-211 UGT1A1 allele produced an additive effect on the risk for the development of CRC [observed OR (2.34) greater than expected OR (1.59)]. For the 268 patients, the results of simple logistical regressions indicated that the OR of developing metastases was 4.90 (P<0.001) and 4.89 (P<0.001) for the individuals possessing UGT1A7*3 allele and variant-211 UGT1A1 allele, respectively. The results of multivariate logistical regressions confirmed these findings (OR = 2.51, P= 0.01; and OR=2.71,P=0.01,respectively).The interaction of these two variants resulted in an additive effect on the risk for metastases amongst patients [observed OR (6.83) greater than expected OR (4.56)]. CONCLUSION: In conclusion, carriage of the UGT1A7*3 allele, as well as variant-211 UGT1A1 allele represents a risk factor for the development of, and a determinant for, metastases associated with CRC patients.

No association between cyclooxygenase-2 and uridine diphosphate glucuronosyltransferase 1A6 genetic polymorphisms and colon cancer risk

AIM：To investigate the association of variations in the cyclooxygenase-2 （COX2） and uridine diphosphate glucuronosyltransferase 1A6 （UGTIA6） genes and non-steroidal anti-inflammatory drugs （NSAIDs） use with risk of colon cancer.METHODS： NSAIDs, which are known to reduce the risk of colon cancer, act directly on COX2 and reduce its activity. Epidemiological studies have associated variations in the COX2 gene with colon cancer risk, but others were unable to replicate this finding. Similarly,enzymes in the UGT1A6 gene have been demonstrated to modify the therapeutic effect of NSAIDs on colon adenomas. Polymorphisms in the UGTIA6 gene have been statistically shown to interact with NSAID intake to influence risk of developing colon adenomas, but not colon cancer. Here we examined the association of tagging single nucleotide polymorphisms （SNPs） in the COX2 and UGTIA6 genes, and their interaction with NSAID consumption, on risk of colon cancer in a population of 422 colon cancer cases and 481 population controls.RESULTS： No SNP in either gene was individually statistically significantly associated with colon cancer, nor did they statistically significantly change the protective effect of NSAID consumption in our sample. Like others, we were unable to replicate the association of variants in the COX2 gene with colon cancer risk （P 〉 0.05）,and we did not observe that these variants modify the protective effect of NSAIDs （P 〉 0.05）. We were able to confirm the lack of association of variants in UGT1A6 with colon cancer risk, although further studies will have to be conducted to confirm the association of these variants with colon adenomas.CONCLUSION： Our study does not support a role of COX2 and UGTIA6 genetic variations in the development of colon cancer.

Polymorphisms of uridine-diphosphoglucuronosyltransferase 1A7 gene in Taiwan Chinese

