Your search keyword '"Polycystic Kidney Diseases metabolism"' showing total 16 results

1. Multiomics profiling of mouse polycystic kidney disease progression at a single-cell resolution.

Author

Muto Y, Yoshimura Y, Wu H, Chang-Panesso M, Ledru N, Woodward OM, Outeda P, Cheng T, Mahjoub MR, Watnick TJ, and Humphreys BD

Subjects

Animals, Mice, Transcriptome, Polycystic Kidney Diseases genetics, Polycystic Kidney Diseases metabolism, Polycystic Kidney Diseases pathology, TRPP Cation Channels genetics, TRPP Cation Channels metabolism, Polycystic Kidney, Autosomal Dominant genetics, Polycystic Kidney, Autosomal Dominant pathology, Polycystic Kidney, Autosomal Dominant metabolism, Humans, Gene Expression Profiling, Epigenesis, Genetic, Multiomics, Disease Progression, Single-Cell Analysis methods, Disease Models, Animal

Abstract

Autosomal dominant polycystic kidney disease (ADPKD) is the most common hereditary kidney disease and causes significant morbidity, ultimately leading to kidney failure. PKD pathogenesis is characterized by complex and dynamic alterations in multiple cell types during disease progression, hampering a deeper understanding of disease mechanism and the development of therapeutic approaches. Here, we generate a single-nucleus multimodal atlas of an orthologous mouse PKD model at early, mid, and late timepoints, consisting of 125,434 single-nucleus transcriptomic and epigenetic multiomes. We catalog differentially expressed genes and activated epigenetic regions in each cell type during PKD progression, characterizing cell-type-specific responses to Pkd1 deletion. We describe heterogeneous, atypical collecting duct cells as well as proximal tubular cells that constitute cyst epithelia in PKD. The transcriptional regulation of the cyst lining cell marker GPRC5A is conserved between mouse and human PKD cystic epithelia, suggesting shared gene regulatory pathways. Our single-nucleus multiomic analysis of mouse PKD provides a foundation to understand the earliest changes molecular deregulation in a mouse model of PKD at a single-cell resolution., Competing Interests: Competing interests statement:B.D.H. is a consultant for Janssen Research & Development, LLC, Pfizer and Chinook Therapeutics. B.D.H holds equity in Chinook Therapeutics. B.D.H holds grant funding from Chinook Therapeutics and Janssen Research & Development, LLC. O.M.W has received grants from AstraZeneca unrelated to the current work.

Published

2024

2. A synthetic agent ameliorates polycystic kidney disease by promoting apoptosis of cystic cells through increased oxidative stress.

Author

Fedeles BI, Bhardwaj R, Ishikawa Y, Khumsubdee S, Krappitz M, Gubina N, Volpe I, Andrade DC, Westergerling P, Staudner T, Campolo J, Liu SS, Dong K, Cai Y, Rehman M, Gallagher AR, Ruchirawat S, Croy RG, Essigmann JM, Fedeles SV, and Somlo S

Subjects

Mice, Animals, Cell Proliferation, Apoptosis, Oxidative Stress, DNA metabolism, Kidney metabolism, TRPP Cation Channels genetics, Polycystic Kidney, Autosomal Dominant drug therapy, Polycystic Kidney, Autosomal Dominant genetics, Polycystic Kidney, Autosomal Dominant metabolism, Polycystic Kidney Diseases metabolism, Cysts metabolism

Abstract

Autosomal dominant polycystic kidney disease (ADPKD) is the most common monogenic cause of chronic kidney disease and the fourth leading cause of end-stage kidney disease, accounting for over 50% of prevalent cases requiring renal replacement therapy. There is a pressing need for improved therapy for ADPKD. Recent insights into the pathophysiology of ADPKD revealed that cyst cells undergo metabolic changes that up-regulate aerobic glycolysis in lieu of mitochondrial respiration for energy production, a process that ostensibly fuels their increased proliferation. The present work leverages this metabolic disruption as a way to selectively target cyst cells for apoptosis. This small-molecule therapeutic strategy utilizes 11beta-dichloro, a repurposed DNA-damaging anti-tumor agent that induces apoptosis by exacerbating mitochondrial oxidative stress. Here, we demonstrate that 11beta-dichloro is effective in delaying cyst growth and its associated inflammatory and fibrotic events, thus preserving kidney function in perinatal and adult mouse models of ADPKD. In both models, the cyst cells with homozygous inactivation of Pkd1 show enhanced oxidative stress following treatment with 11beta-dichloro and undergo apoptosis. Co-administration of the antioxidant vitamin E negated the therapeutic benefit of 11beta-dichloro in vivo, supporting the conclusion that oxidative stress is a key component of the mechanism of action. As a preclinical development primer, we also synthesized and tested an 11beta-dichloro derivative that cannot directly alkylate DNA, while retaining pro-oxidant features. This derivative nonetheless maintains excellent anti-cystic properties in vivo and emerges as the lead candidate for development., Competing Interests: Competing interests statement:The patent US9982009 was granted to B.I.F., R.G.C., J.M.E., S.V.F., and S.S., and assigned to Massachusetts Institute of Technology and Yale University. The patent covers the use of the 11beta-dipropyl and related compounds as therapeutics for polycystic kidney disease and polycystic liver disease. All other authors declare no competing interests.

