Your search keyword '"Guay-Woodford, Lisa"' showing total 56 results

1. Estimating risk of rapid disease progression in pediatric patients with autosomal dominant polycystic kidney disease: a randomized trial of tolvaptan.

Author

Mekahli, Djalila, Guay-Woodford, Lisa M., Cadnapaphornchai, Melissa A., Goldstein, Stuart L., Dandurand, Ann, Jiang, Huan, Jadhav, Pravin, and Debuque, Laurie

Subjects

*RISK assessment, *VASOPRESSIN, *RESEARCH funding, *RETROSPECTIVE studies, *DESCRIPTIVE statistics, *POLYCYSTIC kidney disease, *CONFIDENCE intervals, *COMPARATIVE studies, *DISEASE progression, *CELL receptors, *GLOMERULAR filtration rate, *CHEMICAL inhibitors, *ADOLESCENCE, *CHILDREN

Abstract

Background: Tolvaptan preserves kidney function in adults with autosomal dominant polycystic kidney disease (ADPKD) at elevated risk of rapid progression. A trial (NCT02964273) evaluated tolvaptan safety and pharmacodynamics in children (5–17 years). However, progression risk was not part of study eligibility criteria due to lack of validated criteria for risk assessment in children. As risk estimation is important to guide clinical management, baseline characteristics of the study participants were retrospectively evaluated to determine whether risk of rapid disease progression in pediatric ADPKD can be assessed and to identify parameters relevant for risk estimation. Methods: Four academic pediatric nephrologists reviewed baseline data and rated participant risk from 1 (lowest) to 5 (highest) based on clinical judgement and the literature. Three primary reviewers independently scored all cases, with each case reviewed by two primary reviewers. For cases with discordant ratings (≥ 2-point difference), the fourth reviewer provided a secondary rating blinded to the primary evaluations. Study participants with discordant ratings and/or for whom data were lacking were later discussed to clarify parameters relevant to risk estimation. Results: Of 90 evaluable subjects, primary reviews of 69 (77%) were concordant. The proportion considered at risk of rapid progression (final mean rating ≥ 3.5) by age group was: 15–17 years, 27/34 (79%); 12– < 15, 9/32 (28%); 4– < 12, 8/24 (33%). The panelists agreed on characteristics important for risk determination: age, kidney imaging, kidney function, blood pressure, urine protein, and genetics. Conclusions: High ratings concordance and agreement among reviewers on relevant clinical characteristics support the feasibility of pediatric risk assessment. A higher resolution version of the Graphical abstract is available as Supplementary information [ABSTRACT FROM AUTHOR]

Published

2024

2. Extracellular vesicles in renal disease.

Author

Hartung, Erum A., Guay-Woodford, Lisa M., Karpman, Diana, Ståhl, Anne-Lie, and Arvidsson, Ida

Subjects

*AUTOSOMAL recessive polycystic kidney, *KIDNEY function tests, *HEPATIC fibrosis, *HYPERTENSION, *GENETIC mutation

Abstract

Extracellular vesicles, such as exosomes and microvesicles, are host cell-derived packages of information that allow cell-cell communication and enable cells to rid themselves of unwanted substances. The release and uptake of extracellular vesicles has important physiological functions and may also contribute to the development and propagation of inflammatory, vascular, malignant, infectious and neurodegenerative diseases. This Review describes the different types of extracellular vesicles, how they are detected and the mechanisms by which they communicate with cells and transfer information. We also describe their physiological functions in cellular interactions, such as in thrombosis, immune modulation, cell proliferation, tissue regeneration and matrix modulation, with an emphasis on renal processes. We discuss how the detection of extracellular vesicles could be utilized as biomarkers of renal disease and how they might contribute to disease processes in the kidney, such as in acute kidney injury, chronic kidney disease, renal transplantation, thrombotic microangiopathies, vasculitides, IgA nephropathy, nephrotic syndrome, urinary tract infection, cystic kidney disease and tubulopathies. Finally, we consider how the release or uptake of extracellular vesicles can be blocked, as well as the associated benefits and risks, and how extracellular vesicles might be used to treat renal diseases by delivering therapeutics to specific cells. [ABSTRACT FROM AUTHOR]

Published

2017

3. Renal cystic diseases: diverse phenotypes converge on the cilium/centrosome complex.

Author

Guay-Woodford, Lisa

Subjects

*CYSTIC kidney disease, *KIDNEY diseases, *CENTROSOMES, *CELLS, *KARYOKINESIS, *PHENOTYPES

Abstract

Inherited renal cystic diseases constitute an important set of single-gene disorders that frequently progress to end stage renal disease (ESRD). Transmitted as autosomal dominant, autosomal recessive, or X-linked traits, renal cystic diseases are phenotypically diverse with respect to age at onset, rate of disease progression, and associated extra-renal manifestations. These disorders involve defects in a set of gene products commonly referred to as cystoproteins that, while functionally distinct, appear to co-localize, at least in part, with the cilia/centrosome complex. Therefore, investigations are increasingly focused on the role of this complex in the pathogenesis of renal cystic disease. Sorting out the functional relationship between these cystoproteins and the cilia/centrosome complex will undoubtedly provide a better understanding of renal cystic disease pathogenesis and, potentially, identify new targets for therapeutic intervention. [ABSTRACT FROM AUTHOR]

Published

2006

4. Murine models of polycystic kidney disease: molecular and therapeutic insights.

Author

Guay-Woodford, Lisa M.

Subjects

*POLYCYSTIC kidney disease, *KIDNEY diseases, *NEPHROLOGY

Abstract

Numerous murine (mouse and rat) models of polycystic kidney disease (PKD) have been described in which the mutant phenotype results from a spontaneous mutation or engineering via chemical mutagenesis, transgenic technologies, or gene-specific targeting in mouse orthologs of human PKD genes. These murine phenotypes closely resemble human PKD, with common abnormalities observed in tubular epithelia, the interstitial compartment, and the extracellular matrix of cystic kidneys. In both human and murine PKD, genetic background appears to modulate the renal cystic phenotype. In murine models, these putative modifying effects have been dissected into discrete factors called quantitative trait loci and genetically mapped. Several lines of experimental evidence support the hypothesis that PKD genes and their modifiers may define pathways involved in cystogenesis and PKD progression. Among the various pathway abnormalities described in murine PKD, recent provocative data indicate that structural and/or functional defects in the primary apical cilia of tubular epithelia may play a key role in PKD pathogenesis. This review describes the most widely studied murine models; highlights the data regarding specific gene defects and genetic modifiers; summarizes the data from these models that have advanced our understanding of PKD pathogenesis; and examines the effect of various therapeutic interventions in murine PKD. [ABSTRACT FROM AUTHOR]

Published

2003

5. Renal structure in early autosomal-dominant polycystic kidney disease (ADPKD): The Consortium for Radiologic Imaging Studies of Polycystic Kidney Disease (CRISP) cohort1.

Author

Chapman, Arlene B., Guay-Woodford, Lisa M., Grantham, Jared J., Torres, Vicente E., Bae, Kyongtae T., Baumgarten, Deborah A., Kenney, Philip J., King, Bernard F., Glockner, James F., Wetzel, Louis H., Brummer, Marijn E., O'Neill, W. Charles, Robbin, Michelle L., Bennett, William M., Klahr, Saulo, Hirschman, Gladys H., Kimmel, Paul L., Thompson, Paul A., and Miller, J. Philip

Subjects

*POLYCYSTIC kidney disease, *RADIOGRAPHY, *CYSTIC kidney disease, *DIAGNOSTIC imaging

Abstract

Renal structure in early autosomal-dominant polycystic kidney disease (ADPKD): The Consortium for Radiologic Imaging Studies of Polycystic Kidney Disease (CRISP) cohort Background. Autosomal-dominant polycystic kidney disease (ADPKD) is characterized by gradual renal enlargement and cyst growth prior to loss of renal function. Standard radiographic imaging has not provided the resolution and accuracy necessary to detect small changes in renal volume or to reliably measure renal cyst volumes. The Consortium for Radiologic Imaging Studies in Polycystic Kidney Disease (CRISP) is longitudinally observing ADPKD individuals using high-resolution magnetic resonance (MR) imaging to determine if change in renal and cyst volumes can be detected over a short period of time, and if they correlate with decline in renal function early in disease. Methods. Standardization studies were conducted in phantoms and four subjects at each participating clinical center. After, in the full-scale protocol, healthy ADPKD individuals 15 to 45 years old with creatinine clearance>70 mL/min underwent standardized MR renal imaging, renal iothalamate clearance, comprehensive clinical evaluation, and determination of 24-hour urinary albumin and electrolyte excretion. Stereology was used from T1-weighted images to quantify renal volume, and region-growing thresholding was used from T2-weighted images to determine cyst volume. Renal structures were evaluated in relation to demographic, clinical, and biochemical variables using means/medians, standard deviations, and Pearson correlations. Results. Reliability coefficients for MR renal and cyst volume measurements in phantoms were 99.9% and 89.2%, respectively. In the full-scale protocol, 241 ADPKD individuals (145 women and 96 men) were enrolled. Total renal, cyst, and % cyst volume were significantly greater in each decade group. Hypertensive individuals demonstrated greater renal, cyst, and % cyst volume than normotensive subjects. Age-adjusted renal (r = -0.31, P < 0.0001), cyst (r = -0.36, P < 0.0001), and % cyst volume (r = -0.35, P < 0.0001) were inversely related to glomerular filtration rate (GFR). Age-adjusted renal volume (r = 0.42, P < 0.0001), cystic (r = 0.39, P < 0.0001, and % cyst volume (r = 0.41, P < 0.0001) were related with urinary albumin excretion. Conclusion. MR measures of renal and cyst volume are reliable and accurate in patients with ADPKD. ADPKD is characterized by significant cystic involvement that increases with age. Structure (renal and cyst volume) and function (GFR) are inversely related and directly related with the presence of hypertension and urinary albumin excretion in individuals with normal renal function. [ABSTRACT FROM AUTHOR]

Published

2003

6. Autosomal Recessive Polycystic Kidney Disease: The Clinical Experience in North America.

Author

Guay-Woodford, Lisa M. and Desmond, Renee A.

