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13. Discussion on the meeting on 'Statistical modelling and analysis of genetic data'

Author

Balding, Dj, Carothers, Ad, Marchini, Jl, Cardon, Lr, Vetta, A., Griffiths, B., Weir, Bs, Hill, Wg, Goldstein, D., Strimmer, K., Myers, S., Beaumont, Ma, Glasbey, Ca, Mayer, Cd, Richardson, S., Marshall, C., Durrett, R., Nielsen, R., Peter Visscher, Knott, Sa, Haley, Cs, Ball, Rd, Hackett, Ca, Holmes, S., Husmeier, D., Jansen, Rc, Ter Braak, Cjf, Maliepaard, Ca, Boer, Mp, Joyce, P., Li, N., Stephens, M., Marcoulides, Ga, Drezner, Z., Mardia, K., Mcvean, G., Meng, Xl, Ochs, Mf, Pagel, M., Sha, N., Vannucci, M., Sillanpaa, Mj, Sisson, S., Yandell, Bs, Jin, Cf, Satagopan, Jm, Gaffney, Pj, Zeng, Zb, Broman, Kw, Speed, Tp, Fearnhead, P., Donnelly, P., Larget, B., Simon, Dl, Kadane, Jb, Nicholson, G., Smith, Av, Jonsson, F., Gustafsson, O., Stefansson, K., Parmigiani, G., Garrett, Es, Anbazhagan, R., Gabrielson, E., and University of Groningen

Subjects
Statistics and Probability, EVOLUTIONARY TREES, Maximum likelihood, bayesian-analysis, CHAIN MONTE-CARLO, half-sib populations, Space (commercial competition), AFFECTING WING SHAPE, HALF-SIB POPULATIONS, BAYESIAN-ANALYSIS, Mathematics education, Econometrics, chain monte-carlo, Statistical analysis, MAXIMUM-LIKELIHOOD, Mathematics, QUANTITATIVE TRAIT LOCI, HUMAN LIPOPROTEIN-LIPASE, drosophila-melanogaster, MULTIVARIATE REGRESSION, evolutionary trees, Genetic data, Statistical model, human lipoprotein-lipase, PRI Biometris, DROSOPHILA-MELANOGASTER, quantitative trait loci, maximum-likelihood, multivariate regression, Statistics, Probability and Uncertainty, affecting wing shape
Abstract

David J. Balding .Imperial College School of Medicine, London/ I extendmy apologies to the authors that an unavoidable commitment arising unexpectedly in the 18 hours before the meeting robbed me of my final preparation, so that my comments at the meeting were poorly presented. I shall try to do a better job in this written version, and to leave enough space I shall omit my introductory comments about the role of statisticians in bioinformatics.

Published
2002

14. Data and theory point to mainly additive genetic variance for complex traits

Author

Mackay, TFC, Hill, WG, Goddard, ME, Visscher, PM, Mackay, TFC, Hill, WG, Goddard, ME, and Visscher, PM

Abstract

The relative proportion of additive and non-additive variation for complex traits is important in evolutionary biology, medicine, and agriculture. We address a long-standing controversy and paradox about the contribution of non-additive genetic variation, namely that knowledge about biological pathways and gene networks imply that epistasis is important. Yet empirical data across a range of traits and species imply that most genetic variance is additive. We evaluate the evidence from empirical studies of genetic variance components and find that additive variance typically accounts for over half, and often close to 100%, of the total genetic variance. We present new theoretical results, based upon the distribution of allele frequencies under neutral and other population genetic models, that show why this is the case even if there are non-additive effects at the level of gene action. We conclude that interactions at the level of genes are not likely to generate much interaction at the level of variance.

Published
2008

19. The impact of gender role conflict on multidimensional social support in older men.

Author

Hill WG and Donatelle RJ

Abstract

This study examines the impact of gender role conflict on the perceived social support in a sample of older men aged 40-86. Three-hundred eighty-nine men completed a survey measuring gender role conflict and multidimensional social support. Canonical correlation was used to explore possible dimensions between the four gender role conflict factors and differing dimensions of social support. Only one canonical variate was interpretable and indicated that all four subscales of the Gender Role Conflict Scale appeared inversely and significantly related to Emotional/Informational Support, Affective Support, and Positive Social Interaction. These findings suggest that gender role conflict in older men may limit their perception of the availability of social support thereby restricting men's ability to appreciate the beneficial effects of supporting relationships. Study limitations and directions for future research are discussed. [ABSTRACT FROM AUTHOR]

Published
2005

24. DREADD agonist compound 21 causes acute diuresis in wild-type mice.

Author

MacIver B, Wu A, Hill WG, and Yu W

Abstract

The targeted activation or inhibition of specific cell populations using chemogenetics allows the precise dissection of cellular signaling and function. Designer receptors exclusively activated by designer drugs (DREADDs) is a chemogenetic platform initially developed by mutating human muscarinic receptors to be unresponsive to endogenous acetylcholine but exclusively activated by an "inert" designer drug. Compound 21 (C21) is a new and potent DREADD agonist; however, radioligand assays from a recent report indicated its ability to bind to endogenous G protein-coupled receptors (GPCRs), including muscarinic M1-3 receptors. Whether this binding causes off-target effects is unclear. Renal innervation is important for the regulation of renal function, and the advent of chemogenetic tools provides significant opportunities for the mechanistic understanding of renal innervation and function. GPCRs such as adrenergic and muscarinic receptors play a role in renal function; thus, a careful pharmacological characterization of C21 in renal function is a prerequisite for this approach. Unexpectedly, an infusion of 1.0 mg/kg C21 in anesthetized mice caused an ∼4-fold increase in urine output and correspondingly increased the glomerular filtration rate (GFR), suggesting a C21-mediated acute diuretic effect. This acute diuresis effect was further confirmed in awake mice using voiding spot assays. The exact molecular mechanism for C21-mediated diuresis is unclear; however, we demonstrated by in vitro myography that C21 can effectively inhibit bladder smooth muscle contraction by antagonizing M3 receptors at the micromolar level, causing increased voiding size in vivo . In summary, C21 functions as a GPCR antagonist and has significant dose-dependent off-target effects in the renal system., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 MacIver, Wu, Hill and Yu.)

