Collecting duct-specific knockout of renin attenuates angiotensin II-induced hypertension

Ramkumar, Nirupama; Stuart, Deborah; Rees, Sara; Hoek, Alfred N. Van; Sigmund, Curt D.; Kohan, Donald E.

doi:10.1152/ajprenal.00367.2014

Cited by 55 publications

(76 citation statements)

References 25 publications

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Section: Discussionmentioning

confidence: 99%

“…A recent study showed that deletion of renin in the collecting duct principal cells (using an aquaporin 2-Cre mouse) did not affect blood pressure, even varying Na intake (16). However, those mice had an attenuated response to ANG II-induced hypertension (16). Whether renin expression in the collecting duct plays a role during pathological processes still remains to be investigated, but in our study, deletion of renin in the tubular compartment did not result in any discernible morphological or physiological changes.…”

Section: Discussionmentioning

confidence: 99%

“…A recent study showed that ANG II-induced hypertension is attenuated in a principal cell-specific conditional knockout for renin, using a mouse expressing Cre-recombinase under the control of the Aquaporin 2 promoter (16). Whereas the contribution of RAS genes in ureteric bud branching and renal medulla development has been implied in a number of studies (11, 24 -26, 33), the contribution of tubular renin in overall kidney morphogenesis and development of the renal vasculature has not been established.…”

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Vascular versus tubular renin: role in kidney development

Sequeira-Lόpez

Nagalakshmi

et al. 2015

American Journal of Physiology-Regulatory, Integrative and Comp

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-Renin, the key regulated enzyme of the renin-angiotensin system regulates blood pressure, fluid-electrolyte homeostasis, and renal morphogenesis. Whole body deletion of the renin gene results in severe morphological and functional derangements, including thickening of renal arterioles, hydronephrosis, and inability to concentrate the urine. Because renin is found in vascular and tubular cells, it has been impossible to discern the relative contribution of tubular versus vascular renin to such a complex phenotype. Therefore, we deleted renin independently in the vascular and tubular compartments by crossing Ren1 c fl/fl mice to Foxd1-cre and Hoxb7-cre mice, respectively. Deletion of renin in the vasculature resulted in neonatal mortality that could be rescued with daily injections of saline. The kidneys of surviving mice showed the absence of renin, hypertrophic arteries, hydronephrosis, and negligible levels of plasma renin. In contrast, lack of renin in the collecting ducts did not affect kidney morphology, intra-renal renin, or circulating renin in basal conditions or in response to a homeostatic stress, such as sodium depletion. We conclude that renin generated in the renal vasculature is fundamental for the development and integrity of the kidney, whereas renin in the collecting ducts is dispensable for normal kidney development and cannot compensate for the lack of renin in the vascular compartment. Further, the main source of circulating renin is the kidney vasculature.arterioles; conditional knockout; medulla; renin angiotensin system RENIN IS CRITICAL FOR THE control of blood pressure and fluid/ electrolyte homeostasis. In adult mammals, renin is synthesized and released from juxtaglomerular (JG) cells located in the wall of the afferent arterioles at the entrance to the glomeruli. However, within the embryonic (E) kidney, renin precursors appear before arteriolar development is discernible around E12.5-E14.5 days of gestation (22). JG cells descend from a group of stromal cells, which express the forkhead transcription factor Foxd1 and, in turn, differentiate into all the mural cells of the renal arterioles, pericytes, and glomerular mesangium (23). During this developmental process, renin cells regulate elongation and branching of the renal vasculature, where they are distributed broadly along large intrarenal arteries, in each tip of newly appearing arteriolar branches and inside glomerular cells, which differentiate into mesangial cells (7,8,18,21). Thus, during fetal and postnatal life, there is a widespread distribution and progressive shifting pattern of renin throughout the renal vasculature, and it is not until arteriolar development is finalized that these cells are circumscribed to their "classical" JG location, as typically seen in the adult mammal. Interestingly, Ren1 c KO mice display abnormal renal vascular development, with fewer, shorter, and prominently thicker renal interlobular arteries and afferent arterioles (28). In addition to the vascular abnormalities, the kidneys of Ren1 c KO ...