Subjects

*POLYCYSTIC kidney disease, *PEDIATRICS

Abstract

ABSTRACT. Objective. We designed a longitudinal clinical database for autosomal recessive polycystic kidney disease (ARPKD), recruited patients from pediatric nephrology centers in the United States and Canada, and examined their clinical morbidities and survival characteristics. We initially targeted enrollment to children who were born and diagnosed after January 1, 1990, so as to capture a cohort that is representative of ARPKD patients born in the last decade. When a significant number of older ARPKD patients were also referred, we extended our database to include all patients who met our inclusion criteria, thereby allowing direct comparisons between a long-term survivor subset and a cohort that included both neonatal survivors and nonsurvivors. Design. Patient entry into our database required either compatible histopathology or ultrasonographic evidence of enlarged, echogenic kidneys and the presence of at least 1 of the following additional criteria: a) biopsyproven ARPKD in a sibling; b) biliary fibrosis based on either clinical or histopathologic evidence; c) no sonographic evidence of renal cysts in the parents (parents must be >30 years of age); or d) parental consanguinity, eg, first-cousin marriage. Clinical questionnaires (primary data form and follow-up data form) were developed to collect initial patient data and follow-up data at yearly intervals. Results. Thirty-four centers provided clinical information for 254 patients and of these, 209 had sufficient data for analyses. When stratified by date of birth, 166 (79.4%) were born on or after January 1, 1990 (younger cohort) and 43 children (20.6%) were born before 1990 (older cohort). The gender distribution was equal in both cohorts. The median age at diagnosis was significantly later in the older cohort and no deaths were reported among these patients, suggesting that this group is biased toward long-term survivors. In the younger cohort, 74.7% of the patients are alive, with a median age of... [ABSTRACT FROM AUTHOR]

Published

2003

7. Proceedings of the Eighth International Workshop on Developmental Nephrology: Genes, Morphogenesis, and Function. The Sessions.

Author

Satlin, Lisa M., Guay-Woodford, Lisa, and Chevalier, Robert L.

Subjects

*NEPHROLOGY, *CONFERENCES & conventions, *GROWTH factors, *NEOVASCULARIZATION

Abstract

Presents the proceedings of the sessions of the 'Eighth International Workshop on Developmental Nephrology: Genes, Morphogenesis, and Function,' held in Victoria on August 29-31, 2001. Molecular control of nephrogenesis; Discussion on growth factors and receptors; Initiation of the proceedings on angiogenesis and vasculogenesis.

Published

2003

8. Diffuse renal cystic disease in children: morphologic and genetic correlations.

Author

Guay-Woodford, Lisa M., Galliani, Carlos A., Musulman-Mroczek, Elizabeth, Spear, Gerald S., Guillot, Ann P., and Bernstein, Jay

Subjects

*POLYCYSTIC kidney disease, *PEDIATRIC nephrology, *HUMAN molecular genetics

Abstract

During a 5-year period, we evaluated seven infants and two fetuses who presented with enlarged, hyperechoic kidneys. In each, the initial clinical diagnosis was autosomal recessive polycystic kidney disease (ARPKD). Among the seven unrelated infants were three Caucasian and four African-American infants. No syndromic stigmata were evident in any of these infants. At the time of the initial evaluation, the family data were incomplete for four infants. The two fetuses were presumed to be at-risk for ARPKD based on the diagnosis in previous siblings. Renal histopathology was evaluated in all nine cases and revealed a spectrum of cystic disease ranging from ARPKD to glomerulocystic kidney disease to autosomal dominant polycystic kidney disease to diffuse cystic dysplasia. In the eight cases for whom liver histopathology was available, varying degrees of biliary dysgenesis were evident. We present a detailed analysis of the key histopathological features in each case and discuss the histopathological findings in an embryological context. In addition, we address the current role of molecular genetics in the diagnostic evaluation. [ABSTRACT FROM AUTHOR]

Published

1998

9. Bartter syndrome: unraveling the pathophysiologic enigma.

Author

Guay-Woodford, Lisa M. and Guay-Woodford, L M

Subjects

*SYNDROMES, *BARTTER syndrome, *DIFFERENTIAL diagnosis, *KIDNEY tubules, *PROGNOSIS

Abstract

Familial hypokalemic, hypochloremic metabolic alkalosis, or Bartter syndrome, is not a single disorder but rather a set of closely related disorders. These Bartter-like syndromes share many of the same physiologic derangements, but differ with regard to the age of onset, the presenting symptoms, the magnitude of urinary potassium (K) and prostaglandin excretion, and the extent of urinary calcium excretion. At least three clinical phenotypes have been distinguished: (1) classic Bartter syndrome; (2) the hypocalciuric-hypomagnesemic Gitelman variant; and (3) the antenatal hypercalciuric variant (also termed hyperprostaglandin E syndrome). The fundamental pathogenesis of this complex set of disorders has long fascinated and stymied investigators. Physiologic investigations have suggested numerous pathogenic models. The cloning of genes encoding renal transport proteins has provided molecular tools to begin testing these hypotheses. To date, molecular genetic analyses have determined that mutations in the gene encoding the thiazide-sensitive sodium-chloride (Na-Cl) cotransporter underlie the pathogenesis of the Gitelman variant. In comparison, the antenatal variant is genetically heterogeneous with mutations in the genes encoding either the bumetanide-sensitive sodium-potassium-chloride (Na-K-2Cl) cotransporter or the luminal, ATP-regulated, K channel. With these data, investigators have begun to unravel the pathophysiologic enigma of the Bartter-like syndromes. Further studies will help refine pathogenic models for this set of disorders as well as provide new insights into the normal mechanisms of renal electrolyte transport. [ABSTRACT FROM AUTHOR]

Published

1998

10. RIP-ed and ready to dance: new mechanisms for polycystin-1 signaling.

Author

Guay-woodford, Lisa M.

Subjects

*POLYCYSTIC kidney disease, *HUMAN chromosome abnormalities, *PROTEOLYSIS, *PROTEIN metabolism, *GENETIC transcription, *PROTEINS

Abstract

Polycystin-1, the protein encoded by the principal gene involved in autosomal dominant polycystic kidney disease, has been implicated in extracellular sensing as well as in cell-cell and cell-matrix interactions. However, the precise mechanisms involved in polycystin-1 signaling are not well defined. A report in this issue of the JCI demonstrates that the C-terminal tail of polycystin-1 is cleaved from the membrane through regulated intramembrane proteolysis (RIP) and that this domain translocates to the nucleus, where it activates the AP-1 transcription pathway (see the related article beginning on page 1433). This translocation appears to be modulated by polycystin-2, with which polycystin-1 is thought to interact. These findings provide what we believe to be the first evidence that polycystin-1 can signal directly to the nucleus and that polycystin-1-polycystin-2 interactions do not require colocalization of these proteins in the same membrane compartment. [ABSTRACT FROM AUTHOR]

Published

2004

11. Increased risk of kidney failure in patients with genetic kidney disorders.

Author

Elliott, Mark D., Vena, Natalie, Marasa, Maddalena, Cocchi, Enrico, Bheda, Shiraz, Bogyo, Kelsie, Ning Shang, Zanoni, Francesca, Verbitsky, Miguel, Chen Wang, Kolupaeva, Victoria, Gina Jin, Sofer, Maayan, Pena, Rafael Gras, Canetta, Pietro A., Bomback, Andrew S., Guay-Woodford, Lisa M., Jean Hou, Gillespie, Brenda W., and Robinson, Bruce M.

Subjects

*GENETIC disorders, *KIDNEY failure, *DISEASE risk factors, *MEDICAL genetics, *WHOLE genome sequencing, *FAMILY history (Medicine), *MOLECULAR diagnosis

Abstract

BACKGROUND. It is unknown whether the risk of kidney disease progression and failure differs between patients with and without genetic kidney disorders. METHODS. Three cohorts were evaluated: the prospective Cure Glomerulonephropathy Network (CureGN) and 2 retrospective cohorts from Columbia University, including 5,727 adults and children with kidney disease from any etiology who underwent whole-genome or exome sequencing. The effects of monogenic kidney disorders and APOL1 kidney-risk genotypes on the risk of kidney failure, estimated glomerular filtration rate (eGFR) decline, and disease remission rates were evaluated along with diagnostic yields and the impact of American College of Medical Genetics secondary findings (ACMG SFs). RESULTS. Monogenic kidney disorders were identified in 371 patients (6.5%), high-risk APOL1 genotypes in 318 (5.5%), and ACMG SFs in 100 (5.2%). Family history of kidney disease was the strongest predictor of monogenic disorders. After adjustment for traditional risk factors, monogenic kidney disorders were associated with an increased risk of kidney failure (hazard ratio [HR] = 1.72), higher rate of eGFR decline (-3.06 vs. 0.25 mL/min/1.73 m² /year), and lower risk of complete remission (odds ratioNot achieving CR = 5.25). High-risk APOL1 genotypes were associated with an increased risk of kidney failure (HR = 1.67) and faster eGFR decline (-2.28 vs. 0.25 mL/min/1.73 m² ), replicating prior findings. ACMG SFs were not associated with personal or family history of associated diseases, but were predicted to impact care in 70% of cases. CONCLUSIONS. Monogenic kidney disorders were associated with an increased risk of kidney failure, faster eGFR decline, and lower rates of complete remission, suggesting opportunities for early identification and intervention based on molecular diagnosis. [ABSTRACT FROM AUTHOR]

Published

2024

12. Phenotypic variability in PKD1: The family as a starting point.

Author

Guay-Woodford, Lisa M.

Subjects

*POLYCYSTIC kidney disease, *KIDNEY diseases, *GENETICS

Abstract

Editorial. Focuses on phenotypic variability in polycystic kidney disease (PKD). Characteristics of the disease; Progression of renal cystic lesion; Clinical expression of PKD1-related diseases.

Published

1999

13. Pkhd1cyli/cyli mice have altered renal Pkhd1 mRNA processing and hormonally sensitive liver disease.

Author

Yang, Chaozhe, Harafuji, Naoe, Caldovic, Ljubica, Yu, Weiying, Boddu, Ravindra, Bhattacharya, Surajit, Barseghyan, Hayk, Gordish-Dressman, Heather, Foreman, Oded, Bebok, Zsuzsa, Eicher, Eva M., and Guay-Woodford, Lisa M.

Subjects

*AUTOSOMAL recessive polycystic kidney, *POLYCYSTIC kidney disease, *LIVER diseases, *GENE expression, *DELETION mutation, *HEPATORENAL syndrome

Abstract

Autosomal-recessive polycystic kidney disease (ARPKD; MIM #263200) is a severe, hereditary, hepato-renal fibrocystic disorder that causes early childhood morbidity and mortality. Mutations in the polycystic kidney and hepatic disease 1 (PKHD1) gene, which encodes the protein fibrocystin/polyductin complex (FPC), cause all typical forms of ARPKD. Several mouse lines carrying diverse, genetically engineered disruptions in the orthologous Pkhd1 gene have been generated, but none expresses the classic ARPKD renal phenotype. In the current study, we characterized a spontaneous mouse Pkhd1 mutation that is transmitted as a recessive trait and causes cysticliver (cyli), similar to the hepato-biliary disease in ARPKD, but which is exacerbated by age, sex, and parity. We mapped the mutation to Chromosome 1 and determined that an insertion/deletion mutation causes a frameshift within Pkhd1 exon 48, which is predicted to result in a premature termination codon (UGA). Pkhd1cyli/cyli (cyli) mice exhibit a severe liver pathology but lack renal disease. Further analysis revealed that several alternatively spliced Pkhd1 mRNA, all containing exon 48, were expressed in cyli kidneys, but in lower abundance than in wild-type kidneys, suggesting that these transcripts escaped from nonsense-mediated decay (NMD). We identified an AAAAAT motif in exon 48 upstream of the cyli mutation which could enable ribosomal frameshifting, thus potentially allowing production of sufficient amounts of FPC for renoprotection. This mechanism, expressed in a species-specific fashion, may help explain the disparities in the renal phenotype observed between Pkhd1 mutant mice and patients with PKHD1-related disease. Key messages: The Pkhd1cyli/cyli mouse expresses cystic liver disease, but no kidney phenotype. Pkhd1 mRNA expression is decreased in cyli liver and kidneys compared to wild-type. Ribosomal frameshifting may be responsible for Pkhd1 mRNA escape from NMD. Pkhd1 mRNA escape from NMD could contribute to the absent kidney phenotype. [ABSTRACT FROM AUTHOR]

Published

2023

14. Cystin is required for maintaining fibrocystin (FPC) levels and safeguarding proteome integrity in mouse renal epithelial cells: A mechanistic connection between the kidney defects in cpk mice and human ARPKD.

