Insulin-like growth factor binding protein 7 and tissue inhibitor of metalloproteinases-2: differential expression and secretion in human kidney tubule cells

Emlet, David R.; Pastor-Soler, Núria M.; Marciszyn, Allison L.; Wen, Xiang; Gómez, Hernando; Humphries, William H.; Morrisroe, Seth; Volpe, J; Kellum, John A.

doi:10.1152/ajprenal.00271.2016

Cited by 107 publications

(86 citation statements)

References 71 publications

(68 reference statements)

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“…mesoderm, by which originate vasculature, connective tissue, skeleton, and urinary tract. All considered variants affect genes associated to connective tissue, glomerulus, and skeleton impairment (Demirdas et al, 2017;Emlet et al, 2017;Schock et al, 2017;Wunnenburger et al, 2017). However, a critical point regards the clinical significance of variants detected by the analysis.…”

Section: Discussionmentioning

confidence: 99%

High-Throughput Sequencing to Detect Novel Likely Gene-Disrupting Variants in Pathogenesis of Sporadic Brain Arteriovenous Malformations

et al. 2020

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Molecular signaling that leads to brain arteriovenous malformation (bAVM) is to date elusive and this is firstly due to the low frequency of familial cases. Conversely, sporadic bAVM is the most diffuse condition and represents the main source to characterize the genetic basis of the disease. Several studies were conducted in order to detect both germ-line and somatic mutations linked to bAVM development and, in this context, next generation sequencing technologies offer a pivotal resource for the amount of outputted information. We performed whole exome sequencing on a young boy affected by sporadic bAVM. Paired-end sequencing was conducted on an Illumina platform and filtered variants were validated by Sanger sequencing. We detected 20 likely gene-disrupting variants affecting as many loci. Of these variants, 11 are inherited novel variants and one is a de novo nonsense variant, affecting STK4 gene. Moreover, we also considered rare known variants affecting loci involved in vascular differentiation. In order to explain their possible involvement in bAVM pathogenesis, we analyzed molecular networks at Cytoscape platform. In this study we focus on some genetic point variations detected in a child affected by bAVM. Therefore, we suggest these novel affected loci as prioritized for further investigation on pathogenesis of bAVM lesions.

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Section: Discussionmentioning

confidence: 99%

High-Throughput Sequencing to Detect Novel Likely Gene-Disrupting Variants in Pathogenesis of Sporadic Brain Arteriovenous Malformations

et al. 2020

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“…Proximal tubule cells were procured, isolated, and characterized from cortices of whole adult human kidneys obtained from the Center for Organ Recovery and Education (CORE, Pittsburgh, PA, USA) through a University of Pittsburgh approved protocol as previously described (Emlet et al, 2017). Renal cortices from four male donors with a median age of 54 years (IQR of 44-64) were subjected to enzymatic and mechanical dissociation by razor blade mincing and digestion with 200 u/ml Collagenase IV, and 100 u/ml DNAse in HBSS for 1 h at 37 °C, followed by sieving with a 250 μm sieve (Gilson, Lewis Center, OH, USA) to remove undigested material.…”

Section: Star Methods Textmentioning

confidence: 99%

PEBP1 Wardens Ferroptosis by Enabling Lipoxygenase Generation of Lipid Death Signals

Wenzel

Tyurina

Zhao

et al. 2017

Cell

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SUMMARY Ferroptosis is a form of programmed cell death pathogenic to several acute and chronic diseases and executed via oxygenation of polyunsaturated phosphatidylethanolamines (PE) by 15-lipoxygenases (15-LO) that normally use free polyunsaturated fatty acids as substrates. Mechanisms of the altered 15-LO substrate specificity are enigmatic. We sought a common ferroptosis regulator for 15LO. We discovered that PEBP1, a scaffold protein inhibitor of protein kinase cascades, complexes with two 15LO isoforms, 15LO1 and 15LO2, and changes their substrate competence to generate hydroperoxy-PE. Inadequate reduction of hydroperoxy-PE due to insufficiency or dysfunction of a selenoperoxidase, GPX4, leads to ferroptosis. We demonstrated the importance of PEBP1-dependent regulatory mechanisms of ferroptotic death in airway epithelial cells in asthma, kidney epithelial cells in renal failure and cortical and hippocampal neurons in brain trauma. As master regulators of ferroptotic cell death with profound implications for human disease, PEBP1/15LO complexes represent a new target for drug discovery.

