Aberrant Tubuloglomerular Feedback and HIF-1α Confer Resistance to Ischemia after Subtotal Nephrectomy

Singh, Prabhleen; Blantz, Roland C.; Rosenberger, Christian; Gabbai, Francis B.; Schoeb, Trenton R.; Thomson, Scott C.

doi:10.1681/asn.2011020130

Cited by 24 publications

(29 citation statements)

References 53 publications

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“…9 Most prior investigations of the relationships between severe RMR and AKI were limited to the examination of acute injury, usually shorter than 40 minutes in duration, 24 hours after I/R. 14,16 In the only study where the impact of RMR on subsequent AKI was studied over longer periods, subtotal RMR by UNX+ablation/infarction 10 weeks before I/R decreased AKI severity compared with I/R of both intact kidneys, but AKI after I/R in UNX kidneys was more severe. 15 However, there were no differences in repair, which was essentially complete by 10 days in all groups.…”

Section: Discussionmentioning

confidence: 99%

“…13 AKI-CKD relationships have also been questioned on the grounds that mechanisms for AKI-CKD interactions are ill-defined and controversial. [14][15][16] We addressed these uncertainties by investigating the impact of normotensive renal mass reduction (RMR; 0%, 50%, and 75%) of 2-weeks duration on AKI induced by ischemia-reperfusion (I/R) in rats. We addressed three questions.…”

mentioning

confidence: 99%

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Severe Renal Mass Reduction Impairs Recovery and Promotes Fibrosis after AKI

Polichnowski¹,

Lan

Geng

et al. 2014

Journal of the American Society of Nephrology

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Preexisting CKD may affect the severity of and/or recovery from AKI. We assessed the impact of prior graded normotensive renal mass reduction on ischemia-reperfusion-induced AKI. Rats underwent 40 minutes of ischemia 2 weeks after right uninephrectomy and surgical excision of both poles of the left kidney (75% reduction of renal mass), right uninephrectomy (50% reduction of renal mass), or sham reduction of renal mass. The severity of AKI was comparable among groups, which was reflected by similarly increased serum creatinine (S Cr ; approximately 4.5 mg/dl) at 2 days, tubule necrosis at 3 days, and vimentinexpressing regenerating tubules at 7 days postischemia-reperfusion. However, S Cr remained elevated compared with preischemia-reperfusion values, and more tubules failed to differentiate during late recovery 4 weeks after ischemia-reperfusion in rats with 75% renal mass reduction relative to other groups. Tubules that failed to differentiate continued to produce vimentin, exhibited vicarious proliferative signaling, and expressed less vascular endothelial growth factor but more profibrotic peptides. The disproportionate failure of regenerating tubules to redifferentiate in rats with 75% renal mass reduction associated with more severe capillary rarefaction and greater tubulointerstitial fibrosis. Furthermore, initially normotensive rats with 75% renal mass reduction developed hypertension and proteinuria, 2-4 weeks postischemia-reperfusion. In summary, severe (.50%) renal mass reduction disproportionately compromised tubule repair, diminished capillary density, and promoted fibrosis with hypertension after ischemia-reperfusion-induced AKI in rats, suggesting that accelerated declines of renal function may occur after AKI in patients with preexisting CKD. 25: 149625: -150725: , 201425: . doi: 10.1681 Clinical studies suggest that AKI worsens preexisting CKD and accelerates progression to end stage because of residual structural and functional deficits. 1-7 CKD, per se, may increase the risk and severity of AKI and the likelihood of incomplete recovery from AKI. 8 Thus, AKI and CKD reinforce each other to increase nephron loss and tubulointerstitial fibrosis (TIF). 9 Nevertheless, causal relationships for both aspects of the AKI-CKD nexus 10 (AKI resulting in CKD/ESRD and CKD, per se, predisposing to AKI) have been questioned. 11,12 These concerns were recently reviewed. 13 AKI-CKD relationships have also been questioned on the grounds that mechanisms for AKI-CKD interactions are ill-defined and controversial. [14][15][16] We addressed these uncertainties by investigating the impact of normotensive renal mass reduction (RMR; 0%, 50%, and 75%) of 2-weeks duration on AKI induced by ischemia-reperfusion (I/R) in rats. We addressed three questions. (1) Does prior RMR increase AKI severity? (2) Does prior RMR impair recovery from AKI? (3) Does prior RMR predispose to the development of more severe TIF during J Am Soc Nephrol

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Severe Renal Mass Reduction Impairs Recovery and Promotes Fibrosis after AKI

Polichnowski¹,

Lan

Geng

et al. 2014

Journal of the American Society of Nephrology

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“…Indeed, MD-TGF responses were effectively abolished within 7 days of RRM in most, but not all, rat nephrons (1372,1373). The immediate response of MD-TGF is less clear.…”

