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3. The role of insulin receptor substrate 2 in hypothalamic and β cell function

Author

Choudhury, A.I., Heffron, H., Smith, M.A., Al-Qassab, H., Xu, A.W., Selman, C., Simmgen, M., Clements, M., Claret, M., MacColl, G., Bedford, D.C., Hisadome, K., Diakonov, I., Moosajee, V., Bell, J.D., Speakman, J.R., Batterham, R.L., Barsh, G.S., Ashford, M.L.J., and Withers, D.J.

Subjects
nervous system, digestive, oral, and skin physiology, hormones, hormone substitutes, and hormone antagonists
Abstract

Insulin receptor substrate 2 (Irs2) plays complex roles in energy homeostasis. We generated mice lacking Irs2 in β cells and a population of hypothalamic neurons (RIPCreIrs2KO), in all neurons (NesCreIrs2KO), and in proopiomelanocortin neurons (POMCCreIrs2KO) to determine the role of Irs2 in the CNS and β cell. RIPCreIrs2KO mice displayed impaired glucose tolerance and reduced β cell mass. Overt diabetes did not ensue, because β cells escaping Cre-mediated recombination progressively populated islets. RIPCreIrs2KO and NesCreIrs2KO mice displayed hyperphagia, obesity, and increased body length, which suggests altered melanocortin action. POMCCreIrs2KO mice did not display this phenotype. RIPCreIrs2KO and NesCreIrs2KO mice retained leptin sensitivity, which suggests that CNS Irs2 pathways are not required for leptin action. NesCreIrs2KO and POMCCreIrs2KO mice did not display reduced β cell mass, but NesCreIrs2KO mice displayed mild abnormalities of glucose homeostasis. RIPCre neurons did not express POMC or neuropeptide Y. Insulin and a melanocortin agonist depolarized RIPCre neurons, whereas leptin was ineffective. Insulin hyperpolarized and leptin depolarized POMC neurons. Our findings demonstrate a critical role for IRS2 in β cell and hypothalamic function and provide insights into the role of RIPCre neurons, a distinct hypothalamic neuronal population, in growth and energy homeostasis.

Published
2005

4. Molecular modelling and experimental studies of mutation and cell-adhesion sites in the fibronectin type III and whey acidic protein domains of human anosmin-1

Author

Robertson, A, MacColl, G S, Nash, J A, Boehm, M K, Perkins, S J, and Bouloux, P M

Subjects
Models, Molecular, Neurons, Extracellular Matrix Proteins, Sequence Homology, Amino Acid, Protein Conformation, Amino Acid Motifs, DNA Mutational Analysis, Molecular Sequence Data, Mutation, Missense, Nerve Tissue Proteins, Milk Proteins, Fibronectins, Protein Structure, Tertiary, Amino Acid Substitution, Cell Adhesion, Humans, Amino Acid Sequence, Heparitin Sulfate, Peptides, Cells, Cultured, Research Article
Abstract

Anosmin-1, the gene product of the KAL gene, is implicated in the pathogenesis of X-linked Kallmann's syndrome. Anosmin-1 protein expression is restricted to the basement membrane and interstitial matrix of tissues affected in this syndrome during development. The anosmin-1 sequence indicates an N-terminal cysteine-rich domain, a whey acidic protein (WAP) domain, four fibronectin type III (FnIII) domains and a C-terminal histidine-rich region, and shows similarity with cell-adhesion molecules, such as neural cell-adhesion molecule, TAG-1 and L1. We investigated the structural and functional significance of three loss-of-function missense mutations of anosmin-1 using comparative modelling of the four FnIII and the WAP domains based on known NMR and crystal structures. Three missense mutation-encoded amino acid substitutions, N267K, E514K and F517L, were mapped to structurally defined positions on the GFCC' beta-sheet face of the first and third FnIII domains. Electrostatic maps demonstrated large basic surfaces containing clusters of conserved predicted heparan sulphate-binding residues adjacent to these mutation sites. To examine these modelling results anosmin-1 was expressed in insect cells. The incorporation of the three mutations into recombinant anosmin-1 had no effect on its secretion. The removal of two dibasic motifs that may constitute potential physiological cleavage sites for anosmin-1 had no effect on cleavage. Peptides based on the anosmin-1 sequences R254--K285 and P504--K527 were then synthesized in order to assess the effect of the three mutations on cellular adhesion, using cell lines that represented potential functional targets of anosmin-1. Peptides (10 microg/ml) incorporating the N267K and E514K substitutions promoted enhanced adhesion to 13.S.1.24 rat olfactory epithelial cells and canine MDCK1 kidney epithelial cells (P