Author

Zhang, Yiming J., Yang, Chaozhe, Wang, Wei, Harafuji, Naoe, Stasiak, Piotr, Bell, P. Darwin, Caldovic, Ljubica, Sztul, Elizabeth, Guay‐Woodford, Lisa M., and Bebok, Zsuzsanna

Abstract

Autosomal recessive polycystic kidney disease (ARPKD) is caused primarily by mutations in PKHD1, encoding fibrocystin (FPC), but Pkhd1 mutant mice failed to reproduce the human phenotype. In contrast, the renal lesion in congenital polycystic kidney (cpk) mice, with a mutation in Cys1 and cystin protein loss, closely phenocopies ARPKD. Although the nonhomologous mutation diminished the translational relevance of the cpk model, recent identification of patients with CYS1 mutations and ARPKD prompted the investigations described herein. We examined cystin and FPC expression in mouse models (cpk, rescued‐cpk (r‐cpk), Pkhd1 mutants) and mouse cortical collecting duct (CCD) cell lines (wild type (wt), cpk). We found that cystin deficiency caused FPC loss in both cpk kidneys and CCD cells. FPC levels increased in r‐cpk kidneys and siRNA of Cys1 in wt cells reduced FPC. However, FPC deficiency in Pkhd1 mutants did not affect cystin levels. Cystin deficiency and associated FPC loss impacted the architecture of the primary cilium, but not ciliogenesis. No reduction in Pkhd1 mRNA levels in cpk kidneys and CCD cells suggested posttranslational FPC loss. Studies of cellular protein degradation systems suggested selective autophagy as a mechanism. In support of the previously described function of FPC in E3 ubiquitin ligase complexes, we demonstrated reduced polyubiquitination and elevated levels of functional epithelial sodium channel in cpk cells. Therefore, our studies expand the function of cystin in mice to include inhibition of Myc expression via interaction with necdin and maintenance of FPC as functional component of the NEDD4 E3 ligase complexes. Loss of FPC from E3 ligases may alter the cellular proteome, contributing to cystogenesis through multiple, yet to be defined, mechanisms. [ABSTRACT FROM AUTHOR]

Published

2023

15. Introduction to the Proceedings of the Eighth International Workshop on Developmental Nephrology: Genes, Morphogenesis, and Function.

Author

Satlin, Lisa M., Guay-Woodford, Lisa, and Chevalier, Robert L.

Subjects

*NEPHROLOGY, *CONFERENCES & conventions

Abstract

Discusses the organization of the 'Eight International Workshop on Developmental Nephrology: Genes, Morphogenesis, and Function,' held in Victoria, British Columbia on August 29-31, 2001. Provision of a comprehensive analysis in developmental nephrology; Assembly of investigators involved in the field of developmental renal physiology; Integration of topics on genetics of renal development.

Published

2003

16. Genetic Disorders of Renal Electrolyte Transport.

Author

Scheinman, Steven J., Guay-Woodford, Lisa M., Thakker, Rajesh V., and Warnock, David G.

Subjects

*KIDNEY diseases, *RENAL tubular transport disorders, *SODIUM channels, *GENETIC disorders, *GENETICS

Abstract

Discusses genetic disorders of renal electrolyte transport. Mutations affecting the epithelial sodium channel; Renal tubular disorders inherited by mendelian traits; Mutations affecting diuretic-sensitive sodium-transport proteins; Mutations associated with X-linked hypophoshatemic rickets; Conclusions.

Published

1999

17. Founder mutation in the PMM2 promotor causes hyperinsulinemic hypoglycaemia/polycystic kidney disease (HIPKD).

Author

Islam, Sumaya, Tekman, Mehmet, Flanagan, Sarah E., Guay‐Woodford, Lisa, Hussain, Khalid, Ellard, Sian, Kleta, Robert, Bockenhauer, Detlef, Stanescu, Horia, and Iancu, Daniela

Subjects

*POLYCYSTIC kidney disease, *HAPLOTYPES, *SINGLE nucleotide polymorphisms, *HYPOGLYCEMIA, *HETEROZYGOSITY, *PROMOTERS (Genetics)

Abstract

Background: Polycystic kidney disease with hyperinsulinaemic hypoglycaemia (HIPKD) is a recently described disease caused by a single nucleotide variant, c.‐167G>T, in the promoter region of PMM2 (encoding phosphomannomutase 2), either in homozygosity or compound heterozygosity with a pathogenic coding variant in trans. All patients identified so far are of European descent, suggesting a possible founder effect. Methods: We generated high density genotyping data from 11 patients from seven unrelated families, and used this information to identify a common haplotype that included the promoter variant. We estimated the age of the promoter mutation with DMLE+ software, using demographic parameters corresponding to the European population. Results: All patients shared a 0.312 Mb haplotype which was absent in 503 European controls available in the 1000 Genomes Project. The age of this mutation was estimated as 105–110 generations, indicating its occurrence around 600 BC, a time of intense migration, which might explain the presence of the same mutations in Europeans around the globe. Conclusion: The shared unique haplotype among seemingly unrelated patients is consistent with a founder effect in Europeans. [ABSTRACT FROM AUTHOR]

Published

2021

18. Cystin genetic variants cause autosomal recessive polycystic kidney disease associated with altered Myc expression.

Author

Yang, Chaozhe, Harafuji, Naoe, O'Connor, Amber K., Kesterson, Robert A., Watts, Jacob A., Majmundar, Amar J., Braun, Daniela A., Lek, Monkol, Laricchia, Kristen M., Fathy, Hanan M., Mane, Shrikant, Shril, Shirlee, Hildebrandt, Friedhelm, and Guay-Woodford, Lisa M.

Subjects

*POLYCYSTIC kidney disease, *MYC proteins, *PROTEIN expression, *EPITHELIAL cells, *LABORATORY mice

Abstract

Mutation of the Cys1 gene underlies the renal cystic disease in the Cys1cpk/cpk (cpk) mouse that phenocopies human autosomal recessive polycystic kidney disease (ARPKD). Cystin, the protein product of Cys1, is expressed in the primary apical cilia of renal ductal epithelial cells. In previous studies, we showed that cystin regulates Myc expression via interaction with the tumor suppressor, necdin. Here, we demonstrate rescue of the cpk renal phenotype by kidney-specific expression of a cystin-GFP fusion protein encoded by a transgene integrated into the Rosa26 locus. In addition, we show that expression of the cystin-GFP fusion protein in collecting duct cells down-regulates expression of Myc in cpk kidneys. Finally, we report the first human patient with an ARPKD phenotype due to homozygosity for a deleterious splicing variant in CYS1. These findings suggest that mutations in Cys1/CYS1 cause an ARPKD phenotype in mouse and human, respectively, and that the renal cystic phenotype in the mouse is driven by overexpression of the Myc proto-oncogene. [ABSTRACT FROM AUTHOR]

Published

2021

19. Heterozygous Pkhd1C642* mice develop cystic liver disease and proximal tubule ectasia that mimics radiographic signs of medullary sponge kidney.

Author

Shan, Dan, Rezonzew, Gabriel, Mullen, Sean, Roye, Ronald, Juling Zhou, Chumley, Phillip, Revell, Dustin Z., Challa, Anil, Kim, Harrison, Lockhart, Mark E., Schoeb, Trenton R., Croyle, Mandy J., Kesterson, Robert A., Yoder, Bradley K., Guay-Woodford, Lisa M., and Mrug, Michal

Subjects

*AUTOSOMAL recessive polycystic kidney, *CYSTIC kidney disease, *HEPATIC echinococcosis, *LIVER diseases, *KIDNEY diseases, *BILE ducts

Abstract

Heterozygosity for human polycystic kidney and hepatic disease 1 (PKHD1) mutations was recently associated with cystic liver disease and radiographic findings resembling medullary sponge kidney (MSK). However, the relevance of these associations has been tempered by a lack of cystic liver or renal disease in heterozygous mice carrying Pkhd1 gene trap or exon deletions. To determine whether heterozygosity for a smaller Pkhd1 defect can trigger cystic renal disease in mice, we generated and characterized mice with the predicted truncating Pkhd1C642** mutation in a region corresponding to the middle of exon 20 cluster of five truncating human mutations (between PKHD1G617fs and PKHD1G644*). Mouse heterozygotes or homozygotes for the Pkhd1C642** mutation did not have noticeable liver or renal abnormalities on magnetic resonance images during their first weeks of life. However, when aged to ~1.5 yr, the Pkhd1C642** heterozygotes developed prominent cystic liver changes; tissue analyses revealed biliary cysts and increased number of bile ducts without signs of congenital hepatic fibrosis-like portal field inflammation and fibrosis that was seen in Pkhd1C642** homozygotes. Interestingly, aged female Pkhd1C642** heterozygotes, as well as homozygotes, developed radiographic changes resembling MSK. However, these changes correspond to proximal tubule ectasia, not an MSK-associated collecting duct ectasia. In summary, by demonstrating that cystic liver and kidney abnormalities are triggered by heterozygosity for the Pkhd1C642** mutation, we provide important validation for relevant human association studies. Together, these investigations indicate that PKHD1 mutation heterozygosity (predicted frequency 1 in 70 individuals) is an important underlying cause of cystic liver disorders and MSK-like manifestations in a human population. [ABSTRACT FROM AUTHOR]

Published

2019

20. CTSA Consortium Consensus Scientific Review Committee (SRC) Working Group Report on the SRC Processes.

Author

Selker, Harry P., Buse, John B., Califf, Robert M., Carter, Robert, Cooper, Dan M., Davis, Jonathan, Ford, Daniel E., Galassetti, Pietro, Guay‐Woodford, Lisa, Huggins, Gordon S., Kasper, Amanda, Kieburtz, Karl, Kirby, Aaron, Klein, Andreas K., Kline, Joel, O’ Neill, Robert T., Rape, Marie, Reichgott, Douglas J., Rojevsky, Svetlana, and Rosenthal, Gary E.

