慢性HBV感染者载脂蛋白E基因多态性分析
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摘要
目的
探讨慢性HBV感染者(CHB)外周血白介素-2(IL-2)、γ-干扰素(IFN-γ)活性与病毒载量、肝功能状态以及肝纤维化的关系。
探讨各临床分型HBV感染者ApoE基因多态性的分布情况,并分析其对慢性HBV感染性免疫的影响。
方法
测定慢性HBV感染者外周血Th1型细胞因子IL-2、IFN-γ水平,IL-2检测采用放射免疫法(RIA法),IFN-γ检测采用双抗夹心法(ELISA法)。
对慢性HBV感染者外周静脉抗凝血进行DNA抽提,PCR扩增ApoE基因片段,用荧光偏振的方法检测ApoE基因型。
3、根据病毒载量不同选出低载量组和高载量组;根据病情及肝功能状况分为CHB携带组、轻度组、中度组及重度组;根据有无肝纤维化分为肝硬化组和非肝硬化组;根据ApoE三种基因型不同分为ApoEε2组、ApoEε3组及ApoEε4组。
结果
1、HBV DNA高载量组与低载量组相比IL-2水平显著低下(P﹤0.05),两组间INF-γ水平无明显差异。随着肝功能损害程度增加IL-2含量逐渐降低,INF-γ逐渐增高;与非肝硬化组比较肝硬化组的IL-2的含量显著降低,IFN-γ显著升高(均P﹤0.01)。
2、三种ApoE基因型在慢性HBV感染者中的分布频率ApoEε3:ApoEε4:ApoEε2为0.74:0.16:0.10,与正常人群频率相比无明显差异。轻度组ApoEε4(0.22)高于正常值范围(0.04(0.17),并与中度、重度组相比有显著差异(均P(0.05);肝硬化组与非肝硬化组之间ApoE基因频率无差异;与ApoEε3、ApoEε2组相比ApoEε4组有较高的IL-2和总胆固醇水平。
结论
在乙肝慢性化过程中,IL-2与HBV清除有关,其降低的程度与肝损伤严重程度及肝纤维化相关;IFN-γ的抗病毒作用不明显,但它作为炎症介质参与了肝脏炎症坏死和肝纤维化的形成过程。
高水平的ApoEε4基因可通过调节IL-2和血脂水平减轻HBV感染后引起的肝细胞炎症反应,对抗HBV感染后的肝损伤。
Objective
1. To explore the relationship among IL-2, IFN-γin sera and HBV load , hepatic function condition and liver fibrosis in patients with chronic hepatitis B (CHB).
2. To deserve the frequency distribution of ApoE phenotypes and alleles in chronic HBV infected with different clinical manifestations, and the effects of ApoE gene polymorphism in HBV infective immunity were analyzed.
Methods
1. The quantity of IL-2 and IFN-γin sera were measured, the RIA and ELISA technique were separately used to detect IL-2 and IFN-γ.
2. The blood genome DNA of chronic hepatitis B were extracted, PCR and TDI-FP technique were separately used to copy the ApoE gene and detection of ApoE gene types.
3. According to the virus load the low-quantity group and high-quantity group was choosed out . According to the hepatic function condition the patients was divided into the chronic CHB Virus taking, light-degree, mid-degree and severe-degree group. According to liver fibrosis condition the cirrhosis group and non-cirrhosis group were divided. According to the ApoE gene polymorphism the patients were divided into the ApoEε2 group, ApoEε3 group and ApoEε4 group.
Results
1. Compared with the low-quantity group the IL-2 in high-quantity group was significantly decreased (P﹤0.05), there was no difference of IFN-γ between them. Along with the severer of hepatic function the IL-2 quantity was decreased and the IFN-γ was increased. Compared with the non-cirrhosis group the IL-2 in cirrhosis group was significantly decreased and the IFN-γwas increased(P﹤0.01).
2. The allele frequencies of ApoE in the chronic hepatitis B ApoEε3: ApoEε4: ApoEε2 were 0.74: 0.16: 0.10, There was no significant difference in the chronic HBV-infected compared with previously published population data, however, the frequency of the ApoEε4 in light-degree(0.22) was higher than the population data(0.04(0.17),and compared with the CHB mid-degree and severe-degree groups, it was significantly higher (P﹤0.05).The ApoE allele frequencies were similar in cirrhosis group and non-cirrhosis group. Compared with the ApoEε3 and ApoEε2 the IL-2 and TC in ApoEε4 were higher.