Published
2001

10. Multicystic dysplastic kidney and Kallmann's syndrome: a new association?

Author

Deeb, A, Robertson, A, MacColl, G, Bouloux, P M, Gibson, M, Winyard, P J, Woolf, A S, Moghal, N E, and Cheetham, T D

Abstract

Kallmann's syndrome is characterized by anosmia and hypogonadotrophic hypogonadism. Radiographic studies of teenagers and older subjects with the X-linked form of the syndrome have shown that up to 40% have an absent kidney unilaterally. Although this has been attributed to renal "agenesis", a condition in which the kidney fails to form, little is known about the appearance of the developing urinary tract either pre- or post-natally in individuals with Kallmann's syndrome.

Published
2001
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11. Impact of regulatory safety notices on valproate prescribing and pregnancy outcome among women of child-bearing potential in Scotland: a population-based cohort study.

Author

McTaggart S, MacColl G, Gronkowski K, Wood R, Leach JP, and Bennie M

Subjects
Cohort Studies, Female, Humans, Pregnancy, Pregnancy Outcome epidemiology, Scotland epidemiology, Abortion, Spontaneous, Valproic Acid adverse effects
Abstract

Objective: To examine the impact of Medicines and Healthcare products Regulatory Agency (MHRA) safety alerts on valproate prescribing among women aged 14-45 years in Scotland and examine trends in pregnancies exposed to valproate., Design: Population-based cohort study., Participants: 21 983 women of all ages who received valproate between January 2011 and December 2019., Methods: All valproate prescriptions issued to women in Scotland between January 2011 and December 2019 were identified and prevalence/incidence rates per 10 000 population derived. The impact of regulatory safety alerts on prescribing was analysed using Joinpoint models. Linked pregnancy records for January 2011 to September 2019 were identified and annual rates of pregnancy per 1000 valproate-treated women aged 14-45 years were calculated for each pregnancy outcome: live birth, stillbirth, miscarriage and termination., Results: Annual prevalent and incident rates of valproate prescribing declined in women aged 14-45 years between 2011 and 2019 from 40.5 to 18.3 per 10 000 population (54.8% reduction) and 7.9 to 1.3 per 10 000 population (83.5% reduction), respectively. Statistically significant changes occurred around the times of the MHRA safety alerts. The number of valproate-exposed pregnancies conceived each year fell from 70 in 2011 to 20 in 2018, a 71.4% reduction, and the number of live births fell from 52 to 14, a 73.0% reduction. Expressed as a rate this was a 46.4% decrease from 15.3 to 8.2 per 1000 valproate-treated women aged 14-45 years in 2011 and 2018, respectively. Live birth was the most common pregnancy outcome., Conclusion: This study demonstrates, for the first time, the capabilities of national data sets to identify drug exposure and derive pregnancy outcome at scale across Scotland. Building on this as part of an evolving national/UK surveillance capability will continue efforts to minimise in-utero exposure to valproate; enabling ongoing surveillance to understand better long-term outcomes, and to inform better provision of health and wider support services., Competing Interests: Competing interests: In the last 10 years JPL has received speaker’s fees and Advisory Board honoraria from UCB Pharma, EISAI, Desitin, GlaxoSmithKline, GW Pharmaceuticals, Biogen and Arvelle. There has been an award of an unrestricted Independent Investigator Award from UCB in 2015 to fund a research fellow. SM, GM, KG, RW and MB have no competing interests to declare., (© Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published
2022
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12. Fall in peptic ulcer mortality associated with increased consultant input, prompt surgery and use of high dependency care identified through peer-review audit.