Subjects

*REVIEW committees, *TRANSLATIONAL research, *RESEARCH, *TECHNICAL specifications, *SOCIETIES

Abstract

Human research projects must have a scientifically valid study design, analytic plan, and be operationally feasible in order to be successfully completed and thus to have translational impact. To ensure this, institutions that conduct clinical research should have a scientific review process prior to submission to the Institutional Review Committee (IRB). This paper reports the Clinical and Translational Science Award (CTSA) Consortium Scientific Review Committee (SRC) Consensus Working Group's proposed framework for a SRC process. Recommendations are provided for institutional support and roles of CTSAs, multisite research, criteria for selection of protocols that should be reviewed, roles of committee members, application process, and committee process. Additionally, to support the SCR process effectively, and to ensure efficiency, the Working Group recommends information technology infrastructures and evaluation metrics to determine outcomes are provided. [ABSTRACT FROM AUTHOR]

Published

2015

21. The cpk model of recessive PKD shows glutamine dependence associated with the production of the oncometabolite 2-hydroxyglutarate.

Author

Hwang, Vicki J., Kim, Jeffrey, Rand, Amy, Yang, Chaozhe, Sturdivant, Steve, Hammock, Bruce, Bell, P. Darwin, Guay-Woodford, Lisa M., and Weiss, Robert H.

Subjects

*CREATINE kinase, *POLYCYSTIC kidney disease treatment, *GLUTAMINE

Abstract

Since polycystic kidney disease (PKD) was first noted over 30 years ago to have neoplastic parallels, there has been a resurgent interest in elucidating neoplasia-relevant pathways in PKD. Taking a nontargeted metabolomics approach in the B6(Cg)-Cys 1cpk/ J(cpk) mouse model of recessive PKD, we have now characterized metabolic reprogramming in these tissues, leading to a glutamine-dependent TCA cycle shunt toward total 2-hydroxyglutarate (2-HG) production in cpk compared with B6 wild-type kidney tissue. After confirmation of increased 2-HG expression in immortalized collecting duct cpk cells as well as in human autosomal recessive PKD tissue using targeted analysis, we show that the increase in 2-HG is likely due to glutamine-sourced-ketoglutarate. In addition, cpk cells require exogenous glutamine for growth such that inhibition of glutaminase-1 decreases cell viability as well as proliferation. This study is a demonstration of the striking parallels between recessive PKD and cancer metabolism. Our data, once confirmed in other PKD models, suggest that future therapeutic approaches targeting this pathway, such as using glutaminase inhibitors, have the potential to open novel treatment options for renal cystic disease. [ABSTRACT FROM AUTHOR]

Published

2015

22. Genetic and Informatic Analyses Implicate Kif12 as a Candidate Gene within the Mpkd2 Locus That Modulates Renal Cystic Disease Severity in the Cys1cpk Mouse.

Author

Mrug, Michal, Zhou, Juling, Yang, Chaozhe, Aronow, Bruce J., Cui, Xiangqin, Schoeb, Trenton R., Siegal, Gene P., Yoder, Bradley K, and Guay-Woodford, Lisa M.

Subjects

*POLYCYSTIC kidney disease, *LABORATORY mice, *CHROMOSOMES, *CYSTIC kidney disease, *GENE expression, *NEPHRONS, *PATIENTS, *DIAGNOSIS

Abstract

We have previously mapped the interval on Chromosome 4 for a major polycystic kidney disease modifier (Mpkd) of the B6(Cg)-Cys1cpk/J mouse model of recessive polycystic kidney disease (PKD). Informatic analyses predicted that this interval contains at least three individual renal cystic disease severity-modulating loci (Mpkd1-3). In the current study, we provide further validation of these predicted effects using a congenic mouse line carrying the entire CAST/EiJ (CAST)-derived Mpkd1-3 interval on the C57BL/6J background. We have also generated a derivative congenic line with a refined CAST-derived Mpkd1-2 interval and demonstrated its dominantly-acting disease-modulating effects (e.g., 4.2-fold increase in total cyst area; p<0.001). The relative strength of these effects allowed the use of recombinants from these crosses to fine map the Mpkd2 effects to a <14 Mbp interval that contains 92 RefSeq sequences. One of them corresponds to the previously described positional Mpkd2 candidate gene, Kif12. Among the positional Mpkd2 candidates, only expression of Kif12 correlates strongly with the expression pattern of Cys1 across multiple anatomical nephron structures and developmental time points. Also, we demonstrate that Kif12 encodes a primary cilium-associated protein. Together, these data provide genetic and informatic validation of the predicted renal cystic disease-modulating effects of Mpkd1-3 loci and implicate Kif12 as the candidate locus for Mpkd2. [ABSTRACT FROM AUTHOR]

Published

2015

23. Magnetic resonance microscopy of renal and biliary abnormalities in excised tissues from a mouse model of autosomal recessive polycystic kidney disease.

Author

Lee, Choong H., O'Connor, Amber K., Yang, Chaozhe, Tate, Joshua M., Schoeb, Trenton R., Flint, Jeremy J., Blackband, Stephen J., and Guay‐Woodford, Lisa M.

Subjects

*AUTOSOMAL recessive polycystic kidney, *MAGNETIC resonance microscopy, *BILE duct diseases, *KIDNEYS, *LABORATORY mice, *MAGNETIC resonance imaging

Abstract

Polycystic kidney disease ( PKD) is transmitted as either an autosomal dominant or recessive trait and is a major cause of renal failure and liver fibrosis. The cpk mouse model of autosomal recessive PKD ( ARPKD) has been extensively characterized using standard histopathological techniques after euthanasia. In the current study, we sought to validate magnetic resonance microscopy ( MRM) as a robust tool for assessing the ARPKD phenotype. We used MRM to evaluate the liver and kidney of wild-type and cpk animals at resolutions <100 μm and generated three-dimensional (3D) renderings for pathological evaluation. Our study demonstrates that MRM is an excellent method for evaluating the complex, 3D structural defects in this ARPKD mouse model. We found that MRM was equivalent to water displacement in assessing kidney volume. Additionally, using MRM we demonstrated for the first time that the cpk liver exhibits less extensive ductal arborization, that it was reduced in volume, and that the ductal volume was disproportionately smaller. Histopathology indicates that this is a consequence of bile duct malformation. With its reduced processing time, volumetric information, and 3D capabilities, MRM will be a useful tool for future in vivo and longitudinal studies of disease progression in ARPKD. In addition, MRM will provide a unique tool to determine whether the human disease shares the newly appreciated features of the murine biliary phenotype. [ABSTRACT FROM AUTHOR]

Published

2015

24. Clinical and genetic characterization of a founder PKHD1 mutation in Afrikaners with ARPKD.

Author

Lambie, Lindsay, Amin, Rasheda, Essop, Fahmida, Cnaan, Avital, Krause, Amanda, and Guay-Woodford, Lisa

Subjects

*DNA analysis, *ETHNIC groups, *GENETIC mutation, *POLYMERASE chain reaction, *SURVIVAL analysis (Biometry), *SURVIVAL, *RETROSPECTIVE studies, *DATA analysis software, *HAPLOTYPES, *DESCRIPTIVE statistics, *AUTOSOMAL recessive polycystic kidney, *GENETICS

Abstract

Background: Autosomal recessive polycystic kidney disease (ARPKD; MIM 263200) occurs in 1:20,000 live births. Disease expression is widely variable, with approximately 30 % of affected neonates dying perinatally, while others survive to adulthood. Mutations at the PKHD1 locus are responsible for all typical presentations. The objectives of this study were to define the clinical and genetic characteristics in a cohort of South African patients of Afrikaner origin, a population with a high prevalence of ARPKD. Methods: DNA from the cohort was analyzed for background haplotypes and the p.M627K mutation previously identified in two unrelated Afrikaner patients. The clinical phenotype of the homozygous group was characterized. Results: Analysis of 36 Afrikaner families revealed that 27 patients, from 24 (67 %) families, were homozygous for the p.M627K substitution, occurring on a common haplotype. The clinical phenotype of the homozygous individuals was variable. Conclusions: Our data provide strong evidence that the p.M627K substitution is a founder mutation in the Afrikaner population and can be used for streamlined diagnostic testing for at-risk pregnancies. The observed clinical variability suggests that disease expression is modulated by other genetic loci or by gene-environment interactions. [ABSTRACT FROM AUTHOR]

Published

2015

25. Intragenic motifs regulate the transcriptional complexity of Pkhd1/PKHD1.

Author

Boddu, Ravindra, Yang, Chaozhe, O'Connor, Amber, Hendrickson, Robert, Boone, Braden, Cui, Xiangqin, Garcia-Gonzalez, Miguel, Igarashi, Peter, Onuchic, Luiz, Germino, Gregory, and Guay-Woodford, Lisa

Subjects

*AUTOSOMAL recessive polycystic kidney, *COMPLEMENTATION (Genetics), *GENE regulatory networks, *ANIMAL models in research, *PROTEINS, *DIAGNOSIS

Abstract

Autosomal recessive polycystic kidney disease (ARPKD) results from mutations in the human PKHD1 gene. Both this gene, and its mouse ortholog, Pkhd1, are primarily expressed in renal and biliary ductal structures. The mouse protein product, fibrocystin/polyductin complex (FPC), is a 445-kDa protein encoded by a 67-exon transcript that spans >500 kb of genomic DNA. In the current study, we observed multiple alternatively spliced Pkhd1 transcripts that varied in size and exon composition in embryonic mouse kidney, liver, and placenta samples, as well as among adult mouse pancreas, brain, heart, lung, testes, liver, and kidney. Using reverse transcription PCR and RNASeq, we identified 22 novel Pkhd1 kidney transcripts with unique exon junctions. Various mechanisms of alternative splicing were observed, including exon skipping, use of alternate acceptor/donor splice sites, and inclusion of novel exons. Bioinformatic analyses identified, and exon-trapping minigene experiments validated, consensus binding sites for serine/arginine-rich proteins that modulate alternative splicing. Using site-directed mutagenesis, we examined the functional importance of selected splice enhancers. In addition, we demonstrated that many of the novel transcripts were polysome bound, thus likely translated. Finally, we determined that the human PKHD1 R760H missense variant alters a splice enhancer motif that disrupts exon splicing in vitro and is predicted to truncate the protein. Taken together, these data provide evidence of the complex transcriptional regulation of Pkhd1/PKHD1 and identified motifs that regulate its splicing. Our studies indicate that Pkhd1/PKHD1 transcription is modulated, in part by intragenic factors, suggesting that aberrant PKHD1 splicing represents an unappreciated pathogenic mechanism in ARPKD. Key messages: [ABSTRACT FROM AUTHOR]