Section: Carlström Et Almentioning

confidence: 94%

Renal Autoregulation in Health and Disease

Carlström

Wilcox

Arendshorst

2015

Physiological Reviews

391

383

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Intrarenal autoregulatory mechanisms maintain renal blood flow (RBF) and glomerular filtration rate (GFR) independent of renal perfusion pressure (RPP) over a defined range (80-180 mmHg). Such autoregulation is mediated largely by the myogenic and the macula densa-tubuloglomerular feedback (MD-TGF) responses that regulate preglomerular vasomotor tone primarily of the afferent arteriole. Differences in response times allow separation of these mechanisms in the time and frequency domains. Mechanotransduction initiating the myogenic response requires a sensing mechanism activated by stretch of vascular smooth muscle cells (VSMCs) and coupled to intracellular signaling pathways eliciting plasma membrane depolarization and a rise in cytosolic free calcium concentration ([Ca(2+)]i). Proposed mechanosensors include epithelial sodium channels (ENaC), integrins, and/or transient receptor potential (TRP) channels. Increased [Ca(2+)]i occurs predominantly by Ca(2+) influx through L-type voltage-operated Ca(2+) channels (VOCC). Increased [Ca(2+)]i activates inositol trisphosphate receptors (IP3R) and ryanodine receptors (RyR) to mobilize Ca(2+) from sarcoplasmic reticular stores. Myogenic vasoconstriction is sustained by increased Ca(2+) sensitivity, mediated by protein kinase C and Rho/Rho-kinase that favors a positive balance between myosin light-chain kinase and phosphatase. Increased RPP activates MD-TGF by transducing a signal of epithelial MD salt reabsorption to adjust afferent arteriolar vasoconstriction. A combination of vascular and tubular mechanisms, novel to the kidney, provides for high autoregulatory efficiency that maintains RBF and GFR, stabilizes sodium excretion, and buffers transmission of RPP to sensitive glomerular capillaries, thereby protecting against hypertensive barotrauma. A unique aspect of the myogenic response in the renal vasculature is modulation of its strength and speed by the MD-TGF and by a connecting tubule glomerular feedback (CT-GF) mechanism. Reactive oxygen species and nitric oxide are modulators of myogenic and MD-TGF mechanisms. Attenuated renal autoregulation contributes to renal damage in many, but not all, models of renal, diabetic, and hypertensive diseases. This review provides a summary of our current knowledge regarding underlying mechanisms enabling renal autoregulation in health and disease and methods used for its study.

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“…15 Thus, although restoration of RBF and GFR might be a logical strategy in early prerenal states, hypofiltration mediated by the persistence of the tubuloglomerular feedback system may be protective in the presence of significant renal injury. 16 It must be stressed, however, that the importance of tubuloglomerular feedback in mediating the link between prominent decline in GFR and focal tubular injury has been suggested for ischemiareperfusion and nephrotoxic AKI 17,18 but remains unproven in models of septic AKI and clinical AKI caused by multiple insults. Finally, internephron heterogeneity, the focal distribution of lesions and accessibility limited to a subgroup of superficial nephrons, should be kept in mind when interpreting the results of micropuncture techniques.…”

Section: Renal Microcirculation Glomerular Hemodynamics In Akimentioning

confidence: 99%

Renal Hemodynamics in AKI

Matějovič

İnce

Chawla

et al. 2016

Journal of the American Society of Nephrology

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Novel therapeutic interventions are required to prevent or treat AKI. To expedite progress in this regard, a consensus conference held by the Acute Dialysis Quality Initiative was convened in April of 2014 to develop recommendations for research priorities and future directions. Here, we highlight the concepts related to renal hemodynamics in AKI that are likely to reveal new treatment targets on investigation. Overall, we must better understand the interactions between systemic, total renal, and glomerular hemodynamics, including the role of tubuloglomerular feedback. Furthermore, the net consequences of therapeutic maneuvers aimed at restoring glomerular filtration need to be examined in relation to the nature, magnitude, and duration of the insult. Additionally, microvascular blood flow heterogeneity in AKI is now recognized as a common occurrence; timely interventions to preserve the renal microcirculatory flow may interrupt the downward spiral of injury toward progressive kidney failure and should, therefore, be investigated. Finally, development of techniques that permit an integrative physiologic approach, including direct visualization of renal microvasculature and measurement of oxygen kinetics and mitochondrial function in intact tissue in all nephron segments, may provide new insights into how the kidney responds to various injurious stimuli and allow evaluation of new therapeutic strategies.

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Aberrant Tubuloglomerular Feedback and HIF-1α Confer Resistance to Ischemia after Subtotal Nephrectomy

Cited by 24 publications

References 53 publications

Severe Renal Mass Reduction Impairs Recovery and Promotes Fibrosis after AKI

Severe Renal Mass Reduction Impairs Recovery and Promotes Fibrosis after AKI

Renal Autoregulation in Health and Disease

Renal Hemodynamics in AKI

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