中华病理学杂志
中華病理學雜誌
중화병이학잡지
Chinese Journal of Pathology
2014年
10期
663-667
,共5页
姚坤%段泽君%胡泽良%边宇%齐雪岭
姚坤%段澤君%鬍澤良%邊宇%齊雪嶺
요곤%단택군%호택량%변우%제설령
少突神经胶质瘤%杂合子丢失%异柠檬酸脱氢酶
少突神經膠質瘤%雜閤子丟失%異檸檬痠脫氫酶
소돌신경효질류%잡합자주실%이저몽산탈경매
Oligodendroglioma%Loss of heterozygosity%Isocitrate dehydrogenase
目的 观察少突胶质细胞起源肿瘤及少突-星形细胞起源肿瘤1p/19q杂合性缺失与人IDH1-R132H突变蛋白表达的相关性,探索预测少突胶质细胞起源肿瘤及少突-星形细胞起源肿瘤化疗敏感性的分子标志物.方法 选择病理学诊断为各类型和级别的少突胶质细胞起源肿瘤38例及少突-星形细胞起源肿瘤37例,共75例,采用荧光原位杂交方法检测1p/19q杂合性缺失,免疫组织化学法检测其IDH1-R132H突变蛋白表达.结果 75例少突胶质细胞起源肿瘤及少突-星形细胞起源肿瘤1p/19q杂合性缺失为37例(37/75,49.3%),其中34例1p和19q同时发生缺失,1p缺失与19q缺失二者密切相关(P<0.01).在少突胶质细胞瘤(WHOⅡ级)中,1p/19q杂合性缺失检出率比间变性少突胶质细胞瘤(WHOⅢ级)高,但差异无统计学意义(P>0.05).少突胶质细胞起源肿瘤(WHOⅡ级和WHOⅢ级)中1p/19q杂合性缺失率高于少突-星形细胞起源肿瘤(WHOⅡ级和WHOⅢ级,P <0.05).而且少突胶质细胞起源肿瘤中1p/19q杂合性缺失均为联合缺失,1p和19q的单独缺失仅发生在少突-星形细胞起源肿瘤中.在75例中51例(68.0%)少突胶质细胞起源肿瘤及少突-星形细胞起源肿瘤出现IDH1-R132H突变蛋白表达.少突胶质细胞起源肿瘤IDH1-R132H突变蛋白检测阳性率高于少突-星形细胞起源肿瘤.而且少突胶质细胞起源肿瘤及少突-星形细胞起源肿瘤中,IDH1-R132H突变蛋白阳性表达与1p/19q杂合性缺失均有明显相关性(P<0.05).结论 IDH1-R132H突变蛋白表达与1p/19q杂合性缺失有明显相关性,IDH1-R132H蛋白是预测少突胶质细胞起源肿瘤及少突-星形细胞起源肿瘤1p/19q是否杂合性缺失的潜在分子标志物.
目的 觀察少突膠質細胞起源腫瘤及少突-星形細胞起源腫瘤1p/19q雜閤性缺失與人IDH1-R132H突變蛋白錶達的相關性,探索預測少突膠質細胞起源腫瘤及少突-星形細胞起源腫瘤化療敏感性的分子標誌物.方法 選擇病理學診斷為各類型和級彆的少突膠質細胞起源腫瘤38例及少突-星形細胞起源腫瘤37例,共75例,採用熒光原位雜交方法檢測1p/19q雜閤性缺失,免疫組織化學法檢測其IDH1-R132H突變蛋白錶達.結果 75例少突膠質細胞起源腫瘤及少突-星形細胞起源腫瘤1p/19q雜閤性缺失為37例(37/75,49.3%),其中34例1p和19q同時髮生缺失,1p缺失與19q缺失二者密切相關(P<0.01).在少突膠質細胞瘤(WHOⅡ級)中,1p/19q雜閤性缺失檢齣率比間變性少突膠質細胞瘤(WHOⅢ級)高,但差異無統計學意義(P>0.05).少突膠質細胞起源腫瘤(WHOⅡ級和WHOⅢ級)中1p/19q雜閤性缺失率高于少突-星形細胞起源腫瘤(WHOⅡ級和WHOⅢ級,P <0.05).而且少突膠質細胞起源腫瘤中1p/19q雜閤性缺失均為聯閤缺失,1p和19q的單獨缺失僅髮生在少突-星形細胞起源腫瘤中.在75例中51例(68.0%)少突膠質細胞起源腫瘤及少突-星形細胞起源腫瘤齣現IDH1-R132H突變蛋白錶達.少突膠質細胞起源腫瘤IDH1-R132H突變蛋白檢測暘性率高于少突-星形細胞起源腫瘤.而且少突膠質細胞起源腫瘤及少突-星形細胞起源腫瘤中,IDH1-R132H突變蛋白暘性錶達與1p/19q雜閤性缺失均有明顯相關性(P<0.05).結論 IDH1-R132H突變蛋白錶達與1p/19q雜閤性缺失有明顯相關性,IDH1-R132H蛋白是預測少突膠質細胞起源腫瘤及少突-星形細胞起源腫瘤1p/19q是否雜閤性缺失的潛在分子標誌物.