Published

2014

26. Neurocognition in children with autosomal recessive polycystic kidney disease in the CKiD cohort study.

Author

Hartung, Erum, Matheson, Matthew, Lande, Marc, Dell, Katherine, Guay-Woodford, Lisa, Gerson, Arlene, Warady, Bradley, Hooper, Stephen, and Furth, Susan

Subjects

*CARDIOVASCULAR disease diagnosis, *HYPERTENSION, *COGNITIVE testing, *FISHER exact test, *GLOMERULAR filtration rate, *NEUROPSYCHOLOGICAL tests, *NEUROPSYCHOLOGY, *REGRESSION analysis, *RESEARCH funding, *STATISTICS, *DATA analysis, *CROSS-sectional method, *DATA analysis software, *DESCRIPTIVE statistics, *AUTOSOMAL recessive polycystic kidney, *DISEASE complications

Abstract

Background: Autosomal recessive polycystic kidney disease (ARPKD) is an inherited disorder characterized by enlarged, cystic kidneys with progressive chronic kidney disease (CKD), systemic hypertension, and congenital hepatic fibrosis. Children with ARPKD can have early onset CKD and severe hypertension, both of which are known to have adverse neurocognitive effects. The objectives of this study were (1) to determine whether ARPKD patients have greater neurocognitive deficits compared to that of children with other causes of CKD, and (2) to examine the relative prevalence of hypertension in ARPKD, a known risk factor for neurocognitive dysfunction. Methods: We performed a cross-sectional, control-matched analysis of 22 ARPKD patients with mild-to-moderate CKD in the Chronic Kidney Disease in Children (CKiD) cohort study, compared with a control group of 44 children with other causes of CKD, matched based on glomerular filtration rate, age at study entry, and age at diagnosis. Results: Children with ARPKD in this cohort had neurocognitive functioning comparable to children with other causes of CKD in domains of intellectual functioning, academic achievement, attention regulation, executive functioning, and behavior. Blood pressure parameters were similar between the two groups; however, ARPKD patients required a significantly greater number of antihypertensive medications to achieve similar BP levels. Conclusions: ARPKD patients are potentially at risk for neurocognitive dysfunction due to early onset CKD and more severe hypertension. However, this study of children with mild-to-moderate CKD in the CKiD cohort did not demonstrate increased risk in children with ARPKD compared to children with other causes of CKD. Further studies are needed to determine if these findings are applicable to children with more severe manifestations of ARPKD. [ABSTRACT FROM AUTHOR]

Published

2014

27. Expanding the phenotype of proteinuria in Dent disease. A case series.

Author

Cramer, Monica, Charlton, Jennifer, Fogo, Agnes, Fathallah-Shaykh, Sahar, Askenazi, David, and Guay-Woodford, Lisa

Subjects

*GENETIC disorder diagnosis, *GLOMERULONEPHRITIS, *BIOPSY, *KIDNEY tubules, *GENETIC mutation, *PROTEINURIA, *PHENOTYPES, *DESCRIPTIVE statistics, *DIAGNOSIS

Abstract

Background: Dent disease is an X-linked recessive renal tubular disorder characterized by low molecular weight proteinuria, hypercalciuria, nephrocalcinosis, nephrolithiasis, and progressive renal failure (MIM 300009). A recent case series identified four patients with CLCN5 mutations who presented with nephrotic-range proteinuria, histologic evidence of focal segmental and/or global sclerosis, and low molecular weight proteinuria. Case-Diagnosis/Treatment: We characterize the clinical, genetic, and histopathological features of seven unrelated adolescent males with nephrotic-range proteinuria and CLCN5 mutations. Six patients underwent renal biopsy prior to assessing tubular proteinuria. All biopsied patients had either segmental sclerosis (3/6) or segmental increase in mesangial matrix (3/6). Five patients revealed some degree of foot process effacement, but only one patient biopsy revealed >50 % foot process effacement. The attenuated foot process effacement suggests the glomerulosclerosis is not due to a primary podocytopathy. Conclusions: These data suggest that clinicians should consider a diagnostic evaluation for Dent disease in young males presenting with high-grade proteinuria. [ABSTRACT FROM AUTHOR]

Published

2014

28. Renal Macrophages in Autosomal Recessive Polycystic Kidney Disease.

Author

Mrug, Michal, Zhou, Juling, Guay‐Woodford, Lisa M, and Smythies, Lesley E

Subjects

*KIDNEY diseases, *MACROPHAGES

Abstract

A letter to the editor is presented in response to the article related with renal macrophages in autosomal recessive polycystic kidney disease.

Published

2013

29. The Ciliary Protein Cystin Forms a Regulatory Complex with Necdin to ModulateMyc Expression.

Author

Wu, Maoqing, Yang, Chaozhe, Tao, Binli, Bu, Su, and Guay-Woodford, Lisa M.

Subjects

*LABORATORY mice, *AUTOSOMAL recessive polycystic kidney, *ANIMAL models in research, *CYSTINE, *GENETIC regulation, *GENE expression

Abstract

Cystin is a novel cilia-associated protein that is disrupted in the cpk mouse, a well-characterized mouse model of autosomal recessive polycystic kidney disease (ARPKD). Interestingly, overexpression of the Myc gene is evident in animal models of ARPKD and is thought to contribute to the renal cystic phenotype. Using a yeast two-hybrid approach, the growth suppressor protein necdin, known to modulate Myc expression, was found as an interacting partner of cystin. Deletion mapping demonstrated that the C-terminus of cystin and both termini of necdin are required for their mutual interaction. Speculating that these two proteins may function to regulate gene expression, we developed a luciferase reporter assay and observed that necdin strongly activated the Myc P1 promoter, and cystin did so more modestly. Interestingly, the necdin effect was significantly abrogated when cystin was co-transfected. Chromatin immunoprecipitation and electrophoretic mobility shift assays revealed a physical interaction with both necdin and cystin and the Myc P1 promoter, as well as between these proteins. The data suggest that these proteins likely function in a regulatory complex. Thus, we speculate that Myc overexpression in the cpk kidney results from the dysregulation of the cystin-necdin regulatory complex and c-Myc, in turn, contributes to cystogenesis in the cpk mouse. [ABSTRACT FROM AUTHOR]

Published

2013

30. X-ray diffraction studies on merohedrally twinned Δ1-62NtNBCe1-A crystals of the sodium/bicarbonate cotransporter.

Author

Gill, Harindarpal S., Dutcher, Lauren, Boron, Walter F., Patel, Samir, and Guay-Woodford, Lisa M.

Subjects

*SODIUM bicarbonate, *MACROMOLECULES, *BICARBONATE ions, *SODIUM ions, *X-ray diffraction, *CELL membranes

Abstract

NBCe1-A membrane-embedded macromolecules that cotransport sodium and bicarbonate ions across the bilayer serve to maintain acid-base homeostasis throughout the body. Defects result in a number of renal and eye disorders, including type-II renal tubular acidosis and cataracts. Here, crystals of a human truncated mutant of the cytoplasmic N-terminal domain of NBCe1 (Δ1-62NtNBCe1-A) are reported that diffract X-rays to 2.4 Å resolution. The crystal symmetry of Δ1-62NtNBCe1-A is of space group P31 with pseudo- P3121 symmetry and it has a hemihedral twin fraction of 33.0%. The crystals may provide insight into the pathogenic processes observed in a subset of patients with truncating and point mutations in the gene encoding NBCe1. [ABSTRACT FROM AUTHOR]

Published

2013

31. Telomerase immortalization of principal cells from mouse collecting duct.

Author

Steele, Stacy L., Yongren Wu, Kolb, Robert J., Gooz, Monika, Haycraft, Courtney J., Keyser, Kent T., Guay-Woodford, Lisa, Hai Yao, and Bell, P. Darwin

Subjects

*TELOMERASE, *REVERSE transcriptase, *BENZAMIDE, *GENETIC engineering, *DNA polymerases

Abstract

Recently, the use of overexpression of telomerase reverse transcriptase (TERT) has led to the generation of immortalized human cell lines. However, this cell immortalization approach has not been reported in well-differentiated mouse cells, such as renal epithelial cells. We sought to establish and then characterize a mouse collecting duct cell line, using ectopic expression of mTERT. Isolated primary cortical collecting duct (CCD) cell lines were transduced with mouse (m)TERT, using a lentiviral vector. mTERT-negative cells did not survive blasticidin selection, whereas mTERT-immortalized cells proliferated in selection media for over 40 subpassages. mTERT messenger RNA and telomerase activity was elevated in these cells, compared with an SV40-immortalized cell line. Flow cytometry with Dolichos biflorus agglutinin was used to select the CCD principal cells, and we designated this cell line mTERT-CCD. Cells were well differentiated and exhibited morphological characteristics typically found in renal epithelial cells, such as tight junction formation, microvilli, and primary cilia. Further characterization using standard immunofluorescence revealed abundant expression of aquaporin-2 and the vasopressin type 2 receptor. mTERT-CCD cells exhibited cAMP-stimulated/benzamil-inhibited whole cell currents. Whole cell patch-clamp currents were also enhanced after a 6-day treatment with aldosterone. In conclusion, we have successfully used mTERT to immortalize mouse collecting duct cells that retain the basic in vivo phenotypic characteristics of collecting duct cells. This technique should be valuable in generating cell lines from genetically engineered mouse models. [ABSTRACT FROM AUTHOR]

Published

2010

32. Renal CD14 expression correlates with the progression of cystic kidney disease.

Author

Juling Zhou, Xiaosen Ouyang, Xiangqin Cui, Schoeb, Trenton R., Smythies, Lesley E., Johnson, Martin R., Guay-Woodford, Lisa M., Chapman, Arlene B., and Mrug, Michal

Subjects

*KIDNEY diseases, *MONOCYTES, *ACUTE kidney failure, *HEREDITY, *NEPHROLOGY

Abstract

Monocyte and macrophage markers are among the most highly overexpressed genes in cpk mouse kidneys with severely progressive renal cystic disease. We show here that one of these markers, CD14, is abnormally transcribed, activated and shed in cystic kidneys. However, these abnormalities were not associated with an increased number of interstitial CD14-positive mononuclear cells. Instead, we found that most non-cystic and cystic renal tubular epithelia were CD14-positive; even distal nephron-derived principal cells. Cd14 was significantly overexpressed in the kidneys of 5-day-old cpk mice and further increased as the disease progressed. In the cpk model with variable rates of cystic kidney enlargement (due to an intercross of two distinct genetic backgrounds), Cd14 expression positively correlated with kidney volume, exceeding the correlation with MCP-1, an established marker of autosomal-dominant polycystic kidney disease (ADPKD). In 16 patients with ADPKD, the baseline urinary CD14 level showed some tendency to correlate with the 2-year change in total kidney volume; however, the tendency was not statistically significant. But the association was significant when the analysis was confined to males. Clearly more studies need to be done to evaluate the utility of CD14 as a marker for outcomes in ADPKD. [ABSTRACT FROM AUTHOR]

Published

2010

33. The C3H/HeJ inbred mouse is a model of vesico-ureteric reflux with a susceptibility locus on chromosome 12.

Author

Murawski, Inga J., Maina, Rita W., Malo, Danielle, Guay-Woodford, Lisa M., Gros, Philippe, Fujiwara, Mary, Morgan, Kenneth, and Gupta, Indra R.

