Transcriptional analysis of kidneys during repair from AKI reveals possible roles for NGAL and KIM-1 as biomarkers of AKI-to-CKD transition

Ko, Gang Jee; Grigoryev, Dmitry N.; Linfert, Douglas R.; Jang, Hye Ryoun; Watkins, Tonya; Cheadle, Chris; Racusen, Lorraine C.; Rabb, Hamid

doi:10.1152/ajprenal.00619.2009

Cited by 173 publications

(144 citation statements)

References 44 publications

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“…These clinical findings are supported by preclinical data that mirror those risk factors identified in large observational studies (17,(32)(33)(34).…”

Section: Aki To Ckd In Adultssupporting

confidence: 61%

“…The main mechanisms incriminated in CKD progression include inappropriate vascular, interstitial, and tubular regeneration after AKI (17). These maladaptive processes appear to be linked to impaired angiogenesis and reduced endothelial proliferation (35,36), cell cycle arrest (37), persistent fibrosis (38), epigenetic changes (33), increased expression in kidney tissue microRNAs associated with renal fibrosis (39), and ongoing inflammation (34). Further research to identify potential therapeutic targets to mitigate CKD progression after AKI in humans is urgently needed.…”

Section: Aki To Ckd In Adultsmentioning

confidence: 99%

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AKI Transition of Care

Goldstein

Jaber

Faubel

et al. 2013

Clinical Journal of the American Society of Nephrology

178

124

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SummaryThe incidence rate of AKI is increasing across the spectrum of hospitalized children and adults. Given the increased morbidity and mortality associated with AKI, significant research effort has been appropriately focused on standardizing AKI definitions, identifying risk factors, and discovering and validating novel, earlier structural biomarkers of kidney injury. In addition, a growing body of evidence demonstrates that AKI is a risk factor for the future development or accelerated progression of CKD. Unfortunately, prospective observational studies have not consistently followed survivors of episodes of AKI for longitudinal outcomes after hospital discharge, which could lead to ascertainment bias in terms of over-or underestimation of CKD development. Furthermore, data show that clinical follow-up of AKI survivors is low. This lack of systematic study and clinical follow-up represents a potential missed opportunity to prevent chronic disease after an acute illness and improve outcomes. Therefore, prospective study of transitions of care after episodes of AKI is needed to identify which patients are at risk for CKD development and to optimally target therapeutic interventions.

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“…These clinical findings are supported by preclinical data that mirror those risk factors identified in large observational studies (17,(32)(33)(34).…”

Section: Aki To Ckd In Adultssupporting

confidence: 61%

Section: Aki To Ckd In Adultsmentioning

confidence: 99%

AKI Transition of Care

Goldstein

Jaber

Faubel

et al. 2013

Clinical Journal of the American Society of Nephrology

178

124

View full text Add to dashboard Cite

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“…Preliminary studies have reported on the potential utility of KIM-1 as a CKD biomarker (23,24). Animal models of AKI-to-CKD transition have identified NGAL and KIM-1 as two of the most upregulated genes and proteins in the kidney, revealing a possible role for these proteins as potential biomarkers to predict risk of CKD after AKI (25). The persistent elevation in KIM-1 and IL-18 in AKIpositive patients suggests ongoing kidney injury.…”

Section: Discussionmentioning

confidence: 99%

Follow-Up Renal Assessment of Injury Long-Term After Acute Kidney Injury (FRAIL-AKI)

Cooper

Claes

Goldstein

et al. 2016

Clinical Journal of the American Society of Nephrology

112

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Background and objectives Novel urinary kidney damage biomarkers detect AKI after cardiac surgery using cardiopulmonary bypass (CPB-AKI). Although there is growing focus on whether AKI leads to CKD, no studies have assessed whether novel urinary biomarkers remain elevated long term after CPB-AKI. We assessed whether there was clinical or biomarker evidence of long-term kidney injury in patients with CPB-AKI.Design, setting, participants, & measurements We performed a cross-sectional evaluation for signs of chronic kidney injury using both traditional measures and novel urinary biomarkers in a population of 372 potentially eligible children (119 AKI positive and 253 AKI negative) who underwent surgery using cardiopulmonary bypass for congenital heart disease at Cincinnati Children's Hospital Medical Center between 2004 and 2007. A total of 51 patients (33 AKI positive and 18 AKI negative) agreed to long-term assessment. We also compared the urinary biomarker levels in these 51 patients with those in healthy controls of similar age.Results At long-term follow-up (mean duration6SD, 760.98 years), AKI-positive and AKI-negative patients had similarly normal assessments of kidney function by eGFR, proteinuria, and BP measurement. However, AKI-positive patients had higher urine concentrations of IL-18 (48.5 pg/ml versus 20.3 pg/ml [P=0.01] and 20.5 pg/ml [P,0.001]) and liver-type fatty acid-binding protein (L-FABP) (5.9 ng/ml versus 3.9 ng/ml [P=0.001] and 3.2 ng/ml [P,0.001]) than did AKI-negative patients and healthy controls.Conclusions Novel urinary biomarkers remain elevated 7 years after an episode of CPB-AKI in children. However, there is no conventional evidence of CKD in these children. These biomarkers may be a more sensitive marker of chronic kidney injury after CPB-AKI. Future studies are needed to understand the clinical relevance of persistent elevations in IL-18, kidney injury molecule-1, and L-FABP in assessments for potential long-term kidney consequences of CPB-AKI.

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“…Several promising biomarkers have emerged from these studies (16,17). Analysis of temporal and spatial differences in their expression highlights the cellular complexity of the AKI response (ref.…”

Section: Introductionmentioning

confidence: 99%

Cell-specific translational profiling in acute kidney injury

et al. 2014

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Acute kidney injury (AKI) promotes an abrupt loss of kidney function that results in substantial morbidity and mortality. Considerable effort has gone toward identification of diagnostic biomarkers and analysis of AKI-associated molecular events; however, most studies have adopted organ-wide approaches and have not elucidated the interplay among different cell types involved in AKI pathophysiology. To better characterize AKI-associated molecular and cellular events, we developed a mouse line that enables the identification of translational profiles in specific cell types. This strategy relies on CRE recombinase-dependent activation of an EGFP-tagged L10a ribosomal protein subunit, which allows translating ribosome affinity purification (TRAP) of mRNA populations in CRE-expressing cells. Combining this mouse line with cell type-specific CRE-driver lines, we identified distinct cellular responses in an ischemia reperfusion injury (IRI) model of AKI. Twenty-four hours following IRI, distinct translational signatures were identified in the nephron, kidney interstitial cell populations, vascular endothelium, and macrophages/monocytes. Furthermore, TRAP captured known IRI-associated markers, validating this approach. Biological function annotation, canonical pathway analysis, and in situ analysis of identified response genes provided insight into cell-specific injury signatures. Our study provides a deep, cell-based view of early injury-associated molecular events in AKI and documents a versatile, genetic tool to monitor cell-specific and temporal-specific biological processes in disease modeling.

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Transcriptional analysis of kidneys during repair from AKI reveals possible roles for NGAL and KIM-1 as biomarkers of AKI-to-CKD transition

Cited by 173 publications

References 44 publications

AKI Transition of Care

AKI Transition of Care

Follow-Up Renal Assessment of Injury Long-Term After Acute Kidney Injury (FRAIL-AKI)

Cell-specific translational profiling in acute kidney injury

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