Published
2024
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25. Dietary restriction impacts health and lifespan of genetically diverse mice.

Author

Di Francesco A, Deighan AG, Litichevskiy L, Chen Z, Luciano A, Robinson L, Garland G, Donato H, Vincent M, Schott W, Wright KM, Raj A, Prateek GV, Mullis M, Hill WG, Zeidel ML, Peters LL, Harding F, Botstein D, Korstanje R, Thaiss CA, Freund A, and Churchill GA

Subjects
Animals, Female, Mice, Adiposity genetics, Adiposity physiology, Resilience, Psychological, Lymphocytes, Erythrocytes, Body Weight genetics, Body Weight physiology, Caloric Restriction adverse effects, Fasting adverse effects, Fasting metabolism, Fasting physiology, Genetic Variation, Health, Longevity genetics, Longevity physiology
Abstract

Caloric restriction extends healthy lifespan in multiple species 1 . Intermittent fasting, an alternative form of dietary restriction, is potentially more sustainable in humans, but its effectiveness remains largely unexplored 2-8 . Identifying the most efficacious forms of dietary restriction is key for developing interventions to improve human health and longevity 9 . Here we performed an extensive assessment of graded levels of caloric restriction (20% and 40%) and intermittent fasting (1 and 2 days fasting per week) on the health and survival of 960 genetically diverse female mice. We show that caloric restriction and intermittent fasting both resulted in lifespan extension in proportion to the degree of restriction. Lifespan was heritable and genetics had a larger influence on lifespan than dietary restriction. The strongest trait associations with lifespan included retention of body weight through periods of handling-an indicator of stress resilience, high lymphocyte proportion, low red blood cell distribution width and high adiposity in late life. Health effects differed between interventions and exhibited inconsistent relationships with lifespan extension. 40% caloric restriction had the strongest lifespan extension effect but led to a loss of lean mass and changes in the immune repertoire that could confer susceptibility to infections. Intermittent fasting did not extend the lifespan of mice with high pre-intervention body weight, and two-day intermittent fasting was associated with disruption of erythroid cell populations. Metabolic responses to dietary restriction, including reduced adiposity and lower fasting glucose, were not associated with increased lifespan, suggesting that dietary restriction does more than just counteract the negative effects of obesity. Our findings indicate that improving health and extending lifespan are not synonymous and raise questions about which end points are the most relevant for evaluating aging interventions in preclinical models and clinical trials., (© 2024. The Author(s).)

Published
2024
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26. Targeting NADPH Oxidase as an Approach for Diabetic Bladder Dysfunction.

Author

Silveira THR, Silva FH, Hill WG, Antunes E, and de Oliveira MG

Abstract

Diabetic bladder dysfunction (DBD) is the most prevalent complication of diabetes mellitus (DM), affecting >50% of all patients. Currently, no specific treatment is available for this condition. In the early stages of DBD, patients typically complain of frequent urination and often have difficulty sensing when their bladders are full. Over time, bladder function deteriorates to a decompensated state in which incontinence develops. Based on studies of diabetic changes in the eye, kidney, heart, and nerves, it is now recognized that DM causes tissue damage by altering redox signaling in target organs. NADPH oxidase (NOX), whose sole function is the production of reactive oxygen species (ROS), plays a pivotal role in other well-known and bothersome diabetic complications. However, there is a substantial gap in understanding how NOX controls bladder function in health and the impact of NOX on DBD. The current review provides a thorough overview of the various NOX isoforms and their roles in bladder function and discusses the importance of further investigating the role of NOXs as a key contributor to DBD pathogenesis, either as a trigger and/or an effector and potentially as a target., Competing Interests: The authors declare no conflicts of interest.

Published
2024
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27. A Spectrum of Age- and Gender-Dependent Lower Urinary Tract Phenotypes in Three Mouse Models of Type 2 Diabetes.

Author

MacIver B, Bien EM, de Oliveira MG, and Hill WG

Abstract

Lower urinary tract symptoms are extremely common in people with diabetes and obesity, but the causes are unclear. Furthermore, it has proven difficult to reliably demonstrate bladder dysfunction in diabetic mouse models, thus limiting the ability to gain mechanistic insights. Therefore, the main objective of this experimental study was to characterize diabetic bladder dysfunction in three promising polygenic mouse models of type 2 diabetes. We performed periodic assessments of glucose tolerance and micturition (void spot assay) for eight to twelve months. Males and females and high-fat diets were tested. NONcNZO10/LtJ mice did not develop bladder dysfunction over twelve months. TALLYHO/JngJ males were severely hyperglycemic from two months of age (fasted blood glucose ~550 mg/dL), while females were moderately so. Although males exhibited polyuria, neither they nor the females exhibited bladder dysfunction over nine months. KK.Cg-A y /J males and females were extremely glucose intolerant. Males exhibited polyuria, a significant increase in voiding frequency at four months (compensation), followed by a rapid drop in voiding frequency by six months (decompensation) which was accompanied by a dramatic increase in urine leakage, indicating loss of outlet control. At eight months, male bladders were dilated. Females also developed polyuria but compensated with larger voids. We conclude KK.Cg-A y /J male mice recapitulate key symptoms noted in patients and are the best model of the three to study diabetic bladder dysfunction.