Subjects

*KIDNEY abnormalities, *LABORATORY mice, *URINARY organs, *CHROMOSOMES, *GENOMES

Abstract

Vesico-ureteric reflux is the most common congenital anomaly of the urinary tract, characterized by a defective uretero-vesical junction with retrograde urine flow from the bladder toward the kidneys. Because there is strong evidence for a genetic basis for some cases of vesico-ureteric reflux, we screened 11 inbred mouse strains for reflux and kidney size and identified one strain, C3H/HeJ, that has a 100 percent incidence of vesico-ureteric reflux with otherwise normal kidneys at birth. These mice are predisposed to reflux as a result of a defective uretero-vesical junction characterized by a short intravesical ureter. This defect results from a delay in urinary tract development initially manifested by a ureteric bud arising from a more caudal location along the mesonephric duct. In contrast, C57BL/6J mice (resistant to reflux at birth) have long intravesical ureters, normally positioned ureteric buds, and no delay in urinary tract development. Genome-wide and additional fine mapping of backcross mice, derived from C3H/HeJ and C57BL/6J crosses, identified a significant reflux susceptibility locus, Vurm1, on chromosome 12 (peak logarithm of the odds=7.39). The C3H/HeJ mouse is a model of vesico-ureteric reflux without renal malformation, and further characterization of this model will allow for the identification of a pathway important for urinary tract development, a finding that will serve as a model for the human disorder. [ABSTRACT FROM AUTHOR]

Published

2010

34. PKHD1 sequence variations in 78 children and adults with autosomal recessive polycystic kidney disease and congenital hepatic fibrosis

Author

Gunay-Aygun, Meral, Tuchman, Maya, Font-Montgomery, Esperanza, Lukose, Linda, Edwards, Hailey, Garcia, Angelica, Ausavarat, Surasawadee, Ziegler, Shira G., Piwnica-Worms, Katie, Bryant, Joy, Bernardini, Isa, Fischer, Roxanne, Huizing, Marjan, Guay-Woodford, Lisa, and Gahl, William A.

Subjects

*POLYCYSTIC kidney disease, *NUCLEOTIDE sequence, *PATHOGENIC microorganisms, *LIVER diseases, *COHORT analysis, *KIDNEY disease diagnosis, *GENETICS

Abstract

Abstract: PKHD1, the gene mutated in autosomal recessive polycystic kidney disease (ARPKD)/congenital hepatic fibrosis (CHF), is an exceptionally large and complicated gene that consists of 86 exons and has a number of alternatively spliced transcripts. Its longest open reading frame contains 67 exons that encode a 4074 amino acid protein called fibrocystin or polyductin. The phenotypes caused by PKHD1 mutations are similarly complicated, ranging from perinatally-fatal PKD to CHF presenting in adulthood with mild kidney disease. To date, more than 300 mutations have been described throughout PKHD1. Most reported cohorts include a large proportion of perinatal-onset ARPKD patients; mutation detection rates vary between 42% and 87%. Here we report PKHD1 sequencing results on 78 ARPKD/CHF patients from 68 families. Differing from previous investigations, our study required survival beyond 6months and included many adults with a CHF-predominant phenotype. We identified 77 PKHD1 variants (41 novel) including 19 truncating, 55 missense, 2 splice, and 1 small in-frame deletion. Using computer-based prediction tools (GVGD, PolyPhen, SNAP), we achieved a mutation detection rate of 79%, ranging from 63% in the CHF-predominant group to 82% in the remaining families. Prediction of the pathogenicity of missense variants will remain challenging until a functional assay is available. In the meantime, use of PKHD1 sequencing data for clinical decisions requires caution, especially when only novel or rare missense variants are identified. [Copyright &y& Elsevier]

Published

2010

35. Characterization of large rearrangements in autosomal dominant polycystic kidney disease and the PKD1/TSC2 contiguous gene syndrome.

Author

Consugar, Mark B., Wong, Wai C., Lundquist, Patrick A., Rossetti, Sandro, Kubly, Vickie J., Walker, Denise L., Rangel, Laureano J., Aspinwall, Richard, Niaudet, W. Patrick, Özen, Seza, David, Albert, Velinov, Milen, Bergstralh, Eric J., Bae, Kyongtae T., Chapman, Arlene B., Guay-Woodford, Lisa M., Grantham, Jared J., Torres, Vicente E., Sampson, Julian R., and Dawson, Brian D.

Subjects

*DNA damage, *POLYCYSTIC kidney disease, *REARRANGEMENTS (Chemistry), *MICROBIOLOGICAL assay, *GENETIC regulation, *PATIENTS

Abstract

Large DNA rearrangements account for about 8% of disease mutations and are more common in duplicated genomic regions, where they are difficult to detect. Autosomal dominant polycystic kidney disease (ADPKD) is caused by mutations in either PKD1 or PKD2. PKD1 is located in an intrachromosomally duplicated region. A tuberous sclerosis gene, TSC2, lies immediately adjacent to PKD1 and large deletions can result in the PKD1/TSC2 contiguous gene deletion syndrome. To rapidly identify large rearrangements, a multiplex ligation-dependent probe amplification assay was developed employing base-pair differences between PKD1 and the six pseudogenes to generate PKD1-specific probes. All changes in a set of 25 previously defined deletions in PKD1, PKD2 and PKD1/TSC2 were detected by this assay and we also found 14 new mutations at these loci. About 4% of the ADPKD patients in the CRISP study were found to have gross rearrangements, and these accounted for about a third of base-pair mutation negative families. Sensitivity of the assay showed that about 40% of PKD1/TSC contiguous gene deletion syndrome families contained mosaic cases. Characterization of a family found to be mosaic for a PKD1 deletion is discussed here to illustrate family risk and donor selection considerations. Our assay improves detection levels and the reliability of molecular testing of patients with ADPKD.Kidney International (2008) 74, 1468–1479; doi:10.1038/ki.2008.485; published online 24 September 2008 [ABSTRACT FROM AUTHOR]

Published

2008

36. Loss of primary cilia results in deregulated and unabated apical calcium entry in ARPKD collecting duct cells.

Author

Siroky, Brian J., Ferguson, William B., Fuson, Amanda L., Yi Xie, Fintha, Attila, Komlosi, Peter, Yoder, Bradley K., Schwiebert, Erik M., Guay-Woodford, Lisa M., and Bell, P. Darwin

Subjects

*EPITHELIAL cells, *CYSTS (Pathology), *POLYCYSTIC kidney disease, *CILIA & ciliary motion, *HUMAN chromosome abnormalities, *FLUORESCENCE microscopy, *IMMUNOCYTOCHEMISTRY

Abstract

Recent genetic analysis has identified a pivotal role of primary cilia in the pathogenesis of polycystic kidney disease (PKD). However, little is known regarding how cilia loss/dysfunction contributes to cyst development. In epithelial cells, changes in apical fluid flow induce cilia-mediated Ca2+ entry via polycystin-2 (PC2), a cation channel. The Oak Ridge Polycystic Kidney (orpk) mouse contains a mutated Tg737 gene that disrupts expression of polaris, a protein required for ciliogenesis. These studies examine the effect of cilia malformation on Ca2+ entry in orpk cilia(-) collecting duct principal cells, and in orpk cells in which wild-type Tg737 was reintroduced, orpk cilia(+). [Ca2+]i was monitored in confluent cell monolayers using fluorescence microscopy. Intrinsic apical Ca2+ entry was measured by Mn2+ quenching and Ca2+ depletion/readdition under flow conditions below the threshold for stimulation. We found that unstimulated apical Ca2+ entry was markedly increased in cilia(-) cells and was sensitive to Gd3+, an inhibitor of PC2. Electrophysiological measurements demonstrate increased abundance of an apical channel, consistent with PC2, in cilia(-) cells. Immunofluorescence studies revealed that PC2, normally expressed on and at the base of cilia in orpk cilia(+) cells, was observed throughout the apical membrane in cilia(-) cells. Furthermore, cilia(-) cells displayed elevated subapical Ca2+ levels measured with the near-membrane Ca2+ indicator FFP-18. We propose that cilia exert a tonic regulatory influence on apical Ca2+ entry, and absence of cilia results in loss of spatial organization of PC2, causing unregulated Ca2+ entry and elevations in subapical [Ca2+], a factor which may contribute to cyst formation. [ABSTRACT FROM AUTHOR]

Published

2006

37. Predominant extrahepatic biliary disease in autosomal recessive polycystic kidney disease: A new association.

Author

Goilav, Beatrice, Norton, Karen I., Satlin, Lisa M., Guay-Woodford, Lisa, Chen, Frank, Magid, Margret S., Emre, Sukru, and Shneider, Benjamin L.

Subjects

*BILE duct diseases, *POLYCYSTIC kidney disease, *KIDNEY diseases, *HYPERTENSION, *PORTAL hypertension, *CELL membranes, *ENDOSCOPIC retrograde cholangiopancreatography

Abstract

Autosomal recessive polycystic kidney disease (ARPKD) is characterized by dilation of ectatic renal collecting ducts, intrahepatic biliary dysgenesis, and portal fibrosis. Portal hypertension and recurrent bacterial cholangitis can dominate the clinical picture in long-term survivors. Predominant extrahepatic bile duct disease was revealed in four patients who underwent magnetic resonance cholangiopancreatography. All four patients had portal hypertension, although liver biochemistries did not suggest biliary disease. In two of the patients, cholangitis was clinically ascribed to the bile duct disease. Western blot analysis of plasma membranes from normal rat extrahepatic bile duct and kidney revealed the presence of polyductin as a single ∼440 kDa protein. Although the exact function of polyductin in the extrahepatic duct is unknown, it may have a role in the development and control of lumenal size. Clinical management of patients with ARPKD should include consideration of potential problems related to extrahepatic bile duct disease. [ABSTRACT FROM AUTHOR]

Published

2006

38. Heightened epithelial Na+ channel-mediated Na+ absorption in a murine polycystic kidney disease model epithelium lacking apical monocilia.

Author

Olteanu, Dragos, Yoder, Bradley K., Wen Liu, Croyle, Mandy J., Welty, Elisabeth A., Rosborough, Kelley, Wyss, J. Michael, Bell, P. Darwin, Guay-Woodford, Lisa M., Bevensee, Mark O., Satlin, Lisa M., and Schwiebert, Erik M.

