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1. Quality standards for the management of non-alcoholic fatty liver disease (NAFLD): consensus recommendations from the British Association for the Study of the Liver and British Society of Gastroenterology NAFLD Special Interest Group

Author

McPherson S, Armstrong MJ, Cobbold JF, Corless L, Anstee QM, Aspinall RJ, Barclay ST, Brennan PN, Cacciottolo TM, Goldin RD, Hallsworth K, Hebditch V, Jack K, Jarvis H, Johnson J, Li W, Mansour D, McCallum M, Mukhopadhya A, Parker R, Ross V, Rowe IA, Srivastava A, Thiagarajan P, Thompson AI, Tomlinson J, Tsochatzis EA, Yeoman A, Alazawi W

Published
2022
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3. Scientific Business Abstracts of the 113th Annual Meeting of the Association of Physicians of Great Britain and Ireland

Author

Cacciottolo, TM, Perikari, A, van der Klaauw, A, Henning, E, Stadler, LKJ, Keogh, J, Farooqi, IS, Tenin, G, Keavney, B, Ryan, E, Budd, R, Bewley, M, Coelho, P, Rumsey, W, Sanchez, Y, McCafferty, J, Dockrell, D, Walmsley, S, Whyte, M, Liu, Y, Choy, M-K, Abraham, S, Black, G, Ford, T, Stanley, B, Good, R, Rocchiccioli, P, McEntegart, M, Watkins, S, Eteiba, H, Shaukat, A, Lindsay, M, Robertson, K, Hood, S, McGeoch, R, McDade, R, Sidik, N, McCartney, P, Corcoran, D, Collison, D, Rush, C, McConnachie, A, Touyz, R, Oldroyd, K, Berry, Colin, Gazdagh, G, Diver, L, Marshall, J, McGowan, R, Ahmed, F, Tobias, E, Curtis, E, Parsons, C, Maslin, K, D’Angelo, S, Moon, R, Crozier, S, Gossiel, F, Bishop, N, Kennedy, S, Papageorghiou, A, Fraser, R, Gandhi, S, Prentice, A, Inskip, H, Godfrey, K, Schoenmakers, I, Javaid, MK, Eastell, R, Cooper, C, Harvey, N, Watt, ER, Howden, A, Mirchandani, A, Hukelmann, JL, Sadiku, P, Plant, TM, Cantrell, DA, Whyte, MKB, Walmsley, SR, Mordi, I, Forteath, C, Wong, A, Mohan, M, Palmer, C, Doney, A, Rena, G, Lang, C, Gray, EH, Azarian, S, Riva, A, Edwards, H, McPhail, MJW, Williams, R, Chokshi, S, Patel, VC, Edwards, LA, Page, D, Miossec, M, Williams, S, Monaghan, R, Fotiou, E, Santibanez-Koref, M, Badat, M, Mettananda, S, Hua, P, Schwessinger, R, Hughes, J, Higgs, D, Davies, J, Cacciottolo, TM, Perikari, A, van der Klaauw, A, Henning, E, Stadler, LKJ, Keogh, J, Farooqi, IS, Tenin, G, Keavney, B, Ryan, E, Budd, R, Bewley, M, Coelho, P, Rumsey, W, Sanchez, Y, McCafferty, J, Dockrell, D, Walmsley, S, Whyte, M, Liu, Y, Choy, M-K, Abraham, S, Black, G, Ford, T, Stanley, B, Good, R, Rocchiccioli, P, McEntegart, M, Watkins, S, Eteiba, H, Shaukat, A, Lindsay, M, Robertson, K, Hood, S, McGeoch, R, McDade, R, Sidik, N, McCartney, P, Corcoran, D, Collison, D, Rush, C, McConnachie, A, Touyz, R, Oldroyd, K, Berry, Colin, Gazdagh, G, Diver, L, Marshall, J, McGowan, R, Ahmed, F, Tobias, E, Curtis, E, Parsons, C, Maslin, K, D’Angelo, S, Moon, R, Crozier, S, Gossiel, F, Bishop, N, Kennedy, S, Papageorghiou, A, Fraser, R, Gandhi, S, Prentice, A, Inskip, H, Godfrey, K, Schoenmakers, I, Javaid, MK, Eastell, R, Cooper, C, Harvey, N, Watt, ER, Howden, A, Mirchandani, A, Hukelmann, JL, Sadiku, P, Plant, TM, Cantrell, DA, Whyte, MKB, Walmsley, SR, Mordi, I, Forteath, C, Wong, A, Mohan, M, Palmer, C, Doney, A, Rena, G, Lang, C, Gray, EH, Azarian, S, Riva, A, Edwards, H, McPhail, MJW, Williams, R, Chokshi, S, Patel, VC, Edwards, LA, Page, D, Miossec, M, Williams, S, Monaghan, R, Fotiou, E, Santibanez-Koref, M, Badat, M, Mettananda, S, Hua, P, Schwessinger, R, Hughes, J, Higgs, D, and Davies, J