Published
2023
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28. Selective Pharmacological Inhibition of NOX2 by GSK2795039 Improves Bladder Dysfunction in Cyclophosphamide-Induced Cystitis in Mice.

Author

de Oliveira MG, Monica FZ, Passos GR, Victorio JA, Davel AP, Oliveira ALL, Parada CA, D'Ancona CAL, Hill WG, and Antunes E

Abstract

Interstitial cystitis/bladder pain syndrome (IC/BPS) is a chronic inflammatory disease without consistently effective treatment. Among the many mediators implicated in cystitis, the overproduction of reactive oxygen species (ROS) seems to play a key role, although the main source of ROS remains unclear. This study aimed to investigate the contribution of NADPH oxidase (NOX) isoforms in ROS generation and the voiding dysfunction of cyclophosphamide (CYP, 300 mg/Kg, ip, 24 h)-induced cystitis in adult female mice, a well-recognized animal model to study IC/BPS, by using GKT137831 (5 mg/Kg, ip, three times in a 24 h period) or GSK2795039 (5 mg/Kg, ip, three times in a 24 h period) to inhibit NOX1/4 or NOX2, respectively. Our results showed that treatment with GSK2795039 improved the dysfunctional voiding behavior induced by CYP, reduced bladder edema and inflammation, and preserved the urothelial barrier integrity and tight junction occludin expression, besides inhibiting the characteristic vesical pain and bladder superoxide anion generation. In contrast, the NOX1/4 inhibitor GKT137831 had no significant protective effects. Taken together, our in vivo and ex vivo data demonstrate that NOX2 is possibly the main source of ROS observed in cystitis-induced CYP in mice. Therefore, selective inhibition of NOX2 by GSK2795039 may be a promising target for future therapies for IC/BPS.

Published
2022
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29. Deletion of Mechanosensory β1-integrin From Bladder Smooth Muscle Results in Voiding Dysfunction and Tissue Remodeling.

Author

Yu W, MacIver B, Zhang L, Bien EM, Ahmed N, Chen H, Hanif SZ, de Oliveira MG, Zeidel ML, and Hill WG

Abstract

The bladder undergoes large shape changes as it fills and empties and experiences complex mechanical forces. These forces become abnormal in diseases of the lower urinary tract such as overactive bladder, neurogenic bladder, and urinary retention. As the primary mechanosensors linking the actin cytoskeleton to the extracellular matrix (ECM), integrins are likely to play vital roles in maintaining bladder smooth muscle (BSM) homeostasis. In a tamoxifen-inducible smooth muscle conditional knockout of β1-integrin, there was concomitant loss of α1- and α3-integrins from BSM and upregulation of αV- and β3-integrins. Masson's staining showed a reduction in smooth muscle with an increase in collagenous ECM. Functionally, mice exhibited a changing pattern of urination by voiding spot assay up to 8 wk after tamoxifen. By 8 wk, there was increased frequency with reductions in voided volume, consistent with overactivity. Cystometrograms confirmed that there was a significant reduction in intercontractile interval with reduced maximal bladder pressure. Muscle strip myography revealed a loss of contraction force in response to electrical field stimulation, that was entirely due to the loss of muscarinic contractility. Quantitative western blotting showed a loss of M3 receptor and no change in P2X 1 . qPCR on ECM and interstitial genes revealed loss of Ntpd2, a marker of an interstitial cell subpopulation; and an upregulation of S100A4, which is often associated with fibroblasts. Collectively, the data show that the loss of appropriate mechanosensation through integrins results in cellular and extracellular remodeling, and concomitant bladder dysfunction that resembles lower urinary tract symptoms seen in older people., Competing Interests: The authors have no conflicts of interest to disclose., (© The Author(s) 2022. Published by Oxford University Press on behalf of American Physiological Society.)

Published
2022
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30. Urine and Tissue Bacterial Loads Correlate With Voiding Behaviors in a Murine Urinary Tract Infection Model.

Author

Zhu K, Hill WG, Li F, Shi B, and Chai TC

Subjects
Animals, Correlation of Data, Disease Models, Animal, Female, Mice, Mice, Inbred C57BL, Urine microbiology, Bacterial Load, Kidney microbiology, Urinary Bladder microbiology, Urinary Tract Infections microbiology, Urinary Tract Infections physiopathology, Urinary Tract Infections urine, Urination
Abstract

Objectives: To describe associations between voiding behavior and bacterial loads in a murine model of urinary tract infection (UTI)., Methods: Fourteen female C57BL/6J mice were transurethrally inoculated with 10 8 colony-forming unit uropathogenic E. coli (UPEC) UTI89 in 50 μL two times, 24 hours apart. Voiding spot assays were used to measure voiding behavior. Voiding spot assays and urine cultures were performed at various time points between 1 and 28 days postinfection (dpi). Bladder and kidney bacterial loads were measured at 28 dpi. Correlations were calculated between voiding spot assay variables and bacterial loads at different dpi. In a separate experiment, 3 female mice were infected with UPEC in the same manner for histology changes at 28-dpi in chronic UTI., Results: During the 28 days, among 14 mice, 8 developed chronic cystitis and 11 developed chronic pyelonephritis based on a priori definitions. All infected mice showed increased urinary frequency, polyuria, and decreased bladder capacity. Tissue fibrosis was also observed in the infected bladder. At 1 dpi and 28 dpi, the urinary bacterial loads were positively associated with frequency and polyuria. Bladder and kidney bacterial loads at 28 dpi were positively with frequency and polyuria., Conclusions: Urine and tissue bacterial loads were associated with changes of voiding behavior at both 1 and 28 dpi., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published
2021
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31. Molecular mechanisms of voiding dysfunction in a novel mouse model of acute urinary retention.

