PDF下载 ( 1389 KB)
Expression and significance of OX40/OX40L in peripheral blood of patients with autoimmune hepatitis,primary biliary cholangitis,and their overlap syndrome
-
摘要:
目的探讨自身免疫性肝炎(AIH)、原发性胆汁性胆管炎(PBC)及其重叠综合征患者经规范化治疗前后外周血中OX40/OX40L(CD134/CD134L)在CD4+T淋巴细胞、CD8+T淋巴细胞、单核细胞、B淋巴细胞的表达情况及其临床意义。方法选取2015年8月-2019年8月在江苏省苏北人民医院就诊的74例确诊AIH、PBC及其重叠综合征患者,按照相关诊断标准分为AIH组(29例)、PBC组(26例)、重叠综合征组(19例)(即A、P、C组),同时设置健康对照30例。在规范化治疗前后抽取患者外周血标本,采用免疫荧光标记流式细胞术检测OX40/OX40L在外周血细胞表面的表达情况,比较OX40/OX40L在治疗前后、健康对照组的表达差异。多组间比较采用单因素方差分析,进一步两两比较采用LSD-t检验,配对样本两组间比较采用配对t检验。结果 3组在性别年龄构成上差异均无统计学意义(P值均> 0. 05)。治疗前:A、P、C 3组外周血中CD4+T淋巴细胞的OX40阳性率依次升高,且均高于对照组,依次为:(14. 80±4. 99)%、(17. 11±2. 71)%、(25. 18±5...
Abstract:Objective To investigate the expression and clinical significance of OX40/OX40 L( CD134/CD134 L) in CD4 + T cells,CD8 +T cells,monocytes,and B lymphocytes in peripheral blood of patients with autoimmune hepatitis( AIH),primary biliary cholangitis( PBC),and their overlap syndrome before and after standardized treatment. Methods A total of 74 patients with AIH,PBC,and their o-verlap syndrome who were diagnosed in Subei People's Hospital of Jiangsu from August 2015 to August 2019 were enrolled,and according to related diagnostic criteria,they were divided into AIH group( group A) with 29 patients,PBC group( group P) with 26 patients,and overlap syndrome group( group C) with 19 patients. A healthy control group with 30 individuals was also established. Peripheral blood samples were collected before and after standardized treatment to measure the expression of OX40/OX40 L on the surface of peripheral blood cells by immunofluorescence flow cytometry,and the expression of OX40/OX40 L was compared before and after treatment and between the three groups and the healthy control group to investigate its clinical significance. A one-way analysis of variance was used for comparison between multiple groups,and the least significant difference t-test was used for further comparison between two groups; the paired t-test was used for comparison of paired samples between two groups. Results There were no significant differences in sex composition and age composition between the three groups( P > 0. 05). Before treatment,the positive rate of OX40 in peripheral blood CD4+T cells gradually increased in groups A,P,and C,and groups A,P,and C had a significantly higher positive rate of OX40 than the control group( 14. 80% ± 4. 99%/17. 11% ± 2. 71%/25. 18% ± 5. 55% vs 6. 67% ± 2. 26%,F = 14. 823,P < 0. 001); groups A,P,and C had a significantly higher positive rate of OX40 in CD8+T cells than the control group( 4. 86% ± 1. 54%/6. 40% ± 1. 88%/7. 33% ± 2. 12% vs 4. 09% ± 2. 69%,F =5. 486,P < 0. 001); the positive rate of OX40 L in CD14+monocytes was 19. 84% ± 6. 11% in group A,21. 17% ± 4. 35% in group P,29. 13% ± 6. 32% in group C,and 4. 86% ± 2. 34% in the control group,and there was a significant difference between groups( F =17. 004,P < 0. 001); the positive rate of OX40 L in CD19+B cells was 17. 62% ± 3. 86% in group A,14. 75% ± 4. 32% in group P,10. 13% ± 2. 56% in group C,and 4. 50% ± 1. 