Published

2024

3. Agonists of prostaglandin E 2 receptors as potential first in class treatment for nephronophthisis and related ciliopathies.

Author

Garcia H, Serafin AS, Silbermann F, Porée E, Viau A, Mahaut C, Billot K, Birgy É, Garfa-Traore M, Roy S, Ceccarelli S, Mehraz M, Rodriguez PC, Deleglise B, Furio L, Jabot-Hanin F, Cagnard N, Del Nery E, Fila M, Sin-Monnot S, Antignac C, Lyonnet S, Krug P, Salomon R, Annereau JP, Benmerah A, Delous M, Briseño-Roa L, and Saunier S

Subjects

Animals, Cilia metabolism, Female, Humans, Kidney Diseases, Cystic congenital, Male, Mice, Prostaglandins metabolism, Receptors, Prostaglandin E metabolism, Zebrafish, Ciliopathies drug therapy, Ciliopathies genetics, Ciliopathies metabolism, Polycystic Kidney Diseases metabolism

Abstract

Nephronophthisis (NPH) is an autosomal recessive tubulointerstitial nephropathy belonging to the ciliopathy disorders and known as the most common cause of hereditary end-stage renal disease in children. Yet, no curative treatment is available. The major gene, NPHP1, encodes a protein playing key functions at the primary cilium and cellular junctions. Using a medium-throughput drug-screen in NPHP1 knockdown cells, we identified 51 Food and Drug Administration-approved compounds by their ability to alleviate the cellular phenotypes associated with the loss of NPHP1; 11 compounds were further selected for their physicochemical properties. Among those compounds, prostaglandin E1 (PGE1) rescued ciliogenesis defects in immortalized patient NPHP1 urine-derived renal tubular cells, and improved ciliary and kidney phenotypes in our NPH zebrafish and Nphp1 knockout mouse models. Furthermore, Taprenepag, a nonprostanoid prostaglandin E2 receptor agonist, alleviated the severe retinopathy observed in Nphp1−/− mice. Finally, comparative transcriptomics allowed identification of key signaling pathways downstream PGE1, including cell cycle progression, extracellular matrix, adhesion, or actin cytoskeleton organization. In conclusion, using in vitro and in vivo models, we showed that prostaglandin E2 receptor agonists can ameliorate several of the pleotropic phenotypes caused by the absence of NPHP1; this opens their potential as a first therapeutic option for juvenile NPH-associated ciliopathies.

Published

2022

4. Ttc30a affects tubulin modifications in a model for ciliary chondrodysplasia with polycystic kidney disease.

Author

Getwan M, Hoppmann A, Schlosser P, Grand K, Song W, Diehl R, Schroda S, Heeg F, Deutsch K, Hildebrandt F, Lausch E, Köttgen A, and Lienkamp SS

Subjects

Animals, Bone and Bones metabolism, Bone and Bones pathology, Ciliopathies genetics, Ciliopathies metabolism, Craniosynostoses genetics, Craniosynostoses metabolism, Cytoskeletal Proteins genetics, Disease Models, Animal, Ectodermal Dysplasia genetics, Ectodermal Dysplasia metabolism, Embryo, Nonmammalian metabolism, Musculoskeletal Abnormalities genetics, Musculoskeletal Abnormalities metabolism, Phenotype, Polycystic Kidney Diseases genetics, Polycystic Kidney Diseases metabolism, Tubulin metabolism, Xenopus laevis, Bone and Bones abnormalities, Ciliopathies pathology, Craniosynostoses pathology, Cytoskeletal Proteins metabolism, Ectodermal Dysplasia pathology, Embryo, Nonmammalian pathology, Musculoskeletal Abnormalities pathology, Polycystic Kidney Diseases pathology, Tubulin chemistry

Abstract

Skeletal ciliopathies (e.g., Jeune syndrome, short rib polydactyly syndrome, and Sensenbrenner syndrome) are frequently associated with nephronophthisis-like cystic kidney disease and other organ manifestations. Despite recent progress in genetic mapping of causative loci, a common molecular mechanism of cartilage defects and cystic kidneys has remained elusive. Targeting two ciliary chondrodysplasia loci ( ift80 and ift172 ) by CRISPR/Cas9 mutagenesis, we established models for skeletal ciliopathies in Xenopus tropicalis Froglets exhibited severe limb deformities, polydactyly, and cystic kidneys, closely matching the phenotype of affected patients. A data mining-based in silico screen found ttc30a to be related to known skeletal ciliopathy genes. CRISPR/Cas9 targeting replicated limb malformations and renal cysts identical to the models of established disease genes. Loss of Ttc30a impaired embryonic renal excretion and ciliogenesis because of altered posttranslational tubulin acetylation, glycylation, and defective axoneme compartmentalization. Ttc30a/b transcripts are enriched in chondrocytes and osteocytes of single-cell RNA-sequenced embryonic mouse limbs. We identify TTC30A/B as an essential node in the network of ciliary chondrodysplasia and nephronophthisis-like disease proteins and suggest that tubulin modifications and cilia segmentation contribute to skeletal and renal ciliopathy manifestations of ciliopathies in a cell type-specific manner. These findings have implications for potential therapeutic strategies., Competing Interests: The authors declare no competing interest., (Copyright © 2021 the Author(s). Published by PNAS.)