Author

Xie X, Chen H, Zhang L, Chan D, Hill WG, Zeidel ML, and Yu W

Subjects
Animals, Biomechanical Phenomena, Female, Gene Expression Regulation, Mice, Muscle Contraction, Muscle, Smooth pathology, Urinary Bladder injuries, Urinary Bladder metabolism, Urinary Retention metabolism, Urodynamics, Disease Models, Animal, Urinary Bladder pathology, Urinary Retention pathology
Abstract

Acute urinary retention (AUR) is a common urological emergency and affects a significant patient population. The inability to eliminate urine may lead to permanent damage to the bladder's structure and functioning. However, we know little about the underlying molecular sequelae to the urine retention. To closely mirror the potential high pressures that patients with AUR could experience, we catheterized anesthetized female mice via the urethra and filled the bladder by pumping saline (25 µL/min) into the bladder lumen to 50 cm or 80 cm water pressure. A water column with designated height (50 or 80 cm) was then adjusted to maintain constant pressure in the bladder lumen for 30 minutes. Functional and morphological evaluations were performed from 0 to 24 hours after AUR treatment. Mice exhibited incontinence and overactivity with diminished voiding pressure. Significant injury was confirmed which revealed bladders with disrupted urothelial barrier, edematous lamina propria, and distorted muscle bundles. Bladder smooth muscle (BSM) from pressure-treated mice have significantly diminished contraction force, suggesting that bladder voiding dysfunction can be attributed to impaired BSM contractility. Indeed, dysregulation of acetylcholine and purinergic signaling pathways were demonstrated, indicating that reduced efficacy of these pathways contributes to impaired BSM contractility. Finally, altered expression of β1-integrin and extracellular matrix mediated mechanotransduction pathways were detected, suggesting a profound remodeling process. These data demonstrated an easy to perform, quantifiable, and reproducible AUR mouse model, which mimics well the characteristics of human AUR patients, and our data generate new insights into the molecular mechanisms that occur following AUR., (© 2021 Federation of American Societies for Experimental Biology.)

Published
2021
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32. Early Increased Urinary IL-2 and IL-10 Levels Were Associated With Development of Chronic UTI in a Murine Model.

Author

Zhu K, Hill WG, Li F, Shi B, and Chai TC

Subjects
Animals, Bacterial Load, Biomarkers urine, Chemokines urine, Chronic Disease, Disease Models, Animal, Disease Progression, Escherichia coli Infections complications, Female, Mice, Mice, Inbred C57BL, Urinary Tract Infections microbiology, Urination, Urine microbiology, Interleukin-10 urine, Interleukin-2 urine, Urinary Tract Infections urine
Abstract

Objectives: To analyze factors during early stage of urinary tract infection (UTI) that are associated with development of chronic UTI., Methods: Mice were inoculated with Uropathogenic Escherichia coli (UPEC) 2 times 24 hours apart. At 1, 3, 7, 10, 14, 21 and 28 days post infection (dpi), urine bacterial loads and voiding behavior (voiding spot assay, VSA) were measured. At 1 and 28 dpi, 32 urine inflammatory cytokines/chemokines were measured using enzyme-linked immunosorbent assay (ELISA). Bladder and kidney cytokines/chemokines were measured on 28 dpi. Mice that had no more than 1 episode of urine bacterial load < 10 4 colony forming unit/ml during the entire 4 weeks were defined as susceptible to chronic UTI, otherwise, mice were considered resistant., Results: At 28 dpi, 64.3% mice developed chronic UTI (susceptible group) and 35.7% mice did not (resistant group). Factors at 1 dpi that were predictive of chronic UTI included increased urine IL-2 (OR 11.9, 95%CI 1.1-130.8, P = .043) and increased urine IL-10 (OR 14.0, 95%CI 1.0-201.2, P = .052). At 28 dpi, there were several significant differences between the susceptible vs resistant groups including urine/tissue bacterial loads and certain urine/tissue cytokines/chemokines., Conclusions: Higher urine IL-2 and IL-10 at 1 dpi predicted chronic UTI infection in this model. There have been recent publications associating both of these cytokines to UTI susceptibility. Further explorations into IL-2 and IL-10 mediated pathways could shed light on the biology of recurrent and chronic UTI which are difficult to treat., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published
2020
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33. Effect of heterogeneity in recombination rate on variation in realised relationship.

Author

White IMS and Hill WG

Subjects
Animals, Chickens, Humans, Chromosomes genetics, Evolution, Molecular, Models, Genetic, Recombination, Genetic
Abstract

Individuals of a specified pedigree relationship vary in the proportion of the genome they share identical by descent, i.e. in their realised or actual relationship. Predictions of the variance in realised relationship have previously been based solely on the proportion of the map length shared, which requires the implicit assumption that both recombination rate and genetic information are uniformly distributed along the genome. This ignores the possible existence of recombination hotspots, and fails to distinguish between coding and non-coding sequences. In this paper, we therefore quantify the effects of heterogeneity in recombination rate at broad and fine-scale levels on the variation in realised relationship. Variance is usually greater on a chromosome with a non-uniform recombination rate than on a chromosome with the same map length and uniform recombination rate, especially if recombination rates are higher towards chromosome ends. Reductions in variance can also be obtained, however, and the overall pattern of change is quite complex. In general, local (fine-scale) variation in recombination rate, e.g. hotspots, has a small influence on the variance in realised relationship. Differences in rates across longer regions and between chromosome ends can increase or decrease the variance in a realised relationship, depending on the genomic architecture.