목적 관찰소돌효질세포기원종류급소돌-성형세포기원종류1p/19q잡합성결실여인IDH1-R132H돌변단백표체적상관성,탐색예측소돌효질세포기원종류급소돌-성형세포기원종류화료민감성적분자표지물.방법 선택병이학진단위각류형화급별적소돌효질세포기원종류38례급소돌-성형세포기원종류37례,공75례,채용형광원위잡교방법검측1p/19q잡합성결실,면역조직화학법검측기IDH1-R132H돌변단백표체.결과 75례소돌효질세포기원종류급소돌-성형세포기원종류1p/19q잡합성결실위37례(37/75,49.3%),기중34례1p화19q동시발생결실,1p결실여19q결실이자밀절상관(P<0.01).재소돌효질세포류(WHOⅡ급)중,1p/19q잡합성결실검출솔비간변성소돌효질세포류(WHOⅢ급)고,단차이무통계학의의(P>0.05).소돌효질세포기원종류(WHOⅡ급화WHOⅢ급)중1p/19q잡합성결실솔고우소돌-성형세포기원종류(WHOⅡ급화WHOⅢ급,P <0.05).이차소돌효질세포기원종류중1p/19q잡합성결실균위연합결실,1p화19q적단독결실부발생재소돌-성형세포기원종류중.재75례중51례(68.0%)소돌효질세포기원종류급소돌-성형세포기원종류출현IDH1-R132H돌변단백표체.소돌효질세포기원종류IDH1-R132H돌변단백검측양성솔고우소돌-성형세포기원종류.이차소돌효질세포기원종류급소돌-성형세포기원종류중,IDH1-R132H돌변단백양성표체여1p/19q잡합성결실균유명현상관성(P<0.05).결론 IDH1-R132H돌변단백표체여1p/19q잡합성결실유명현상관성,IDH1-R132H단백시예측소돌효질세포기원종류급소돌-성형세포기원종류1p/19q시부잡합성결실적잠재분자표지물.
Objective To correlate the presence of chromosome 1p/19q deletion with the expression of R132H mutant IDH1 status in oligodendroglial tumors,and to explore molecular markers for predicting chemosensitivity of oligodendroglial tumors.Methods The study included 75 oligodendroglial tumors (38 oligodendrogliomas and 37 oligoastrocytomas).Immunohistochemistry was used to detect the expression of R132H mutant IDH1 protein,and fluorescence in situ hybridization (FISH) was employed to detect 1p/19q deletion.Results Deletion of chromosome 1p and/or 19q was detected in 37 cases(37/75,49.3%),among which co-deletion of 1p and 19q was seen in 34 cases (closely correlated,P < 0.01).Oligodendrogliomas WHO Ⅱ had a slightly higher deletion rate than oligodendrogliomas WHO Ⅲ,although without statistical significance.Oligodendrogliomas WHO Ⅱ and WHO Ⅲ had a significantly higher deletion rate of chromosome 1p/19q than oligoastrocytomas WHO Ⅱ and WHO Ⅲ (P <0.05).While combined loss of 1p/19q was always detected in oligodendrogliomas when FISH was positive,isolated 1p or 19q deletion was only found in oligoastrocytomas.The expression of R132H mutant IDH1 was detected in 51 of 75 cases (68.0%),in which oligodendrogliomas had a higher positive rate than oligoastrocytomas.Statistical analysis demonstrated a significant correlation between the expression of R132H mutant IDH1 protein and the presence of combined 1p/19q deletion in oligodendrogliomas (P < 0.05).Conclusions A significant correlation was observed between the expression of R132H mutant protein and 1p/19q LOH.Expression of 132H mutant IDH1 protein is the potential biomarker for predicating the presence of 1p/19q deletion in oligodendrogliomas.