Author

Aga H, Readhead D, Maccoll G, and Thompson A

Abstract

Objectives: Patients with peptic ulceration continue to present to surgeons with complications of bleeding or perforation and to die under surgical care. This study sought to examine whether improved consultant input, timely interventions and perioperative care could reduce mortality from peptic ulcer., Design: Prospective collection of peer-review mortality data using Scottish Audit of Surgical Mortality methodologies (http://www.SASM.org) and analysed using SPSS., Setting: Secondary care; all hospitals in Scotland, UK, admitting surgical patients over 13 years (1994-2006)., Participants: 42 736 patients admitted (38 782 operative and 3954 non-operative) with peptic ulcer disease; 1952 patients died (1338 operative and 614 non-operative deaths) with a diagnosis of peptic ulcer., Primary and Secondary Outcome Measures: Adverse events; consultant presence at operation, operations performed within 2 h and high dependency/intensive therapy unit (HDU/ITU) use., Results: Annual mortality fell from 251 in 1994 to 83 in 2006, proportionately greater than the reduction in hospital admissions with peptic ulcer. Adverse events declined over time and were rare for non-operative patients. Consultant surgeon presence at operation rose from 40.0% in 1994 to 73.4% in 2006, operations performed within 2 h of admission from 10.3% in 1994 to 28.1% in 2006 and HDU/ITU use from 52.7% in 1994 to 84.4% in 2006. Consultant involvement (p=0.005) and HDU/ITU care (p=0.026) were significantly associated with a reduction in operative deaths., Conclusion: Patients with complications of peptic ulceration admitted under surgical care should be offered consultant surgeon input, timely surgery and HDU/ITU care.

Published
2012
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13. Overexpression of 5-HT2C receptors in forebrain leads to elevated anxiety and hypoactivity.

Author

Kimura A, Stevenson PL, Carter RN, Maccoll G, French KL, Simons JP, Al-Shawi R, Kelly V, Chapman KE, and Holmes MC

Subjects
Animals, Anxiety genetics, COS Cells, Chlorocebus aethiops, Male, Mice, Mice, Inbred C57BL, Mice, Inbred CBA, Mice, Transgenic, Rats, Receptor, Serotonin, 5-HT2C genetics, Anxiety metabolism, Gene Expression, Motor Activity physiology, Prosencephalon physiology, Receptor, Serotonin, 5-HT2C biosynthesis
Abstract

The 5-HT(2C) receptor has been implicated in mood and eating disorders. In general, it is accepted that 5-HT(2C) receptor agonists increase anxiety behaviours and induce hypophagia. However, pharmacological analysis of the roles of these receptors is hampered by the lack of selective ligands and the complex regulation of receptor isoforms and expression levels. Therefore, the exact role of 5-HT(2C) receptors in mood disorders remain controversial, some suggesting agonists and others suggesting antagonists may be efficacious antidepressants, while there is general agreement that antagonists are beneficial anxiolytics. In order to test the hypothesis that increased 5-HT(2C) receptor expression, and thus increased 5-HT(2C) receptor signalling, is causative in mood disorders, we have undertaken a transgenic approach, directly altering the 5-HT(2C) receptor number in the forebrain and evaluating the consequences on behaviour. Transgenic mice overexpressing 5-HT(2C) receptors under the control of the CaMKIIalpha promoter (C2CR mice) have elevated 5-HT(2C) receptor mRNA levels in cerebral cortex and limbic areas (including the hippocampus and amygdala), but normal levels in the hypothalamus, resulting in > 100% increase in the number of 5-HT(2C) ligand binding sites in the forebrain. The C2CR mice show increased anxiety-like behaviour in the elevated plus-maze, decreased wheel-running behaviour and reduced activity in a novel environment. These behaviours were observed in the C2CR mice without stimulation by exogenous ligands. Our findings support a role for 5-HT(2C) receptor signalling in anxiety disorders. The C2CR mouse model offers a novel and effective approach for studying disorders associated with 5-HT(2C) receptors.

Published
2009
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14. Digenic mutations account for variable phenotypes in idiopathic hypogonadotropic hypogonadism.

Author

Pitteloud N, Quinton R, Pearce S, Raivio T, Acierno J, Dwyer A, Plummer L, Hughes V, Seminara S, Cheng YZ, Li WP, Maccoll G, Eliseenkova AV, Olsen SK, Ibrahimi OA, Hayes FJ, Boepple P, Hall JE, Bouloux P, Mohammadi M, and Crowley W

Subjects
Adult, Amino Acid Sequence, Base Sequence, Conserved Sequence, DNA genetics, Female, Fibroblast Growth Factor 8 metabolism, Genotype, Gonadotropin-Releasing Hormone deficiency, Heterozygote, Humans, Hypogonadism etiology, Hypogonadism metabolism, Kallmann Syndrome genetics, Male, Models, Genetic, Models, Molecular, Molecular Sequence Data, Pedigree, Phenotype, Receptor, Fibroblast Growth Factor, Type 1 chemistry, Receptor, Fibroblast Growth Factor, Type 1 genetics, Receptor, Fibroblast Growth Factor, Type 1 metabolism, Receptors, LHRH genetics, Sequence Deletion, Sequence Homology, Amino Acid, Transcription Factors genetics, Hypogonadism genetics, Mutation
Abstract