Published
2020
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34. Urological complications of obesity and diabetes in males and females of three mouse models: temporal manifestations.

Author

Kim AK, Hamadani C, Zeidel ML, and Hill WG

Subjects
Animals, Body Weight physiology, Diabetes Mellitus, Type 1 physiopathology, Disease Models, Animal, Female, Insulin Resistance physiology, Male, Mice, Obesity physiopathology, Urologic Diseases physiopathology, Diabetes Mellitus, Type 1 complications, Obesity complications, Urinary Bladder physiopathology, Urologic Diseases etiology
Abstract

Diabetic bladder dysfunction is a frequent complication of diabetes. Although many mouse models of diabetes now exist, there has been little systematic effort to characterize them for the timing of onset and severity of bladder dysfunction. We monitored metabolic status and tested bladder function by void spot assay and limited anesthetized cystometry in both male and female mice of three models of obesity and diabetes: a type 1 diabetes model (the Akita mouse) and two type 2 diabetes models [the diet-induced obese (DIO) model and the ob/ob mouse]. Akita mice had insulin pellets implanted subcutaneously every 3 mo to mimic poorly controlled type 1 diabetes in humans. Mice were hyperglycemic by 48 days after implants. Female mice exhibited no bladder dysfunction at any age up to 20 mo and gained weight normally. In contrast, by 7 mo, male Akita mice developed a profound polyuria and failed to show normal weight gain. There were no observable signs of bladder dysfunction in either sex. DIO mice on high/low-fat diets for 16 mo exhibited mild hyperglycemia in female mice (not in male mice), mild weight gain, and no evidence of bladder dysfunction. Ob/ob mice were followed for 8 mo and became extremely obese. Male and female mice were glucose intolerant, insulin intolerant, and hyperinsulinemic at 4 mo. By 8 mo, their metabolic status had improved but was still abnormal. Urine volume increased in male mice but not in female mice. Bladder dysfunction was observed in the spotting patterns of female mice at 4 and 6 mo of age, resolving by 8 mo. We conclude there are dramatic sex-related differences in lower urinary tract function in these models. Male Akita mice may be a good model for polyuria-related bladder remodeling, whereas female ob/ob mice may better mimic storage problems related to loss of outlet control in a setting of type 2 diabetes complicated by obesity.

Published
2020
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35. Targetable purinergic receptors P2Y12 and A2b antagonistically regulate bladder function.

Author

Hao Y, Wang L, Chen H, Hill WG, Robson SC, Zeidel ML, and Yu W

Subjects
Animals, Cells, Cultured, Female, Mice, Mice, Inbred C57BL, Mice, Knockout, Models, Biological, Muscle Contraction, Muscle, Smooth physiology, Pregnancy, Signal Transduction, Urinary Bladder Diseases metabolism, Receptor, Adenosine A2B physiology, Receptors, Purinergic P2Y12 physiology, Urinary Bladder physiology
Abstract

Abnormalities in purine availability or purinergic receptor density are commonly seen in patients with lower urinary tract symptoms (LUTS), but the underlying mechanisms relating altered receptor function to LUTS are unknown. Here we provide extensive evidence for the reciprocal interplay of multiple receptors responding to ATP, ADP (adenosine diphosphate), and adenosine, agonists that regulate bladder function significantly. ADP stimulated P2Y12 receptors, causing bladder smooth muscle (BSM) contraction, whereas adenosine signaling through potentially newly defined A2b receptors, actively inhibited BSM purinergic contractility. The modulation of adenylyl cyclase-cAMP signaling via A2b and P2Y12 interaction actively regulated bladder contractility by modulating intracellular calcium levels. KO mice lacking the receptors display diametrically opposed bladder phenotypes, with P2Y12-KO mice exhibiting an underactive bladder (UAB) phenotype with increased bladder capacity and reduced voiding frequency, whereas A2b-KO mice have an overactive bladder (OAB), with decreased capacity and increased voiding frequency. The opposing phenotypes in P2Y12-KO and A2b-KO mice not only resulted from dysregulated BSM contractility, but also from abnormal BSM cell growth. Finally, we demonstrate that i.p. administration of drugs targeting P2Y12 or A2b receptor rescues these abnormal phenotypes in both KO mice. These findings strongly indicate that P2Y12 and A2b receptors are attractive therapeutic targets for human patients with LUTS.

Published
2019
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39. Mouse urothelial genes associated with voiding behavior changes after ovariectomy and bladder lipopolysaccharide exposure.