AIM: Single nucleotide polymorphisms (SNPs) of uridinediphosphoglucuro -nosyltransferase 1A7 (UGT1A7) gene are associated with the development of orolaryngeal cancer, hepatocellular carcinoma, and colorectal cancer. We performed this research to establish the techniques for determining UGT1A7 gene and basic data of this gene for Taiwan Chinese. METHODS: We collected blood samples from 112 healthy adults and 505 subjects carrying different genotypes of UGT1A1, and determined the promoter area and the entire sequence of UGT1A7 exon 1 by polymerase chain reaction. We designed appropriate primers and restriction enzymes to detect variant UGT1A7 genotypes found in the study subjects. RESULTS: Six SNPs at nucleotides 33, 387, 391, 392, 622, and 756 within the coding region of UGT1A7 exon 1 were found. The incidence of UGT1A7*l/*2 (N129R131W208/ K129K131W208) was predominant (35.7%) while that of UGT1A7 *3/*3 (K129K131R208/K129K131R208) was the least (2.7%). The allele frequency of UGT1A7*3, which exists in a considerable proportion of Caucasians (0.361) and Japanese (0.255), was identified only to be 0.152 in our study subjects. A novel variation at nucleotide -57 in the upstream was found, which was associated with SNPs at nucleotides 33, 387, 391, 392, and 622 in one of the variant haplotypes. The nucleotide changes at positions 387, 391, 392 and 756 were in linkage in another variant haplotype. The allele frequency of UGT1A7*3 was 0.018, 0.158, 0.242, 0.433, and 0.920 in subjects carrying wild, A(TA)6TAA/A(TA)7TAA, A(TA)7TAA/A(TA)7TAA, 211G/211A, and 211A/211A variants of UGT1A1 gene, respectively. By using natural or mutagenesis primers, we successfully detected the variations at nucleotides -57, 33, 387, and 622 with the restriction enzymes HpyCH4 Ⅳ, TaqⅠ, AflⅡ, and Rsa Ⅰ, respectively. CONCLUSION: The results indicate that the allele frequencies of UGT1A7 gene in Taiwan Chinese are different from those in Caucasians and Japanese. Carriage of the nucleotide 211- variant UGT1A gene is highly associated with UGT1A7*3. The restriction-enzymedigestion method for the determination of nucleotides-57 (or 33, or 622) and 387 can rapidly identify genotypes of UGT1A7 in an individual.

中国人UGT1A1＊28的基因多态性以及与伊立替康毒性和疗效的关系

【目的】研究中国肿瘤患者UGT1A1的基因多态性与伊立替康的化学治疗在进展期消化道肿瘤患者不良反应的发生率和严重程度的关系。【方法】采用PCR法扩增目的基因片段,直接测序法分析UGT1A基因多态性的方法,检测2010年3月至2011年3月在我院住院治疗的317例肿瘤患者UGT1A1基因多态性的分布情况,并对其中44例采用含伊立替康方案化疗的进展期胃肠肿瘤患者,观察并记录化疗中出现的不良反应情况,比较不同基因型患者使用伊立替康后Ⅲ度以上不良反应发生率的差异。【结果】317例恶性肿瘤患者中UGT1A1基因启动子区TA序列6次重复的纯合野生型TA6/6有250例(78.9%);基因型为TA序列6次和7次重复的杂合型TA6/7有59例(18.6%);基因型TA序列7次重复的纯合突变型TA7/7有8例(2.5%)。在44例采用含伊立替康方案化疗的进展期胃肠肿瘤患者中,TA6/6、TA6/7和TA7/7各基因型发生Ⅲ度以上中性粒细胞减少者分别为8.6%、12.5%和100%;发生Ⅲ度以上腹泻者分别为14.3%、12.5%和100%。【结论】中国患者UGT1A1*28多态性频率低,TA7/7纯合变异型患者应用伊立替康化疗发生Ⅲ度以上中性粒细胞减少和腹泻的风险增加,而TA6/7杂合子与TA6/6野生型相似,并不增加患者发生Ⅲ度以上中性粒细胞减少和腹泻的风险,对野生型TA6/6能否通过筛查,选择合适患者适当增加伊立替康剂量以提高疗效,值得临床进一步深入研究。