Idiopathic hypogonadotropic hypogonadism (IHH) due to defects of gonadotropin-releasing hormone (GnRH) secretion and/or action is a developmental disorder of sexual maturation. To date, several single-gene defects have been implicated in the pathogenesis of IHH. However, significant inter- and intrafamilial variability and apparent incomplete penetrance in familial cases of IHH are difficult to reconcile with the model of a single-gene defect. We therefore hypothesized that mutations at different IHH loci interact in some families to modify their phenotypes. To address this issue, we studied 2 families, one with Kallmann syndrome (IHH and anosmia) and another with normosmic IHH, in which a single-gene defect had been identified: a heterozygous FGF receptor 1 (FGFR1) mutation in pedigree 1 and a compound heterozygous gonadotropin-releasing hormone receptor (GNRHR) mutation in pedigree 2, both of which varied markedly in expressivity within and across families. Further candidate gene screening revealed a second heterozygous deletion in the nasal embryonic LHRH factor (NELF) gene in pedigree 1 and an additional heterozygous FGFR1 mutation in pedigree 2 that accounted for the considerable phenotypic variability. Therefore, 2 different gene defects can synergize to produce a more severe phenotype in IHH families than either alone. This genetic model could account for some phenotypic heterogeneity seen in GnRH deficiency.

Published
2007
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15. The role of insulin receptor substrate 2 in hypothalamic and beta cell function.

Author

Choudhury AI, Heffron H, Smith MA, Al-Qassab H, Xu AW, Selman C, Simmgen M, Clements M, Claret M, Maccoll G, Bedford DC, Hisadome K, Diakonov I, Moosajee V, Bell JD, Speakman JR, Batterham RL, Barsh GS, Ashford ML, and Withers DJ

Subjects
Animals, Body Weight, Electrophysiology, Genotype, Glucose metabolism, Hypothalamus cytology, Insulin administration & dosage, Insulin metabolism, Insulin Receptor Substrate Proteins, Intracellular Signaling Peptides and Proteins, Islets of Langerhans cytology, Leptin administration & dosage, Leptin metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Neurons cytology, Phosphoproteins genetics, Pro-Opiomelanocortin metabolism, Receptor, Insulin metabolism, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Energy Metabolism, Homeostasis, Hypothalamus metabolism, Islets of Langerhans metabolism, Neurons metabolism, Phosphoproteins metabolism
Abstract

Insulin receptor substrate 2 (Irs2) plays complex roles in energy homeostasis. We generated mice lacking Irs2 in beta cells and a population of hypothalamic neurons (RIPCreIrs2KO), in all neurons (NesCreIrs2KO), and in proopiomelanocortin neurons (POMCCreIrs2KO) to determine the role of Irs2 in the CNS and beta cell. RIPCreIrs2KO mice displayed impaired glucose tolerance and reduced beta cell mass. Overt diabetes did not ensue, because beta cells escaping Cre-mediated recombination progressively populated islets. RIPCreIrs2KO and NesCreIrs2KO mice displayed hyperphagia, obesity, and increased body length, which suggests altered melanocortin action. POMCCreIrs2KO mice did not display this phenotype. RIPCreIrs2KO and NesCreIrs2KO mice retained leptin sensitivity, which suggests that CNS Irs2 pathways are not required for leptin action. NesCreIrs2KO and POMCCreIrs2KO mice did not display reduced beta cell mass, but NesCreIrs2KO mice displayed mild abnormalities of glucose homeostasis. RIPCre neurons did not express POMC or neuropeptide Y. Insulin and a melanocortin agonist depolarized RIPCre neurons, whereas leptin was ineffective. Insulin hyperpolarized and leptin depolarized POMC neurons. Our findings demonstrate a critical role for IRS2 in beta cell and hypothalamic function and provide insights into the role of RIPCre neurons, a distinct hypothalamic neuronal population, in growth and energy homeostasis.

Published
2005
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16. Kallmann syndrome: adhesion, afferents, and anosmia.

