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基因组甲基化与慢性荨麻疹发病机制间的关系的初步探索 被引量:1

Association of genome DNA methylation with pathogenesis of chronic urticaria
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摘要 目的通过检测慢性特发性荨麻疹和自身免疫性荨麻疹的基因组甲基化水平,初步探讨基因组甲基化与其发病机制间的关系。方法采用ASST方法将45例慢性荨麻疹患者分为慢性特发性荨麻疹组和自身免疫性荨麻疹组。分离血清,分别检测血清中TgAb、TPOAb、ANA、SAM和SAH水平,并对结果进行统计分析。结果慢性荨麻疹患者ASST阳性率46.7%,对照组ASST全部阴性,两组比较差异有统计学意义(P〈0.01)。自身免疫荨麻疹组自身抗体检出率最高,TGAb、TPOAb和ANA的阳性率分别是23.80%、14.29%、14.29%;与慢性特发性荨麻疹组及对照组比较,自身免疫荨麻疹组TGAb差异均有统计学意义(P〈0.05),TPOAb和ANA的差异均无统计学意义(P〉O.05);慢性特发性荨麻疹组与对照组比较,三种自身抗体差异均无统计学意义(P〉0.05)。自身免疫性荨麻疹组SAM较其它两组低,而SAH高于其它两组,SAM/SAH也较其它两组小,但差异均无统计学意义(P〉0.05)。慢性特发性荨麻疹组SAM、SAH和SAM/SAH与对照组比较,差异均无统计学意义(P〉0.05)。结论我科门诊慢性荨麻疹患者中,自身免疫性荨麻疹所占比例达46.7%;TGAb在自身免疫性荨麻疹患者中阳性率显著高于慢性特发性荨麻疹,能否作为一种有价值的自身免疫性荨麻疹的临床检测指标有待进一步研究;SAM、SAH及其比值在自身免疫性荨麻疹、慢性特发性荨麻疹及对照组中无统计学差异,似乎甲基化并不参与到自身免疫性荨麻疹的发病机制中,但有待更大的样本量证实。 Objective To explore the association of genome methylation with the pathogenesis of chronic urticaria by detecting genome methylation level of chronic idiopathic urticaria and autoimmune urticaria. Methods 45 patients with chronic urticaria were divided into chronic idiopathic urticaria group and autoimmune urticaria group using ASST method. Serum TgAb, TPOAb, ANA, SAM, and SAH were detected. Results The positive rate of ASST was 46.7% in patients with chronic urticaria, as compared with 0% in control group. There was a statistical significance between the two groups. The positive rates of TgAb, TPOAb, and ANA were 23.80%, 14.29%, and 14.29% in autoimmune urticaria group, 4.16%, 4.16%, and 0 in chronic idiopathic urticaria group, and 5%, 0%, and 0% in the control group. TgAb differed significantly between autoimmune urticaria group and the other two groups, but not between chronic idiopathic urticaria group and the control group. TPOAb and ANA did not differ statistically between the two groups. SAM, SAH, and SAM/SAH did not differ significantly. Conclusions Autoimmune urticaria accounts for 46.7% in patients with chronic urticaria. TGAb is significantly higher in autoimmune urticaria patients than in those with chronic idiopathic urticaria. Further research should be done to confirm whether TGAb can be a kind of valuable clinical detection index of autoimmune urticaria. There is no statistical significance in SAM, SAH, and SAM/SAH between the two groups, which is likely to suggest that methylation is not involved in the pathogenesis of autoimmune urticaria. But this conclusion needs to be confirmed by bigger samples.
作者 宋彪 房思宁 郑利雄 梅忠喜 黄小芳
机构地区 深圳市人民医院暨南大学第二临床医学院皮肤科
出处 《国际医药卫生导报》 2013年第15期2267-2271,共5页 International Medicine and Health Guidance News
基金 深圳市科技计划项目(201003023)
关键词 荨麻疹 DNA甲基化 S-腺苷蛋氨酸 S-腺苷同型半胱氨酸 Urticaria DNA methylation S-adenosylmethionine S-adenosylhomosysteine
分类号 R758.24 [医药卫生—皮肤病学与性病学]
  • 相关文献

参考文献16

  • 1李尊忠,郑敏.DNA低甲基化与系统性红斑狼疮关系的研究进展[J].浙江大学学报(医学版),2006,35(4):458-462. 被引量:7
  • 2杨文彪,林健才,蒋卫民,李健雄.慢性特发性荨麻疹与甲状腺自身免疫性的关系研究[J].实用医学杂志,2003,19(3):244-245. 被引量:4
  • 3Asero R, Tedeschi A, Riboldi P, et al. Plasma of patients with chronic urticaria shows signs of thrombin generation, and its intradermal injection causes wheal-and-flare reactions much more frequently than autologous serum[J]. J Allergy Clin Immunol, 2006, 117(5) : 1113-1117.
  • 4Sabroe RA, Greaves MW. The pathogenesis of chronic idiopathic urticaria[J]. Arch Dermatol, 1997, 133(8): 1003-1005.
  • 5Gaig P, Garc f a-Ortega P, Enrique E, et al. Successful treatment of chronic idiopathic urticaria associated with thyroid autoimmunity[J]. J Investig Allergol Clin Immunol, 2000, 10(6) : 342-345.
  • 6Greaves MW. Chronic urticaria[J]. N Engl J Med, 1995, 332(26): 1767-1772.
  • 7Tong LJ, Balakrishnan G, Kochan JP, et al. Assessment of autoimmunity in patients with chronic urticaria[J]. J Allergy ClinImmunol, 1997, 99(4): 461-465.
  • 8Fiebiger E, Maurer D, Holub H, et al. Serum IgG autoantibodies directed against the alpha chain of Fc epsilon RI: a selective marker and pathogenetic factor for a distinct subset of chronic urticaria patients?[J]. J Clin Invest, 1995, 96(6): 2606-2612.
  • 9孙蔚凌,夏济平,毕志刚.慢性荨麻疹患者血清中抗FcεRⅠα自身抗体及其功能性的检测[J].中国麻风皮肤病杂志,2007,23(4):280-282. 被引量:3
  • 10Greaves M. Chronic urticaria[J]. J Allergy Clin Immunol, 2000, 105: 664-672.