Conclusions
1. The activity of IL-2 shows a beneficial effects on eliminating HBV, the quantity of IL-2 has relationship with liver damage and fibrosis formation. There is no beneficial effects of IFN-γon eliminating HBV, and it can accelerate the liver necrosis and fibrosis formation.
2. The high carriage of ApoEε4 allele may lighten the hepatic inflammatory damage through regulate the quantity of IL-2 and plasma lipid levels in sera.
探讨慢性HBV感染者(CHB)外周血白介素-2(IL-2)、γ-干扰素(IFN-γ)活性与病毒载量、肝功能状态以及肝纤维化的关系。
探讨各临床分型HBV感染者ApoE基因多态性的分布情况,并分析其对慢性HBV感染性免疫的影响。
方法
测定慢性HBV感染者外周血Th1型细胞因子IL-2、IFN-γ水平,IL-2检测采用放射免疫法(RIA法),IFN-γ检测采用双抗夹心法(ELISA法)。
对慢性HBV感染者外周静脉抗凝血进行DNA抽提,PCR扩增ApoE基因片段,用荧光偏振的方法检测ApoE基因型。
3、根据病毒载量不同选出低载量组和高载量组;根据病情及肝功能状况分为CHB携带组、轻度组、中度组及重度组;根据有无肝纤维化分为肝硬化组和非肝硬化组;根据ApoE三种基因型不同分为ApoEε2组、ApoEε3组及ApoEε4组。
结果
1、HBV DNA高载量组与低载量组相比IL-2水平显著低下(P﹤0.05),两组间INF-γ水平无明显差异。随着肝功能损害程度增加IL-2含量逐渐降低,INF-γ逐渐增高;与非肝硬化组比较肝硬化组的IL-2的含量显著降低,IFN-γ显著升高(均P﹤0.01)。
2、三种ApoE基因型在慢性HBV感染者中的分布频率ApoEε3:ApoEε4:ApoEε2为0.74:0.16:0.10,与正常人群频率相比无明显差异。轻度组ApoEε4(0.22)高于正常值范围(0.04(0.17),并与中度、重度组相比有显著差异(均P(0.05);肝硬化组与非肝硬化组之间ApoE基因频率无差异;与ApoEε3、ApoEε2组相比ApoEε4组有较高的IL-2和总胆固醇水平。
结论
在乙肝慢性化过程中,IL-2与HBV清除有关,其降低的程度与肝损伤严重程度及肝纤维化相关;IFN-γ的抗病毒作用不明显,但它作为炎症介质参与了肝脏炎症坏死和肝纤维化的形成过程。
高水平的ApoEε4基因可通过调节IL-2和血脂水平减轻HBV感染后引起的肝细胞炎症反应,对抗HBV感染后的肝损伤。
Objective
1. To explore the relationship among IL-2, IFN-γin sera and HBV load , hepatic function condition and liver fibrosis in patients with chronic hepatitis B (CHB).
2. To deserve the frequency distribution of ApoE phenotypes and alleles in chronic HBV infected with different clinical manifestations, and the effects of ApoE gene polymorphism in HBV infective immunity were analyzed.
Methods
1. The quantity of IL-2 and IFN-γin sera were measured, the RIA and ELISA technique were separately used to detect IL-2 and IFN-γ.
2. The blood genome DNA of chronic hepatitis B were extracted, PCR and TDI-FP technique were separately used to copy the ApoE gene and detection of ApoE gene types.
3. According to the virus load the low-quantity group and high-quantity group was choosed out . According to the hepatic function condition the patients was divided into the chronic CHB Virus taking, light-degree, mid-degree and severe-degree group. According to liver fibrosis condition the cirrhosis group and non-cirrhosis group were divided. According to the ApoE gene polymorphism the patients were divided into the ApoEε2 group, ApoEε3 group and ApoEε4 group.
Results
1. Compared with the low-quantity group the IL-2 in high-quantity group was significantly decreased (P﹤0.05), there was no difference of IFN-γ between them. Along with the severer of hepatic function the IL-2 quantity was decreased and the IFN-γ was increased. Compared with the non-cirrhosis group the IL-2 in cirrhosis group was significantly decreased and the IFN-γwas increased(P﹤0.01).