Published
2019

4. Loss of transient receptor potential channel 5 causes obesity and postpartum depression.

Author

Li Y, Cacciottolo TM, Yin N, He Y, Liu H, Liu H, Yang Y, Henning E, Keogh JM, Lawler K, Mendes de Oliveira E, Gardner EJ, Kentistou KA, Laouris P, Bounds R, Ong KK, Perry JRB, Barroso I, Tu L, Bean JC, Yu M, Conde KM, Wang M, Ginnard O, Fang X, Tong L, Han J, Darwich T, Williams KW, Yang Y, Wang C, Joss S, Firth HV, Xu Y, and Farooqi IS

Subjects
Animals, Female, Mice, Male, Humans, Paraventricular Hypothalamic Nucleus metabolism, Mice, Inbred C57BL, Oxytocin metabolism, Maternal Behavior, Obesity metabolism, Obesity genetics, TRPC Cation Channels metabolism, TRPC Cation Channels genetics, Depression, Postpartum metabolism, Neurons metabolism
Abstract

Hypothalamic neural circuits regulate instinctive behaviors such as food seeking, the fight/flight response, socialization, and maternal care. Here, we identified microdeletions on chromosome Xq23 disrupting the brain-expressed transient receptor potential (TRP) channel 5 (TRPC5). This family of channels detects sensory stimuli and converts them into electrical signals interpretable by the brain. Male TRPC5 deletion carriers exhibited food seeking, obesity, anxiety, and autism, which were recapitulated in knockin male mice harboring a human loss-of-function TRPC5 mutation. Women carrying TRPC5 deletions had severe postpartum depression. As mothers, female knockin mice exhibited anhedonia and depression-like behavior with impaired care of offspring. Deletion of Trpc5 from oxytocin neurons in the hypothalamic paraventricular nucleus caused obesity in both sexes and postpartum depressive behavior in females, while Trpc5 overexpression in oxytocin neurons in knock-in mice reversed these phenotypes. We demonstrate that TRPC5 plays a pivotal role in mediating innate human behaviors fundamental to survival, including food seeking and maternal care., Competing Interests: Declaration of interests I.S.F. has consulted for a number of companies developing weight loss drugs (including Eli Lilly, Novo Nordisk, and Rhythm Pharmaceuticals) and investors (Goldman Sachs, SV Health). I.S.F. is a member of the Advisory Board of Cell. J.R.B.P. is an employee and shareholder of Insmed, receives research funding from GSK, and is a paid consultant for WW International. K.W.W. holds shares in Novo Nordisk and Eli Lilly., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2024
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5. Spleen Size Does Not Correlate With Histological Stage of Liver Disease in People With Nonalcoholic Fatty Liver Disease.