38% in the control group,showing a trend of gradual reduction,and groups A,P,and C had a significantly higher positive rate than the control group( F = 12. 221,P < 0. 001). After treatment,the positive rate of OX40 in CD8+T cells decreased significantly to a similar level as the control group,and there was no significant difference between groups( F =0. 731,P = 0. 538). For the other three types of cells,although there were varying degrees of reduction in the positive rate of OX40/OX40 L after treatment,groups A,P,and C still had a significantly higher positive rate than the control group; in CD4+T cells,the positive rate of OX40 was 11. 00% ± 1. 98% in group A,13. 72% ± 1. 03% in group P,19. 72% ± 3. 47% in group C,and 6. 67% ± 2. 26% in the control group,and groups A,P,and C had a significantly higher positive rate than the control group( F = 11. 365,P < 0. 001); in CD14+monocytes,the positive rate of OX40 L was 11. 82% ± 2. 23% in group A,15. 19% ± 4. 42% in group P,24. 51% ± 4. 09% in group C,and 4. 86% ± 2. 34% in the control group,and groups A,P,and C had a significantly higher positive rate than the control group( F =13. 748,P < 0. 001); in CD19+B cells,the positive rate of OX40 L was 9. 09% ± 3. 25% in group A,6. 81% ± 2. 20% in group P,7. 48% ± 2. 85% in group C,and 4. 50% ± 1. 38% in the control group,and groups A,P,and C had a significantly higher positive rate than the control group( F = 8. 052,P < 0. 001). Groups A,P,and C had significant reductions in the expression of OX40/OX40 L in peripheral blood CD4+T cells,CD8+T cells,CD14+monocytes,and CD19+B lymphocytes after treatment( all P < 0. 05). Conclusion The expression of OX40/OX40 L in peripheral blood increases in patients with AIH,PBC,and their overlap syndrome and decreases after treatment,indicating that the OX40/OX40 L pathway is involved in the pathogenesis of the above diseases,and the role of OX40 on the surface of CD8+T cells may better reflect the treatment outcome.
-
Key words:
- hepatitis,autoimmune /
- primary biliary cholangitis /
- overlap syndrome /
- receptors,OX40 /
- OX40 ligand
-
[1] LLEO A,LEUNG P,HIRSCHFIELD GM,et al. The pathogenesis of primary biliary cholangitis:A comprehensive review[J].Semin Liver Dis,2020,40(1):34-48. [2] ARNDTZ K,HIRSCHFIELD GM. The pathogenesis of autoimmune liver disease[J]. Dig Dis,2016,34(4):327-333. [3] SEBODE M,HARTL J,VERGANI D,et al. Autoimmune hepatitis:From current knowledge and clinical practice to future research agenda[J]. Liver Int,2018,38(1):15-22. [4] WILLOUGHBY J,GRIFFITHS J,TEWS I,et al. OX40:Structure and function-What questions remain?[J]. Mol Immunol,2017,83:13-22. [5] DENG J,ZHAO S,ZHANG X,et al. OX40(CD134)and OX40 ligand,important immune checkpoints in cancer[J].Onco Targets Ther,2019,12:7347-7353. [6] LEI W,ZENG D,LIU G,et al. Crucial role of OX40/OX40L signaling in a murine model of asthma[J]. Mol Med Rep,2018,17(3):4213-4220. [7] WEBB GJ,HIRSCHFIELD GM,LANE PJ. OX40,OX40L and autoimmunity:A comprehensive review[J]. Clin Rev Allergy Immunol,2016,50(3):312-332. [8] HENNES EM,ZENIYA M,CZAJA AJ,et al. Simplified criteria for the diagnosis of autoimmune hepatitis[J]. Hepatology,2008,48(1):169-176. [9] Chinese Society of Hepatology,Chinese Medical Association;Chinese Society of Gastroenterology,Chinese Medical Association; Chinese Society of Infectious Diseases,Chinese Medical Association. Consensus on the diagnosis and management of primary biliary cirrhosis(cholangitis)(2015)[J]. J Clin Hepatol,2015,31(12):1980-1988.