YKL40 expression in CD14~+ liver cells in acute and chronic injury

被引:0
|
作者
Oscar Pizano-Martínez [1 ]
Irinea Yaez-Sánchez [1 ]
Pilar Alatorre-Carranza [1 ]
Alejandra Miranda-Díaz [1 ]
Pablo C Ortiz-Lazareno [2 ]
Trinidad García-Iglesias [1 ]
Adrian Daneri-Navarro [1 ]
Mónica Vázquez-Del Mercado [1 ]
Mary Fafutis-Morris [1 ]
Vidal Delgado-Rizo [1 ]
机构
[1] Department of Physiology,CUCS,University of Guadalajara,Guadalajara,Jalisco 44340,México
[2] Division of Immunology,Centro de Investigación Biomédica de OccidenteIMSS.Guadalajara,Jalisco 44340,México
关键词
YKL40; Kupffer cells; Liver cirrhosis; CD14 + cells;
D O I
暂无
中图分类号
R575 [肝及胆疾病];
学科分类号
1002 ; 100201 ;
摘要
AIM:To demonstrate that CD14 + cells are an important source of the growth factor YKL40 in acute and chronic liver damage.METHODS:Rats were inoculated with one dose of CCl4 to induce acute damage.Liver biopsies were obtained at 0,6,12,24,48 and 72 h.For chronic damage,CCl4 was administered three days per week for 6 or 8 wk.Tissue samples were collected,and cellular populations were isolated by liver digestion and purified by cell sorting.YKL40 mRNA and protein expression were evaluated by realtime polymerase chain reaction and western blot.RESULTS:Acute liver damage induced a rapid increase of YKL40 mRNA beginning at 12 h.Expression peaked at 24 h,with a 26fold increase over basal levels.By 72 h however,YKL40 expression levels had nearly returned to control levels.On the other hand,chronic damage induced a sustained increase in YKL40 expression,with 7and 9fold higher levels at 6 and 8 wk,respectively.The pattern of YKL40 expression in different subpopulations showed that CD14+cells,which include Kupffer cells,are a source of YKL40 after acute damage at 72 h[0.09 relative expression units(REU)]as well as after chronic injury at 6 wk(0.11 REU).Hepatocytes,in turn,accounted for 0.06 and 0.01 REU after 72 h(acute)or 6 wk(chronic),respectively.The rest of the CD14cells(including T lymphocytes,B lymphocytes,natural killer and natural killer T cells) yielded 0.07 and 0.15 REU at 72 h and 6 wk,respectively.YKL40 protein expression in liver was detected at 72 h as well as 6 and 8 wk,with the highest expression relative to controls(11fold;P≤0.05)seen at 6 wk.Macrophages were stimulated by lipopolysaccharide.We demonstrate that under these conditions,these cells showed maximum expression of YKL40 at 12 h,with P<0.05 compared with controls.CONCLUSION:Hepatic CD14 + cells are an YKL40 mRNA and protein source in acute and chronic liver injury,with expression patterns similar to growth factors implicated in inflammationfibrogenesis.
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页码:3830 / 3835
页数:6
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