UGT1A1*28基因多态性与中药预防伊立替康腹泻效果的关系

目的:探讨中药对伊立替康化疗后腹泻的预防作用,同时结合尿苷二磷酸葡萄糖醛酸转移酶1A1*28(UGT1A1*28)基因多态性进行中药疗效分析。方法:自2011年10月至2013年5月共200例患者被随机分为对照组(单纯化疗)和中药组(化疗联合中药)。全部患者在化疗开始前均接受UGT1A1*28基因多态性的检测。化疗采用标准FOLFIRI方案,中药于化疗前2 d开始服用,至伊立替康化疗后第5天结束。期间记录患者不良反应,并进行疗效评价。结果:200例患者中TA6/6野生基因型144例,非野生基因型56例(TA7/7纯合型12例和TA6/7杂合型44例)。2级以上腹泻者共58例,中药组腹泻发生率较对照组下降14%(22%vs.36%,P=0.029)。除腹泻以外,2级以上呕吐发生率中药组也明显低于对照组(15%vs.27%,P=0.037)。患者总体有效率为37.5%,中药组和对照组相比差异无统计学意义(40%vs.35%,P=0.465)。UGT1A1*28野生基因型患者2级以上腹泻发生率(22.9%vs.44.6%,P=0.002)和呕吐发生率(16.7%vs.23.2%,P=0.016)均低于与非野生基因型患者。在中药治疗组中,非野生基因型与野生型相比,2级以上腹泻发生率(22.2%vs.21.9%,P=0.974)和呕吐发生率(18.5%vs.13.7%,P=0.777)差异无统计学意义。结论:中药可有效预防伊立替康引起的迟发性腹泻,对于UGT1A1*28非野生基因型患者的迟发性腹泻同样具有预防作用。UGT1A1*28基因非野生基因型腹泻发生率明显高于野生基因型,在使用伊立替康治疗前应检测患者的该基因状态。

UGT1A1基因多态性与转移性结直肠癌伊立替康化疗毒性及疗效的关系

目的:探讨UGT1A1*28和UGT1A1*6基因多态性与伊立替康治疗转移性结直肠癌患者的不良反应和疗效之间的关系。方法:外周血中抽提基因组DNA,采用PCR扩增目的基因片段,直接测序法分析2010年4月至2012年3月在我院做基因检测的207例消化道肿瘤患者UGT1A1*28和UGT1A1*6基因多态性的分布情况,并对其中56例采用含伊立替康方案化疗的转移性结直肠癌患者出现的不良反应情况、肿瘤进展时间及化疗疗效进行观察并记录,比较不同基因型患者之间的差异。结果:207例消化道肿瘤患者中,UGT1A1*28位点野生型TA6/6有164例(79.2%),杂合突变型TA6/7有41例(19.8%),纯合突变型TA7/7有2例(1.0%);UGT1A1*6位点野生型G/G有154例(74.4%),杂合突变型G/A有51例(24.6%),纯合突变型A/A有2例(1.0%)。在56例转移性结直肠癌患者中,*6位点突变型(G/A和A/A)可以增加发生3级以上腹泻(38.9%vs 7.9%,P<0.05)和中性粒细胞减少(61.1%vs 29.0%,P<0.05)的风险;*28位点突变型(6/7和7/7)可以增加发生3级以上血小板减少(33.3%vs 2.1%,P<0.05)的风险;肿瘤进展时间和化疗疗效在*28和*6位点各基因型之间差异无统计学意义。结论:在采用含伊立替康方案化疗的转移性结直肠癌患者中,UGT1A1*6位点突变型增加发生3级以上腹泻和中性粒细胞减少的风险;UGT1A1*28位点突变型增加发生3级以上血小板减少的风险。

