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ISSN 1001-5256 (Print)
ISSN 2097-3497 (Online)
CN 22-1108/R
Issue 11
Nov.  2016
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Article Navigation >  Journal of Clinical Hepatology  > 2016  >  32(11): 2130-2133

Role of reproductive factors in female patients with primary biliary cholangitis

DOI: 10.3969/j.issn.1001-5256.2016.11.025
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  • Published Date: 2016-11-20
    Abstract
  • Objective To investigate the role of productive factors in the development of primary biliary cholangitis( PBC). Methods A total of 273 female patients with a definite diagnosis of PBC who visited Xijing Hospital from October 2013 to August 2015 were enrolled. The patients with autoimmune hepatitis,primary sclerosing cholangitis overlap syndrome,and hepatic encephalopathy and those with incomplete data after telephone follow- up were excluded,and 54 female PBC patients who had female relatives were finally enrolled( PBC group).The female relatives who were less than 10 years older or younger than the patients were collected,and those with severe systemic diseases and incomplete data after telephone follow- up were excluded; finally 88 relatives were enrolled( relative group). The questionnaire for female reproductive factors in PBC was used to survey all these enrolled patients and collect data. The t- test was used for comparison of continuous data between groups,the chi- square test was used for comparison of categorical data between groups,and a multivariate logistic regression analysis was used for the analysis of dose- response relationship. Results The PBC group had a significantly higher number of births than the relative group( 2. 55 ± 1. 84 vs 1. 84 ± 0. 95,t = 2. 708,P = 0. 009). Furthermore,there was a significant dose- response pattern between the number of births and the development of PBC( P = 0. 002). Conclusion The number of births may be associated with the development of PBC in a dose- response manner. As for the female population susceptible to PBC,a reduction in the number of births may reduce the possibility of PBC.

     

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    • References(28)
  • [1]CAREY EJ,ALI AH,LINDOR KD.Primary biliary cirrhosis[J].Lancet,2015,386(10003):1565-1575.
    [2]PARIKH-PATEL A,GOLD EB,UTTS J,et al.The association between gravidity and primary biliary cirrhosis[J].Ann Epidemiol,2002,12(4):264-272.
    [3]PRINCE MI,DUCKER SJ,JAMES OF.Case-control studies of risk factors for primary biliary cirrhosis in two United Kingdom populations[J].Gut,2010,59(4):508-512.
    [4]PARIKH-PATEL A,GOLD EB,WORMAN HJ,et al.Risk factors for primary biliary cirrhosis in a cohort of patients from the united states[J].Hepatology,2001,33(1):16-21.
    [5]CORPECHOT C,CHRETIEN Y,CHAZOUILLERES O,et al.Demographic,lifestyle,medical and familial factors associated with primary biliary cirrhosis[J].J Hepatol,2010,53(1):162-169.
    [6]GERSHWIN ME,SELMI C,WORMAN HJ,et al.Risk factors and comorbidities in primary biliary cirrhosis:a controlled interview-based study of 1032 patients[J].Hepatology,2005,42(5):1194-1202.
    [7]LAMMERT C,NGUYEN DL,JURAN BD,et al.Questionnaire based assessment of risk factors for primary biliary cirrhosis[J].Dig Liver Dis,2013,45(7):589-594.
    [8]LINDOR KD,GERSHWIN ME,POUPON R,et al.Primary biliary cirrhosis[J].Hepatology,2009,50(1):291-308.
    [9]FLOREANI A,PATERNOSTER D,MEGA A,et al.Sex hormone profile and endometrial cancer risk in primary biliary cirrhosis:a case-control study[J].Eur J Obstet Gynecol Reprod Biol,2002,103(2):154-157.
    [10]BECKER U,ALMDAL T,CHRISTENSEN E,et al.Sex hormones in postmenopausal women with primary biliary cirrhosis[J].Hepatology,1991,13(5):865-869.
    [11]NEWTON JL,BHALA N,BURT J,et al.Characterisation of the associations and impact of symptoms in primary biliary cirrhosis using a disease specific quality of life measure[J].J Hepatol,2006,44(4):776-783.
    [12]ALPINI G,GLASER SS,UENO Y,et al.Bile acid feeding induces cholangiocyte proliferation and secretion:evidence for bile acid-regulated ductal secretion[J].Gastroenterology,1999,116(1):179-186.
    [13]WOOLBRIGHT BL,DORKO K,ANTOINE DJ,et al.Bile acidinduced necrosis in primary human hepatocytes and in patients with obstructive cholestasis[J].Toxicol Appl Pharmacol,2015,283(3):168-177.
    [14]ALEKSUNES LM,YEAGER RL,WEN X,et al.Repression of hepatobiliary transporters and differential regulation of classic and alternative bile acid pathways in mice during pregnancy[J].Toxicol Sci,2012,130(2):257-268.
    [15]FLOREANI A,INFANTOLINO C,FRANCESCHET I,et al.Pregnancy and primary biliary cirrhosis:a case-control study[J].Clin Rev Allergy Immunol,2015,48(2-3):236-242.
    [16]SUN Y,HAAPANEN K,LI B,et al.Women and primary biliary cirrhosis[J].Clin Rev Allergy Immunol,2015,48(2-3):285-300.
    [17]ALVARO D,ALPINI G,ONORI P,et al.Estrogens stimulate proliferation of intrahepatic biliary epithelium in rats[J].Gastroenterology,2000,119(6):1681-1691.
    [18]ALVARO D,INVERNIZZI P,ONORI P,et al.Estrogen receptors in cholangiocytes and the progression of primary biliary cirrhosis[J].J Hepatol,2004,41(6):905-912.
    [19]NELSON JL,FURST DE,MALONEY S,et al.Microchimerism and HLA-compatible relationships of pregnancy in scleroderma[J].Lancet,1998,351(9102):559-562.
    [20]NELSON JL.Maternal-fetal immunology and autoimmune disease:is some autoimmune disease auto-alloimmune or allo-autoimmune?[J].Arthritis Rheum,1996,39(2):191-194.
    [21]MURAJI T.Maternal microchimerism in biliary atresia:are maternal cells effector cells,targets,or just bystanders?[J].Chimerism,2014,5(1):1-5.
    [22]WAKAE T,TAKATSUKA H,SETO Y,et al.Similarity between hepatic graft-versus-host disease and primary biliary cirrhosis[J].Hematology,2002,7(5):305-310.
    [23]KOGAN J,ILAN I.Combined liver damage from primary biliary cirrhosis,primary sclerosing cholangitis,liver allograft rejection and graft-versus-host disease[J].Harefuah,2000,138(1):38-41.
    [24]LUPPI P,HALUSZCZAK C,BETTERS D,et al.Monocytes are progressively activated in the circulation of pregnant women[J].J Leukoc Biol,2002,72(5):874-884.
    [25]SOUTHCOMBE J,REDMAN C,SARGENT I.Peripheral blood invariant natural killer T cells throughout pregnancy and in preeclamptic women[J].J Reprod Immunol,2010,87(1-2):52-59.
    [26]DING J,ZHU BT.Unique dose-dependent effects of the human pregnancy hormone estriol on the ratio of blood IgM to IgG in female mice[J].Mol Med Rep,2016,13(1):447-452.
    [27]ROBINSON DP,KLEIN SL.Pregnancy and pregnancy-associated hormones alter immune responses and disease pathogenesis[J].Horm Behav,2012,62(3):263-271.
    [28]CORTINA ME,LITWIN S,ROUX ME,et al.Impact of mouse pregnancy on thymic T lymphocyte subsets[J].Reprod Fertil Dev,2012,24(8):1123-1133.
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