NIX介导的线粒体自噬研究进展

自噬是指细胞在缺氧、饥饿等不利条件下,利用溶酶体降解细胞器和大分子蛋白等物质,以利于细胞存活的过程。根据对降解底物的选择性,自噬可分为选择性自噬和非选择性自噬。线粒体自噬(mitophagy)是一种典型的选择性自噬,最早于2005年提出[1]。线粒体自噬是指细胞在受到高水平活性氧自由基(reactive oxygen species,ROS)等危害下,线粒体发生去极化即线粒体膜电位下降,线粒体内膜两侧质子及其他离子浓度的不对称分布而形成线粒体膜电位,当H+跨膜梯度形成发生障碍时,导致外正、内负的线粒体膜电位下降,线粒体从而受到损伤,受损的线粒体被特异性的包裹进自噬体中,并与溶酶体融合后完成降解的过程。

熊去氧胆酸抑制人肝星状细胞活化和NIX蛋白表达的实验研究

目的研究NIX蛋白的表达变化与熊去氧胆酸(UDCA)抑制人肝星状细胞(HSC)活化作用的关系。方法人肝星状细胞-LX2细胞实验分为四组:溶媒对照组、UDCA(0.5μM)组、TGF-β1(5 ng/ml)组、TGF-β1(5 ng/ml)+UDCA(0.5μM)组。通过Western blot检测比较各组间α-SMA、NIX的表达差异。结果TGF-β1刺激LX2细胞后,α-SMA、NIX表达分别较对照组增加60.9%、51.0%;UDCA抑制TGF-β1活化LX2细胞后,α-SMA的表达抑制率达55.6%,与其显著下调NIX的表达呈正相关。结论 UDCA下调HSC细胞NIX蛋白的表达,可能为UDCA抗肝纤维化的药理新机制。

Post-translational modification of Parkin and its research progress in cancer

Clinical practice has shown that Parkin is the major causative gene found in an autosomal recessive juvenile parkin-sonism(AR-JP)via Parkin mutations and that the Parkin protein is the core expression product of the Parkin gene,which itself belongs to an E3 ubiquitin ligase.Since the discovery of the Parkin gene in the late 1990s,researchers in many countries have begun extensive research on this gene and found that in addition to AR-JP,the Parkin gene is associated with many diseases,including type 2 diabetes,leprosy,Alzheimer’s,autism,and cancer.Recent studies have found that the loss or dysfunction of Parkin has a certain relationship with tumorigenesis.In general,the Parkin gene,a well-established tumor suppressor,is deficient and mutated in a variety of malignancies.Parkin overexpres-sion inhibits tumor cell growth and promotes apoptosis.However,the functions of Parkin in tumorigenesis and its regulatory mechanisms are still not fully understood.This article describes the structure,functions,and post-transla-tional modifications of Parkin,and summarizes the recent advances in the tumor suppressive function of Parkin and its underlying mechanisms.