CBP and p300 are essential for renin cell identity and morphological integrity of the kidney

Gómez, R. Ariel; Pentz, Ellen S.; Jin, Xuan; Cordaillat, Magali; López, María Luisa S. Sequeira

doi:10.1152/ajpheart.01266.2008

Cited by 78 publications

(88 citation statements)

References 35 publications

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“…Recently, in vitro and in vivo studies demonstrate the crucial role of the cAMP pathway on the acquisition and maintenance of the renin cell identity. 51,52 Activation of the cAMP pathway was proven to be of importance not only for the well known stimulation of renin release but also for vascular development early in fetal life. Conditional deletion of G␣ s in cells from the renin lineage such as arteriolar SMCs and mesangial cells results in almost complete absence of renin-expressing cells in the fetal kidney accompanied by blunted development of the preglomerular arterial tree.…”

Section: Role Of the Camp Pathwaymentioning

confidence: 99%

Development of the Renal Arterioles

López

Gómez

2011

Journal of the American Society of Nephrology

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125

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Section: Role Of the Camp Pathwaymentioning

confidence: 99%

Development of the Renal Arterioles

López

Gómez

2011

Journal of the American Society of Nephrology

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125

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“…Serial sections (5 m) were deparaffinized in xylenes and graded alcohols. Sections were processed for immunohistochemistry for renin and ␣-smooth muscle actin and stained with hematoxylin or with Masson's trichrome (to assess collagen deposition) as previously described (8,32). To visualize renin granules, 2 m kidney sections were deparaffinized through xylenes and graded alcohols followed by a wash with PBS for 5 min.…”

Section: Generationmentioning

confidence: 99%

“…RNA extraction and cDNA generation by reverse transcription and quantitative real-time PCR using SYBR Green (Invitrogen, Eugene, OR) were performed as previously described (8). Renin mRNA expression was normalized to GAPDH expression.…”

Section: Rna Isolation and Qrt-pcr Analysismentioning

confidence: 99%

Transcriptional regulator RBP-J regulates the number and plasticity of renin cells

Rivera

Monteagudo²,

Pentz³

et al. 2011

Physiological Genomics

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scriptional regulator RBP-J regulates the number and plasticity of renin cells. Physiol Genomics 43: 1021-1028, 2011. First published July 12, 2011 doi:10.1152 doi:10. /physiolgenomics.00061.2011 cells are crucial in the control of blood pressure and fluidelectrolyte homeostasis. Notch receptors convey cell-cell signals that may regulate the renin cell phenotype. Because the common downstream effector for all Notch receptors is the transcription factor RBP-J, we used a conditional knockout approach to delete RBP-J in cells of the renin lineage. The resultant RBP-J conditional knockout (cKO) mice displayed a severe reduction in the number of reninpositive juxtaglomerular apparatuses (JGA) and a reduction in the total number of renin positive cells per JGA and along the afferent arterioles. This reduction in renin protein was accompanied by a decrease in renin mRNA expression, decreased circulating renin, and low blood pressure. To investigate whether deletion of RBP-J altered the ability of mice to increase the number of renin cells normally elicited by a physiological threat, we treated RBP-J cKO mice with captopril and sodium depletion for 10 days. The resultant treated RBP-J cKO mice had a 65% reduction in renin mRNA levels (compared with treated controls) and were unable to increase circulating renin. Although these mice attempted to increase the number of renin cells, the cells were unusually thin and had few granules and barely detectable amounts of immunoreactive renin. As a consequence, the cells were incapable of fully adopting the endocrine phenotype of a renin cell. We conclude that RBP-J is required to maintain basal renin expression and the ability of smooth muscle cells along the kidney vasculature to regain the renin phenotype, a fundamental mechanism to preserve homeostasis. juxtaglomerular cells; cell identity; homeostasis; recruitment; conditional knockout; recombination signal binding protein for immunoglobulin kappa J region

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“…Using a cultured renin linage cell system, studies observed that its gene expression memory is maintained in the cultured cells and may be re-enacted by cAMP and chromatin remodeling (histone H4 acetylation) (44). Other investigators also noted that CREB-binding protein and p300 (which possess histone acetyltransferase activity) are vital for renin cell distinctiveness, as well as the integrity of the renal architecture (45).…”

Section: Role Of Epigenetics In Ckdmentioning

confidence: 99%

Chronic kidney disease in children and the role of epigenetics: Future therapeutic trajectories

et al. 2016

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Abstract. Global differences in the observed causes of chronic kidney disease (CKD) in children are well documented and are attributed to dissimilarities in clime, race, hereditary, and ancestry. Thus, familial clustering and disparities in CKD prevalence rates across ethnic and racial groups indicate that the progression of renal disease has a strong genetic component. Mammalian studies have demonstrated a feasible nexus between nutrition and non-genetic exposure (around the time of conception and in epigenetic changes) in the expression of major genes identified in renal organogenesis. The major consequence is a reduction in the number of nephrons, with subsequent predisposition to hypertension and CKD.

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CBP and p300 are essential for renin cell identity and morphological integrity of the kidney

Cited by 78 publications

References 35 publications

Development of the Renal Arterioles

Development of the Renal Arterioles

Transcriptional regulator RBP-J regulates the number and plasticity of renin cells

Chronic kidney disease in children and the role of epigenetics: Future therapeutic trajectories

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