Author

MacColl G, Bouloux P, and Quinton R

Subjects
Animals, Cell Adhesion genetics, Cell Adhesion Molecules deficiency, Cell Adhesion Molecules genetics, Humans, Kallmann Syndrome metabolism, Kallmann Syndrome physiopathology, Nerve Tissue Proteins deficiency, Nerve Tissue Proteins genetics, Olfactory Pathways metabolism, Olfactory Pathways physiopathology, Cell Differentiation genetics, Cell Movement genetics, Extracellular Matrix Proteins, Kallmann Syndrome genetics, Olfaction Disorders genetics, Olfactory Pathways abnormalities
Abstract

Three new studies into the function of human anosmin-1 and related proteins in C. elegans and rodents show that these influence axon branching and axon targeting. The rodent anosmin appears to work at two stages of development, initially promoting axon outgrowth from the olfactory bulb and then stimulating branching from axons into the olfactory cortex. CeKal-1 further influences morphogenesis, and, as the human and nematode anosmins are functionally conserved, these studies provide insights into the pathogenesis of Kallmann syndrome (KS).

Published
2002
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17. GnRH neuronal development: insights into hypogonadotrophic hypogonadism.

Author

MacColl G, Quinton R, and Bouloux PM

Subjects
Animals, Central Nervous System physiology, Gonadotropin-Releasing Hormone analogs & derivatives, Humans, Hypogonadism etiology, Hypogonadism genetics, Kallmann Syndrome complications, Kallmann Syndrome genetics, Kallmann Syndrome physiopathology, Olfaction Disorders genetics, Olfaction Disorders physiopathology, Cell Movement physiology, Gonadotropin-Releasing Hormone physiology, Hypogonadism physiopathology, Neurons physiology
Abstract

Pulsatile secretion of the hypothalamic decapeptide gonadotrophin-releasing hormone (GnRH) regulates activity of the pituitary-gonadal reproductive axis. Defects of this neuroendocrine axis necessarily result in hypogonadotrophic hypogonadism. In many vertebrate species studied, the main population of GnRH neurones originates extracranially within the olfactory system. In humans, both olfactory and GnRH systems are affected in Kallmann's syndrome--resulting in isolated hypogonadotrophic hypogonadism (IHH) combined with anosmia (loss of sense of smell). Familial IHH is also caused by other genetic conditions, which prevent GnRH from activating luteinizing hormone/follicle-stimulating hormone release from pituitary gonadotrophs. However, many cases of IHH have no defined chromosomal abnormality and, in the absence of pedigree analysis, studying the biological mechanisms controlling migration of GnRH neurones through the olfactory system into the developing central nervous system might reveal additional genetic pathways that play a role in the pathogenesis of IHH.

Published
2002
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18. Recent advances in the pathogenesis of Kallmann's syndrome.

Author

Bouloux PM, Hu Y, and MacColl G

Subjects
Female, Humans, Incidence, Kallmann Syndrome epidemiology, Kallmann Syndrome genetics, Male, Nerve Tissue Proteins genetics, Neurons physiology, Sex Characteristics, Extracellular Matrix Proteins, Gonadotropin-Releasing Hormone deficiency, Kallmann Syndrome physiopathology
Published
2002
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19. Molecular modelling and experimental studies of mutation and cell-adhesion sites in the fibronectin type III and whey acidic protein domains of human anosmin-1.

Author

Robertson A, MacColl GS, Nash JA, Boehm MK, Perkins SJ, and Bouloux PM

Subjects
Amino Acid Motifs, Amino Acid Sequence, Amino Acid Substitution, Cell Adhesion physiology, Cells, Cultured, DNA Mutational Analysis, Fibronectins genetics, Fibronectins metabolism, Heparitin Sulfate metabolism, Humans, Milk Proteins chemistry, Models, Molecular, Molecular Sequence Data, Mutation, Missense, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Neurons chemistry, Neurons metabolism, Peptides metabolism, Protein Conformation, Protein Structure, Tertiary, Sequence Homology, Amino Acid, Extracellular Matrix Proteins, Fibronectins chemistry, Nerve Tissue Proteins chemistry
Abstract