Author

Cacciottolo TM, Kumar A, Godfrey EM, Davies SE, and Allison M

Subjects
Humans, Spleen pathology, Splenomegaly etiology, Liver pathology, Liver Cirrhosis pathology, Non-alcoholic Fatty Liver Disease pathology, Hypertension, Portal complications
Abstract

Splenomegaly in the context of liver disease is classically associated with advanced cirrhosis and portal hypertension. 1 More recently, we observed an increasing number of patients with splenomegaly and nonalcoholic fatty liver disease (NAFLD), but in whom intensive work-up revealed no evidence of advanced liver disease or portal hypertension. In this study, we found no correlation between spleen size and histological stage of NAFLD, and a strong correlation between body weight, height and serum high density lipoprotein (HDL) levels., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2023
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6. Quality standards for the management of non-alcoholic fatty liver disease (NAFLD): consensus recommendations from the British Association for the Study of the Liver and British Society of Gastroenterology NAFLD Special Interest Group.

Author

McPherson S, Armstrong MJ, Cobbold JF, Corless L, Anstee QM, Aspinall RJ, Barclay ST, Brennan PN, Cacciottolo TM, Goldin RD, Hallsworth K, Hebditch V, Jack K, Jarvis H, Johnson J, Li W, Mansour D, McCallum M, Mukhopadhya A, Parker R, Ross V, Rowe IA, Srivastava A, Thiagarajan P, Thompson AI, Tomlinson J, Tsochatzis EA, Yeoman A, and Alazawi W

Subjects
Consensus, Delphi Technique, Humans, Societies, Medical, United Kingdom, Disease Management, Non-alcoholic Fatty Liver Disease diagnosis, Non-alcoholic Fatty Liver Disease therapy, Quality Indicators, Health Care standards
Abstract

Non-alcoholic fatty liver disease (NAFLD) is common, affecting approximately 25% of the general population. The evidence base for the investigation and management of NAFLD is large and growing, but there is currently little practical guidance to support development of services and delivery of care. To address this, we produced a series of evidence-based quality standard recommendations for the management of NAFLD, with the aim of improving patient care. A multidisciplinary group of experts from the British Association for the Study of the Liver and British Society of Gastroenterology NAFLD Special Interest Group produced the recommendations, which cover: management of people with, or at risk of, NAFLD before the gastroenterology or liver clinic; assessment and investigations in secondary care; and management in secondary care. The quality of evidence for each recommendation was evaluated by the Grading of Recommendation Assessment, Development and Evaluation tool. An anonymous modified Delphi voting process was conducted individually by each member of the group to assess the level of agreement with each statement. Statements were included when agreement was 80% or greater. From the final list of statements, a smaller number of auditable key performance indicators were selected to allow services to benchmark their practice. It is hoped that services will review their practice against our recommendations and key performance indicators and institute service development where needed to improve the care of patients with NAFLD., Competing Interests: Declaration of interests SM personal fees outside the submitted work from Gilead, Intercept, and Novo Nordisk. MJA has received fees for consultancy, advisory boards, and speaking from Novo Nordisk and Norgine. JFC has received fees for consultancy, advisory boards, and speaking from Intercept, Novo Nordisk, canNASH, and AstraZeneca. EAT has received fees for advisory boards and speaking from Falk Pharma, Intercept, Gilead, and Pfizer. AS has received fees for consultancy and speaking from Siemens. STB has received payment for advisory boards and speaking from AbbVie, Gilead, and Intercept. RJA has received honoraria for speaking and advisory board membership from Falk Pharma, Gilead, Intercept, Novartis, and Norgine. DM has received fees for consultancy from Intercept. PNB has received speaking and educational fees from Takeda. RP has received speaking fees and advisory board fees from Siemens, Norgine, Novo Nordisk, and Shionogi. AY has taken part in advisory boards and consultancy for Intercept and Novo Nordisk. HJ has received speaker fees from Intercept. WA has received fees for consultancy and lecturing from AstraZeneca, Janssen, Novo Nordisk, Gilead Science, Intercept, and Coherus and has received competitive grant funding from GSK and Gilead Science. LC has received personal fees outside the submitted work from Norgine, Intercept, and Novo Nordisk. JT has received personal fees outside the submitted work from Novartis and Poxel. QMA is coordinator of the IMI2 LITMUS consortium, which is funded by the EU Horizon 2020 programme and EFPIA. He reports research grant funding from Allergan/Tobira, AstraZeneca, GlaxoSmithKline, Glympse Bio, Novartis Pharma AG, Pfizer Ltd, and Vertex, consultancy on behalf of Newcastle University for 89Bio, Allergan/Tobira, Altimmune, AstraZeneca, Axcella, Blade, BMS, BNN Cardio, Cirius, CymaBay, EcoR1, E3Bio, Eli Lilly & Company, Galmed, Genentech, Genfit, Gilead, Grunthal, HistoIndex, Indalo, Intercept, Inventiva, IQVIA, Janssen, Madrigal, MedImmune, Medpace, Metacrine, NGMBio, North Sea Therapeutics, Novartis, Novo Nordisk A/S, PathAI, Pfizer Ltd, Poxel, ProSciento, Raptor Pharma, Roche, Servier, Terns, The Medicines Company, and Viking Therapeutics, and speaker fees from Abbott Laboratories, Allergan/Tobira, BMS, Clinical Care Options, Falk, Fishawack, Genfit SA, Gilead, Integritas Communications, Kenes, and MedScape. All other authors declared no competing interests., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published
2022
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7. Obesity Due to Steroid Receptor Coactivator-1 Deficiency Is Associated With Endocrine and Metabolic Abnormalities.