Published

2021

5. TAZ/Wnt-β-catenin/c-MYC axis regulates cystogenesis in polycystic kidney disease.

Author

Lee EJ, Seo E, Kim JW, Nam SA, Lee JY, Jun J, Oh S, Park M, Jho EH, Yoo KH, Park JH, and Kim YK

Subjects

Adaptor Proteins, Signal Transducing, Animals, Axin Protein, Cell Proliferation, Disease Models, Animal, Epithelial Cells metabolism, Humans, Kidney metabolism, Kidney pathology, Mice, Mice, Knockout, Polycystic Kidney Diseases pathology, Polycystic Kidney, Autosomal Dominant genetics, Polycystic Kidney, Autosomal Dominant pathology, Protein Kinase C deficiency, Protein Kinase C genetics, TRPP Cation Channels genetics, Transcriptome, Polycystic Kidney Diseases genetics, Polycystic Kidney Diseases metabolism, Polycystic Kidney, Autosomal Dominant metabolism, Proto-Oncogene Proteins c-myc metabolism, Trans-Activators metabolism, Wnt Signaling Pathway physiology, beta Catenin metabolism

Abstract

Autosomal-dominant polycystic kidney disease (ADPKD) is the most common genetic renal disease, primarily caused by germline mutation of PKD1 or PKD2 , leading to end-stage renal disease. The Hippo signaling pathway regulates organ growth and cell proliferation. Herein, we demonstrate the regulatory mechanism of cystogenesis in ADPKD by transcriptional coactivator with PDZ-binding motif (TAZ), a Hippo signaling effector. TAZ was highly expressed around the renal cyst-lining epithelial cells of Pkd1 -deficient mice. Loss of Taz in Pkd1 -deficient mice reduced cyst formation. In wild type, TAZ interacted with PKD1, which inactivated β-catenin. In contrast, in PKD1-deficient cells, TAZ interacted with AXIN1, thus increasing β-catenin activity. Interaction of TAZ with AXIN1 in PKD1-deficient cells resulted in nuclear accumulation of TAZ together with β-catenin, which up-regulated c-MYC expression. Our findings suggest that the PKD1-TAZ-Wnt-β-catenin-c-MYC signaling axis plays a critical role in cystogenesis and might be a potential therapeutic target against ADPKD., Competing Interests: The authors declare no competing interest., (Copyright © 2020 the Author(s). Published by PNAS.)

Published

2020

6. Small-molecule allosteric activators of PDE4 long form cyclic AMP phosphodiesterases.

Author

Omar F, Findlay JE, Carfray G, Allcock RW, Jiang Z, Moore C, Muir AL, Lannoy M, Fertig BA, Mai D, Day JP, Bolger G, Baillie GS, Schwiebert E, Klussmann E, Pyne NJ, Ong ACM, Bowers K, Adam JM, Adams DR, Houslay MD, and Henderson DJP

Subjects

Animals, Cell Line, Cyclic AMP metabolism, Cyclic AMP-Dependent Protein Kinases metabolism, Cyclic Nucleotide Phosphodiesterases, Type 4 drug effects, Dogs, Enzyme Activation drug effects, Humans, Madin Darby Canine Kidney Cells, Phosphorylation, Polycystic Kidney Diseases metabolism, Protein Isoforms, Cyclic Nucleotide Phosphodiesterases, Type 4 metabolism

Abstract

Cyclic AMP (cAMP) phosphodiesterase-4 (PDE4) enzymes degrade cAMP and underpin the compartmentalization of cAMP signaling through their targeting to particular protein complexes and intracellular locales. We describe the discovery and characterization of a small-molecule compound that allosterically activates PDE4 long isoforms. This PDE4-specific activator displays reversible, noncompetitive kinetics of activation (increased V max with unchanged K m ), phenocopies the ability of protein kinase A (PKA) to activate PDE4 long isoforms endogenously, and requires a dimeric enzyme assembly, as adopted by long, but not by short (monomeric), PDE4 isoforms. Abnormally elevated levels of cAMP provide a critical driver of the underpinning molecular pathology of autosomal dominant polycystic kidney disease (ADPKD) by promoting cyst formation that, ultimately, culminates in renal failure. Using both animal and human cell models of ADPKD, including ADPKD patient-derived primary cell cultures, we demonstrate that treatment with the prototypical PDE4 activator compound lowers intracellular cAMP levels, restrains cAMP-mediated signaling events, and profoundly inhibits cyst formation. PDE4 activator compounds thus have potential as therapeutics for treating disease driven by elevated cAMP signaling as well as providing a tool for evaluating the action of long PDE4 isoforms in regulating cAMP-mediated cellular processes., Competing Interests: Conflict of interest statement: D.J.P.H., F.O., J.E.F., R.W.A., Z.J., G.C., C.M., A.L.M., K.B., J.M.A., D.R.A., and M.D.H. are employees of Mironid, Limited. N.J.P., E.K., and A.C.M.O. act as consultants to Mironid, Limited., (Copyright © 2019 the Author(s). Published by PNAS.)