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“…Kidney Expression of RGS14-The RGS14 gene is located on chromosome 5, adjacent to SLC34A1, which encodes the NPT2A protein, a renal phosphate transporter. Therefore, we examined the expression of RGS14 in human kidney samples and in proximal and distal tubule cells isolated from these samples (33). As shown in Fig To extend these findings, we sought to determine and characterize the action of RGS14 on PTH-sensitive phosphate transport in RPTEC, a non-transformed line of human proximal tubule cells (34).…”

Section: Resultsmentioning

confidence: 99%

“…Tissue and Cell Preparation-Human adult kidney (HAK10, 65yo M; HAK55, 63yo/M; HAK57, 53yo/M; HAK58, 63yo/F); CD13 (proximal tubule), and CD227 (distal tubule) cells were from male and female donors, as indicated. Tissue procurement and processing have been described (33). CD13 and CD227 cells were seeded on 6 well plates.…”

Section: Methodsmentioning

confidence: 99%

Genetic variants disrupt human RGS₁₄ binding to NHERF₁ and regulation of NPT₂A-mediated phosphate transport

Friedman

Mamonova

Magyar

et al. 2019

Preprint

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RGS14 has been implicated in disordered phosphate metabolism. The human RGS14 gene is adjacent to SLC34A1 that encodes the NPT2A sodium-phosphate cotransporter. Hormone-regulated NPT2A requires the PDZ protein NHERF1 which contains two PDZ domains (PDZ1 and PDZ2). NHERF1 binds the PDZ ligand carboxy tail of NPT2A to regulate phosphate uptake, and this NPT2A:NHERF1 complex is inhibited by parathyroid hormone (PTH). Studies here define roles for RGS14 in NHERF1-dependent, PTH-sensitive phosphate transport. We found that RGS14 binds to NHERF1 via the PDZ2 domain. PTH inhibits NPT2A-mediated phosphate transport and RGS14 blocked this action. Several rare human mutations have been reported in the RGS14 PDZ ligand located at residues 563 (D563N, D563G) and 565 (A565S, A565V). D563N disrupted RGS14 binding to NHERF1 and did not interfere with PTH action, whereas D563G, A565S, and A565V bound NHERF1 and were functionally equivalent to wild-type RGS14. Computational analysis and molecular dynamics modeling of NHERF1 PDZ2 binding to the RGS14 C-terminal PDZ ligands refined the structural determinants of this interaction. Additional studies demonstrated that RGS14 is expressed in human kidney proximal and distal tubule cells. Together, our findings are consistent with the view that RGS14 contributes to PTH-sensitive phosphate transport in humans. RGS14 coding variants may cause disordered phosphate metabolism.

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Insulin-like growth factor binding protein 7 and tissue inhibitor of metalloproteinases-2: differential expression and secretion in human kidney tubule cells

Cited by 107 publications

References 71 publications

High-Throughput Sequencing to Detect Novel Likely Gene-Disrupting Variants in Pathogenesis of Sporadic Brain Arteriovenous Malformations

High-Throughput Sequencing to Detect Novel Likely Gene-Disrupting Variants in Pathogenesis of Sporadic Brain Arteriovenous Malformations

PEBP1 Wardens Ferroptosis by Enabling Lipoxygenase Generation of Lipid Death Signals

Genetic variants disrupt human RGS₁₄ binding to NHERF₁ and regulation of NPT₂A-mediated phosphate transport

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Insulin-like growth factor binding protein 7 and tissue inhibitor of metalloproteinases-2: differential expression and secretion in human kidney tubule cells

Cited by 107 publications

References 71 publications

High-Throughput Sequencing to Detect Novel Likely Gene-Disrupting Variants in Pathogenesis of Sporadic Brain Arteriovenous Malformations

High-Throughput Sequencing to Detect Novel Likely Gene-Disrupting Variants in Pathogenesis of Sporadic Brain Arteriovenous Malformations

PEBP1 Wardens Ferroptosis by Enabling Lipoxygenase Generation of Lipid Death Signals

Genetic variants disrupt human RGS14 binding to NHERF1 and regulation of NPT2A-mediated phosphate transport

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Genetic variants disrupt human RGS₁₄ binding to NHERF₁ and regulation of NPT₂A-mediated phosphate transport