2. The allele frequencies of ApoE in the chronic hepatitis B ApoEε3: ApoEε4: ApoEε2 were 0.74: 0.16: 0.10, There was no significant difference in the chronic HBV-infected compared with previously published population data, however, the frequency of the ApoEε4 in light-degree(0.22) was higher than the population data(0.04(0.17),and compared with the CHB mid-degree and severe-degree groups, it was significantly higher (P﹤0.05).The ApoE allele frequencies were similar in cirrhosis group and non-cirrhosis group. Compared with the ApoEε3 and ApoEε2 the IL-2 and TC in ApoEε4 were higher.
Conclusions
1. The activity of IL-2 shows a beneficial effects on eliminating HBV, the quantity of IL-2 has relationship with liver damage and fibrosis formation. There is no beneficial effects of IFN-γon eliminating HBV, and it can accelerate the liver necrosis and fibrosis formation.
2. The high carriage of ApoEε4 allele may lighten the hepatic inflammatory damage through regulate the quantity of IL-2 and plasma lipid levels in sera.
引文
病毒性肝炎防治方案(中华医学会传染病与寄生虫病学分会、肝病学分会联合修订).中华传染病杂志,2001,19(1):56(62
Jiang R,Feng X,Guo Y,et al.T helper cells in patients with chronic hepatitis B virus infection.Chin Med J (Engl),2002,115(3):422(444
姜荣龙,卢桥声,骆抗先,等.慢性乙型肝炎病毒感染者外周血T辅助细胞1、2型细胞因子的表达.中华传染病杂志,2000,18(1):26(28
Bataller R,North KE,Brenner DA.Genetic polymorphisms and the progression of liver fibrosis: a critical appraisal.Hepatology,2003,37(3):493~503
赵彩彦,刘金星,汤慧华,等.病毒性肝炎和原发性肝癌IL-2相关指标的意义.华人消化杂志,1998,6(6):479(481
Huang YC,Chen Y,Tian DY.Effect of IFN-αon serum IL-2 and SIL-2R in the patients with chronic hepatitis B.J Clin Intern Med,2000,17(6):362~367
王静艳,孙金良,刘沛,等.乙型病毒性肝炎患者血清TNF-α、IFN-γ、IL-6和IL-8的检测及意义.中国公共卫生,1998,14(5):262~263
顾长海,王宇明.肝功能衰竭.北京:人民卫生出版社,2002,94
Wang Y,Lawson JA,Jaeschke H.Differential effect of α-amino-ethyl-isothioureea, an inhibitor of the inducible nitric oxide synthase, on microvascular blood flow and organ injury in models of hepatic ischermia-reperfusion and endotoxemia.Shock,1998,10(1):20~25
王子强,徐章,李毅,等.TNF-α、IFN-γ在肝纤维化中的发病学意义探讨.医学新知杂志,2000,4(10):184(186
章以法,冯岚,王林伦,等.肝炎肝硬化患者血清IFN-γ水平与 HA、PⅢP、Ⅳ-C、LN水平关系的分析.临床肝胆杂志,2001,17(1):30~31
蔡卫民,陈峰.近年来肝纤维化主要进展(上)—发病机理研究.临床肝胆病杂志,1998,14(1):655~656
周俊英,赵彩彦,甄真,等.病毒性肝炎患者血清IFN-γ与肝纤维化关系的研究.中国免疫学杂志,2000,16(6):333~335
Korhonen T, Hannuksela ML,Seppanen S.The effect of the apolipoprotein E phenotype on cholesteryl ester transfer protein activity, plasma lipids and apolipoprotein AI levels in hypercholesterolaemic patients on colestipol and lovastatin treatment.Eur J Clin Pharmacol ,1999,54(12):903~910
Ginsberg HN.Lipoprotein physiology.Endocrinol Metab Clin North Am,1998,27(3):503~519
张雪梅,刘秉文.载脂蛋白E研究进展.中国动脉硬化杂志,2001,9(2):165~168