Published

2019

7. Green mamba peptide targets type-2 vasopressin receptor against polycystic kidney disease.

Author

Ciolek J, Reinfrank H, Quinton L, Viengchareun S, Stura EA, Vera L, Sigismeau S, Mouillac B, Orcel H, Peigneur S, Tytgat J, Droctové L, Beau F, Nevoux J, Lombès M, Mourier G, De Pauw E, Servent D, Mendre C, Witzgall R, and Gilles N

Subjects

Animals, Benzazepines pharmacology, CHO Cells, Cricetinae, Cricetulus, Crystallography, X-Ray, Cyclic AMP metabolism, Female, HEK293 Cells, Humans, Mice, Mice, Inbred C57BL, Polycystic Kidney Diseases metabolism, Signal Transduction, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Time Factors, Tolvaptan, Trypsin chemistry, Antidiuretic Hormone Receptor Antagonists pharmacology, Dendroaspis, Natriuretic Peptides pharmacology, Peptides pharmacology, Polycystic Kidney Diseases drug therapy, Receptors, Vasopressin genetics, Snake Venoms pharmacology

Abstract

Polycystic kidney diseases (PKDs) are genetic disorders that can cause renal failure and death in children and adults. Lowering cAMP in cystic tissues through the inhibition of the type-2 vasopressin receptor (V2R) constitutes a validated strategy to reduce disease progression. We identified a peptide from green mamba venom that exhibits nanomolar affinity for the V2R without any activity on 155 other G-protein-coupled receptors or on 15 ionic channels. Mambaquaretin-1 is a full antagonist of the V2R activation pathways studied: cAMP production, beta-arrestin interaction, and MAP kinase activity. This peptide adopts the Kunitz fold known to mostly act on potassium channels and serine proteases. Mambaquaretin-1 interacts selectively with the V2R through its first loop, in the same manner that aprotinin inhibits trypsin. Injected in mice, mambaquaretin-1 increases in a dose-dependent manner urine outflow with concomitant reduction of urine osmolality, indicating a purely aquaretic effect associated with the in vivo blockade of V2R. CD1-pcy/pcy mice, a juvenile model of PKD, daily treated with 13 [Formula: see text]g of mambaquaretin-1 for 99 d, developed less abundant (by 33%) and smaller (by 47%) cysts than control mice. Neither tachyphylaxis nor apparent toxicity has been noted. Mambaquaretin-1 represents a promising therapeutic agent against PKDs., Competing Interests: The authors declare no conflict of interest.

Published

2017

8. Cilium transition zone proteome reveals compartmentalization and differential dynamics of ciliopathy complexes.

Author

Dean S, Moreira-Leite F, Varga V, and Gull K

Subjects

Bardet-Biedl Syndrome genetics, Bardet-Biedl Syndrome metabolism, Basal Bodies metabolism, Basal Bodies ultrastructure, Cell Compartmentation, Cilia genetics, Ciliary Motility Disorders genetics, Ciliary Motility Disorders metabolism, Ciliopathies genetics, Cytoskeleton metabolism, Cytoskeleton ultrastructure, Encephalocele genetics, Encephalocele metabolism, Flagella genetics, Flagella metabolism, Flagella ultrastructure, Humans, Microscopy, Electron, Transmission, Microscopy, Fluorescence, Mutation, Polycystic Kidney Diseases genetics, Polycystic Kidney Diseases metabolism, Proteome genetics, Protozoan Proteins genetics, RNA Interference, Retinitis Pigmentosa, Trypanosoma genetics, Trypanosoma ultrastructure, Cilia metabolism, Ciliopathies metabolism, Proteome metabolism, Protozoan Proteins metabolism, Trypanosoma metabolism

Abstract

The transition zone (TZ) of eukaryotic cilia and flagella is a structural intermediate between the basal body and the axoneme that regulates ciliary traffic. Mutations in genes encoding TZ proteins (TZPs) cause human inherited diseases (ciliopathies). Here, we use the trypanosome to identify TZ components and localize them to TZ subdomains, showing that the Bardet-Biedl syndrome complex (BBSome) is more distal in the TZ than the Meckel syndrome (MKS) complex. Several of the TZPs identified here have human orthologs. Functional analysis shows essential roles for TZPs in motility, in building the axoneme central pair apparatus and in flagellum biogenesis. Analysis using RNAi and HaloTag fusion protein approaches reveals that most TZPs (including the MKS ciliopathy complex) show long-term stable association with the TZ, whereas the BBSome is dynamic. We propose that some Bardet-Biedl syndrome and MKS pleiotropy may be caused by mutations that impact TZP complex dynamics., Competing Interests: The authors declare no conflict of interest.