Anosmin-1, the gene product of the KAL gene, is implicated in the pathogenesis of X-linked Kallmann's syndrome. Anosmin-1 protein expression is restricted to the basement membrane and interstitial matrix of tissues affected in this syndrome during development. The anosmin-1 sequence indicates an N-terminal cysteine-rich domain, a whey acidic protein (WAP) domain, four fibronectin type III (FnIII) domains and a C-terminal histidine-rich region, and shows similarity with cell-adhesion molecules, such as neural cell-adhesion molecule, TAG-1 and L1. We investigated the structural and functional significance of three loss-of-function missense mutations of anosmin-1 using comparative modelling of the four FnIII and the WAP domains based on known NMR and crystal structures. Three missense mutation-encoded amino acid substitutions, N267K, E514K and F517L, were mapped to structurally defined positions on the GFCC' beta-sheet face of the first and third FnIII domains. Electrostatic maps demonstrated large basic surfaces containing clusters of conserved predicted heparan sulphate-binding residues adjacent to these mutation sites. To examine these modelling results anosmin-1 was expressed in insect cells. The incorporation of the three mutations into recombinant anosmin-1 had no effect on its secretion. The removal of two dibasic motifs that may constitute potential physiological cleavage sites for anosmin-1 had no effect on cleavage. Peptides based on the anosmin-1 sequences R254--K285 and P504--K527 were then synthesized in order to assess the effect of the three mutations on cellular adhesion, using cell lines that represented potential functional targets of anosmin-1. Peptides (10 microg/ml) incorporating the N267K and E514K substitutions promoted enhanced adhesion to 13.S.1.24 rat olfactory epithelial cells and canine MDCK1 kidney epithelial cells (P<0.01) compared with the wild-type peptides. This result was attributed to the introduction of a lysine residue adjacent to the large basic surfaces. We predict that two of the three missense mutants increase the binding of anosmin-1 to an extracellular target, possibly by enhancing heparan sulphate binding, and that this critically affects the function of anosmin-1.

Published
2001
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20. Idiopathic gonadotrophin deficiency: genetic questions addressed through phenotypic characterization.

Author

Quinton R, Duke VM, Robertson A, Kirk JM, Matfin G, de Zoysa PA, Azcona C, MacColl GS, Jacobs HS, Conway GS, Besser M, Stanhope RG, and Bouloux PM

Subjects
Adolescent, Adult, Craniofacial Abnormalities genetics, Dyskinesias genetics, Female, Genetic Linkage, Gonadotropins genetics, Humans, Kallmann Syndrome genetics, Kidney abnormalities, Male, Nerve Tissue Proteins genetics, Olfaction Disorders genetics, Pedigree, Phenotype, Prospective Studies, Retrospective Studies, X Chromosome, Extracellular Matrix Proteins, Gonadotropins deficiency, Hypogonadism genetics
Abstract