二级参考文献47

  • 1孙蔚凌,毕志刚.慢性荨麻疹患者血清组胺释放活性检测[J].中华皮肤科杂志,2004,37(6):351-353. 被引量:12
  • 2刘暘,郑敏,殷文浩,鲍彰.系统性红斑狼疮患者血清HGF与MMP-9的检测及与疾病活动性的关系[J].浙江大学学报(医学版),2004,33(4):340-343. 被引量:3
  • 3任跃忠,戴巧定,徐荣臻.新的人内源性逆转录病毒NP9基因的分子克隆与病毒蛋白表达[J].浙江大学学报(医学版),2005,34(4):361-364. 被引量:1
  • 4孙蔚凌,毕志刚.人高亲和力IgE受体α链基因克隆及表达[J].中国麻风皮肤病杂志,2005,21(8):609-612. 被引量:3
  • 5ZHUYi-min LAIMao-de(朱益民 来茂德).Role of DNA methylation in the occurrence of tumor[J].浙江大学学报:医学版,2003,32(2):162-166.
  • 6LU Q,KAPLAN M,RAY D,et al.Demethylation of ITGAL(CD11a) regulatory sequences in systemic lupus erythematosus[J].Arthritis Rheum,2002,46(5):1 282-1 291.
  • 7RICHARDSON B C,LIEBLING M R,HUDSON J L.CD4+ cells treated with DNA methylation inhibitors induce autologous B cell differentiation[J].Clin Immunol Immunopathol,1990,55(3):368-381.
  • 8KOBATA T,JACQUOT S,KOZLOWSKI S,et al.CD27-CD70 interaction regulate B-cell activation by T cells[J].Proc Natl Acad Sci U S A,1995,92(24):11 249-11 253.
  • 9OELKE K,LU Q,RICHARDSON D,et al.Overexpression of CD70 and overstimulation of IgG synthesis by lupus T cells and T cells treated with DNA methylation inhibitors[J].Arthritis Rheum,2004,50(6):1 850-1 860.
  • 10KAPLAN M J,RAY D,MO R R,et al.TRAIL (Apo2 ligand) and TWEAK (Apo3 ligand) mediate CD4+T cell killing of antigenpresenting macrophages[J].J Immunol,2000,164(6):2 897-2 904.

共引文献14

同被引文献21

  • 1Kabesch M. Epigenetics in asthma and allergy [J]. Curr Opin Allergy Clin Immunol, 2014, 14 (1): 62-68. DOI: 10.1097/ACI.
  • 2B~gin P, Nadeau KC. Epigenetic regulation of asthma and allergic disease [J ]. Allergy Asthma Clin Immunol, 2014, 10 ( 1 ): 27. DOI: 10.1186/1710-1492-10-27.
  • 3Nakamura T, Sekigawa I, Ogasawara H, et al. Expression of DNMT-1 in patients with atopic dermatitis [J]. Arch Dermatol Res, 2006, 298(5): 253-256. DOI: 10.1007/s00403-006-0682-0.
  • 4Liang Y, Wang P, Zhao M, et al. Demethylation of the FCER1G promoter leads to FceRI overexpression on monocytes of patients with atopic dermatitis[J]. Allergy, 2012, 67(3): 424-430. DOI: 10.1111/j.1398-9995.2011.02760.x.
  • 5Ziyab AH, Karmaus W, Holloway JW, et al. DNA methylation of the filaggrin gene adds to the risk of eczema associated with loss- of-function variants[J]. J Eur Acad Dermatol Venereol, 2013, 27 (3): e420-423. DOI: 10.1111/jdv. 12000.
  • 6Luo Y, Zhou B, Zhao M, et al. Promoter demethylation contributes to TSLP overexpression in skin lesions of patients with atopic dermatitis[J]. Clin Exp Dermatol, 2014, 39 (1): 48- 53. DOI: 10.1111/ced.12206.
  • 7Wang IJ, Chen SL, Lu TP, et al. Prenatal smoke exposure, DNA methylation, and childhood atopic dermatitis [J]. Clin Exp Allergy, 2013, 43 (5): 535-543. DOI: 10.1111/cea.12108.
  • 8Rodr~guez E, Baurecht H, Wahn AF, et al. An integrated epigenetic an d transcriptomic analysis reveals distinct tissue- specific patterns of DNA methylation associated with atopicdermatitis EJ]. J Invest Dermatol, 2014, 134 (7): 1873-1883. DOI: 10.1038/jid.2014.87.
  • 9Chapman VL, Zollinger T, Terranova R, et al. Chemical allergen induced perturbations of the mouse lymph node DNA methylome [J]. Toxicol Sci, 2014, 139 (2): 350-361. DOI: 10.1093/toxsci/ kfu047.
  • 10Chapman VL, Terranova R, Moggs JG, et al. Evaluation of 5- methylcytosine and 5-hydroxymethylcytosine as potential biomarkers for charaeterisation of chemical allergens [J~. Toxicology, 2016, 340(1): 17-26. DOI: 10.1016/j.tux.2015.12. 003.

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国际医药卫生导报
2013年 第15期

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