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急性肾损伤早期诊断生物标志物研究进展 被引量:18

Progression of Biological Marker in Early Diagnosis Acute Kidney Injury:A Review
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摘要 急性肾损伤(acute kidney injury,AKI)既往称为急性肾衰竭"(acute renal failure,ARF),是一种常见的致死性肾病,在一般住院病人中AKI发病率约为5%,但在重症监护病房则高达30%~50%。内科疾病引起的AKI死亡率在23%左右,但由多脏器功能不全所致者死亡率高达60%。迄今,尚无有效治疗AKⅠ药物,一旦发生AKI,临床上只能采取支持治疗,等待肾功能的恢复。因此,早期诊断及早期治疗是防治AKI的最佳策略。生物标记物是近年来研究早期诊断AKI的热点和趋势,研究发现包括NGAL,KIM-1,IL-18,NHE3等多种标记物是早期预测AKI强力指标,本文就急性肾损伤早期诊断生物标志物研究进展进行综述。 Acute kidney injury(AKI),was also called acute renal failure(ARF),is a common fatal nephropathy.Incidence rate of AKI on inpatients approximately 5%,but in ICU(intensive care unit)its more high,attain 30-50%.The mortality of AKI,which induction by internal medical disease approximately 23%,however,in MODS(multiple organ dysfunction)patients,the mortality reach up to 60%.Up to now,still has no active drug to treatment AKI,once to be sick,doctor can only give Supporting Therapy to wait for renal function recovery.So,early diagnosis is the best way in prevention and cure in AKI.For the past few years,the research of biological marker in early diagnosis is the hot spots and tendency,including NGAL,KIM-1,IL-18,NHE3 etc is found valuable in early diagnosis AKI.This review is about biological marker in early diagnosis AKI.
作者 肖燎原 盛珺 孙丽君 梅长林
机构地区 第二军医大学长征医院
出处 《现代生物医学进展》 CAS 2013年第16期3183-3185,共3页 Progress in Modern Biomedicine
基金 国家自然科学基金青年项目(81100487)
关键词 急性肾损伤 生物标记物 中性粒细胞明胶酶相关性脂质运载蛋白 肾损伤因子-1 白介素18 Na+ H+交换子同型体3 胱抑素C 富含半胱氨酸蛋白-61 AKI Biological marker NGAL KIM-1 IL-18 NHE3 Cystatin C Cyr 61
分类号 R692 [医药卫生—泌尿科学]
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参考文献23

  • 1Johnson DW. Early detection of acute kidney injury: Emerging newbiomarkers[J]. Nephrology,2008,13: 91-98. 被引量:1
  • 2American society of nephrology. American society of nephrology renalresearch report [J]. J Am Soc Nephrol, 2005, 16: 1886-1903. 被引量:1
  • 3Devarajan PJ, Mishra S, Supavekin LT, et al. Gene expression in earlyischemic renal injury: Clues towards pathogenesis, biomarker discov-ery, and novel therapeutics[J], Mol. Genet. Metab, 2003,80: 365-376. 被引量:1
  • 4Mishra J, Ma Q, Prada A, et al. Identification of neutrophil gelati-nase-associated lipocalin as a novel early urinary biomarker for is-chemic renal injury[J]. J Am Soc Nephrol, 2003,14:2534-2543. 被引量:1
  • 5Mishra J, Dent C, Tarabishi R, et al. Neutrophil gelatinase-associatedlipocalin (NGAL) as a biomarker for acute renal injury after cardiacsurgery[J]. Lancet, 2005, 365: 1231-1238. 被引量:1
  • 6Mori K, Lee HT, Rapoport D,et al. Endocytic delivery of lipocalin-siderophore-iron complex rescues the kidney fromischemia-reperfu-sion injury [J]. J Clin Invest, 2006,115:610-621. 被引量:1
  • 7Bachorzewska-Gajewska H, Malyszko J,Sitniewska E, et al. Neu-trophil gelatinase-associated lipocalin (NGAL) correlations with cys-tatin C, serum creatinine and eGFR in patients with normal serumcreatinine undergoing coronary angiography [J]. Nephrol Dial Trans-plant, 2007,22: 295-296. 被引量:1
  • 8Trachtman H, Christen E, Cnaan A, et al. Urinary neutrophil gelati-nase-associated lipocalcin in D+HUS: A novel marker of renal injury[J]. Pediatr Nephrol, 2006,21: 989-994. 被引量:1
  • 9Zhou H, Hewitt SM, Yuen PST, et al. Acute kidney injury biomarkers-needs, present status and future promise [J]. NephSAP, 2006, 5:63-71. 被引量:1
  • 10Yang SA, Stevens JL, Bonventre XV. Kidney injury molecule-1: a tis-sue and urinary biomarker for nephrotoxicant-induced renal injury [J].Am J Physiol Renal Physiol, 2004,286:F552-F563. 被引量:1

二级参考文献32

  • 1Sutters M, Germino GG. Autosomal dominant polycystic kidney disease: molecular genetics and pathophysiology. J Lab Clin Med,2003,141: 91-101. 被引量:1
  • 2Kireeva ML, Mo FE, Yang GP, et al. Cyr61, product of a growth factor-inducible immediate-early gene, promote cell proliferation,migration, and adhesion. Mol Cell Biol. 1996,16: 1326-1334. 被引量:1
  • 3Brigstock DR. Regulation of angiogenesis and endothelial cell function by connective tissue growth factor (CTGF) and cysteine-rich 61 (CYR61). Angiogenesis,2002,5: 153-165. 被引量:1
  • 4Murica NS, Sweeney WE Jr, Avner ED. New insights into the molecular pathophysioology of polycystic kidney disease. J Kidney Int, 1999, 55:1187-1197. 被引量:1
  • 5Joly D, Morel V, Hummel A, et al. Beta4 integrin and laminin 5are aberrantly expressed in polycystic kidney disease: role in increased cell adhesion and migration. Am J Pathol, 2003, 163:1791-1800. 被引量:1
  • 6Jay P, Berge-Lefranc JL, Marsollier C, et al. The human growth factor-inducible immediate early gene, CYR61, maps to chromosome 1p. Oncogene, 1997,10; 14: 1753-1757. 被引量:1
  • 7Yang GP, Lau LF. Cyr61, product of a growth factor-inducible immediate early gene, is associated with the extracellular matrix and the cell surface. Cell Growth Differ, 1991,2: 351-357. 被引量:1
  • 8Kireeva ML, MO FE, Yang GP, et al. Cyr61, a product of a growth factor-inducible immediate-early gene, promotes cell proliferation, migration, and adhesion. Mol Cell Biol, 1996, 16:1326-1334. 被引量:1
  • 9Lewis MP, Fine LG; Norman JT . Pexicrine effects of basement membrane components on paracrine signaling by renal tubular cells. Kidney Int,1996,49: 48-58. 被引量:1
  • 10Chen CC, Chen N, Lau LF. The angiogenic factors Cyr61 and connective tissue growth factor induce adhesive signaling in primary human skin fibroblasts. J Biol Chem, 2001, 276:10443-10452. 被引量:1

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现代生物医学进展
2013年 第16期

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