中国部分地区肿瘤患者UGT1A1*28和UGT1A1*6位点基因多态性分布的差异研究

目的调查我国部分地区肿瘤患者UGT1A1^＊28和UGT1A1^＊6位点基因多态性分布情况,明确二者在肿瘤患者中分布的差异。方法收集2011年8月—2014年4月山东大学附属临沂市人民医院、临沂市肿瘤医院、兰州大学第一附属医院、西安交通大学第一附属医院、西京医院应用伊立替康治疗的住院肿瘤患者241例,均进行了UGT1A1^＊28位点基因多态性检测,其中177例同时进行了UGT1A1^＊6位点基因多态性检测,提取基因组DNA,PCR扩增UGT1A1基因片段,检测UGT1A1^＊28和UGT1A1^＊6位点基因型分布。结果 241例检测UGT1A1^＊28位点基因多态性的患者中,UGT1A1^＊28位点基因启动子区TA序列呈6次重复的野生型（TA6/6）即野生型纯合子180例（74.7%）,TA序列6次和7次重复的杂合突变型（TA6/7）即突变型杂合子56例（23.2%）,TA序列7次重复的纯合突变型（TA7/7）即突变型纯合子5例（2.1%）;177例检测UGT1A1^＊6位点基因多态性的患者中,UGT1A1^＊6位点基因型为野生型（G/G）即野生型纯合子106例（59.9%）,杂合突变型（G/A）即突变型杂合子62例（35.0%）,纯合突变型（A/A）即突变型纯合子9例（5.1%）。UGT1A1^＊28和UGT1A1^＊6位点基因型分布比较,差异有统计学意义（P〈0.05）。不同性别、年龄、肿瘤部位、地区来源肿瘤患者UGT1A1^＊28位点基因型分布比较,差异均无统计学意义（P〉0.05）。不同性别、年龄、地区来源肿瘤患者UGT1A1^＊6位点基因型分布比较,差异均无统计学意义（P〉0.05）;不同肿瘤部位患者UGT1A1^＊6位点基因型分布比较,差异有统计学意义（P〈0.05）。男性、〈40岁、肠道、山东地区、甘肃地区肿瘤患者UGT1A1^＊28与UGT1A1^＊6位点基因型分布比较,差异有统计学意义（P〈0.05）;女性、40~60岁、〉60岁、肺部、胃部、其他部位、陕西地区、其他地区肿瘤患者UGT1A1^＊28与UGT1A1^＊6位点基因型分布比较,差异无统计学意义（P〉0.05）。结论国内肿瘤患者中UGT1A1^＊28和UGT1A1^＊6位点基因野生型纯合子频率均较高,但两位点基因型分布有差异,所以研究UGT1A1基因与伊立替康毒副作用时应联合检测UGT1A1^＊28和UGT1A1^＊6两个突变位点,并且应同时注意患者的性别、年龄、肿瘤部位及地区来源。

UGT1A6、UGT1A9基因多态性对汉族癫痫患者丙戊酸血药浓度的影响

目的:考察尿苷二磷酸葡萄糖醛酸转移酶(UGT)1A6和1A9基因多态性对汉族癫痫患者丙戊酸血药浓度的影响。方法:选取2014年1月—2015年4月于我院门诊就诊的汉族癫痫患者107例,均使用丙戊酸单药治疗,治疗时间为3个月~6年。采用酶放大免疫法测定患者体内丙戊酸稳态血药浓度,采用基质辅助激光解吸电离飞行时间质谱法检测其UGT1A6(rs2070959、rs6759892)和UGT1A9(rs13418420、rs2741045、rs2741049、rs6731242、rs72551330)基因型,并考察基因多态性与丙戊酸标准化血药浓度(CDR)的相关性。结果:未检出UGT1A9 rs72551330突变型,其余6个位点基因型频率均符合Hardy-Weinberg平衡(P>0.05)。UGT1A6 rs2070959、rs6759892突变基因携带(AG+GG或TG+GG型)者丙戊酸CDR值显著低于其野生纯合子携带(AA或TT型)者,差异均有统计学意义(P<0.05);而携带UGT1A9 rs13418420、rs2741045、rs2741049和rs6731242野生纯合子和突变基因的患者丙戊酸CDR值比较,差异均无统计学意义(P>0.05)。结论:汉族癫痫患者UGT1A6 rs2070959、rs6759892基因多态性与丙戊酸血药浓度有关,且UGT1A6 rs2070959、rs6759892突变基因携带者可能需要更高的丙戊酸剂量。

