Sun Rong,Wu Zhouguang,Ye Yongqin,et al.Preliminary study on the expression level and clinical significance of GPC1 in liver tissues of children with biliary atresia[J].Journal of Clinical Pediatric Surgery,,18():211-215.[doi:10.3969/j.issn.1671-6353.2019.03.010]
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Preliminary study on the expression level and clinical significance of GPC1 in liver tissues of children with biliary atresia

Journal of Clinical Pediatric Surgery[ISSN:1671-6353/CN:43-1380/R] volume: 第18卷 Number: 2019 03 Page: 211-215 Column: 论著 Date of publication: 2019-03-25
Author(s):
Sun Rong1 Wu Zhouguang2 Ye Yongqin2 Zhang Dahao2 Wang Bin2
1. Zhuhai Campus of Zunyi Medical University, Zhuhai 519000, China;
2. Shenzhen Children’s Hospital, Shenzhen 518000, China
Keywords:
GPC1Biliary AtresiaLiver/Anatomy & HistologyGene Expression Regulation
CLC:
R729;R657.4+4;R393
DOI:
10.3969/j.issn.1671-6353.2019.03.010
Abstract:
Objective To explore the clinical significance of GPC1 in the pathogenesis of children with biliary atresia (BA).Methods A total of 35 hospitalized BA children at Children’s Hospital of Shenzhen from July 2016 to February 2018 were recruited into observation group.And another 42 hospitalized children with congenital choledochal dilatation were selected as control group.The distribution of GPC1 protein in observation group was detected by immunohistochemistry and the expression levels of GPC1 and protein expression in liver samples of two groups were detected by quantitative polymerase chain reaction (qPCR) and Western blot.Results GPC1 was distributed predominantly at the top of cholangiocarcinoma cells.The expression of GPC1 mRNA in observation and control groups (0.65±0.05 vs. 2.54±0.12,P<0.05) and protein expression (1.31±0.14 vs. 2.83±0.25,P<0.05) showed statistical differences.Conclusion The expression of GPC1 may be closely correlated with the pathogenesis of BA.

References:

1 Asai A, Miethke A, Bezerra JA.Pathogenesis of biliary atresia:defining biology to understand clinical phenotypes[J].Nat Rev Gastroenterol Hepatol, 2015, 12(6):342-345.DOI:10.1038/nrgastro.2015.74.
2 Wen J, Xiao Y, Wang J, et al.Low doses of CMV induce autoimmune-mediated and inflammatory responses in bile duct epithelia of regulatory T cell-depleted neonatal mice[J].Lab Invest, 2015, 95(2):180-192.DOI:10.1038/labinvest.2014.148.
3 郭振亚, 张若岩, 柳明江, 等.先天性胆道闭锁的病因研究进展[J].临床肝胆病杂志, 2015, 31(8):1343-1346.DOI:10.3969/j.issn.1001-5256.2015.08.043. Guo ZY, Zhang RY, Liu MG, et al.Etiology of congenital biliary atresia[J].Journal of Clinical Hepatobiliary Diseases, 2015, 31(8):1343-1346.DOI:10.3969/j.issn.1001-5256.2015.08.043.
4 Tang V, Cofer ZC, Cui S, et al.Loss of a candidate biliary atresia susceptibility gene, add3a, causes biliary developmental defects in zebrafish[J].J Pediatr Gastroenterol Nutr, 2016, 63(5):524-530.DOI:10.1097/MPG.0000000000001375.
5 李智涵, 王斌.Ⅲ型胆道闭锁手术治疗的研究进展[J].临床小儿外科杂志, 2016, 15(1):11-13.DOI:10.3969/j.issn.1671-6353.2016.01.004.Li ZH, Wang B.Advances in surgical treatment of biliary atresia of type Ⅲ[J].J Clin Ped Sur, 2016, 15(1):11-13.DOI:10.3969/j.issn.1671-6353.2016.01.004.
6 Asai A, Miethke A, Bezerra JA.Pathogenesis of biliary atresia:defining biology to understand clinical phenotypes[J].Nat Rev Gastroenterol Hepatol, 2015, 12(6):342-352.DOI:10.1038/nrgastro.2015.74.
7 Hill JJ, Tremblay TL, Fauteux F, et al.Glycoproteomic comparison of clinical triple-negative and luminal breast tumors[J].Journal of Proteome Research, 2015, 14(3):1376-1388.DOI:10.1021/pr500987r.
8 Sadek KH, Ezzat S, Abdel-Aziz SA, et al.Macrophage migration inhibitory factor (MIF) gene promotor polymorphism is associated with increased fibrosis in biliary atresia patients, but not with disease susceptibility[J].Ann Hum Genet, 2017, 81(5):177-183.DOI:10.1111/ahg.12199.
9 Tang V, Cofer ZC, Cui S, et al.Loss of a candidate biliary atresia susceptibility gene, add3a, causes biliary developmental defects in zebrafish[J].J Pediatr Gastroenterol Nutr, 2016, 63(5):524-530.DOI:10.1097/MPG.0000000000001375.
10 Leyva-Vega M, Gerfen J, Thiel BD, et al.Genomic alterations in biliary atresia suggest region of potential disease susceptibility in 2q37.3[J].Am J.Med.Genet.A, 2010, 152A(4):886-895.DOI:10.1002/ajmg.a.33332.
11 Cui S, Leyva-Vega M, Tsai EA, et al.Evidence from human and zebrafish that GPC1 is a biliary atresia susceptibility gene[J].Gastroenterology, 2013, 144(5):1107-1115.DOI:10.1053/j.gastro.2013.01.022.
12 Ke J, Zeng S, Mao J, et al.Common genetic variants of GPC1 gene reduce risk of biliary atresia in a Chinese population[J].J Pediatr.Surg, 2016, 51(10):1661-1664.DOI:10.1016/j.jpedsurg.2016.05.009.
13 Melo SA, Luecke LB, Kahlert C, et al.Glypican-1 identifies cancer exosomes and detects early pancreatic cancer[J].Nature, 2015, 523(7559):177-182.DOI:10.1038/nature14581.
14 Lu H, Niu F, Liu F, et al.Elevated glypican-1 expression is associated with an unfavorable prognosis in pancreatic ductal adenocarcinoma[J].Cancer Med, 2017, 6(6):1181-1191.DOI:10.1002/cam4.1064.
15 Hara H, Takahashi T, Serada S, et al.Overexpression of glypican-1 implicates poor prognosis and their chemoresistance in oesophageal squamous cell carcinoma[J].Br J Cancer, 2016, 115(1):66-75.DOI:10.1038/bjc.2016.183.
16 Lai X, Wang M, McElyea SD, et al.A microRNA signature in circulating exosomes is superior to exosomal glypican-1 levels for diagnosing pancreatic cancer[J].Cancer letters, 2017, 393(1):86-93.DOI:10.1016/j.canlet.2017.02.019.
17 Li J, Li B, Ren C, et al.The clinical significance of circulating GPC1 positive exosomes and its regulative miRNAs in colon cancer patients[J].Oncotarget, 2017, 8(60):101189-101202.DOI:10.18632/oncotarget.20516.
18 Chamorro-Jorganes A, Araldi E, Rotllan N, et al.Autoregulation of glypican-1 by intronic microRNA-149 fine tunes the angiogenic response to FGF2 in humanendothelial cells[J].J Cell Sci, 2014, 127(6):1169-1178.DOI:10.1242/jcs.130518.

Memo

收稿日期:2018-09-13。
基金项目:国家自然科学基金(编号:81770512)
通讯作者:王斌,Email:szwb1967@126.com

Last Update: 1900-01-01