Subjects

*POLYCYSTIC kidney disease, *CILIA & ciliary motion, *HYPERTENSION, *EPITHELIAL cells, *ELECTROPHYSIOLOGY

Abstract

The Tg737orpk autosomal recessive polycystic kidney disease (ARPKD) mouse carries a hypomorphic mutation in the Tg737 gene. Because of the absence of its protein product Polaris, the nonmotile primary monocilium central to the luminal membrane of ductal epithelia, such as the cortical collecting duct (CCD) principal cell (PC), is malformed. Although the functions of the renal monocilium remain elusive, primary monocilia or flagella on neurons act as sensory organelles. Thus we hypothesized that the PC monocilium functions as a cellular sensor. To test this hypothesis, we assessed the contribution of Polaris and cilium structure and function to renal epithelial ion transport electrophysiology. Properties of Tg737orpk mutant CCD PC clones were compared with clones genetically rescued with wild-type Tg737 cDNA. All cells were grown as polarized cell monolayers with similarly high transepithelial resistance on permeable filter supports. Three- to fourfold elevated transepithelial voltage (Vte) and short-circuit current (Isc) were measured in mutant orpk monolayers vs. rescued controls. Pharmacological and cell biological examination of this enhanced electrical end point in mutant monolayers revealed that epithelial Na! channels (ENaCs) were upregulated. Amiloride, ENaC-selective amiloride analogs (benzamil and phenamil), and protease inhibitors (aprotinin and leupeptin) attenuated heightened Vte and Isc. Higher concentrations of additional amiloride analogs (ethylisopropylamiloride and dimethyl-amiloride) also revealed inhibition of Vte. Cell culture requirements and manipulations were also consistent with heightened ENaC expression and function. Together, these data suggest that ENaC expression and/or function are upregulated in the luminal membrane of mutant, cilium-deficient orpk CCD PC monolayers vs. cilium-competent controls. When the genetic lesion causes loss or malformation of the monocilium, ENaC-driven Na+ hyperabsorption may explain the rapid emergence of severe hypertension in a majority of patients with ARPKD. [ABSTRACT FROM AUTHOR]

Published

2006

39. Polyductin, thePKHD1gene product, comprises isoforms expressed in plasma membrane, primary cilium, and cytoplasm.

Author

Menezes, Luis F.C., Cali, Yiqiang, Nagasawa, Yasuyuki, Silva, Ana M.G., Watkins, Mary L., Da Silva, Aline M., Somlo, Stefan, Guay-Woodford, Lisa M., Germino, Gregory G., and Onuchic, Luiz F.

Subjects

*GENES, *CELL membranes, *CYTOPLASM, *POLYCYSTIC kidney disease, *CYSTIC kidney disease, *PROTEINS

Abstract

Polyductin, thePKHD1gene product, comprises isoforms expressed in plasma membrane, primary cilium, and cytoplasm.Background. PKHD1, the autosomal-recessive polycystic kidney disease (ARPKD) gene, encodes multiple alternatively spliced transcripts predicted to generate membrane-bound and secreted proteins. The longest open reading frame encodes polyductin (fibrocystin), a putative 4074 amino acid protein with a single transmembrane domain and an intracellular C-terminus.Methods.To characterize thePKHD1products and their expression profile, we raised polyclonal antibodies against different portions of polyductin and analyzed different organs using various methods.Results.Western blot analyses demonstrated specific bands of>440 kD in human adult kidney, liver, and pancreas and∼230 kD in kidney and liver, predominantly observed in membrane fractions. The>440-kD putative membrane protein was immunoprecipitated from kidney and subsequently detected by Western blotting using two distinct antisera. An additional product of∼140 kD was specifically recognized by affinity-purified antisera predominantly in soluble fractions. Immunohistochemistry studies revealed specific staining in cortical and medullary collecting ducts and thick ascending limbs of Henle (TALH). Serial sections were stained with antibodies against aquaporin-2 and Tamm-Horsfall protein to confirm the nephron segment localization. Positive staining was also detected in biliary and pancreatic duct epithelia. Analyses of mouse developing tissues showed specific staining in the ureteric bud branches, intra- and extrahepatic biliary ducts, pancreatic ducts, and salivary glands. Immunofluorescence studies in inner medullary collecting duct cultured cells and immunoelectron microscopy analysis of medullary collecting ducts demonstrated that the protein localizes to the primary cilium. Positive signal was also detected in the apical membrane and in cytoplasm.Conclusion.The results indicate that polyductin is part of the group of polycystic kidney disease (PKD)-related proteins expressed in primary apical cilia. Our data also suggest that, in addition to its likely involvement in cilia function, polyductin probably serves in other subcellular functional roles. The detection of three different products using two antisera, with evidence for distinct subcellular localizations, suggests thatPKHD1encodes membrane-bound and soluble isoforms. [ABSTRACT FROM AUTHOR]

Published

2004

40. Comparative Genomics Identifies a Flagellar and Basal Body Proteome that Includes the BBS5 Human Disease Gene

Author

Li, Jin Billy, Gerdes, Jantje M., Haycraft, Courtney J., Fan, Yanli, Teslovich, Tanya M., May-Simera, Helen, Li, Haitao, Blacque, Oliver E., Li, Linya, Leitch, Carmen C., Lewis, Richard Allan, Green, Jane S., Parfrey, Patrick S., Leroux, Michel R., Davidson, William S., Beales, Philip L., Guay-Woodford, Lisa M., Yoder, Bradley K., Stormo, Gary D., and Katsanis, Nicholas

Subjects

*GENOMICS, *DISEASES, *GENES, *CENTRIOLES

Abstract

Cilia and flagella are microtubule-based structures nucleated by modified centrioles termed basal bodies. These biochemically complex organelles have more than 250 and 150 polypeptides, respectively. To identify the proteins involved in ciliary and basal body biogenesis and function, we undertook a comparative genomics approach that subtracted the nonflagellated proteome of Arabidopsis from the shared proteome of the ciliated/flagellated organisms Chlamydomonas and human. We identified 688 genes that are present exclusively in organisms with flagella and basal bodies and validated these data through a series of in silico, in vitro, and in vivo studies. We then applied this resource to the study of human ciliation disorders and have identified BBS5, a novel gene for Bardet-Biedl syndrome. We show that this novel protein localizes to basal bodies in mouse and C. elegans, is under the regulatory control of daf-19, and is necessary for the generation of both cilia and flagella. [Copyright &y& Elsevier]

Published

2004

41. Magnetic resonance measurements of renal blood flow as a marker of disease severity in autosomal-dominant polycystic kidney disease.

Author

King, Bernard F., Torres, Vicente E., Brummer, Marijn E., Chapman, Arlene B., Bae, Kyongtae T., Glockner, James F., Arya, Kraisthith, Felmlee, Joel P., Grantham, Jared J., Guay-Woodford, Lisa M., Bennett, William M., Klahr, Saulo, Hirschman, Gladys H., Kimmel, Paul L., Thompson, Paul A., and Miller, J. Phillip

Subjects

*POLYCYSTIC kidney disease, *MAGNETIC resonance, *BLOOD flow

Abstract

Magnetic resonance measurements of renal blood flow as a marker of disease severity in autosomal-dominant polycystic kidney disease. Background. Autosomal-dominant polycystic kidney disease (ADPKD) is an inherited disorder characterized by renal cyst growth, early development of hypertension, and late occurrence of renal insufficiency. Despite evidence for the importance of nephroangiosclerosis in the progression of renal insufficiency in ADPKD, evaluation of renal blood flow (RBF) as a surrogate marker of disease severity has received little attention. Methods. Flow phantoms and repeat RBF measurements assessed accuracy and reproducibility. One hundred twenty-seven ADPKD subjects with creatinine clearances >70 mL/min underwent measurements of RBF, total, and cyst renal volumes, and % cyst volumes by magnetic resonance (MR) and of glomerular filtration rate (GFR). Renal vascular resistance (RVR) was calculated. MR blood flow sequences utilized a two-dimensional cine phase-contrast breath-hold pulse sequence perpendicular to the renal arteries. Flow rates were calculated utilizing FLOW software. Volumetric analysis was performed using stereology and region-based thresholding. Results. Excellent accuracy and intraobserver and interobserver reproducibility were demonstrated. Anatomic (total kidney volume, total cyst volume, and % cyst volume), hemodynamic (RBF and RVR), and functional (GFR) parameters were strongly correlated. Left polycystic kidneys were larger and had more severe disease. Regression analysis showed that age, diagnosis of hypertension, anatomic parameters and hemodynamic parameters were significant predictors of GFR. Multiple linear regression analysis identified age and hemodynamic parameters only as separate predictors of GFR. Anatomic, hemodynamic, and functional parameters discriminated between normotensive and hypertensive subjects despite antihypertensive treatments. Conclusion. Renal hemodynamic parameters measured by MR correlate with anatomic and functional indices of disease severity, are the strongest predictors of renal function, and deserve further consideration as an outcome measure in clinical trials to guide therapy in ADPKD. [ABSTRACT FROM AUTHOR]

Published

2003

42. Positional cloning of jcpk/bpk locus of the mouse.

Author

Cogswell, Cathy, Price, Sarah J., Xiaoying Hou, Guay-Woodford, Lisa M., Flaherty, Lorraine, and Bryda, Elizabeth C.

Subjects

*POLYCYSTIC kidney disease, *DROSOPHILIDAE, *HUMAN chromosome abnormalities, *KIDNEY diseases, *HOMOLOGY (Biology), *GENETIC mutation

Abstract

By positional cloning techniques, we have identified the gene that is disrupted in the jcpk and bpk mouse models for polycystic kidney disease. This gene is the mouse homolog of the Drosophila Bicaudal C gene. Both of these mutations have been mapped to a very short stretch of Chromosome (Chr) 10. By sequencing the bicaudal C gene, Bicc1, in these models, it was found that the jcpk mutation results in a shortened and abnormal transcript, whereas the bpk mutation results in an abnormal 3′ coding region. In Drosophila, this gene encodes a protein known to influence developmental processes. The mammalian homolog contains three KH (K homology) domains and a SAM (sterile alpha motif) domain and is expressed in the developing embryo, indicating that it may be important in RNA-binding and/or protein interactions during embryogenesis. [ABSTRACT FROM AUTHOR]

Published

2003

43. Confirmation of the ATP6B1 gene as responsible for distal renal tubular acidosis.

Author

Ruf, Rainer, Rensing, Cornelia, Topaloglu, Rezan, Guay-Woodford, Lisa, Klein, Cornelia, Vollmer, Martin, Otto, Edgar, Beekmann, Frank, Haller, Maria, Wiedensohler, Alexander, Leumann, Ernst, Antignac, Corinne, Rizzoni, Gianfranco, Filler, Guido, Brandis, Matthias, Weber, James L., and Hildebrandt, Friedhelm

Subjects

*ACIDOSIS, *KIDNEY tubules, *KIDNEY calcification

Abstract

Primary distal renal tubular acidosis (dRTA) type I is a hereditary renal tubular disorder, which is characterized by impaired renal acid secretion resulting in metabolic acidosis. Clinical symptoms are nephrocalcinosis, nephrolithiasis, osteomalacia, and growth retardation. Biochemical alterations consist of hyperchloremic metabolic acidosis, hypokalemia with muscle weakness, hy- percalciuria, and inappropriately raised urinary pH. Autosomal dominant and rare forms of recessive dRTA are known to be caused by mutations in the gene for the anion exchanger AE1. In order to identify a gene responsible for recessive dRTA, we performed a total genome scan with 303 polymorphic microsatellite markers in six consanguineous families with recessive dRTA from Turkey. In four of these there was an association with sensorineural deathess. The total genome scan yielded regions of homozygosity by descent in all six families on chromosomes 1, 2, and 10 as positional candidate region. In one of these regions the gene ATP6B1 for the β1 subunit of the vacuolar H[sup +]-ATPase is localized, which has recently been identified as causative for recessive dRTA with sensorineural deafness. Therefore, we conducted mutational analysis in 15 families and identified potential loss-of-function mutations in ATP6B1 in 8. We thus confirmed that defects in this gene are responsible for recessive dRTA with sensorineural deafness. [ABSTRACT FROM AUTHOR]

Published

2003

44. Autosomal recessive polycystic kidney disease: outcomes from a single-center experience.

Author

Capisonda, Rhona, Phan, Veronique, Traubuci, Jeffrey, Daneman, Alan, Balfe, J. Williamson, and Guay-Woodford, Lisa M.