Fernndez-Miranda C,Cancelas P,de la Calle A,et al.Changes in Phenotypes of ApoliproteinE and Apoliprotein[a] in liver transplant recipients.Clin transplant,1997,11(4):325~337
王新利,王国荃,徐臻荣,等.新疆维吾尔族长寿老人及长寿家族ApoE等位基因频率分析.中国老年学杂志,1999,19(2):106~108
刘晓春,彭怀燕,覃桂芳.冠心病ApoE基因多态性及其与血清ApoE的关系.上海医学检验杂志,2003,18(1):36~40
苏净,谭兰.载脂蛋白E基因多态性与血管性痴呆的关系.国外医学脑血管病分册,2001,9(4):209~211
曹方,赵瑛.载脂蛋白E与Alzheimer’s病关系的研究进展.医学综述,2001,7(4):206~208
申海莲,刘丽梅,项坤三,等.ApoE基因多态性与中国人2型糖尿病及其肾病并发症的关系.中国糖尿病杂志,2002,10(1):4~6
Schiefermeier M,Kollegger H,made C,etal.The impact of a-polipoprotein E genetypes on ages at onset of symptoms and phenotypic expression in Wilson’s disease.Brain,2002,123(5):585~590
Itzhaiki RF,Irving WL,Wozniak MA,etal.Apolipoprotein E and hepatitis C virus.Hepatology,2003,38(4):1060~1069
顾牛范,冯国鄞,江三多,等.中国汉族ApoE等位基因频率的初步研
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Muros M,Rodriguez-Ferrer C.Apolipoprotein E polymorphism influence on lipids, apolipoproteins and Lp(a) in a Spanish population un-derexpressing apoE4.Atherosclerosis.,1996,121(1):13~21
Bataller R,North KE,Brenner DA.Genetic polymorphisms and the progression of liver fibrosis: a critical appraisal.Hepatology,2003,37(3):493~503.
Percy ME,Potyomkina Z,Dalton AJ,etal.Relation between apolipoprotein E genotype, hepatitis B virus status, and thyroid status in a sample of older persons with Down syndrome.Am J Med Genet,2003,120A(2):191~198
Wozniak MA,Itzhaki RF,Faragher EB,et al.Apolipoprotein E-epsilon 4 protects gainst severe liver disease caused by hepatitis C virus.Hepatology,2002,36(2):456(463
李 晖,李可基,张保惠,等.ApoE基因缺陷鼠免疫、血液、稳态和抗氧化功能改变.北京大学学报(医学版),2001,33(4):347~350
Mistry MJ,Clay MA,Kelly ME,et al.Apolipoprotein E restricts interleukin-dependent T lymphocyte proliferation at the G1A/G1B boundary.Cell Immunol,1995,160(1):14~23
刘春红,夏德全,周廉,等.肝病患者血清载脂蛋白E浓度测定的临床意义.上海医科大学学报,1997,24(6):429~431
范萍,张祖辉,刘宇,等.成都地区362名汉族成人载脂蛋白E表型分布及其与血脂和载脂蛋白之间的关系.华西医科大学学报,1999,30(4):373~374
潘永瑜,胡洁,李冬霞,等.ApoE基因多态性与血脂水平及冠心病的关系.临床内科杂志,2001,18(4):267~269
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Jiang R,Feng X,Guo Y,et al.T helper cells in patients with chronic hepatitis B virus infection.Chin Med J (Engl),2002,115(3):422(444
姜荣龙,卢桥声,骆抗先,等.慢性乙型肝炎病毒感染者外周血T辅助细胞1、2型细胞因子的表达.中华传染病杂志,2000,18(1):26(28
Bataller R,North KE,Brenner DA.Genetic polymorphisms and the progression of liver fibrosis: a critical appraisal.Hepatology,2003,37(3):493~503
赵彩彦,刘金星,汤慧华,等.病毒性肝炎和原发性肝癌IL-2相关指标的意义.华人消化杂志,1998,6(6):479(481
Huang YC,Chen Y,Tian DY.Effect of IFN-αon serum IL-2 and SIL-2R in the patients with chronic hepatitis B.J Clin Intern Med,2000,17(6):362~367
王静艳,孙金良,刘沛,等.乙型病毒性肝炎患者血清TNF-α、IFN-γ、IL-6和IL-8的检测及意义.中国公共卫生,1998,14(5):262~263
顾长海,王宇明.肝功能衰竭.北京:人民卫生出版社,2002,94