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Vascular versus tubular renin: role in kidney development

Sequeira-Lόpez

Nagalakshmi

et al. 2015

American Journal of Physiology-Regulatory, Integrative and Comp

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“…Notably, weak renin staining was only observed in the juxtaglomerular apparatus of normal kidneys ( Figure 5F, open arrow), whereas renin was predominantly induced in renal tubular epithelial cells after kidney injury ( Figure 5F, solid arrows), consistent with previous observations. [31][32][33] We further investigated the effects of exogenous Wnt1 on matrix gene expression and renal fibrotic lesions after AKI. As shown in Figure 6, A-D, in vivo expression of exogenous Wnt1 significantly induced the mRNA expression of a-smooth muscle actin (a-SMA), fibronectin, and types I and III collagens in the kidneys after IRI as shown by qRT-PCR analyses.…”

Section: In Vivo Expression Of Wnt Augments Renal Fibrosis After Akimentioning

confidence: 99%

Sustained Activation of Wnt/β-Catenin Signaling Drives AKI to CKD Progression

Lin

Zhou²,

Tan

et al. 2015

JASN

202

214

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AKI is increasingly recognized as a major risk factor for progression to CKD. However, the factors governing AKI to CKD progression are poorly understood. In this study, we investigated this issue using moderate (20 minutes) and severe (30 minutes) ischemia/reperfusion injury (IRI) in mice. Moderate IRI led to acute kidney failure and transient Wnt/b-catenin activation, which was followed by the restoration of kidney morphology and function. However, severe IRI resulted in sustained and exaggerated Wnt/ b-catenin activation, which was accompanied by development of renal fibrotic lesions characterized by interstitial myofibroblast activation and excessive extracellular matrix deposition. To assess the role of sustained Wnt/b-catenin signaling in mediating AKI to CKD progression, we manipulated this signaling by overexpression of Wnt ligand or pharmacologic inhibition of b-catenin. In vivo, overexpression of Wnt1 at 5 days after IRI induced b-catenin activation and accelerated AKI to CKD progression. Conversely, blockade of Wnt/b-catenin by small molecule inhibitor ICG-001 at this point hindered AKI to CKD progression. In vitro, Wnt ligands induced renal interstitial fibroblast activation and promoted fibronectin expression. However, activated fibroblasts readily reverted to a quiescent phenotype after Wnt ligands were removed, suggesting that fibroblast activation requires persistent Wnt signaling. These results indicate that sustained, but not transient, activation of Wnt/b-catenin signaling has a decisive role in driving AKI to CKD progression. 27: 172727: -174027: , 201627: . doi: 10.1681 AKI is responsible for about 2 million deaths each year worldwide, and its incidence is rising. 1-3 AKI is increasingly common in critically ill patients, and those patients with severe AKI requiring dialysis have a mortality rate of .50%. In contrast to the traditional belief that survivors of AKI tend to fully recover renal function, there is growing evidence that patients who survive an episode of AKI will have a significant risk of developing progressive CKD and even ESRD. 1,2,4 Evidence is also mounting that the severity and frequency of AKI seem to be closely correlated with poor patient long-term outcome, 5,6 suggesting that AKI may be a predictive and causative factor for subsequent development of CKD. In this context, delineation of the underlying mechanisms governing the different courses of long-term outcome after AKI will not only shed new light on understanding the pathophysiology of AKI-CKD progression but also is instrumental in designing rational strategies for therapeutic intervention. J Am Soc NephrolWnt/b-catenin is a developmental signaling pathway that plays an essential role in regulating

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“…[10][11][12][13] The involvement of an intrarenal renin-angiotensin system now seems to be an important component of the pathophysiological mechanisms involved in essential hypertension. [12][13][14][15][16][17][18][19] In the present review, I will first provide a brief summary of my earlier contributions to the hypertension field, these having been addressed in more detail in a review arising from my Lewis K. Dahl Memorial Lecture in 2010. 20 I will then review my more recent research, which has involved the determination of alterations in gene expression at the transcriptome-wide level in hypertension and the pivotal mechanistic insights this work has provided, especially an intriguing mechanism controlling intrarenal renin.…”

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confidence: 99%

Renin, Genes, MicroRNAs, and Renal Mechanisms Involved in Hypertension

Morris

2015

Hypertension

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Collecting duct-specific knockout of renin attenuates angiotensin II-induced hypertension

Cited by 55 publications

References 25 publications

Vascular versus tubular renin: role in kidney development

Vascular versus tubular renin: role in kidney development

Sustained Activation of Wnt/β-Catenin Signaling Drives AKI to CKD Progression

Renin, Genes, MicroRNAs, and Renal Mechanisms Involved in Hypertension

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