Published

2016

9. Folliculin-interacting proteins Fnip1 and Fnip2 play critical roles in kidney tumor suppression in cooperation with Flcn.

Author

Hasumi H, Baba M, Hasumi Y, Lang M, Huang Y, Oh HF, Matsuo M, Merino MJ, Yao M, Ito Y, Furuya M, Iribe Y, Kodama T, Southon E, Tessarollo L, Nagashima K, Haines DC, Linehan WM, and Schmidt LS

Subjects

Alleles, Animals, Apoptosis Regulatory Proteins genetics, Birt-Hogg-Dube Syndrome genetics, Carrier Proteins genetics, Disease Models, Animal, Female, Kidney pathology, Kidney Neoplasms genetics, Kidney Neoplasms pathology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Phenotype, Polycystic Kidney Diseases metabolism, Proto-Oncogene Proteins genetics, Tumor Suppressor Proteins genetics, Apoptosis Regulatory Proteins metabolism, Carrier Proteins metabolism, Gene Expression Regulation, Neoplastic, Kidney Neoplasms metabolism, Proto-Oncogene Proteins metabolism, Tumor Suppressor Proteins metabolism

Abstract

Folliculin (FLCN)-interacting proteins 1 and 2 (FNIP1, FNIP2) are homologous binding partners of FLCN, a tumor suppressor for kidney cancer. Recent studies have revealed potential functions for Flcn in kidney; however, kidney-specific functions for Fnip1 and Fnip2 are unknown. Here we demonstrate that Fnip1 and Fnip2 play critical roles in kidney tumor suppression in cooperation with Flcn. We observed no detectable phenotype in Fnip2 knockout mice, whereas Fnip1 deficiency produced phenotypes similar to those seen in Flcn-deficient mice in multiple organs, but not in kidneys. We found that absolute Fnip2 mRNA copy number was low relative to Fnip1 in organs that showed phenotypes under Fnip1 deficiency but was comparable to Fnip1 mRNA copy number in mouse kidney. Strikingly, kidney-targeted Fnip1/Fnip2 double inactivation produced enlarged polycystic kidneys, as was previously reported in Flcn-deficient kidneys. Kidney-specific Flcn inactivation did not further augment kidney size or cystic histology of Fnip1/Fnip2 double-deficient kidneys, suggesting pathways dysregulated in Flcn-deficient kidneys and Fnip1/Fnip2 double-deficient kidneys are convergent. Heterozygous Fnip1/homozygous Fnip2 double-knockout mice developed kidney cancer at 24 mo of age, analogous to the heterozygous Flcn knockout mouse model, further supporting the concept that Fnip1 and Fnip2 are essential for the tumor-suppressive function of Flcn and that kidney tumorigenesis in human Birt-Hogg-Dubé syndrome may be triggered by loss of interactions among Flcn, Fnip1, and Fnip2. Our findings uncover important roles for Fnip1 and Fnip2 in kidney tumor suppression and may provide molecular targets for the development of novel therapeutics for kidney cancer.

Published

2015

10. Enhanced stability of Mcl1, a prosurvival Bcl2 relative, blunts stress-induced apoptosis, causes male sterility, and promotes tumorigenesis.

Author

Okamoto T, Coultas L, Metcalf D, van Delft MF, Glaser SP, Takiguchi M, Strasser A, Bouillet P, Adams JM, and Huang DC

Subjects

Alleles, Animals, Cell Death, Cell Survival, Female, Fibroblasts metabolism, Flow Cytometry, Gene Expression Regulation, HEK293 Cells, Humans, Infertility, Male metabolism, Leukemia, Myeloid, Acute metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Myeloid Cell Leukemia Sequence 1 Protein genetics, Polycystic Kidney Diseases metabolism, Protein Structure, Tertiary, Proto-Oncogene Proteins c-bcl-2 genetics, Proto-Oncogene Proteins c-myc metabolism, Spermatogenesis, Testis pathology, Time Factors, Ultraviolet Rays, Apoptosis, Cell Transformation, Neoplastic genetics, Infertility, Male genetics, Myeloid Cell Leukemia Sequence 1 Protein physiology, Proto-Oncogene Proteins c-bcl-2 metabolism