UGT1A1基因多态性与伊立替康安全性和有效性的临床研究

目的：观察57例应用伊立替康治疗进展期消化道肿瘤患者的安全性和有效性。方法：采用全血基因组DNA提取、PCR法扩增目的基因片段，直接测序法分析UGT1A1基因多态性，检测2011年8月至2012年6月在河北医科大学第四医院肿瘤内科住院治疗的57例进展期消化道肿瘤患者应用伊立替康的情况，观察并记录化疗中出现的不良反应以及疗效。结果：57例进展期消化道肿瘤患者中，UGT1A1基因启动子区28位点，TA序列6次重复的纯合野生型TA6／6有43例（75．4％）；基因型为TA序列6次和7次重复的杂合型TA6／7有13例（22．8％）；基因型为TA序列7次重复的纯合突变型TA7／7有1例（1．8％）。UGT1A1基因启动子区6位点野生型G／G有48例（84．2％），杂合突变型吲A有7例（12．3％），纯合突变型A／A有2例（3．5％）。在57例采用含伊立替康方案化疗的进展期消化道肿瘤患者中，UGT1A1基因启动子区28位点，TA6／6、TA6／7和TA7／7野生型和突变型发生3级以上中性粒细胞减少者分别为7．0％、14-3％，发生3级以上腹泻者分31j为9．3％、14．3％，其中纯合突变型仅1例患者，100％的发生率。UGT1A1基因启动子区6位点，G／G、G／A和A／A野生型和突变型发生3级以上中性粒细胞减少者分别为4．2％、55．6％，发生3级以上腹泻者分别为12．5％、44．4％，具有统计学差异。各组之间疗效无统计学差异。结论：患者UGT1A1＋28和UGT1A1＋6多态性分布基本一致，UGT1A1＋6突变型患者应用伊立替康化疗发生3级以上中性粒细胞减少和腹泻的风险增加，而UGT1A1＋28突变型与以上不良反应并无绝对相关性，UGT1A1各基因型之间疗效无明显差异。能否通过对UGT1A1的筛查，选择合适患者安全有效的应用伊立替康，值得临床进一步扩大样本量深入研究。

UGT1A1基因多态性与伊立替康治疗结直肠癌不良反应的关系

背景与目的:尿苷二磷酸葡萄糖醛酸转移酶1A1(uridine diphosphoglucu-ronosyl transferase 1A1,UGTlA1)是伊立替康代谢关键酶,其活性受基因多态性影响显著。本研究探讨结直肠癌患者中,UGT1A1*28和UGT1A1*6基因多态性与伊立替康治疗相关不良反应之间的关系。方法:入组2013年4月—2013年12月于复旦大学附属中山医院肿瘤内科接受治疗的消化道恶性肿瘤患者160例。抽提外周血中基因组DNA,分别采用STR方法和Sanger测序法,检测UGT1A1*28和UGT1A1*6基因型,分析UGT1A1基因多态性分布情况。对其中82例化疗方案中含伊立替康的结直肠癌患者进行随访,记录不良反应发生情况和严重程度,比较不同基因型患者之间的差异。结果:160例消化道肿瘤患者中,UTG1A1*28(启动子TATA盒区域TA重复次数)野生型TA6/6124例(77.5%);杂合子TA6/7 33例(20.5%);纯合子TA7/7 3例(2.0%)。UGT1A1*6位点(211G>A)野生型GG 105例(65.6%),杂合子GA 48例(30.0%);纯合子AA 7例(4.4%)。82例化疗方案中含伊立替康的结直肠癌患者中,*28基因型(TA6/7和TA7/7)显著增加发生3级以上中性粒细胞减少的风险(58.3%vs 0.0%,P<0.001),并增加整体不良反应发生率(76.0%vs 45.6%,P<0.001);*6基因型(GA和AA)、年龄、性别、化疗方案和伊立替康相关不良反应发生无显著相关性。结论:接受伊立替康化疗的结直肠癌患者,UGT1A1*28位点多态性显著增加中性粒细胞减少发生的风险,可预测伊立替康引起的骨髓抑制性不良反应,辅助临床选择合适的化疗方案。

