中华老年医学杂志
中華老年醫學雜誌
중화노년의학잡지
Chinese Journal of Geriatrics
2015年
9期
1007-1010
,共4页
黄秋红%陈玲%郑亿庆%熊浩%杨海弟
黃鞦紅%陳玲%鄭億慶%熊浩%楊海弟
황추홍%진령%정억경%웅호%양해제
老年性聋%细胞凋亡
老年性聾%細胞凋亡
노년성롱%세포조망
Presbycusis%Apoptosis
目的 探讨MiR-34a/Bcl-2凋亡通路在老年性聋发病机制中的可能作用. 方法 采用C57BL/6年龄相关性聋小鼠模型,4周龄小鼠和12月龄小鼠为研究对象,采用听性脑干诱发电位检查(ABR)进行听力测试,并检测听皮层神经元凋亡情况,采用聚合酶链反应(PCR)及免疫印迹分析(Western Blot)检测miR-34a/Bcl-2通路在年龄相关性聋小鼠听皮层的表达情况,并检测经典凋亡通路Caspase3的活化情况. 结果 ABR结果显示12月龄小鼠在频率为4 kHz、8 kHz、16 kHz、32kHz的阈值分别为(80.0±2.5)dBHL、(74.0±3.5) dBHL、(86.0±4.6)dBHL、(87.0±6.6)dBHL,高于4周龄小鼠的(32.0±4.5)dBHL、(51.0±1.2)dBHL、(51.0±3.5)dBHL、(56.0±1.5)dBHL(均P<0.05).12月龄小鼠听皮层神经元数量减少,凋亡神经元增多,miR-34a的表达升高(t=6.02,P=0.001),Bcl-2的表达下降(t=7.12,P=0.032),Bax的表达升高(t=6.51,P=0.012),Caspase-3表达升高,4周龄小鼠与12月龄小鼠比较,差异有统计学意义(P=0.023). 结论 MiR34a/Bcl-2介导的凋亡通路可能是年龄相关性聋发病的机制之一.
目的 探討MiR-34a/Bcl-2凋亡通路在老年性聾髮病機製中的可能作用. 方法 採用C57BL/6年齡相關性聾小鼠模型,4週齡小鼠和12月齡小鼠為研究對象,採用聽性腦榦誘髮電位檢查(ABR)進行聽力測試,併檢測聽皮層神經元凋亡情況,採用聚閤酶鏈反應(PCR)及免疫印跡分析(Western Blot)檢測miR-34a/Bcl-2通路在年齡相關性聾小鼠聽皮層的錶達情況,併檢測經典凋亡通路Caspase3的活化情況. 結果 ABR結果顯示12月齡小鼠在頻率為4 kHz、8 kHz、16 kHz、32kHz的閾值分彆為(80.0±2.5)dBHL、(74.0±3.5) dBHL、(86.0±4.6)dBHL、(87.0±6.6)dBHL,高于4週齡小鼠的(32.0±4.5)dBHL、(51.0±1.2)dBHL、(51.0±3.5)dBHL、(56.0±1.5)dBHL(均P<0.05).12月齡小鼠聽皮層神經元數量減少,凋亡神經元增多,miR-34a的錶達升高(t=6.02,P=0.001),Bcl-2的錶達下降(t=7.12,P=0.032),Bax的錶達升高(t=6.51,P=0.012),Caspase-3錶達升高,4週齡小鼠與12月齡小鼠比較,差異有統計學意義(P=0.023). 結論 MiR34a/Bcl-2介導的凋亡通路可能是年齡相關性聾髮病的機製之一.
목적 탐토MiR-34a/Bcl-2조망통로재노년성롱발병궤제중적가능작용. 방법 채용C57BL/6년령상관성롱소서모형,4주령소서화12월령소서위연구대상,채용은성뇌간유발전위검사(ABR)진행은력측시,병검측은피층신경원조망정황,채용취합매련반응(PCR)급면역인적분석(Western Blot)검측miR-34a/Bcl-2통로재년령상관성롱소서은피층적표체정황,병검측경전조망통로Caspase3적활화정황. 결과 ABR결과현시12월령소서재빈솔위4 kHz、8 kHz、16 kHz、32kHz적역치분별위(80.0±2.5)dBHL、(74.0±3.5) dBHL、(86.0±4.6)dBHL、(87.0±6.6)dBHL,고우4주령소서적(32.0±4.5)dBHL、(51.0±1.2)dBHL、(51.0±3.5)dBHL、(56.0±1.5)dBHL(균P<0.05).12월령소서은피층신경원수량감소,조망신경원증다,miR-34a적표체승고(t=6.02,P=0.001),Bcl-2적표체하강(t=7.12,P=0.032),Bax적표체승고(t=6.51,P=0.012),Caspase-3표체승고,4주령소서여12월령소서비교,차이유통계학의의(P=0.023). 결론 MiR34a/Bcl-2개도적조망통로가능시년령상관성롱발병적궤제지일.
Objective To explore the possible mechanism of miR 34a/Bcl-2 apoptotic pathway in the mouse model of age-related hearing loss.Methods A C57BL/6 mouse model of age-related hearing loss was conducted,and 4-week-old and 12-month-old mice were considered as the objects.The auditory brainstem response (ABR) was used to test the hearing function.The TdT-mediated dUTP nick end labeling (TUNEL) was used to observe the apoptosis of neuron in auditory cortex.The mRNA and protein levels of miR-34a,Bcl-2 and caspase 3 were detected by real-time PCR and Western bloting,respectively.Results The ABR showed that the hearing threshold level at 4,8,16,32 kHz were higher in 12-month-old mice than in 4-week-old mice [(80.0±2.5) dBHL vs.(32.0 ±4.5) dBHL,(74.0±3.5) dBHL vs.(51.0±1.2) dBHL,(86.0±4.6) dBHL vs.(51.0±3.5) dBHL,(87.0±6.6) dBHL vs.(56.0±1.5) dBHL,all P<0.05].Compared with 4 week-old mice,the total number of neurons in auditory cortex was decreased,the number of apoptosis neurons was increased,the expressions of miR-34a (t=6.02,P=0.001),Bax (t=6.51,P=0.012) and Caspase 3 (P=0.023) rised,and the expression of Bcl-2 (t=7.12,P=0.032) declined in 12 month-old mice.Conclusions The activation of miR-34a/Bcl-2 apoptotic pathway may be one of the mechanisms of age-related hearing loss.