Abstract

The B-cell CLL/lymphoma 2 (Bcl2) relative Myeloid cell leukemia sequence 1 (Mcl1) is essential for cell survival during development and for tissue homeostasis throughout life. Unlike Bcl2, Mcl1 turns over rapidly, but the physiological significance of its turnover has been unclear. We have gained insight into the roles of Mcl1 turnover in vivo by analyzing mice harboring a modified allele of Mcl1 that serendipitously proved to encode an abnormally stabilized form of Mcl1 due to a 13-aa N-terminal extension. Although the mice developed normally and appeared unremarkable, the homozygous males unexpectedly proved infertile due to defective spermatogenesis, which was evoked by enhanced Mcl1 prosurvival activity. Under unstressed conditions, the modified Mcl1 is present at levels comparable to the native protein, but it is markedly stabilized in cells subjected to stresses, such as protein synthesis inhibition or UV irradiation. Strikingly, the modified Mcl1 allele could genetically complement the loss of Bcl2, because introduction of even a single allele significantly ameliorated the severe polycystic kidney disease and consequent runting caused by Bcl2 loss. Significantly, the development of c-MYC-induced acute myeloid leukemia was also accelerated in mice harboring that Mcl1 allele. Our collective findings reveal that, under certain circumstances, the N terminus of Mcl1 regulates its degradation; that some cell types require degradation of Mcl1 to induce apoptosis; and, most importantly, that rapid turnover of Mcl1 can serve as a tumor-suppressive mechanism.

Published

2014

11. Analysis of human samples reveals impaired SHH-dependent cerebellar development in Joubert syndrome/Meckel syndrome.

Author

Aguilar A, Meunier A, Strehl L, Martinovic J, Bonniere M, Attie-Bitach T, Encha-Razavi F, and Spassky N

Subjects

Abnormalities, Multiple, Animals, Antigens, Neoplasm genetics, Antigens, Neoplasm metabolism, Cell Cycle Proteins, Cell Proliferation, Cerebellar Diseases pathology, Cerebellum pathology, Ciliary Motility Disorders pathology, Cytoskeletal Proteins, Encephalocele pathology, Eye Abnormalities pathology, Humans, Immunohistochemistry, In Situ Hybridization, Kidney Diseases, Cystic pathology, Mice, Microscopy, Electron, Transmission, Microscopy, Fluorescence, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Polycystic Kidney Diseases pathology, RNA Interference, Retina abnormalities, Retina metabolism, Retina pathology, Retinitis Pigmentosa, Statistics, Nonparametric, Cerebellar Diseases metabolism, Cerebellum embryology, Cerebellum metabolism, Ciliary Motility Disorders metabolism, Encephalocele metabolism, Eye Abnormalities metabolism, Granulocyte Precursor Cells physiology, Hedgehog Proteins metabolism, Kidney Diseases, Cystic metabolism, Polycystic Kidney Diseases metabolism, Signal Transduction physiology

Abstract

Joubert syndrome (JS) and Meckel syndrome (MKS) are pleiotropic ciliopathies characterized by severe defects of the cerebellar vermis, ranging from hypoplasia to aplasia. Interestingly, ciliary conditional mutant mice have a hypoplastic cerebellum in which the proliferation of cerebellar granule cell progenitors (GCPs) in response to Sonic hedgehog (SHH) is severely reduced. This suggests that Shh signaling defects could contribute to the vermis hypoplasia observed in the human syndromes. As existing JS/MKS mutant mouse models suggest apparently contradictory hypotheses on JS/MKS etiology, we investigated Shh signaling directly on human fetal samples. First, in an examination of human cerebellar development, we linked the rates of GCP proliferation to the different levels and localizations of active Shh signaling and showed that the GCP possessed a primary cilium with CEP290 at its base. Second, we found that the proliferation of GCPs and their response to SHH were severely impaired in the cerebellum of subjects with JS/MKS and Jeune syndrome. Finally, we showed that the defect in GCP proliferation was similar in the cerebellar vermis and hemispheres in all patients with ciliopathy analyzed, suggesting that the specific cause of vermal hypo-/aplasia precedes this defect. Our results, obtained from the analysis of human samples, show that the hemispheres and the vermis are affected in JS/MKS and provide evidence of a defective cellular mechanism in these pathologic processes.

Published

2012

12. Structure of the EF-hand domain of polycystin-2 suggests a mechanism for Ca2+-dependent regulation of polycystin-2 channel activity.

Author

Petri ET, Celic A, Kennedy SD, Ehrlich BE, Boggon TJ, and Hodsdon ME

Subjects

Amino Acid Sequence, Conserved Sequence genetics, Humans, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Polycystic Kidney Diseases metabolism, Sequence Homology, Calcium metabolism, EF Hand Motifs genetics, Models, Molecular, Polycystic Kidney Diseases genetics, Protein Conformation, TRPP Cation Channels chemistry, TRPP Cation Channels metabolism