(in Chinese)中华医学会肝病学分会,中华医学会消化病学分会,中华医学会感染病学分会.原发性胆汁性肝硬化(又名原发性胆汁性胆管炎)诊断和治疗共识(2015)[J].临床肝胆病杂志,2015,31(12):1980-1988. [10] CHAZOUILLRES O,WENDUM D,SERFATY L,et al. Primary biliary cirrhosis-autoimmune hepatitis overlap syndrome:Clinical features and response to therapy[J]. Hepatology,1998,28(2):296-301. [11] ALVAREZ F,BERG PA,BIANCHI FB,et al. International Autoimmune Hepatitis Group Report:Review of criteria for diagnosis of autoimmune hepatitis[J]. J Hepatol,1999,31(5):929-938. [12] LIU F,PAN ZG,YE J,et al. Primary biliary cirrhosis-autoimmune hepatitis overlap syndrome:Simplified criteria may be effective in the diagnosis in Chinese patients[J]. J Dig Dis,2014,15(12):660-668. [13] PATERSON DJ,JEFFERIES WA,GREEN JR,et al. Antigens of activated rat T lymphocytes including a molecule of 50,000Mr detected only on CD4 positive T blasts[J]. Mol Immunol,1987,24(12):1281-1290. [14] WANG WZ,XIANG XX. Immunological mechanism of Treg/Th17and Th1/Th2 balance in autoimmune hepatitis and new targets for diagnosis and treatment[J]. J Clin Hepatol,2019,35(8):1874-1877.(in Chinese)王维钊,向晓星.Treg/Th17、Th1/Th2平衡在自身免疫性肝炎中的免疫学机制及诊疗新靶点[J].临床肝胆病杂志,2019,35(8):1874-1877. [15] UENO H,BLANCO P. OX40/OX40L axis:Not a friend in autoimmunity[J]. Oncotarget,2015,6(26):21779-21780. [16] MIELI-VERGANI G,VERGANI D,CZAJA AJ,et al. Autoimmune hepatitis[J]. Nat Rev Dis Primers,2018,4:18017. [17] LIANG M,LIWEN Z,YUN Z,et al. The imbalance between Foxp3+Tregs and Th1/Th17/Th22 cells in patients with newly diagnosed autoimmune hepatitis[J]. J Immunol Res,2018,2018:3753081. [18] NAKAGAWA R,MUROYAMA R,SAEKI C,et al. CD4+T cells from patients with primary biliary cholangitis show T cell activation and differentially expressed T-cell receptor repertoires[J]. Hepatol Res,2019,49(6):653-662. [19] WEBB GJ,HIRSCHFIELD GM,KRAWITT EL,et al. Cellular and molecular mechanisms of autoimmune hepatitis[J]. Annu Rev Pathol,2018,13:247-292. [20] SITRIN J,SUTO E,WUSTER A,et al. The Ox40/Ox40 ligand pathway promotes pathogenic th cell responses,plasmablast accumulation,and lupus nephritis in NZB/W F1 Mice[J]. J Immunol,2017,199(4):1238-1249. [21] JIANG J,LIU C,LIU M,et al. OX40 signaling is involved in the autoactivation of CD4+CD28-T cells and contributes to the pathogenesis of autoimmune arthritis[J]. Arthritis Res Ther,2017,19(1):67. [22] MIAO Q,BIAN Z,TANG R,et al. Emperipolesis mediated by CD8 T cells is a characteristic histopathologic feature of autoimmune hepatitis[J]. Clin Rev Allergy Immunol,2015,48(2-3):226-235. [23] HIPPCHEN T,SAUER P,GPPERT B,et al. Association between serum IgG level and clinical course in primary sclerosing cholangitis[J]. BMC Gastroenterol,2019,19(1):153. [24] BRAHIM I,BRAHIM I,HAZIME R,et al. Autoimmune hepatitis:Immunological diagnosis[J]. Presse Med,2017,46(11):1008-1019. -
本文二维码
计量
- 文章访问数: 4108
- HTML全文浏览量: 66
- PDF下载量: 66
- 被引次数: 0
下载:
