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您所在的位置:首頁 > 腎內科醫(yī)學進展 > Circulation:阿托伐他汀可降造影劑誘發(fā)急性腎損傷

Circulation:阿托伐他汀可降造影劑誘發(fā)急性腎損傷

2013-01-23 11:51 閱讀:2145 來源:CMT 作者:網(wǎng)* 責任編輯:網(wǎng)絡
[導讀] 意大利學者的一項研究表明,造影劑應用前24小時內單次給予大劑量阿托伐他汀可有效降低造影劑誘發(fā)急性腎損傷(CIAKI)發(fā)生率。論文發(fā)表于《循環(huán)》[Circulation 2012, 126(25):3008]。

 意大利學者的一項研究表明,造影劑應用前24小時內單次給予大劑量阿托伐他汀可有效降低造影劑誘發(fā)急性腎損傷(CIAKI)發(fā)生率。論文發(fā)表于《循環(huán)》[Circulation 2012, 126(25):3008]。

此項研究包括體內和體外試驗兩部分。在體內研究中,慢性腎病患者被隨機分為阿托伐他汀組(造影劑暴露前24小時內給予80 mg阿托伐他??;202例)和對照組(208例)。所有患者均接受大劑量N-乙酰半胱氨酸和碳酸氫鈉溶液治療。以造影劑暴露后24小時內胱蛋白酶抑制劑C濃度升高10%以上定義CIAKI。體外研究評估了阿托伐他汀預治療對造影劑介導修飾胞內通路的影響;該通路可決定腎小管細胞凋亡或存活。
結果顯示,阿托伐他汀組和對照組的CIAKI發(fā)生率分別為4.5%(9/202)和17.8%(37/208;P=0.005)。在阿托伐他汀組中,伴和未伴糖尿病的中度慢性腎病患者均出現(xiàn)CIAKI發(fā)生率降低。體外研究顯示,阿托伐他汀預治療可通過減少激酶活化預防造影劑誘導的腎細胞凋亡,并可恢復由Akt和ERK通路介導的細胞存活信號。
Impact of a High Loading Dose of Atorvastatin on Contrast-Induced Acute Kidney Injury
Background
The role of statins in the prevention of contrast-induced acute kidney injury (CIAKI) is controversial.
Methods and Results
First, we investigated the in vivo effects of atorvastatin on CIAKI. Patients with chronic kidney disease enrolled in the Novel Approaches for Preventing or Limiting Events (NAPLES) II trial were randomly assigned to (1) the atorvastatin group (80 mg within 24 hours before contrast media [CM] exposure; n=202) or (2) the control group (n=208). All patients received a high dose of N-acetylcysteine and sodium bicarbonate solution. Second, we investigated the in vitro effects of atorvastatin pretreatment on CM-mediated modifications of intracellular pathways leading to apoptosis or survival in renal tubular cells. CIAKI (ie, an increase >10% of serum cystatin C concentration within 24 hours after CM exposure) occurred in 9 of 202 patients in the atorvastatin group (4.5%) and in 37 of 208 patients in the control group (17.8%) (P=0.005; odds ratio=0.22; 95% confidence interval, 0.07–0.69). CIAKI rate was lower in the atorvastatin group in both diabetics and nondiabetics and in patients with moderate chronic kidney disease (estimated glomerular filtration rate, 31–60 mL/min per 1.73 m2). In the in vitro model, pretreatment with atorvastatin (1) prevented CM-induced renal cell apoptosis by reducing stress kinases activation and (2) restored the survival signals (mediated by Akt and ERK pathways).
Conclusions
A single high loading dose of atorvastatin administered within 24 hours before CM exposure is effective in reducing the rate of CIAKI. This beneficial effect is observed only in patients at low to medium risk.

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