Abstract

The C-terminal cytoplasmic tail of polycystin-2 (PC2/TRPP2), a Ca(2+)-permeable channel, is frequently mutated or truncated in autosomal dominant polycystic kidney disease. We have previously shown that this tail consists of three functional regions: an EF-hand domain (PC2-EF, 720-797), a flexible linker (798-827), and an oligomeric coiled coil domain (828-895). We found that PC2-EF binds Ca(2+) at a single site and undergoes Ca(2+)-dependent conformational changes, suggesting it is an essential element of Ca(2+)-sensitive regulation of PC2 activity. Here we describe the NMR structure and dynamics of Ca(2+)-bound PC2-EF. Human PC2-EF contains a divergent non-Ca(2+)-binding helix-loop-helix (HLH) motif packed against a canonical Ca(2+)-binding EF-hand motif. This HLH motif may have evolved from a canonical EF-hand found in invertebrate PC2 homologs. Temperature-dependent steady-state NOE experiments and NMR R(1) and R(2) relaxation rates correlate with increased molecular motion in the EF-hand, possibly due to exchange between apo and Ca(2+)-bound states, consistent with a role for PC2-EF as a Ca(2+)-sensitive regulator. Structure-based sequence conservation analysis reveals a conserved hydrophobic surface in the same region, which may mediate Ca(2+)-dependent protein interactions. We propose that Ca(2+)-sensing by PC2-EF is responsible for the cooperative nature of PC2 channel activation and inhibition. Based on our results, we present a mechanism of regulation of the Ca(2+) dependence of PC2 channel activity by PC2-EF.

Published

2010

13. The stumpy gene is required for mammalian ciliogenesis.

Author

Town T, Breunig JJ, Sarkisian MR, Spilianakis C, Ayoub AE, Liu X, Ferrandino AF, Gallagher AR, Li MO, Rakic P, and Flavell RA

Subjects

Animals, Base Sequence, Blotting, Northern, Brain pathology, Cloning, Molecular, Computational Biology, Gene Expression Profiling, Histocytochemistry, Hydrocephalus metabolism, In Situ Hybridization, Kidney pathology, Mice, Mice, Inbred C57BL, Molecular Sequence Data, Polycystic Kidney Diseases metabolism, Reverse Transcriptase Polymerase Chain Reaction, Tubulin metabolism, Cilia physiology, Genetic Predisposition to Disease, Hydrocephalus genetics, Polycystic Kidney Diseases genetics

Abstract

Cilia are present on nearly all cell types in mammals and perform remarkably diverse functions. However, the mechanisms underlying ciliogenesis are unclear. Here, we cloned a previously uncharacterized highly conserved gene, stumpy, located on mouse chromosome 7. Stumpy was ubiquitously expressed, and conditional loss in mouse resulted in complete penetrance of perinatal hydrocephalus (HC) and severe polycystic kidney disease (PKD). We found that cilia in stumpy mutant brain and kidney cells were absent or markedly deformed, resulting in defective flow of cerebrospinal fluid. Stumpy colocalized with ciliary basal bodies, physically interacted with gamma-tubulin, and was present along ciliary axonemes, suggesting that stumpy plays a role in ciliary axoneme extension. Therefore, stumpy is essential for ciliogenesis and may be involved in the pathogenesis of human congenital malformations such as HC and PKD.

Published

2008

14. The polycystic kidney disease protein PKD2 interacts with Hax-1, a protein associated with the actin cytoskeleton.

Author

Gallagher AR, Cedzich A, Gretz N, Somlo S, and Witzgall R

Subjects

Adaptor Proteins, Signal Transducing, Amino Acid Sequence, Animals, Cell Line, Cortactin, Humans, Immunohistochemistry, Membrane Proteins chemistry, Microfilament Proteins metabolism, Molecular Sequence Data, Polycystic Kidney Diseases metabolism, Precipitin Tests, Protein Binding, Recombinant Proteins metabolism, Sequence Homology, Amino Acid, TRPP Cation Channels, Actins metabolism, Cytoskeleton metabolism, Membrane Proteins metabolism, Proteins metabolism

Abstract

Despite the recent positional cloning of the PKD1 and PKD2 genes, which are mutated in the great majority of patients with autosomal-dominant polycystic kidney disease (PKD), the pathogenic mechanism for cyst formation is still unclear. The finding, that the PKD1 and PKD2 proteins interact with each other through their COOH termini, suggests that both proteins are part of the same protein complex or signal transduction pathway. Using a yeast two-hybrid screen with the PKD2 protein, we isolated the PKD2-interacting protein Hax-1. The specificity of the interaction was demonstrated by the fact that PKD2L, a protein closely related to PKD2, failed to interact with Hax-1. Immunofluorescence experiments showed that in most cells PKD2 and Hax-1 colocalized in the cell body, but in some cells PKD2 and Hax-1 also were sorted into cellular processes and lamellipodia. Furthermore we demonstrated an association between Hax-1 and the F-actin-binding protein cortactin, which suggests a link between PKD2 and the actin cytoskeleton. We speculate that PKD2 is involved in the formation of cell-matrix contacts, which are dysfunctional without a wild-type PKD2 protein, thus leading to cystic enlargement of tubular structures in the kidney, liver, and pancreas.

