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细胞内巯基对 CTNS 基因表达的调控。

Modulation of CTNS gene expression by intracellular thiols.

机构信息

Department of Nephrology and Urology, Bambino Gesù Children's Hospital and Research Institute, Rome, Italy.

出版信息

Free Radic Biol Med. 2010 Apr 1;48(7):865-72. doi: 10.1016/j.freeradbiomed.2010.01.011. Epub 2010 Jan 14.

Abstract

The cysteine/cystine (Cys/CySS) couple represents one of the major cell thiol/disulfide systems and is involved in the regulation of several metabolic pathways and the cell redox state. Nephropathic cystinosis (NC) is an autosomal recessive disease characterized by renal cellular dysfunction due to mutations in the CTNS gene, which encodes cystinosin, a CySS lysosomal transporter. To analyze the mechanisms involved in cell damage in NC, we have investigated the effects of CTNS gene overexpression or inhibition on cell thiol/disulfide systems and vice versa. Overexpression of the CTNS gene had no remarkable effect on intracellular Cys/CySS and GSH/GSSG redox state. Silencing the CTNS gene increased cell CySS and Cys and decreased cell GSH and GSSG and increased mildly the redox state of the Cys/CySS-couple. Extracellular CySS and Cys deprivation for 48 h caused an oxidation of the Cys/CySS (73 mV) and GSH/GSSG (100 mV) redox couples and increased CTNS mRNA levels by 1.9+/-0.2-fold (p<0.001). Conversely, a reduced cell environment associated with a GSH/GSSG reduction from -250.1+/-3.10 to -330.6+/-4.70 mV (p<0.001) and a Cys/CySS reduction from -167.0+/-11.30 to -240.0+/-8.17 mV (p<0.005) was associated with a 40% decrease in CTNS mRNA levels (p<0.05). By regression analysis, CTNS gene expression was correlated with intracellular Cys level and with Cys/CySS redox state.

摘要

半胱氨酸/胱氨酸(Cys/CySS)对代表了主要的细胞硫醇/二硫键系统之一,参与调节几种代谢途径和细胞氧化还原状态。遗传性胱氨酸贮积症(NC)是一种常染色体隐性遗传病,其特征是由于 CTNS 基因突变导致胱氨酸酶功能障碍,从而引起肾脏细胞功能障碍,该基因编码胱氨酸酶,是 CySS 溶酶体转运体。为了分析 NC 中细胞损伤的机制,我们研究了 CTNS 基因过表达或抑制对细胞硫醇/二硫键系统的影响,反之亦然。CTNS 基因过表达对细胞内 Cys/CySS 和 GSH/GSSG 氧化还原状态没有显著影响。沉默 CTNS 基因增加了细胞 CySS 和 Cys,降低了细胞 GSH 和 GSSG,并轻度增加了 Cys/CySS 对的氧化还原状态。细胞外 CySS 和 Cys 剥夺 48 小时导致 Cys/CySS(73 mV)和 GSH/GSSG(100 mV)氧化还原对氧化,并使 CTNS mRNA 水平增加 1.9+/-0.2 倍(p<0.001)。相反,与 GSH/GSSG 降低相关的还原细胞环境(从-250.1+/-3.10 到-330.6+/-4.70 mV,p<0.001)和 Cys/CySS 降低(从-167.0+/-11.30 到-240.0+/-8.17 mV,p<0.005)与 CTNS mRNA 水平降低 40%(p<0.05)相关。通过回归分析,CTNS 基因表达与细胞内 Cys 水平和 Cys/CySS 氧化还原状态相关。

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