Antifibrotic Effect of Tamoxifen in a Model of Progressive Renal Disease

Dellê, Humberto; Rocha, José Roberto Coelho da; Cavaglieri, Rita C.; Vieira, J.M.; Malheiros, Denise Maria Avancini Costa; Noronha, Irene L.

doi:10.1681/asn.2011010046

Cited by 77 publications

(84 citation statements)

References 67 publications

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“…Moreover, renoprotection by estrogen is described in other forms of renal injury, including rat models of chronic allograft nephropathy (CAN) (15,24,25), age-related glomerular damage (29), and hypertensive nephrosclerosis (30). The role of estrogen receptors in this process remains a subject of debate.…”

Section: Discussionmentioning

confidence: 99%

Improved renal ischemia tolerance in females influences kidney transplantation outcomes

Aufhauser¹,

Wang²,

Murken³

et al. 2016

Journal of Clinical Investigation

117

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Section: Discussionmentioning

confidence: 99%

Improved renal ischemia tolerance in females influences kidney transplantation outcomes

Aufhauser¹,

Wang²,

Murken³

et al. 2016

Journal of Clinical Investigation

117

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“…[287][288][289][290][291] Tissue damage effected by these species is augmented by intermittent hypoxia reducing renal expression of antioxidants. 292 In addition, intermittent hypoxia induces the sympathetic nervous system to increase vascular resistance, downregulates expression of the kallikrein-kallistatin vasodilator Shelley Transforming growth factor β inhibition 446 Pro-fibrotic metalloproteinase inhibition 447 Anti-fibrotic metalloproteinase activation 447 Destabilization of renal Remote ischemic pre-conditioning [384][385][386][387][388][389][390] hypoxia-inducible factor Prolyl hydroxylase inhibition 244,448 von Hippel-Lindau protein inhibition 449 pathway, and activates the renal renin-angiotensin-aldosterone system to cause vasoconstriction. [293][294][295][296][297][298][299] Together these processes conspire to produce renal fibrosis and sustained hypertension and their associated means of reducing renal oxygenation ( figure 1).…”

Section: Repeated Episodes Of Acute Kidney Injurymentioning

confidence: 99%

Hypoxia: The Force that Drives Chronic Kidney Disease

Colgan

Shelley

2016

Clinical Medicine & Research

125

111

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In the United States the prevalence of end-stage renal disease (ESRD) reached epidemic proportions in 2012 with over 600,000 patients being treated. The rates of ESRD among the elderly are disproportionally high. Consequently, as life expectancy increases and the baby-boom generation reaches retirement age, the already heavy burden imposed by ESRD on the US health care system is set to increase dramatically. ESRD represents the terminal stage of chronic kidney disease (CKD). A large body of evidence indicating that CKD is driven by renal tissue hypoxia has led to the development of therapeutic strategies that increase kidney oxygenation and the contention that chronic hypoxia is the final common pathway to end-stage renal failure. Numerous studies have demonstrated that one of the most potent means by which hypoxic conditions within the kidney produce CKD is by inducing a sustained inflammatory attack by infiltrating leukocytes. Indispensable to this attack is the acquisition by leukocytes of an adhesive phenotype. It was thought that this process resulted exclusively from leukocytes responding to cytokines released from ischemic renal endothelium. However, recently it has been demonstrated that leukocytes also become activated independent of the hypoxic response of endothelial cells. It was found that this endothelium-independent mechanism involves leukocytes directly sensing hypoxia and responding by transcriptional induction of the genes that encode the β2-integrin family of adhesion molecules. This induction likely maintains the long-term inflammation by which hypoxia drives the pathogenesis of CKD. Consequently, targeting these transcriptional mechanisms would appear to represent a promising new therapeutic strategy.

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“…In addition, because tamoxifen has been shown to affect fibrosis, we show that our tamoxifen treatment paradigm did not effect fibrotic response (Supplemental Figure 6). 32 To fate trace Wnt4 expressing cells, we measured baseline recombination 3 days after tamoxifen administration, to be sure that no further recombination would take place. 33,34 Wnt4 GCE/+ ;R26 tdTomato/+ mice were injected with tamoxifen 4 days after UUO injury and euthanized on day 7 and day 14. tdTomato+ cells were counted in coronal kidney sections of five mice at day 7 after UUO, which reflects the Wnt4+ cells present during days 4-7 after UUO ( Figure 5A and Supplemental Figure 7).…”

Section: Wnt4 Is Upregulated In Medullary Interstitial Myofibroblastsmentioning

confidence: 99%

Wnt4/β−Catenin Signaling in Medullary Kidney Myofibroblasts

DiRocco

Kobayashi

Taketo

et al. 2013

Journal of the American Society of Nephrology

159

136

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Injury to the adult kidney induces a number of developmental genes thought to regulate repair, including Wnt4. During kidney development, early nephron precursors and medullary stroma both express Wnt4, where it regulates epithelialization and controls smooth muscle fate, respectively. Expression patterns and roles for Wnt4 in the adult kidney, however, remain unclear. In this study, we used reporters, lineage analysis, and conditional knockout or activation of the Wnt/b-catenin pathway to investigate Wnt4 in the adult kidney. Proliferating, medullary, interstitial myofibroblasts strongly expressed Wnt4 during renal fibrosis, whereas tubule epithelia, except for the collecting duct, did not. Exogenous Wnt4 drove myofibroblast differentiation of a pericyte-like cell line, suggesting that Wnt4 might regulate pericyte-to-myofibroblast transition through autocrine signaling. However, conditional deletion of Wnt4 in interstitial cells did not reduce myofibroblast proliferation, cell number, or myofibroblast gene expression during fibrosis. Because the injured kidney expresses multiple Wnt ligands that might compensate for the absence of Wnt4, we generated a mouse model with constitutive activation of canonical Wnt/b-catenin signaling in interstitial pericytes and fibroblasts. Kidneys from these mice exhibited spontaneous myofibroblast differentiation in the absence of injury. Taken together, Wnt4 expression in renal fibrosis defines a population of proliferating medullary myofibroblasts. Although Wnt4 may be dispensable for myofibroblast transformation, canonical Wnt signaling through b-catenin stabilization is sufficient to drive spontaneous myofibroblast differentiation in interstitial pericytes and fibroblasts, emphasizing the importance of this pathway in renal fibrosis.

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Antifibrotic Effect of Tamoxifen in a Model of Progressive Renal Disease

Cited by 77 publications

References 67 publications

Improved renal ischemia tolerance in females influences kidney transplantation outcomes

Improved renal ischemia tolerance in females influences kidney transplantation outcomes

Hypoxia: The Force that Drives Chronic Kidney Disease

Wnt4/β−Catenin Signaling in Medullary Kidney Myofibroblasts

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