Author

Acevedo-Alvarez M, Yeh J, Alvarez-Lugo L, Lu M, Sukumar N, Hill WG, and Chai TC

Subjects
Animals, Behavior, Animal, Female, Gene Expression drug effects, Mice, Mice, Inbred C57BL, Microarray Analysis, RNA biosynthesis, RNA genetics, Urinary Bladder, Overactive chemically induced, Urinary Bladder, Overactive genetics, Urination drug effects, Urination physiology, Gene Expression physiology, Lipopolysaccharides pharmacology, Ovariectomy, Urinary Bladder drug effects, Urination genetics, Urothelium metabolism
Abstract

Aims: Symptoms from overactive bladder (OAB) and cystitis secondary to urinary tract infection (UTI) can be similar in post-menopausal women. Effects of ovariectomy (OVX) on voiding behavior after lipopolysaccharide (LPS) intravesical exposure (surrogate for cystitis) in mice were measured. Urothelial genes associated with micturition changes were identified., Methods: Female C57BL6/J mice underwent OVX or sham surgeries (n = 10 for each). Voiding spot assays (VSA) were performed prior to surgery, 4 weeks post-surgery, and each time after 3 consecutive days of transurethral instillation of LPS. In another experiment, mice underwent either sham (n = 9) or OVX (n = 9) surgeries. Urothelial RNAs were collected 4 weeks post-surgery, day 1 and day 3 after LPS instillation. Mouse Gene 2.0 ST Arrays (entire 34 K transcripts) were used for microarray hybridization. A set of criteria was utilized to identify gene expression changes that mimicked voiding behavior changes., Results: Three days after LPS exposure, OVX mice persisted with overactive whereas sham mice normalized voiding behavior. Nine urothelial paralleling voiding behavior changes were identified: IL6 (interleukin 6), IL6rα (Interleukin 6 receptor α), Ptgs2 (Prostaglandin-endoperoxide synthase 2 or COX-2), Ereg (epiregulin), Dusp6 (dual specificity phosphatase 6), Zfp948 (zinc finger protein 948), Zfp52 (Zinc finger protein 52), Gch1 (GTP cyclohydrolase 1), and Amd (S-adenosylmethionine decarboxylase). Three other genes, coding unknown proteins, were also identified: GM12840, GM23134, and GM26809., Conclusions: OVX mice persisted with increased voiding frequency after LPS. Urothelial genes that could mediate this voiding behavior include IL6, COX-2, and S-adenosylmethionine decarboxylase., (© 2018 Wiley Periodicals, Inc.)

Published
2018
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40. Void spot assay: recommendations on the use of a simple micturition assay for mice.

Author

Hill WG, Zeidel ML, Bjorling DE, and Vezina CM

Subjects
Animals, Biological Assay standards, Disease Models, Animal, Mice, Reproducibility of Results, Time Factors, Urination Disorders diagnosis, Biological Assay methods, Urinary Bladder physiopathology, Urination, Urination Disorders physiopathology, Urodynamics
Abstract

Investigators have for decades used mouse voiding patterns as end points for studying behavioral biology. It is only recently that mouse voiding patterns were adopted for study of lower urinary tract physiology. The spontaneous void spot assay (VSA), a popular micturition assessment tool, involves placing a mouse in an enclosure lined by filter paper and quantifying the resulting urine spot pattern. The VSA has advantages of being inexpensive and noninvasive, but some investigators challenge its ability to distinguish lower urinary tract function from behavioral voiding. A consensus group of investigators who regularly use the VSA was established by the National Institutes of Health in 2015 to address the strengths and weaknesses of the assay, determine whether it can be standardized across laboratories, and determine whether it can be used as a surrogate for evaluating urinary function. Here we leverage experience from the consensus group to review the history of the VSA and its uses, summarize experiments to optimize assay design for urinary physiology assessment, and make best practice recommendations for performing the assay and analyzing its results.

Published
2018
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41. Void spot assay procedural optimization and software for rapid and objective quantification of rodent voiding function, including overlapping urine spots.

Author

Wegner KA, Abler LL, Oakes SR, Mehta GS, Ritter KE, Hill WG, Zwaans BM, Lamb LE, Wang Z, Bjorling DE, Ricke WA, Macoska J, Marker PC, Southard-Smith EM, Eliceiri KW, and Vezina CM

Subjects
Animals, Goals, Male, Mice, Transgenic, Urinary Bladder physiopathology, Diabetes Mellitus, Experimental physiopathology, Software, Urination physiology, Urodynamics physiology
Abstract

Mouse urinary behavior is quantifiable and is used to pinpoint mechanisms of voiding dysfunction and evaluate potential human therapies. Approaches to evaluate mouse urinary function vary widely among laboratories, however, complicating cross-study comparisons. Here, we describe development and multi-institutional validation of a new tool for objective, consistent, and rapid analysis of mouse void spot assay (VSA) data. Void Whizzard is a freely available software plugin for FIJI (a distribution of ImageJ) that facilitates VSA image batch processing and data extraction. We describe its features, demonstrate them by evaluating how specific VSA method parameters influence voiding behavior, and establish Void Whizzard as an expedited method for VSA analysis. This study includes control and obese diabetic mice as models of urinary dysfunction to increase rigor and ensure relevance across distinct voiding patterns. In particular, we show that Void Whizzard is an effective tool for quantifying nonconcentric overlapping void spots, which commonly confound analyses. We also show that mouse genetics are consistently more influential than assay design parameters when it comes to VSA outcomes. None of the following procedural modifications to reduce overlapping spots masked these genetic-related differences: reduction of VSA testing duration, water access during the assay period, placement of a wire mesh cage bottom on top of or elevated over the filter paper, treatment of mesh with a hydrophobic spray, and size of wire mesh opening. The Void Whizzard software and rigorous validation of VSA methodological parameters described here advance the goal of standardizing mouse urinary phenotyping for comprehensive urinary phenome analyses.

Published
2018
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42. One Hundred Years of Linkage Disequilibrium.