Published

2000

15. Abnormal sodium pump distribution during renal tubulogenesis in congenital murine polycystic kidney disease.

Author

Avner ED, Sweeney WE Jr, and Nelson WJ

Subjects

Aging physiology, Animals, Immunoenzyme Techniques, Kidney pathology, Kidney Cortex enzymology, Kidney Cortex growth & development, Kidney Medulla enzymology, Kidney Medulla growth & development, Kidney Tubules metabolism, Mice, Mice, Inbred C57BL, Polycystic Kidney Diseases genetics, Polycystic Kidney Diseases pathology, Sodium-Potassium-Exchanging ATPase analysis, Kidney metabolism, Kidney Tubules pathology, Polycystic Kidney Diseases metabolism, Sodium-Potassium-Exchanging ATPase metabolism, Sodium-Potassium-Exchanging ATPase physiology

Abstract

Congenital polycystic kidney disease is characterized by the formation of large fluid-filled cysts in kidney tubules. It has been postulated that increased epithelial cell proliferation and altered transtubular fluid transport are necessary for cyst formation. To address the latter problem, we have studied the plasma membrane distribution of the alpha 1 and beta 1 subunits of Na+/K(+)-ATPase during progressive stages of proximal and collecting tubular cyst formation in the CPK mouse, a murine model of autosomal recessive polycystic kidney disease. In both control and cystic proximal tubules, Na+/K(+)-ATPase distribution was restricted to the basal-lateral membrane of cells. However, in newborn through day 5 kidney tissue, 16% of control vs. 47% of cystic outer cortical, 6% of control vs. 46% of cystic inner cortical, and 2% of control vs. 63% of cystic medullary collecting tubules demonstrated apical and lateral membrane distribution of Na+/K(+)-ATPase. In all nephrogenic zones, the percentage of control or cystic collecting tubules demonstrating apical membrane distribution of Na+/K(+)-ATPase decreased over time, but the percentage of cystic collecting tubules with apical membrane Na+/K(+)-ATPase remained significantly greater than in developmentally matched controls. No alterations in the normal distributions of other apical or basal-lateral membrane marker proteins were noted at any stage of control or cystic proximal or collecting tubule development. We conclude that apical-lateral membrane Na+/K(+)-ATPase expression is a normal transient feature of early collecting tubule development. However, apical membrane Na+/K(+)-ATPase persists in cystic kidneys, suggesting that such expression may be a manifestation of the relatively undifferentiated phenotype of epithelial cells lining collecting tubule cysts. The persistence of apical membrane Na+/K(+)-ATPase, if the enzyme is functional, may have pathogenic important in abnormal transtubular fluid transport in polycystic kidney disease.

Published

1992

16. Decreased de novo synthesis of proteoglycans in drug-induced renal cystic disease.

Author

Lelongt B, Carone FA, and Kanwar YS

Subjects

Animals, Glycosaminoglycans biosynthesis, Glycosaminoglycans isolation & purification, Kidney Cortex drug effects, Kidney Cortex ultrastructure, Kidney Medulla drug effects, Kidney Medulla ultrastructure, Kidney Tubules drug effects, Kidney Tubules ultrastructure, Male, Microscopy, Electron, Polycystic Kidney Diseases chemically induced, Rats, Rats, Inbred Strains, Reference Values, Kidney Cortex metabolism, Kidney Medulla metabolism, Kidney Tubules metabolism, Polycystic Kidney Diseases metabolism, Proteoglycans biosynthesis, Thiazoles toxicity

Abstract

Cellular and extracellular (tubular basement membrane, TBM) alterations in the proteoglycans (PGs) of the rat renal tubules in diphenylthiazole-induced cystic disease were investigated. The PGs of normal and cystic kidneys were labeled with [35S]sulfate in an organ-perfusion system. Extracted cellular and TBM PGs were characterized by Sepharose CL-6B chromatography before or after treatment with heparitinase (degrades heparan sulfate) or chondroitinase ABC (degrades chondroitin sulfate). Total radioactivities in cellular, TBM, and medium fractions of cystic kidneys were reduced by factors of 9, 7, and 3, respectively. The PGs obtained from cystic and normal kidneys had similar profiles, namely, two peaks of radioactivity with Kav values of 0.26 (Mr = 130,000-150,000) and 0.40 (Mr = 50,000-55,000). The peaks had variable proportions of radioactivity for cellular and TBM fractions. Besides heparan sulfate, an additional 15-20% of chondroitin sulfate was synthesized in all three fractions obtained from cystic kidneys. The PGs synthesized by cystic kidneys had lower charge-density characteristics as compared to controls by DEAE-Sephacel chromatography. The medium fractions contained mostly glycosaminoglycan chains (Kav = 0.47, Mr = 24,000-26,000) of heparan sulfate. Autoradiograms of tissue samples revealed approximately 50% and approximately 60% decreases of grain densities over the cellular and TBM compartments, respectively. This decrease in de novo PG synthesis may have some relationship in the pathogenesis of polycystic kidney disease.

Published

1988