基于靶基因捕获测序法对海南省汉族寻常型银屑病与维生素D受体基因关系的研究

doi:10.35541/cjd.20200576

中华皮肤科杂志 ›› 2021, Vol. 54 ›› Issue (7): 597-604.doi: 10.35541/cjd.20200576

基于靶基因捕获测序法对海南省汉族寻常型银屑病与维生素D受体基因关系的研究

刘军麟¹ 王薇² 曹智睿¹ 刘琨¹ 万多艳¹ 吴智明³ 罗杨¹ 肖传柳¹ 刘璐⁴ 殷梅⁵

¹海南医学院第二附属医院皮肤性病科，海口 570311；²海口市人民医院皮肤性病科 570208；³海南医学院第二附属医院检验科，海口 570311；⁴安徽医科大学第一附属医院皮肤性病科，合肥 230022；⁵海南医学院第二附属医院体检中心，海口 570311

收稿日期:2020-06-10 修回日期:2021-01-30 发布日期:2021-07-02
通讯作者: 刘璐；殷梅 E-mail:liulu8887@163.com; liujunlin0759@163.com
基金资助:
国家自然科学基金（81860551）；海南省重点研发计划项目（ZDYF2018156）；海南省卫生健康行业科研项目（20A200472）

Analysis of relationship between psoriasis vulgaris and vitamin D receptor gene in a Han population in Hainan Province based on targeted capture sequencing

Liu Junlin¹, Wang Wei², Cao Zhirui¹, Liu Kun¹, Wan Duoyan¹, Wu Zhiming³, Luo Yang¹, Xiao Chuanliu¹, Liu Lu⁴, Yin Mei⁵

¹Department of Dermatology and Venereology, The Second Affiliated Hospital of Hainan Medical University, Haikou 570311, China; ²Department of Dermatology and Venereology, Haikou People′s Hospital, Haikou 570208, China; ³Department of Clinical Laboratory, The Second Affiliated Hospital of Hainan Medical University, Haikou 570311, China; ⁴Department of Dermatology and Venereology, The First Affiliated Hospital, Anhui Medical University, Hefei 230022, China; ⁵Health Examination Center, The Second Affiliated Hospital of Hainan Medical University, Haikou 570311, China

Received:2020-06-10 Revised:2021-01-30 Published:2021-07-02
Contact: Liu Lu; Yin Mei E-mail:liulu8887@163.com; liujunlin0759@163.com
Supported by:
National Natural Science Foundation of China（81860551）; Key Research and Development Plan of Hainan Province（ZDYF2018156）; Hainan Medical and Health Research Program（20A200472）

摘要/Abstract

摘要： 【摘要】目的探讨维生素D受体（VDR）基因多态性与寻常型银屑病的关系。方法 2018年3月至2020年2月在海南医学院第二附属医院皮肤性病科和体检中心分别收集101例海南籍汉族寻常型银屑病患者与79例海南籍健康对照。采用靶基因捕获测序法对VDR基因及其上、下游各2 kb进行全长测序，对于最小等位基因频率大于1%的单核苷酸多态性（SNP）进行基于SNP和单倍型的关联分析。采用生物信息学方法预测风险位点对基因功能的影响。结果基于SNP的关联分析显示，40个SNP（29个位于内含子区、1个位于外显子区及10个位于基因间区）为银屑病的易感位点，其OR值为0.148（95% CI：0.016 ~ 1.294） ~ 2.779（95% CI：1.260 ~ 6.130）， P < 0.001 ~ 0.976。生物信息学预测显示位于外显子2上的rs2228570可引起氨基酸改变（蛋氨酸→苏氨酸），继而导致基因功能改变。基于单倍型的关联分析显示，10个单倍型为寻常型银屑病的保护性单倍型，在健康对照组和银屑病患者组中的频率分别为5.150% ~ 45.570%、1.110% ~ 33.170%，其OR值为0.198 （95% CI：0.040 ~ 0.985） ~ 0.630（95% CI：0.419 ~ 0.947），P值0.002 ~ 0.048。结论在海南籍汉族人群中，发现40个寻常型银屑病相关的风险SNP，分别位于内含子区、外显子区及基因间区域，同时发现10个保护性单倍型。