Author

Sved JA and Hill WG

Subjects
Animals, Evolution, Molecular, Gene Frequency, Genetic Predisposition to Disease, Genetics, Population, Humans, Population Density, Quantitative Trait Loci, Chromosome Mapping methods, Linkage Disequilibrium, Polymorphism, Single Nucleotide
Abstract

One hundred years ago, the first population genetic calculations were made for two loci. They indicated that populations should settle down to a state where the frequency of an allele at one locus is independent of the frequency of an allele at a second locus, even if these loci are linked. Fifty years later it was realized what is obvious in retrospect, that these calculations ignored the effect of chance segregation of linked loci, an effect now widely recognized following the association of closely linked markers (SNPs) with rare genetic diseases. Linkage disequilibrium is now accepted as the norm for closely linked loci, leading to powerful applications in the mapping of disease alleles and quantitative trait loci, in the detection of sites of selection in the human genome, in the application of genomic prediction of quantitative traits in animal and plant breeding, in the estimation of population size, and in the dating of population divergence., (Copyright © 2018 by the Genetics Society of America.)

Published
2018
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44. Role of P2X 4 Receptor in Mouse Voiding Function.

Author

Yu W, Hill WG, Robson SC, and Zeidel ML

Subjects
Animals, Female, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Muscle Contraction physiology, Muscle, Smooth metabolism, Myocytes, Smooth Muscle metabolism, Urinary Bladder metabolism, Receptors, Purinergic P2X4 metabolism
Abstract

Purinergic signalling plays an important role in the regulation of bladder smooth muscle (BSM) contractility, and P2X 4 receptor is expressed in the bladder wall, where it may act by forming heteromeric receptors with P2X 1 , the major purinergic force-generating muscle receptor. To test this hypothesis, we examined mouse BSM contractile properties in the absence and presence of selective P2X 1 (NF449 & NF279) and P2X 4 antagonists (5-BDBD). These drugs inhibited BSM purinergic contraction only partially, suggesting the possibility of a heteromeric receptor. However, carefully controlled co-immunoprecipitation experiments indicated that P2X 1 and P2X 4 do not form physically linked heteromers. Furthermore, immunofluorescence staining showed that P2X 4 is not present in mouse BSM per se, but in an unknown cellular structure among BSM bundles. To investigate whether deletion of P2X 4 could impact voiding function in vivo, P2X 4 null mice were characterized. P2X 4 null mice had normal bladder weight and morphology, normal voiding spot size and number by voiding spot assay, normal voiding interval, pressure and compliance by cystometrogram, and normal BSM contractility by myography. In conclusion, these data strongly suggest that P2X 4 is not present in mouse BSM cells, does not affect smooth muscle contractility and that mice null for P2X 4 exhibit normal voiding function.

Published
2018
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46. Evaluating the voiding spot assay in mice: a simple method with complex environmental interactions.

Author

Chen H, Zhang L, Hill WG, and Yu W

Subjects
Animals, Environment, Female, Mice, Models, Animal, Stress, Psychological, Urinary Bladder physiopathology, Urodynamics genetics, Urodynamics physiology, Behavior, Animal physiology, Urination physiology
Abstract

The voiding spot assay (VSA) on filter paper is an increasingly popular method for studying lower urinary tract physiology in mice. However, the ways VSAs are performed differ significantly between laboratories, and many variables are introduced compared with the mouse's normal housing situation. Rodents are intelligent social animals, and it is increasingly understood that social and environmental stresses have significant effects on their physiology. Surprisingly, little is known about whether change of environment during VSA affects mouse voiding and what the best methodologies are for retaining "natural" micturition patterns. It is well known that stress-related neuropeptide corticotropin-releasing factor is significantly elevated and induces dramatic voiding changes when rodents encounter stresses. Therefore we hypothesized that changes in the environmental situation could potentially alter voiding during VSA. We have examined multiple factors to test whether they affect female mouse voiding patterns during VSA, including cage type, cage floor, water availability, water bottle location, single or group housing, and different handlers. Our results indicate that mice are surprisingly sensitive to changes in cage type and floor surface, water bottle location, and single/group housing, each of which induces significant changes in voiding patterns, indicative of a stress response. In contrast, neither changing handler nor 4 h of water deprivation affected voiding patterns. Our data indicate that VSA should be performed under conditions as close as possible to the mouse's normal housing. Optimizing VSA methodology will be useful in uncovering voiding alterations in both genetic and disease models of lower urinary dysfunctions., (Copyright © 2017 the American Physiological Society.)

Published
2017
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47. "Conversion" of epistatic into additive genetic variance in finite populations and possible impact on long-term selection response.

Author

Hill WG

Subjects
Animals, Humans, Mutation, Population Dynamics, Quantitative Trait, Heritable, Time Factors, Computational Biology methods, Epistasis, Genetic, Genetic Variation, Models, Genetic, Selection, Genetic
Abstract

The role of epistasis in understanding the genetic architecture and variation of quantitative traits and its role, if any, in artificial selection and livestock improvement more generally has a long and sometimes controversial history. Its presence has been clearly demonstrated in, for example, laboratory experiments, but the amount of variation it contributes is likely to be small in outbred populations. In a finite population, although additive x additive epistatic variance is lost by genetic drift, it also contributes by conversion to additive variance through drift sampling and therefore has a potential indirect role in medium and long-term selection response, with superficial similarity to and hard to distinguish from mutation. Whilst predictions of response require knowledge of genetic parameters, an infinitesimal model provides some analytic results. Otherwise there is little quantitative information relevant to animal populations on which to judge this potential role of epistasis and reach firm conclusions., (© 2017 Blackwell Verlag GmbH.)

