1st Department of Dermatology, St. Ann's Faculty Hospital, Masaryk University Brno, Pekarská 53, Brno 656 91, Czech Republic.
Arch Dermatol Res. 2009 Jul;301(6):467-73. doi: 10.1007/s00403-009-0947-5. Epub 2009 Apr 10.
The expression of matrix metalloproteinase-2 was observed to be significantly upregulated in psoriasis. The aim of this study was to associate the DNA polymorphic variants in MMP-2 promoter gene with psoriasis and/or with psoriasis phenotypes related to psoriasis and comorbid heredity. In the total of 582 Czech Caucasian individuals (386 patients with psoriasis and 196 controls of similar age and sex distribution without personal or family history of chronic disease of the skin), four MMP-2 promoter polymorphisms (-1575G/A, -1306C/T, -790T/G and -735C/T) were detected by PCR methods. A significant association of GG genotype of -790 MMP-2 polymorphism with psoriasis was observed (Pcorr = 0.04). Although no significant case-control differences in frequency of associated GG(-1575)CC(-1306)TT(-790) MMP-2 promoter genotype were observed, the genotype was found to be significantly less frequent in patients with family history of psoriasis (close as well as distant), family history of diabetes and personal history of allergy (2/11 vs. 55/32, odds ratio (OR) for GGCCTT 0.11, 95% confidential interval 0.02-0.50, Pcorr = 0.01). The significant difference between psoriatic patients with positive anamnestic data on diabetes, psoriasis and allergy compared with psoriatic patients that have only positive family history of diabetes was also observed (2/11 vs. 38/31, P = 0.009, Pcorr = 0.04; OR 0.15, 95% CI = 0.03-0.72 for psoriatic patients with GGCCTT genotype and family history of psoriasis, diabetes and personal history of allergy). To conclude, the associated GGCCTT genotype in the promoter of MMP-2 gene was less frequent in patients with positive family history of psoriasis, diabetes and personal history of allergy compared with psoriatic patients without them (2/11 vs. 68/57, P = 0.007, Pcorr = 0.04; OR = 0.15, 95% CI = 0.03-0.72 for psoriatic patients with family history of psoriasis and diabetes and with allergy). Based on our results, we suggest that the MMP-2 located in the psoriasis susceptibility region on 16q (psoriasis susceptibility 8, PSORS8) should be considered as a gene modulator of psoriasis in specific subgroups of patients. In the future, similar genetic characteristics could contribute to the data assembly of genetic predisposition to psoriasis and could lead to therapy improvement based on time-proved individual pharmacogenetic aspects detected in psoriasis patients.
基质金属蛋白酶-2 的表达在银屑病中观察到明显上调。本研究的目的是将 MMP-2 启动子基因中的 DNA 多态性变体与银屑病以及与银屑病相关的银屑病表型和合并的遗传疾病相关联。在总共 582 名捷克白种人个体(386 名银屑病患者和 196 名年龄和性别分布相似、无慢性皮肤病个人或家族史的对照者)中,通过 PCR 方法检测了四种 MMP-2 启动子多态性(-1575G/A、-1306C/T、-790T/G 和 -735C/T)。观察到-790 MMP-2 多态性 GG 基因型与银屑病存在显著相关性(Pcorr = 0.04)。尽管未观察到与相关 GG(-1575)CC(-1306)TT(-790)MMP-2 启动子基因型相关的病例对照频率存在显著差异,但在有银屑病家族史(近亲或远亲)、糖尿病家族史和过敏个人史的患者中,该基因型明显较少见(2/11 与 55/32,GGCCTT 的优势比(OR)为 0.11,95%置信区间为 0.02-0.50,Pcorr = 0.01)。与仅具有糖尿病家族史的银屑病患者相比,具有糖尿病、银屑病和过敏阳性病史的银屑病患者之间也观察到显著差异(2/11 与 38/31,P = 0.009,Pcorr = 0.04;对于具有 GGCCTT 基因型和银屑病、糖尿病和过敏家族史的银屑病患者,OR 为 0.15,95%CI = 0.03-0.72)。总之,与无这些病史的银屑病患者相比,具有阳性银屑病、糖尿病和过敏家族史的患者中 MMP-2 基因启动子中的相关 GGCCTT 基因型较少见(2/11 与 68/57,P = 0.007,Pcorr = 0.04;对于具有银屑病和糖尿病家族史且有过敏史的银屑病患者,OR = 0.15,95%CI = 0.03-0.72)。基于我们的结果,我们建议位于 16q 上的银屑病易感区域(银屑病易感 8,PSORS8)中的 MMP-2 应被视为特定银屑病患者亚群中银屑病的基因调节剂。在未来,类似的遗传特征可能有助于银屑病遗传易感性数据的综合,并可能导致基于在银屑病患者中检测到的经过时间验证的个体药物遗传学方面的改进治疗。
