Kidney injury molecule-1: A urinary biomarker for contrast-induced acute kidney injury

Vijayasimha, M; Padma, V. Vijaya; Mujumdar, Saroj Kumar Das; Satyanarayana, P V V; Yadav, Ashok

doi:10.4103/0975-2870.128974

Cited by 10 publications

(11 citation statements)

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“…It has been suggested that KIM-1 plays an important role in regenerating damaged epithelial cells and in removal of dead cells fom the tubular lumen by phagocytosis [53,55]. KIM-1 is found in the urine as early as 24 h after coronary angiography (using the iso-osmolar contrast medium iodixanol or the low-osmolar contrast medium iopromide), while eGFR (based on SCr) did not change significantly during the first 48 h after contrast administration [57]. In adult patients undergoing cardiac surgery, urinary KIM-1 could predict the development of AKI much more than NGAL [58,59].…”

Section: Kim-1mentioning

confidence: 99%

“…In clinical practice, urinary L-FABP is a good biomarker for AKI in cisplatin-induced nephrotoxicity [118], in septic shock induced AKI [78,119], in contrast-induced AKI [120][121][122][123][124][125], in AKI occurring in patients undergoing percutaneous coronary intervention due to unstable angina [84], in AKI following cardiac surgery [118,126], in AKI of patients admitted to the Intensive-Care Unit with sepsis [127], in AKI occurring in pediatric patients following cardiopulmonary bypass surgery [64], in AKI of human kidney transplant patients from living-related donors [35,116]. Under these conditions, urinary L-FABP is detected much earlier than the rise in SCr.…”

Section: L-fabpmentioning

confidence: 99%

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The ischemic/nephrotoxic acute kidney injury and the use of renal biomarkers in clinical practice

Andreucci

Faga

Pisani

et al. 2017

European Journal of Internal Medicine

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The term Acute Renal Failure (ARF) has been replaced by the term Acute Kidney Injury (AKI). AKI indicates an abrupt (within 24-48h) decrease in Glomerular Filtraton Rate, due to renal damage, that causes fluid and metabolic waste retention and alteration of electrolyte and acid-base balance. The renal biomarkers of AKI are substances or processes that are indicators of normal or impaired function of the kidney. The most used renal biomarker is still serum creatinine that is inadequate for several reasons, one of which is its inability to differentiate between hemodynamic changes of renal function ("prerenal azotemia") from intrinsic renal failure or obstructive nephropathy. Cystatin C is no better in this respect. After the description of the pathophysiology of "prerenal azotemia" and of Acute Kidney Injury (AKI) due to ischemia or nephrotoxicity, the renal biomarkers are listed and described: urinary NAG, urinary and serum KIM-1, serum and urinary NGAL, urinary IL-18, urinary L-FABP, serum Midkine, urinary IGFBP7 and TIMP2, urinary α-GST and π-GST, urinary ɣGT and AP, urinary βM, urinary RBP, serum and urinary miRNA. All have been shown to appear much earlier than the rise of serum Creatinine. Some of them have been demonstrated to predict the clinical outcomes of AKI, such as the need for initiation of dialysis and mortality.

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Section: Kim-1mentioning

confidence: 99%

Section: L-fabpmentioning

confidence: 99%

The ischemic/nephrotoxic acute kidney injury and the use of renal biomarkers in clinical practice

Andreucci

Faga

Pisani

et al. 2017

European Journal of Internal Medicine

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“…133 Urinary levels of the L-FABP have been shown to increase in patients who develop AKI after exposure to IV CM. [133][134][135][136][137] Bachorzewska-Gajewska et al 112 studied 25 patients with normal serum creatinine who underwent PCI for unstable angina: urinary L-FABP increased significantly, like urinary NGAL, after 4 hours and remained elevated up to 48 hours.…”

mentioning

confidence: 99%

“…67,69 The use of urinary KIM-1 as a biomarker of AKI is based on the fact that there is no KIM-1 expression in the kidneys of healthy subjects, and on its upregulation in the apical cell membrane of tubules during AKI. 67 Vijayasimha et al 70 have carried out a study to evaluate whether KIM-1 allows the identification of CI-AKI earlier than the rise in serum creatinine. The study involved 100 consecutive patients with normal serum creatinine undergoing angiographic procedure.…”

mentioning

confidence: 99%

The potential use of biomarkers in predicting contrast-induced acute kidney injury

Andreucci¹,

Faga²,

Riccio³

et al. 2016

IJNRD

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Contrast-induced acute kidney injury (CI-AKI) is a problem associated with the use of iodinated contrast media, causing kidney dysfunction in patients with preexisting renal failure. It accounts for 12% of all hospital-acquired kidney failure and increases the length of hospitalization, a situation that is worsening with increasing numbers of patients with comorbidities, including those requiring cardiovascular interventional procedures. So far, its diagnosis has relied upon the rise in creatinine levels, which is a late marker of kidney damage and is believed to be inadequate. Therefore, there is an urgent need for biomarkers that can detect CI-AKI sooner and more reliably. In recent years, many new biomarkers have been characterized for AKI, and these are discussed particularly with their use in known CI-AKI models and studies and include neutrophil gelatinase-associated lipocalin, cystatin C (Cys-C), kidney injury molecule-1, interleukin-18, N-acetyl-β-d-glucosaminidase, and L-type fatty acid-binding protein (L-FABP). The potential of miRNA and metabolomic technology is also mentioned. Early detection of CI-AKI may lead to early intervention and therefore improve patient outcome, and in future any one or a combination of several of these markers together with development in technology for their analysis may prove effective in this respect.

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“…Na prática clínica, a L-FABP tem sido capaz de diagnosticar a LRA antes mesmo da creatinina sérica em pacientes com nefrotoxicidade induzida por cisplatina (Negishi et al 2009), em choque séptico (Nakamura et al 2009;Tsuchimoto et al 2014), após uso de contraste (Nakamura et al 2006;Vijayasimha et al 2013), após cirurgia cardíaca (Katagiri et al 2012) em pacientes de UTI com sepse (Doi et al 2010) e em transplantados renais (Yamamoto et al 2007b). A L-FABP parece ser um biomarcador de lesão renal no geral, pois também se mostrou alterada em pacientes com DRC (Kamijo et al 2006).…”

Section: L-fabpunclassified

Perfil proteômico da lesão renal aguda induzida por isquemia e reperfusão

Malagrino¹

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Kidney injury molecule-1: A urinary biomarker for contrast-induced acute kidney injury

Cited by 10 publications

References 0 publications

The ischemic/nephrotoxic acute kidney injury and the use of renal biomarkers in clinical practice

The ischemic/nephrotoxic acute kidney injury and the use of renal biomarkers in clinical practice

The potential use of biomarkers in predicting contrast-induced acute kidney injury

Perfil proteômico da lesão renal aguda induzida por isquemia e reperfusão

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