UGT1A1*28和UGT1A1*6基因多态性与伊立替康不良反应的关系

目的探讨UGT1A1＊28和UGT1A1＊6基因多态性在中国人中的分布，并评价其与伊立替康不良反应之间的关系。方法收集2011年3月－2012年3月在我科住院治疗的158例恶性肿瘤患者的外周血，检测其UGT1A1＊28和UGT1A1＊6基因型，其中132例使用伊立替康方案化疗，比较不同基因型患者的不良反应差异。结果158例中，UGT1A1＊28野生型TA6／6者126例（79．7％），杂合突变型TA6／7者30例（19．O％），纯合突变型TA7／7者2例（1．3％）；64例进行UGT1A1＊6基因检测，G／G野生型40例（62．5％），G／A杂合突变型23例（35．9％），A／A纯合突变型1例（1．6％）。UGT1A1＊28基因突变可增加2～4级迟发性腹泻发生率（TA6／6者15．0％、TA6／7者34．8％、TA7／7者50．0％，P=0．000）；联合UGT1A1＊28和UGT1A1＊6基因型，野生型（TA6／6且G／G）患者发生2～4级迟发性腹泻和3～4级中性粒细胞减少的概率明显低于单点变异型和双点变异型（13．0％、22．2％、100．0％，P=0．004；8．7％、25．9％、66．7％，P=0．045）。结论UGT1A1＊28和UGT1A1＊6基因突变患者使用含伊立替康化疗方案时不良反应发生率较高。与单一检测一个位点相比，联合检测UGT1A1＊28和UGT1A1＊6基因型能更准确地预测伊立替康不良反应。

根据UGT1A4 142T>G基因多态性和丙戊酸血药浓度定量估算我国汉族癫痫儿童体内拉莫三嗪的血药浓度

目的:探讨尿苷二磷酸葡糖醛酸转移酶(UGT)1A4 142T>G基因多态性和丙戊酸(VPA)血药浓度对我国南方汉族癫痫儿童体内拉莫三嗪(LTG)血药浓度的影响,并建立定量估算LTG血药浓度的预测方程。方法:选取2010年1月-2016年9月于广州市妇女儿童医疗中心就诊的南方汉族癫痫患儿72例,均采用LTG+VPA联合治疗。采用液相色谱-串联质谱法和酶放大免疫分析法分别测定患儿体内LTG和VPA的血药浓度,采用限制性片段长度多态性聚合酶链反应法测定其UGT1A4 142T>G多态性,并考察患儿年龄、性别、VPA血药浓度、UGT1A4 142T>G多态性与LTG标准化血药浓度(CDR)的相关性,并采用多重线性回归分析建立LTG血药浓度的预测方程。结果:患儿年龄、VPA血药浓度与LTG CDR呈正相关(r分别为0.225、0.300,P<0.05);性别对LTG CDR的影响无统计学意义(P>0.05)。共检出UGT1A4 TT、TG、GG基因型各39、29、4例,各基因型频率均符合HardyWeinberg平衡(P>0.05);TT基因型患儿LTG CDR显著低于TG、GG基因型,差异均有统计学意义(P<0.05)。多重线性回归分析结果显示,患儿LTG剂量(x_1)、体质量(x_2)、VPA血药浓度(x_3)、UGT1A4 142T>G多态性(x4)与LTG血药浓度有关(P<0.05);以LTG血药浓度为因变量(c),上述因素为自变量,得回归方程为c=0.794+0.032x_1-0.057x_2+0.010x_3+0.532x_4(R^2=0.616,P<0.05;其中,UGT1A4 TT基因型为0,TG、GG基因型为1),且LTG预测血药浓度和实测血药浓度的相关性良好(r=0.785,P=0.001)。结论:癫痫患儿的LTG剂量、体质量、VPA血药浓度、UGT1A4 142T>G多态性可能与LTG血药浓度有关;本研究建立的预测方程可为我国南方汉族癫痫患儿的精准用药提供参考。