中华儿科杂志
中華兒科雜誌
중화인과잡지
Chinese Journal of Pediatrics
2008年
2期
89-93
,共5页
赵德育%文惯宇%田曼%施圣云%陈荣华
趙德育%文慣宇%田曼%施聖雲%陳榮華
조덕육%문관우%전만%시골운%진영화
RANTES%多态现象,遗传%呼吸道合胞体病毒感染%细支气管炎
RANTES%多態現象,遺傳%呼吸道閤胞體病毒感染%細支氣管炎
RANTES%다태현상,유전%호흡도합포체병독감염%세지기관염
RANTES%Polymorphism,genetic%Respiratory syncytial virus infections%Bronchiolitis
目的 探讨正常T淋巴细胞表达和分泌的活性调节蛋白RANTES的启动子-28C/G基因多态性与呼吸道合胞病毒(RSV)致细支气管炎(既往称毛细支气管炎)易感的关联性.方法 应用聚合酶链反应-限制性片段长度多态性(PCR-RFLP)技术,检测238例RSV细支气管炎患儿及288例正常对照者的RANTES-28C/G多态性,ELISA法检测血清总IgE浓度,全自动血细胞计数仪计数嗜酸性粒细胞,并搜集受检者的特应性体质史、特应性家族史及临床相关资料.结果 RANTES-28C/G基因型分布在RSV细支气管炎组和对照组均符合Hardy-Weinberg平衡.与对照组比较,RANTES-28C/G基因型及等位基因频率在RSV细支气管炎组中的分布差异均有统计学意义(G=10.22,P<0.01;x2=9.708,P<0.01);与CC基因型个体相比,携带G等位基因的个体发生RSV细支气管炎的风险增加了2.09倍(OR:2.09,95% CI=1.32~3.30,P<0.01).在RSV细支气管炎组,携带G等位基因个体具有特应性体质和特应性家族史的风险分别比CC基因型个体增加了1.85倍(OR=1.85,95% CI=1.01~3.38,P<0.05)和1.91倍(OR=1.91,95% CI=1.03~3.54,P<0.05),其嗜酸性粒细胞计数亦显著升高(Z=-2.303,P<0.05).结论 RANTES启动子-28C/G基因多态性与RSV细支气管炎易感性相关联,并且-28G等位基因与RSV细支气管炎患儿的特应性体质及特应性家族史相关联.
目的 探討正常T淋巴細胞錶達和分泌的活性調節蛋白RANTES的啟動子-28C/G基因多態性與呼吸道閤胞病毒(RSV)緻細支氣管炎(既往稱毛細支氣管炎)易感的關聯性.方法 應用聚閤酶鏈反應-限製性片段長度多態性(PCR-RFLP)技術,檢測238例RSV細支氣管炎患兒及288例正常對照者的RANTES-28C/G多態性,ELISA法檢測血清總IgE濃度,全自動血細胞計數儀計數嗜痠性粒細胞,併搜集受檢者的特應性體質史、特應性傢族史及臨床相關資料.結果 RANTES-28C/G基因型分佈在RSV細支氣管炎組和對照組均符閤Hardy-Weinberg平衡.與對照組比較,RANTES-28C/G基因型及等位基因頻率在RSV細支氣管炎組中的分佈差異均有統計學意義(G=10.22,P<0.01;x2=9.708,P<0.01);與CC基因型箇體相比,攜帶G等位基因的箇體髮生RSV細支氣管炎的風險增加瞭2.09倍(OR:2.09,95% CI=1.32~3.30,P<0.01).在RSV細支氣管炎組,攜帶G等位基因箇體具有特應性體質和特應性傢族史的風險分彆比CC基因型箇體增加瞭1.85倍(OR=1.85,95% CI=1.01~3.38,P<0.05)和1.91倍(OR=1.91,95% CI=1.03~3.54,P<0.05),其嗜痠性粒細胞計數亦顯著升高(Z=-2.303,P<0.05).結論 RANTES啟動子-28C/G基因多態性與RSV細支氣管炎易感性相關聯,併且-28G等位基因與RSV細支氣管炎患兒的特應性體質及特應性傢族史相關聯.