Author

Cacciottolo TM, Henning E, Keogh JM, Bel Lassen P, Lawler K, Bounds R, Ahmed R, Perdikari A, Mendes de Oliveira E, Smith M, Godfrey EM, Johnson E, Hodson L, Clément K, van der Klaauw AA, and Farooqi IS

Subjects
Female, Fibrosis, Humans, Male, Nuclear Receptor Coactivator 1 genetics, Obesity, Morbid complications, Obesity, Morbid genetics
Abstract

Context: Genetic variants affecting the nuclear hormone receptor coactivator steroid receptor coactivator, SRC-1, have been identified in people with severe obesity and impair melanocortin signaling in cells and mice. As a result, obese patients with SRC-1 deficiency are being treated with a melanocortin 4 receptor agonist in clinical trials., Objective: Here, our aim was to comprehensively describe and characterize the clinical phenotype of SRC-1 variant carriers to facilitate diagnosis and clinical management., Methods: In genetic studies of 2462 people with severe obesity, we identified 23 rare heterozygous variants in SRC-1. We studied 29 adults and 18 children who were SRC-1 variant carriers and performed measurements of metabolic and endocrine function, liver imaging, and adipose tissue biopsies. Findings in adult SRC-1 variant carriers were compared to 30 age- and body mass index (BMI)-matched controls., Results: The clinical spectrum of SRC-1 variant carriers included increased food intake in children, normal basal metabolic rate, multiple fractures with minimal trauma (40%), persistent diarrhea, partial thyroid hormone resistance, and menorrhagia. Compared to age-, sex-, and BMI-matched controls, adult SRC-1 variant carriers had more severe adipose tissue fibrosis (46.2% vs 7.1% respectively, P = .03) and a suggestion of increased liver fibrosis (5/13 cases vs 2/13 in controls, odds ratio = 3.4), although this was not statistically significant., Conclusion: SRC-1 variant carriers exhibit hyperphagia in childhood, severe obesity, and clinical features of partial hormone resistance. The presence of adipose tissue fibrosis and hepatic fibrosis in young patients suggests that close monitoring for the early development of obesity-associated metabolic complications is warranted., (© The Author(s) 2022. Published by Oxford University Press on behalf of the Endocrine Society.)