关键词: 银屑病, 受体, 骨化三醇, 多态性, 单核苷酸, 单倍型, 病例对照研究, 靶基因捕获测序

Abstract: 【Abstract】 Objective To investigate the relationship between vitamin D receptor （VDR） gene polymorphisms and psoriasis vulgaris. Methods From March 2018 to February 2020， a total of 101 patients with psoriasis vulgaris were collected from Department of Dermatology and Venereology, the Second Affiliated Hospital of Hainan Medical University, and 79 healthy controls from the health examination center in this hospital. All the subjects were of Han nationality from Hainan province. Targeted capture sequencing was performed to sequence the full length of the VDR gene and its 2-kb upstream and downstream regions. Single-nucleotide polymorphism （SNP）- and haplotype-based association analyses were performed for SNPs with minor allele frequency greater than 1%. Bioinformatics methods were used to predict the impact of risk SNPs on gene functions. Results The SNP-based association analysis showed that 40 SNPs, including 29 in the intron region, 1 in the exon region and 10 in the intergenic region, conferred susceptibility to psoriasis vulgaris, with the odds ratio ranging from 0.148 （95% CI: 0.016 - 1.294） to 2.779 （95% CI: 1.260 - 6.130）, and P value ranging from < 0.001 to 0.976. Bioinformatics analysis indicated that rs2228570 in exon 2 could cause the substitution of methionine by threonine, leading to changes in gene functions. The haplotype-based association analysis showed that 10 haplotypes were protective haplotypes for psoriasis vulgaris, and their frequencies were 5.150% - 45.570% in the healthy control group and 1.110% - 33.170% in the psoriasis group, with the odds ratio ranging from 0.198 （95% CI: 0.040 - 0.985） to 0.630 （95%CI: 0.419 - 0.947）, and the P value ranging from 0.002 to 0.048. Conclusion Among the Han population in Hainan Province, 40 risk SNPs for psoriasis vulgaris were identified in intron, exon and intergenic regions of the VDR gene, and 10 protective haplotypes were identified as well.

Key words: Psoriasis, Receptors, calcitriol, Polymorphism, single nucleotide, Haplotypes, Case-control studies, Targeted capture sequencing

刘军麟王薇曹智睿刘琨万多艳吴智明罗杨肖传柳刘璐殷梅. 基于靶基因捕获测序法对海南省汉族寻常型银屑病与维生素D受体基因关系的研究[J]. 中华皮肤科杂志, 2021,54(7):597-604. doi:10.35541/cjd.20200576

Liu Junlin, Wang Wei, Cao Zhirui, Liu Kun, Wan Duoyan, Wu Zhiming, Luo Yang, Xiao Chuanliu, Liu Lu, Yin Mei. Analysis of relationship between psoriasis vulgaris and vitamin D receptor gene in a Han population in Hainan Province based on targeted capture sequencing[J]. Chinese Journal of Dermatology, 2021, 54(7): 597-604.doi:10.35541/cjd.20200576