목적 탐토정상T림파세포표체화분비적활성조절단백RANTES적계동자-28C/G기인다태성여호흡도합포병독(RSV)치세지기관염(기왕칭모세지기관염)역감적관련성.방법 응용취합매련반응-한제성편단장도다태성(PCR-RFLP)기술,검측238례RSV세지기관염환인급288례정상대조자적RANTES-28C/G다태성,ELISA법검측혈청총IgE농도,전자동혈세포계수의계수기산성립세포,병수집수검자적특응성체질사、특응성가족사급림상상관자료.결과 RANTES-28C/G기인형분포재RSV세지기관염조화대조조균부합Hardy-Weinberg평형.여대조조비교,RANTES-28C/G기인형급등위기인빈솔재RSV세지기관염조중적분포차이균유통계학의의(G=10.22,P<0.01;x2=9.708,P<0.01);여CC기인형개체상비,휴대G등위기인적개체발생RSV세지기관염적풍험증가료2.09배(OR:2.09,95% CI=1.32~3.30,P<0.01).재RSV세지기관염조,휴대G등위기인개체구유특응성체질화특응성가족사적풍험분별비CC기인형개체증가료1.85배(OR=1.85,95% CI=1.01~3.38,P<0.05)화1.91배(OR=1.91,95% CI=1.03~3.54,P<0.05),기기산성립세포계수역현저승고(Z=-2.303,P<0.05).결론 RANTES계동자-28C/G기인다태성여RSV세지기관염역감성상관련,병차-28G등위기인여RSV세지기관염환인적특응성체질급특응성가족사상관련.
Objective Respiratory syncytial virus(RSV)infects nearly all children under two years of age.It is poorly understood why a few children who were infected with RSV develop bronchiolitis that require hospital admission while most have a relatively minor illness.Several recent studies have obtained some indications for the involvement of genetic heterogeneity in RSV bronchiolitis,implying that the clinical outcome of RSV infection perhaps is determined by genetic factors.Regulated on activation,normal T cell expressed and secreted RANTES plays a key role in the pathophysiology of RSV bronchiolitis.The purpose of this study was to explore the genetic association between the RANTES gene promoter-28C/G polymorphism and RSV bronchiolitis in Chinese Han ethnic group population.Methods The study recruited 238 hospitalized patients(186 male and 52 female)under 12 months of age.with a clinical diagnosis of bronchiolitis due to RSV,the sex,age,hospital stay,SaO2 at the time of admission,personal and family history of atopy were recorded.The 288 healthy control subjects(206 male and 82 female),who had no evidence of personal or familial history of atopy and no history of wheezing,were chosen at the same
time.Polymerase chain reaction-restriction fragment length polymorphism(PCR-RFLP)was used to identify the polymorphism at position-28C/G of the RANTES promoter.The total IgE concentrations in serum samples were measured by enzyme-linked immunosorbent assay(ELISA).The absolute peripheral blood eosinophil counts were measured by using an automated hematology analyzer.Results The distribution of RANTES-28C/G gene polymorphism was in accordance with Hardy-Weinberg equilibrium.Compared to control subjects,significant difierence was demonstrated for genotypes and allele frequencies of the RANTES -28C/G polymorphism in patients with RSV bronchiolitis(G=10.22,P<0.01;x2=9.708,P<0.01).
Compared with the wild type CC,the-28G allele carriers demonstrated a 2.09-fold increased risk of RSV bronchiolitis(OR=2.09,95% CI=1.32-3.30,P<0.01).Interestingly,both the percentage of personalhistory of atopy and the percentage of family history of atopy for the-28G allele carriers were significantly
higher(P<0.05)than that for those CC homozygotes carriers in RSV bronchiolitis.Compared with the wild type CC.the-28G allele carriers demonstrated a 1.85-fold increased risk of the personal history of atopy (OR=1.85,95% CI=1.01-3.38,P=0.045)and a 1.91-fold increased risk ofthe family history of atopy (OR=1.91,95% CI=1.03-3.54,P=0.037),and tlle absolute peripheral blood eosinophil counts for the -28G allele carriers were significantly higher(P<0.05).Conclusion The RANTES gene promoter-28C/
G polymorphism iS associated with the susceptibility to RSV bronchiolitis,and the-28G allele iS an important predisposing factor for the personal history of atopy and the family history of atopy in RSV bronchiolitis.