Wang Y,Lawson JA,Jaeschke H.Differential effect of α-amino-ethyl-isothioureea, an inhibitor of the inducible nitric oxide synthase, on microvascular blood flow and organ injury in models of hepatic ischermia-reperfusion and endotoxemia.Shock,1998,10(1):20~25
王子强,徐章,李毅,等.TNF-α、IFN-γ在肝纤维化中的发病学意义探讨.医学新知杂志,2000,4(10):184(186
章以法,冯岚,王林伦,等.肝炎肝硬化患者血清IFN-γ水平与 HA、PⅢP、Ⅳ-C、LN水平关系的分析.临床肝胆杂志,2001,17(1):30~31
蔡卫民,陈峰.近年来肝纤维化主要进展(上)—发病机理研究.临床肝胆病杂志,1998,14(1):655~656
周俊英,赵彩彦,甄真,等.病毒性肝炎患者血清IFN-γ与肝纤维化关系的研究.中国免疫学杂志,2000,16(6):333~335
Korhonen T, Hannuksela ML,Seppanen S.The effect of the apolipoprotein E phenotype on cholesteryl ester transfer protein activity, plasma lipids and apolipoprotein AI levels in hypercholesterolaemic patients on colestipol and lovastatin treatment.Eur J Clin Pharmacol ,1999,54(12):903~910
Ginsberg HN.Lipoprotein physiology.Endocrinol Metab Clin North Am,1998,27(3):503~519
张雪梅,刘秉文.载脂蛋白E研究进展.中国动脉硬化杂志,2001,9(2):165~168
Fernndez-Miranda C,Cancelas P,de la Calle A,et al.Changes in Phenotypes of ApoliproteinE and Apoliprotein[a] in liver transplant recipients.Clin transplant,1997,11(4):325~337
王新利,王国荃,徐臻荣,等.新疆维吾尔族长寿老人及长寿家族ApoE等位基因频率分析.中国老年学杂志,1999,19(2):106~108
刘晓春,彭怀燕,覃桂芳.冠心病ApoE基因多态性及其与血清ApoE的关系.上海医学检验杂志,2003,18(1):36~40
苏净,谭兰.载脂蛋白E基因多态性与血管性痴呆的关系.国外医学脑血管病分册,2001,9(4):209~211
曹方,赵瑛.载脂蛋白E与Alzheimer’s病关系的研究进展.医学综述,2001,7(4):206~208
申海莲,刘丽梅,项坤三,等.ApoE基因多态性与中国人2型糖尿病及其肾病并发症的关系.中国糖尿病杂志,2002,10(1):4~6
Schiefermeier M,Kollegger H,made C,etal.The impact of a-polipoprotein E genetypes on ages at onset of symptoms and phenotypic expression in Wilson’s disease.Brain,2002,123(5):585~590
Itzhaiki RF,Irving WL,Wozniak MA,etal.Apolipoprotein E and hepatitis C virus.Hepatology,2003,38(4):1060~1069
顾牛范,冯国鄞,江三多,等.中国汉族ApoE等位基因频率的初步研
究.中国医学遗传学杂志,1996,13(1):8~10
Muros M,Rodriguez-Ferrer C.Apolipoprotein E polymorphism influence on lipids, apolipoproteins and Lp(a) in a Spanish population un-derexpressing apoE4.Atherosclerosis.,1996,121(1):13~21
Bataller R,North KE,Brenner DA.Genetic polymorphisms and the progression of liver fibrosis: a critical appraisal.Hepatology,2003,37(3):493~503.
Percy ME,Potyomkina Z,Dalton AJ,etal.Relation between apolipoprotein E genotype, hepatitis B virus status, and thyroid status in a sample of older persons with Down syndrome.Am J Med Genet,2003,120A(2):191~198
Wozniak MA,Itzhaki RF,Faragher EB,et al.Apolipoprotein E-epsilon 4 protects gainst severe liver disease caused by hepatitis C virus.Hepatology,2002,36(2):456(463
李 晖,李可基,张保惠,等.ApoE基因缺陷鼠免疫、血液、稳态和抗氧化功能改变.北京大学学报(医学版),2001,33(4):347~350
Mistry MJ,Clay MA,Kelly ME,et al.Apolipoprotein E restricts interleukin-dependent T lymphocyte proliferation at the G1A/G1B boundary.Cell Immunol,1995,160(1):14~23
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