参考文献 34

［1］	Nagpal S, Lu J, Boehm MF. Vitamin D analogs: mechanism of action and therapeutic applications［J］. Curr Med Chem, 2001,8（13）:1661⁃1679. doi: 10.2174/0929867013371950.
［2］	Kontula K, Välimäki S, Kainulainen K, et al. Vitamin D receptor polymorphism and treatment of psoriasis with calcipotriol［J］. Br J Dermatol, 1997,136（6）:977⁃978. doi: 10.1111/j.1365⁃2133. 1997.tb03955.x.
［3］	Lee DY, Park BS, Choi KH, et al. Vitamin D receptor genotypes are not associated with clinical response to calcipotriol in Korean psoriasis patients［J］. Arch Dermatol Res, 2002,294（1⁃2）:1⁃5. doi: 10.1007/s00403⁃002⁃0293⁃3.
［4］	Zhou X, Xu LD, Li YZ. The association of polymorphisms of the vitamin D receptor gene with psoriasis in the Han population of northeastern China［J］. J Dermatol Sci, 2014,73（1）:63⁃66. doi: 10.1016/j.jdermsci.2013.08.014.
［5］	Rucevic I, Stefanic M, Tokic S, et al. Lack of association of vitamin D receptor gene 3′⁃haplotypes with psoriasis in Croatian patients［J］. J Dermatol, 2012,39（1）:58⁃62. doi: 10.1111/j.1346⁃8138.2011.01296.x.
［6］	Acikbas I, Sanlı B, Tepeli E, et al. Vitamin D receptor gene polymorphisms and haplotypes （Apa I, Bsm I, Fok I, Taq I） in Turkish psoriasis patients［J］. Med Sci Monit, 2012,18（11）:CR661⁃666. doi: 10.12659/msm.883544.
［7］	Polić MV, Rucević I, Barisić⁃Drusko V, et al. Polymorphisms of vitamin D receptor gene in the population of eastern Croatia with psoriasis vulgaris and diabetes mellitus［J］. Coll Antropol, 2012,36（2）:451⁃457.
［8］	刘军麟, 曾慧明, 林岷格, 等. 维生素D受体基因多态性与寻常性银屑病易感性及卡泊三醇疗效的相关性［J］. 中华皮肤科杂志, 2017,50（12）:889⁃893. doi: 10.3760/cma.j.issn.0412⁃4030.2017.12.007.
［9］	赵辨. 中国临床皮肤病学［M］. 2版. 南京: 江苏科学技术出版社, 2017.
［10］	Reichrath J, Zouboulis CC, Vogt T, et al. Targeting the vitamin D endocrine system （VDES） for the management of inflammatory and malignant skin diseases: An historical view and outlook［J］. Rev Endocr Metab Disord, 2016,17（3）:405⁃417. doi: 10.1007/s11154⁃016⁃9353⁃4.
［11］	Bouillon R, Carmeliet G, Verlinden L, et al. Vitamin D and human health: lessons from vitamin D receptor null mice［J］. Endocr Rev, 2008,29（6）:726⁃776. doi: 10.1210/er.2008⁃0004.
［12］	Wang TT, Tavera⁃Mendoza LE, Laperriere D, et al. Large⁃scale in silico and microarray⁃based identification of direct 1,25⁃dihydroxyvitamin D3 target genes［J］. Mol Endocrinol, 2005,19（11）:2685⁃2695. doi: 10.1210/me.2005⁃0106.
［13］	Kovalenko PL, Zhang Z, Cui M, et al. 1,25 Dihydroxyvitamin D⁃mediated orchestration of anticancer, transcript⁃level effects in the immortalized, non⁃transformed prostate epithelial cell line, RWPE1［J］. BMC Genomics, 2010,11:26. doi: 10.1186/1471⁃2164⁃11⁃26.
［14］	Gombart AF. The vitamin D⁃antimicrobial peptide pathway and its role in protection against infection［J］. Future Microbiol, 2009,4（9）:1151⁃1165. doi: 10.2217/fmb.09.87.
［15］	Verstuyf A, Carmeliet G, Bouillon R, et al. Vitamin D: a pleiotropic hormone［J］. Kidney Int, 2010,78（2）:140⁃145. doi: 10.1038/ki.2010.17.
［16］	Hansen CM, Binderup L, Hamberg KJ, et al. Vitamin D and cancer: effects of 1,25（OH）2D3 and its analogs on growth control and tumorigenesis［J］. Front Biosci, 2001,6:D820⁃848. doi: 10.2741/hansen.
［17］	Janmaat VT, Van De Winkel A, Peppelenbosch MP, et al. Vitamin D receptor polymorphisms are associated with reduced esophageal vitamin D receptor expression and reduced esophageal adenocarcinoma risk［J］. Mol Med, 2015,21:346⁃354. doi: 10.2119/molmed.2012.00336.
［18］	Orlow I, Reiner AS, Thomas NE, et al. Vitamin D receptor polymorphisms and survival in patients with cutaneous melanoma: a population⁃based study［J］. Carcinogenesis, 2016,37（1）:30⁃38. doi: 10.1093/carcin/bgv157.
［19］	de Azevêdo Silva J, Monteiro Fernandes K, Trés Pancotto JA, et al. Vitamin D receptor （VDR） gene polymorphisms and susceptibility to systemic lupus erythematosus clinical manifestations［J］. Lupus, 2013,22（11）:1110⁃1117. doi: 10.1177/ 0961203313500549.