Objective: The association of idiopathic hypogonadotrophic hypogonadism (IHH) with congenital olfactory deficit defines Kallmann's syndrome (KS). Although a small proportion of IHH patients have been found to harbour defined genetic lesions, the genetic basis of most IHH cases remains to be elucidated. Genes currently recognized to be involved comprise KAL (associated with X-linked-KS), the GnRH receptor (associated with resistance to GnRH therapy), DAX 1 (associated with adrenohypoplasia congenita) and three loci also associated with obesity, leptin (OB), leptin receptor (DB) and prohormone convertase (PC1). Because of the rarity of the condition and the observation that patients are almost universally infertile without assistance, familial transmission of IHH is encountered infrequently and pedigrees tend to be small. This has constrained the ability of conventional linkage studies to identify other candidate loci for genetic IHH. We hypothesized that a systematic clinical evaluation of a large patient sample might provide new insights into the genetics of this rare disorder. Specifically, we wished to examine the following propositions. First, whether normosmic (nIHH) and anosmic (KS) forms of IHH were likely to be genetically discrete entities, on the basis of quantitative olfactory testing, analysis of autosomal pedigrees and the prevalence of developmental defects such as cryptorchidism and cleft palate. Second, whether mirror movements and/or unilateral renal agenesis were specific phenotypic markers for X-linked-KS., Design and Patients: We conducted a clinical study of 170 male and 45 female IHH patients attending the endocrinology departments of three London University teaching hospitals. Approximately 80% of data were obtained from case records and 20% collected prospectively. Parameters assessed included olfaction, testicular volume, family history of hypogonadism, anosmia or pubertal delay, and history or presence of testicular maldescent, neurological, renal or craniofacial anomalies. Where possible, the clinical information was correlated with published data on genetic analysis of the KAL locus., Results: Olfactory acuity was bimodally distributed with no evidence for a spectrum of olfactory deficit. Testicular volume, a marker of integrated gonadotrophin secretion, did not differ significantly between anosmic and normosmic patients, at 2.0 ml and 2.2 ml, respectively. Nevertheless, the prevalence of cryptorchidism was nearly three times greater in anosmic (70.3%, of which 75.0% bilateral) than in normosmic (23.2%, of which 43.8% bilateral) patients. Individuals with nIHH, eugonadal isolated anosmia and/or KS were observed to coexist within 6/13 autosomal IHH pedigrees. On three occasions, fertility treatment given to an IHH patient had resulted in the condition being transmitted to the resulting offspring. Mirror movements and unilateral renal agenesis were observed in 24/98 and 9/87 IHH patients, respectively, all of whom were identifiable as X-KS males on the basis of pedigree analysis and/or defective KAL coding sequence. Abnormalities of eye movement and unilateral sensorineural deafness were observed in 10/21 and 6/111 KS patients, respectively, but not in nIHH patients., Discussion: Patients with IHH are almost invariably either anosmic (KS) or normosmic (nIHH), rather than exhibiting intermediate degrees of olfactory deficit. Moreover, the prevalence of cryptorchidism is nearly three times greater in KS than in nIHH despite comparable testicular volumes, suggesting a primary defect of testicular descent in KS independent of gonadotrophin deficiency. Disorders of eye movement and hearing appear only to occur in association with KS. Taken together, these findings indicate a clear phenotypic separation between KS and nIHH. However, pedigree studies suggest that autosomal KS is an heterogeneous condition, with incomplete phenotypic penetrance within pedigrees, and that some cases of autosomal KS, nIHH and even isolated anosmia are likely to have a common genetic basis. The prevalences of anosmia, mirror movements and unilateral renal agenesis among X-KS men are estimated to be 100, 85 and 31%, respectively. In sporadic IHH, mirror movements and unilateral renal agenesis are 100% specific phenotypic markers of de novo X-KS. By comparison, only 7/10 X-KS families harboured KAL coding defects. Clinical ascertainment, using mirror movements, renal agenesis and ichthyosis as X-KS-specific phenotypic markers, suggested that de novo X-KS was unlikely to comprise more than 11% of sporadic cases. The majority of sporadic KS cases are therefore presumed to have an autosomal basis and, hence, the preponderance of affected KS males over females remains unexplained, though reduced penetrance in women would be a possibility.

Published
2001
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21. The relationship between bond strength and orthodontic bracket base surface area with conventional and microetched foil-mesh bases.

Author

MacColl GA, Rossouw PE, Titley KC, and Yamin C

Subjects
Adhesiveness, Aluminum Oxide chemistry, Analysis of Variance, Animals, Cattle, Chi-Square Distribution, Dental Enamel drug effects, Dental Enamel ultrastructure, Dental Stress Analysis instrumentation, Gels, Logistic Models, Maleates administration & dosage, Materials Testing, Microscopy, Electron, Scanning, Orthodontic Appliance Design, Phosphoric Acids administration & dosage, Resin Cements chemistry, Stress, Mechanical, Surface Properties, Acid Etching, Dental, Dental Alloys chemistry, Dental Bonding methods, Orthodontic Brackets
Abstract

The aim of this study was to test the effects on the shear bond strength by sandblasting bracket base surfaces, reducing base surface area, and etching enamel with various acid types. Four different base sizes, used as either standard (untreated), sandblasted or microetched were bonded with Phase II resin (Reliance Orthodontic Products, Inc.) in four groups of 12 bovine enamel specimens after enamel etching with phosphoric acid gel (37%), 37% phosphoric acid aqueous solution, 10% maleic acid gel, or 10% maleic acid aqueous solution. Storage of samples was for 7 days in distilled water at room temperature before shear bond testing with an Instron universal testing machine with a crosshead speed of 0.5 mm/min. Statistical analyses included the analysis of variance, the Student t test, and the Chi-square test at p < 0.05. An increase in shear bond strength was associated with sandblasting and microetching of foil-mesh bases for all base sizes (p < 0.05). No statistically significant difference in shear bond strength existed between the three larger base sizes, which indicated that shear bond strength is independent of surface area between 6.82 and 12.35 mm2. A reduction in bond strength was associated with the reduction of base surface area from 6.82 to 2.38 mm2 (p < 0.05). There appears to be no need to increase base surface area beyond 6.82 mm2. Aqueous maleic acid (10%) etching of the enamel was associated with the highest shear bond strength, with no statistically significant difference between the other three acids used.

Published
1998
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