Subjects

*POLYCYSTIC kidney disease, *PEDIATRIC nephrology

Abstract

Autosomal recessive polycystic kidney disease (ARPKD) is a relatively common form of pediatric polycystic kidney disease with an incidence of 1:20,000 live births. Previous reports, primarily from populations of European origin, indicate that the clinical presentation and disease course are quite variable. Using a retrospective study design, we sought to determine whether the clinical course and outcome of our multi-ethnic patient cohort differs from the published literature. A 10-year (1990-2000) retrospective study was conducted in which we reviewed the clinical, histopathological, and imaging records of our 31 ARPKD patients. Patients were diagnosed between 0 and 14 years of age, with 17 (55%) presenting within the 1st month of life. The mean follow-up was 67 months and age at last follow-up ranged from 0.5 to 16 years. Of the 17 patients diagnosed as neonates, 11 (65%) had respiratory insufficiency complicated by pneumothoraces. Two died shortly after birth and 2 died within the 1st year of life due to respiratory failure. Among the 13 neonatal survivors, 7 (54%) developed progressive renal insufficiency, whereas 6 of 14 (43%) of those children who presented beyond 1 month of age developed renal insufficiency. Hypertension was present in 55% of our patients, with nearly all neonatal survivors requiring antihypertensive management. Evidence of portal hypertension was found in 10 (37%) of the 27 patients who survived the 1st year of life. In our multi-ethnic ARPKD cohort, the 1-year survival rate (87%) and the clinical variability are comparable to those previously reported. With the recent identification of the PKHD1 gene, characterization of disease-causing mutations should provide new insights into the molecular basis for this phenotypic variability. [ABSTRACT FROM AUTHOR]

Published

2003

45. PKHD1, the Polycystic Kidney and Hepatic Disease 1 Gene, Encodes a Novel Large Protein Containing Multiple Immunoglobulin-Like Plexin-Transcription-Factor Domains and Parallel Beta-Helix 1 Repeats.

Author

Onuchic, Luiz F., Furu, Laszlo, Nagasawa, Yasuyuki, Xiaoying Hou, Eggerman, Thomas, Zhiyong Ren, Bergmann, Carsten, Senderek, Jan, Esquivel, Ernie, Zeltner, Raoul, Rudnik-Sch oumi neborn, Sabine, Mrug, Michael, Sweeney, William, Avner, Ellis D., Zerres, Klaus, Guay-Woodford, Lisa M., Somlo, Stefan, and Geronimo, Gregory G.

Subjects

*POLYCYSTIC kidney disease, *HUMAN chromosome abnormalities, *GENETICS

Abstract

Presents a study which described the identification of PKHD1, the gene mutated in autosomal recessive polycystic kidney disease. Materials and methods; Results; Discussion.

Published

2002

46. Autocrine extracellular purinergic signaling in epithelial cells derived from polycystic kidneys.

Author

Schwiebert, Erik M., Wallace, Darren P., Braunstein, Gavin M., King, Sandi R., Peti-Peterdi, Janos, Hanaoka, Kazushige, Guggino, William B., Guay-Woodford, Lisa M., Bell, P. Darwin, Sullivan, Lawrence P., Grantham, Jared J., and Taylor, Amanda L.

Subjects

*AUTOCRINE mechanisms, *EPITHELIAL cells, *POLYCYSTIC kidney disease, *ADENOSINE triphosphate

Abstract

Investigates the occurrence of autocrine extracellular purinergic signaling in epithelial cells from polycystic kidneys (PK). Genetic forms of PK disease; Production of adenosine triphosphate (ATP) in epithelial monolayers; Mechanisms contributing to enhanced ATP release.

Published

2002

47. Cystin, a novel cilia-associated protein, is disrupted in the cpk mouse model of polycystic kidney disease.

Author

Xiaoying Hou, Mrug, Michal, Yoder, Bradley K., Lefkowitz, Elliot J., Kremmidiotis, Gabriel, D'Eustachio, Peter, Beier, David R., and Guay-Woodford, Lisa M.

Subjects

*GENETIC mutation, *PROTEINS, *GENETICS

Abstract

Describes the positional cloning, mutation analysis and expression of cystin, a novel cilia-associated protein, that is disrupted in congenital polycystic kidney (cpk) mice. Application of southern blot analysis; Refinement of the cpk candidate interval and generation of a transcript map; Identification of the cpk transcript and characterization of the genomic sequence.

Published

2002

48. Cystin, a novel cilia-associated protein, is disrupted in the cpk mouse model of polycystic kidney disease.

Author

Hou, Xiaoying, Mrug, Michal, Yoder, Bradley K, Lefkowitz, Elliot J, Kremmidiotis, Gabriel, D'Eustachio, Peter, Beier, David R, and Guay-Woodford, Lisa M

Subjects

*CELL metabolism, *RNA metabolism, *AMINO acids, *ANIMAL experimentation, *BIOLOGICAL models, *COMPARATIVE studies, *DNA, *DOCUMENTATION, *GENE expression, *GENE mapping, *GENETIC techniques, *RESEARCH methodology, *MEDICAL cooperation, *MEMBRANE proteins, *MICE, *GENETIC mutation, *NUCLEOTIDES, *POLYCYSTIC kidney disease, *RESEARCH, *RESEARCH funding, *RNA, *EVALUATION research, *GENOTYPES

Abstract

The congenital polycystic kidney (cpk) mutation is the most extensively characterized mouse model of polycystic kidney disease (PKD). The renal cystic disease is fully expressed in homozygotes and is strikingly similar to human autosomal recessive PKD (ARPKD), whereas genetic background modulates the penetrance of the corresponding defect in the developing biliary tree. We now describe the positional cloning, mutation analysis, and expression of a novel gene that is disrupted in cpk mice. The cpk gene is expressed primarily in the kidney and liver and encodes a hydrophilic, 145-amino acid protein, which we term cystin. When expressed exogenously in polarized renal epithelial cells, cystin is detected in cilia, and its expression overlaps with polaris, another PKD-related protein. We therefore propose that the single epithelial cilium is important in the functional differentiation of polarized epithelia and that ciliary dysfunction underlies the PKD phenotype in cpk mice. [ABSTRACT FROM AUTHOR]

Published

2002

49. Genomic structure of the gene for the human P1 protein (MCM3) and its exclusion as a candidate for autosomal recessive polycystic kidney disease.

Author

Hofmann, Yvonne, Becker, Jutta, Wright, Felicia, Avner, Ellis D, Mrug, Michal, Guay-Woodford, Lisa M, Somlo, Stefan, Zerres, Klaus, Germino, Gregory G, and Onuchic, Luiz F

Subjects

*POLYCYSTIC kidney disease, *PROTEINS, *HUMAN genetics, *HUMAN gene mapping

Abstract

The locus PKHD1 (polycystic kidney and hepatic disease 1) has been linked to all typical forms of the autosomal recessive polycystic kidney disease (ARPKD) and maps to chromosome 61321.1-p12. We previously defined its genetic interval by the flanking markers D6S1714 and D6S1024. In our current work, we have fine-mapped the gene for the human P1 protein (MCM3), thought to be involved in the DNA replication process, to this critical region. We have also established its genomic structure. Mutation analyses using SSCP were performed in ARPKD patients' cDNA samples, leading to the exclusion of this gene as a candidate for this disorder. We also identified two intragenic polymorphisms that allowed families with critical recombination events to be evaluated. Although neither marker was informative in these individuals, they are the closest yet described for PKHD1 and may help to refine the candidate region. [ABSTRACT FROM AUTHOR]

Published

2000

50. Novel mutations in the thiazide-sensitive NaCl cotransporter gene in patients with Gitelman syndrome with predominant localization to the C-terminal domain.

Author

Lemmink, Henny H., Knoers, Nine V.A.M., Károlyi, Lothar, van Dijk, Henk, Niaudet, Patrick, Antignac, Corinne, Guay-Woodford, Lisa M., Goodyer, Paul R., Carel, Jean-Claude, Hermes, Ad, Seyberth, Hansjörg W., Monnens, Leo A. H., and van den Heuvel, Lambert P.W.J.

Subjects

*KIDNEY diseases, *THIAZINES, *HYPOMAGNESEMIA, *ELECTROLYTES

Abstract

Novel mutations in the thiazide-sensitive NaCl cotransporter gene in patients with Gitelman syndrome. Gitelman syndrome (familial hypokalemia-hypomagnesemia syndrome) is an autosomal recessive inherited renal disorder characterized by defective tubular reabsorption of magnesium and potassium. In this study a group of 18 unrelated and 2 related Gitelman patients, collected from six different countries have been screened for mutations in the human thiazide-sensitive sodium-chloride cotransporter (SLC12A3) gene. Fourteen novel SLC12A3 mutations are presented along with six mutations described earlier, and three neutral polymorphisms. Among the tested patients are two who carry a total of three heterozygous SLC12A3 mutations. Two-thirds of the total number of mutant SLC12A3 alleles are amino acid substitutions. Most SLC12A3 gene mutations, 14 out of a total of 20, are localized at the intracellular carboxy-terminal domain of the NCCT protein. The pathogenicity of individual SLC12A3 mutations is based upon their predicted effect on SLC12A3 protein, and segregation in family members. Evolutionary conservation of substituted amino acid residues and their frequency in control chromosomes is presented. Identical mutations have been found in Gitelman families from different geographical origin, suggesting ancient mutations originating from a common ancestor. As yet, we have not found any evidence for a possible genotype-phenotype correlation. [ABSTRACT FROM AUTHOR]

Published

1998