Published
2022
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10. An unusual cause of cholangiopathy.

Author

Aslam SP, Cacciottolo TM, Bowden D, Griffiths WJH, and Godfrey EM

Subjects
Cholangiopancreatography, Magnetic Resonance, Endosonography, Female, Humans, Substance-Related Disorders complications, Young Adult, Anesthetics, Dissociative adverse effects, Bile Duct Diseases chemically induced, Bile Duct Diseases diagnostic imaging, Ketamine adverse effects
Published
2019
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11. Scientific Business Abstracts of the 113th Annual Meeting of the Association of Physicians of Great Britain and Ireland.

Author

Cacciottolo TM, Perikari A, van der Klaauw A, Henning E, Stadler LKJ, Keogh J, Farooqi IS, Tenin G, Keavney B, Ryan E, Budd R, Bewley M, Coelho P, Rumsey W, Sanchez Y, McCafferty J, Dockrell D, Walmsley S, Whyte M, Liu Y, Choy MK, Tenin G, Abraham S, Black G, Keavney B, Ford T, Stanley B, Good R, Rocchiccioli P, McEntegart M, Watkins S, Eteiba H, Shaukat A, Lindsay M, Robertson K, Hood S, McGeoch R, McDade R, Sidik N, McCartney P, Corcoran D, Collison D, Rush C, McConnachie A, Touyz R, Oldroyd K, Berry C, Gazdagh G, Diver L, Marshall J, McGowan R, Ahmed F, Tobias E, Curtis E, Parsons C, Maslin K, D'Angelo S, Moon R, Crozier S, Gossiel F, Bishop N, Kennedy S, Papageorghiou A, Fraser R, Gandhi S, Prentice A, Inskip H, Godfrey K, Schoenmakers I, Javaid MK, Eastell R, Cooper C, Harvey N, Watt ER, Howden A, Mirchandani A, Coelho P, Hukelmann JL, Sadiku P, Plant TM, Cantrell DA, Whyte MKB, Walmsley SR, Mordi I, Forteath C, Wong A, Mohan M, Palmer C, Doney A, Rena G, Lang C, Gray EH, Azarian S, Riva A, Edwards H, McPhail MJW, Williams R, Chokshi S, Patel VC, Edwards LA, Page D, Miossec M, Williams S, Monaghan R, Fotiou E, Santibanez-Koref M, Keavney B, Badat M, Mettananda S, Hua P, Schwessinger R, Hughes J, Higgs D, and Davies J

Published
2019
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12. Steroid receptor coactivator-1 modulates the function of Pomc neurons and energy homeostasis.

Author

Yang Y, van der Klaauw AA, Zhu L, Cacciottolo TM, He Y, Stadler LKJ, Wang C, Xu P, Saito K, Hinton A Jr, Yan X, Keogh JM, Henning E, Banton MC, Hendricks AE, Bochukova EG, Mistry V, Lawler KL, Liao L, Xu J, O'Rahilly S, Tong Q, Inês Barroso, O'Malley BW, Farooqi IS, and Xu Y

Subjects
Alleles, Animals, Body Weight, Cell Line, Tumor, Crosses, Genetic, Gene Deletion, Gene Knock-In Techniques, Genetic Variation, HEK293 Cells, Heterozygote, Homeostasis, Humans, Leptin metabolism, Male, Membrane Potentials, Mice, Mice, Transgenic, Mutation, Missense, Obesity metabolism, Phenotype, Hypothalamus metabolism, Neurons metabolism, Nuclear Receptor Coactivator 1 genetics, Nuclear Receptor Coactivator 1 metabolism, Obesity genetics
Abstract