［20］	Cavalcanti CA, Silva Jde A, Pita Wde B, et al. Vitamin D receptor polymorphisms and expression profile in rheumatoid arthritis Brazilian patients［J］. Mol Biol Rep, 2016,43（1）:41⁃51. doi: 10.1007/s11033⁃015⁃3937⁃z.
［21］	Oh JJ, Byun SS, Lee SE, et al. Genetic variations in VDR associated with prostate cancer risk and progression in a Korean population［J］. Gene, 2014,533（1）:86⁃93. doi: 10.1016/j.gene. 2013.09.119.
［22］	Chang CK, Mulholland HG, Cantwell MM, et al. Vitamin D receptor gene variants and esophageal adenocarcinoma risk: a population⁃based case⁃control study［J］. J Gastrointest Cancer, 2012,43（3）:512⁃517. doi: 10.1007/s12029⁃011⁃9322⁃9.
［23］	Fang Y, Yu B, Yang Y, et al. Association between vitamin D receptor genetic polymorphisms and haplotypes and risk of lumbar degenerative disc disease in a Chinese population［J］. Int J Clin Exp Pathol, 2017,10（8）:8695⁃8702.
［24］	Vimaleswaran KS, Power C, Hyppönen E. Interaction between vitamin D receptor gene polymorphisms and 25⁃hydroxyvitamin D concentrations on metabolic and cardiovascular disease outcomes［J］. Diabetes Metab, 2014,40（5）:386⁃389. doi: 10. 1016/j.diabet.2014.01.003.
［25］	Shen F, Guo C, Wang Y, et al. Low serum 25⁃hydroxyvitamin D levels may increase the detrimental effect of VDR variants on the risk of essential hypertension［J］. Eur J Clin Nutr, 2020,74（7）:1091⁃1099. doi: 10.1038/s41430⁃019⁃0543⁃5.
［26］	Yu F, Wang C, Wang L, et al. Study and evaluation the impact of vitamin D receptor variants on the risk of type 2 diabetes mellitus in Han Chinese［J］. J Diabetes, 2017,9（3）:275⁃284. doi: 10.1111/1753⁃0407.12413.
［27］	Karami S, Brennan P, Rosenberg PS, et al. Analysis of SNPs and haplotypes in vitamin D pathway genes and renal cancer risk［J/OL］. PLoS One, 2009,4（9）:e7013. https://journals.plos.org/plosone/ article?id=10.1371/journal.pone.0007013. doi: 10.1371/journal.pone.0007013.
［28］	Hu Q, Chen Z, Liang G, et al. Vitamin D receptor gene associations with pulmonary tuberculosis in a Tibetan Chinese population［J］. BMC Infect Dis, 2016,16:469. doi: 10.1186/s12879⁃016⁃1699⁃4.
［29］	Kelly JL, Drake MT, Fredericksen ZS, et al. Early life sun exposure, vitamin D⁃related gene variants, and risk of non⁃Hodgkin lymphoma［J］. Cancer Causes Control, 2012,23（7）:1017⁃1029. doi: 10.1007/s10552⁃012⁃9967⁃0.
［30］	Jurutka PW, Remus LS, Whitfield GK, et al. The polymorphic N terminus in human vitamin D receptor isoforms influences transcriptional activity by modulating interaction with transcription factor IIB［J］. Mol Endocrinol, 2000,14（3）:401⁃420. doi: 10.1210/mend.14.3.0435.
［31］	Colin EM, Weel AE, Uitterlinden AG, et al. Consequences of vitamin D receptor gene polymorphisms for growth inhibition of cultured human peripheral blood mononuclear cells by 1, 25⁃dihydroxyvitamin D3［J］. Clin Endocrinol （Oxf）, 2000,52（2）:211⁃216. doi: 10.1046/j.1365⁃2265.2000.00909.x.
［32］	Holt SK, Kwon EM, Koopmeiners JS, et al. Vitamin D pathway gene variants and prostate cancer prognosis［J］. Prostate, 2010,70（13）:1448⁃1460. doi: 10.1002/pros.21180.
［33］	Shi J, Grundy A, Richardson H, et al. Genetic variation in vitamin D⁃related genes and risk of breast cancer among women of European and East Asian descent［J］. Tumour Biol, 2016,37（5）:6379⁃6387. doi: 10.1007/s13277⁃015⁃4417⁃8.
［34］	Jingwi EY, Abbas M, Ricks⁃Santi L, et al. Vitamin D receptor genetic polymorphisms are associated with PSA level, gleason score and prostate cancer risk in African⁃American men［J］. Anticancer Research, 2015, 35（3）:1549⁃1558.

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基于靶基因捕获测序法对海南省汉族寻常型银屑病与维生素D受体基因关系的研究

Analysis of relationship between psoriasis vulgaris and vitamin D receptor gene in a Han population in Hainan Province based on targeted capture sequencing

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