Published
2017
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48. Stage- and subunit-specific functions of polycomb repressive complex 2 in bladder urothelial formation and regeneration.

Author

Guo C, Balsara ZR, Hill WG, and Li X

Subjects
Adult Stem Cells cytology, Adult Stem Cells physiology, Animals, Cell Differentiation genetics, Cell Differentiation physiology, Embryonic Stem Cells cytology, Embryonic Stem Cells physiology, Epigenesis, Genetic, Female, Gene Expression Regulation, Developmental, Hedgehog Proteins genetics, Hedgehog Proteins physiology, Male, Mice, Mice, Knockout, Mice, Transgenic, Polycomb Repressive Complex 2 chemistry, Polycomb Repressive Complex 2 deficiency, Polycomb Repressive Complex 2 genetics, Protein Subunits, Regeneration genetics, Urinary Bladder embryology, Urothelium embryology, Polycomb Repressive Complex 2 physiology, Regeneration physiology, Urinary Bladder growth & development, Urinary Bladder physiology, Urothelium growth & development, Urothelium physiology
Abstract

Urothelium is the protective lining of the urinary tract. The mechanisms underlying urothelial formation and maintenance are largely unknown. Here, we report the stage-specific roles of PRC2 epigenetic regulators in embryonic and adult urothelial progenitors. Without Eed, the obligatory subunit of PRC2, embryonic urothelial progenitors demonstrate reduced proliferation with concomitant dysregulation of genes including Cdkn2a (p16), Cdkn2b (p15) and Shh. These mutants display premature differentiation of keratin 5-positive (Krt5 + ) basal cells and ectopic expression of squamous-like differentiation markers. Deletion of Ezh2, the major enzymatic component of PRC2, causes upregulation of Upk3a + superficial cells. Unexpectedly, Eed and Eed/Ezh2 double mutants exhibit delayed superficial cell differentiation. Furthermore, Eed regulates the proliferative and regenerative capacity of adult urothelial progenitors and prevents precocious differentiation. Collectively, these findings uncover the epigenetic mechanism by which PRC2 controls urothelial progenitor cell fate and the timing of differentiation, and further suggest an epigenetic basis of urothelial maintenance and regeneration., (© 2017. Published by The Company of Biologists Ltd.)

Published
2017
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49. Effect of filling rate on cystometric parameters in young and middle aged mice.

Author

Kim AK and Hill WG

Abstract

Objectives: To investigate the effect of changing the bladder filling rate during cystometry in younger (2-3 months) and older (13-14 months) C57BL/6J male mice., Methods: Cystometry was performed on mice under anesthesia. Voiding cycles were established in each mouse at a pump delivery rate of 17 μl/min. After 30 min, the rate was increased sequentially to 25, 33, 41 and 49 μl/min. Each rate was maintained for 30 min. The following cystometric parameters were quantified: peak pressure amplitude, intercontractile interval (ICI), compliance, micturition pressure threshold and voiding efficiency., Results: Bladder weights were significantly greater in older mice (42 mg vs. 27 mg, P < 0.01), but functional capacities were not different. The pressure amplitudes did not change as filling rate increased, nor did they differ between the 4-month and 13-month-old males. ICIs were not significantly different between young and mature mice. However, both groups exhibited a non-linear reduction in ICI with increasing filling rate, best described by a power curve ( R 2 > 0.93). Compliance was higher in the older mice at low filling rates (17 and 25 μl/min) but this difference diminished at higher rates. Compliance decreased with increasing flow rate in a non-linear manner, again with greater effects at low filling rates. Micturition pressure thresholds increased with increasing flow rate in a linear manner and older mice began voiding at higher pressures than younger. Both young and old mice exhibited voiding efficiencies of ~70%., Conclusions: The rate of volume delivery has complex effects on the timing of voiding and compliance. These findings argue for greater standardization of cystometry protocols and further investigation into afferent signaling to higher centers at different filling rates., Competing Interests: Competing interests: The authors have declared that no competing interests exist.

Published
2017
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50. Oxidative costs of reproduction in mouse strains selected for different levels of food intake and which differ in reproductive performance.

Author

Jothery AH, Vaanholt LM, Mody N, Arnous A, Lykkesfeldt J, Bünger L, Hill WG, Mitchell SE, Allison DB, and Speakman JR

Subjects
Animals, Female, Male, Mice, Oxidation-Reduction, Eating physiology, Reproduction physiology
Abstract

Oxidative damage caused by reactive oxygen species has been hypothesised to underpin the trade-off between reproduction and somatic maintenance, i.e., the life-history-oxidative stress theory. Previous tests of this hypothesis have proved equivocal, and it has been suggested that the variation in responses may be related to the tissues measured. Here, we measured oxidative damage (protein carbonyls, 8-OHdG) and antioxidant protection (enzymatic antioxidant activity and serum antioxidant capacity) in multiple tissues of reproductive (R) and non-reproductive (N) mice from two mouse strains selectively bred for high (H) or low (L) food intake, which differ in their reproductive performance, i.e., H mice have increased milk energy output (MEO) and wean larger pups. Levels of oxidative damage were unchanged (liver) or reduced (brain and serum) in R versus N mice, and no differences in multiple measures of oxidative protection were found between H and L mice in liver (except for Glutathione Peroxidase), brain or mammary glands. Also, there were no associations between an individual's energetic investment (e.g., MEO) and most of the oxidative stress measures detected in various tissues. These data are inconsistent with the oxidative stress theory, but were more supportive of, but not completely consistent, with the 'oxidative shielding' hypothesis.

Published
2016
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