Hypothalamic neurons expressing the anorectic peptide Pro-opiomelanocortin (Pomc) regulate food intake and body weight. Here, we show that Steroid Receptor Coactivator-1 (SRC-1) interacts with a target of leptin receptor activation, phosphorylated STAT3, to potentiate Pomc transcription. Deletion of SRC-1 in Pomc neurons in mice attenuates their depolarization by leptin, decreases Pomc expression and increases food intake leading to high-fat diet-induced obesity. In humans, fifteen rare heterozygous variants in SRC-1 found in severely obese individuals impair leptin-mediated Pomc reporter activity in cells, whilst four variants found in non-obese controls do not. In a knock-in mouse model of a loss of function human variant (SRC-1 L1376P ), leptin-induced depolarization of Pomc neurons and Pomc expression are significantly reduced, and food intake and body weight are increased. In summary, we demonstrate that SRC-1 modulates the function of hypothalamic Pomc neurons, and suggest that targeting SRC-1 may represent a useful therapeutic strategy for weight loss.

Published
2019
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14. Pi*Z heterozygous alpha-1 antitrypsin states accelerate parenchymal but not biliary cirrhosis.

Author

Cacciottolo TM, Gelson WT, Maguire G, Davies SE, and Griffiths WJ

Subjects
Biopsy, Disease Progression, England epidemiology, Fatty Liver diagnosis, Fatty Liver enzymology, Fatty Liver epidemiology, Gene Frequency, Genetic Predisposition to Disease, Genetic Testing, Humans, Liver pathology, Liver Cirrhosis diagnosis, Liver Cirrhosis enzymology, Liver Cirrhosis epidemiology, Liver Cirrhosis, Alcoholic enzymology, Liver Cirrhosis, Alcoholic epidemiology, Liver Cirrhosis, Alcoholic genetics, Liver Cirrhosis, Biliary diagnosis, Liver Cirrhosis, Biliary enzymology, Liver Cirrhosis, Biliary epidemiology, Non-alcoholic Fatty Liver Disease, Phenotype, Predictive Value of Tests, Prevalence, Protein Folding, Retrospective Studies, Risk Factors, Time Factors, alpha 1-Antitrypsin chemistry, alpha 1-Antitrypsin metabolism, Fatty Liver genetics, Heterozygote, Liver enzymology, Liver Cirrhosis genetics, Liver Cirrhosis, Biliary genetics, alpha 1-Antitrypsin genetics
Abstract

Objective: The degree to which heterozygous forms of alpha-1 antitrypsin (A1AT), principally MZ, causes liver disease is uncertain. If heterozygosity is a relevant cofactor, over-representation in patients with end-stage liver disease would be predicted. We therefore assessed the prevalence and disease-related distribution of A1AT heterozygosity in the largest cohort to date for this purpose., Methods: We retrospectively analysed 1036 patients assessed for liver transplantation at our unit between 2003 and 2010. A1AT heterozygotes were identified on the basis of isoelectric focusing and/or histology, showing A1AT globule deposition consistent with an abnormal phenotype., Results: Z-allele frequency was the highest in patients with nonalcoholic steatohepatitis (NASH) cirrhosis (20.3%), followed by patients with 'other parenchymal' diseases (11.9%), alcohol-related liver disease (9.9%), autoimmune disease (8.6%), hepatitis C (6.1%), hepatitis B (3.0%) and biliary disease (1.9%). Compared with the heterozygote frequency in the general European population of 9.0%, the heterozygote frequency was significantly higher among patients with NASH cirrhosis (P≤0.0001) and lower in the biliary subgroup (P=0.004). The prevalence of MZ heterozygosity was significantly increased in cirrhosis because of both alcohol (9.9%) and NASH (17.3%) compared with the general European population (2.8%; P<0.0001)., Conclusion: Accumulation of misfolded A1AT aggregates appears to accelerate progression, in which the hepatocyte is the key injured cell. Heterozygous A1AT states worsen prognosis, particularly in NASH and alcohol-related cirrhosis, and should be identified at presentation. In cases in which genetic screening is not readily available, a low threshold for isoelectric focusing and routine specific histochemical staining of liver biopsy specimens are warranted to identify these patients.

Published
2014
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