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1. Prevalence of atherosclerosis in individuals with prediabetes and diabetes compared to normoglycaemic individuals—a Swedish population-based study

Author

Östgren, Carl Johan, Otten, Julia, Festin, Karin, Angerås, Oskar, Bergström, Göran, Cederlund, Kerstin, Engström, Gunnar, Eriksson, Maria J., Eriksson, Mats, Fall, Tove, Gummesson, Anders, Hagström, Emil, Hellman, Urban, James, Stefan K., Jernberg, Tomas, Kihlberg, Johan, Kylhammar, David, Markstad, Hanna, Nilsson, Peter, Persson, Anders, Persson, Margaretha, Pirazzi, Carlo, Renklint, Rebecka, Rosengren, Annika, Söderberg, Stefan, and Sundström, Johan

Published
2023
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3. Myeloperoxidase Inhibition in Heart Failure With Preserved or Mildly Reduced Ejection Fraction:SATELLITE Trial Results

Author

Lam, Carolyn S.P., Lund, Lars H., Shah, Sanjiv J., Voors, Adriaan A., Erlinge, David, Saraste, Antti, Pirazzi, Carlo, Grove, Erik L., Barasa, Anders, Schou, Morten, Aziz, Ahmed, Svedlund, Sara, Wijngaarden, Jan Van, Lindstedt, Eva-Lotte, Gustavsson, Andreas, Nelander, Karin, Garkaviy, Pavlo, Gan, Li-Ming, Gabrielsen, Anders, Lam, Carolyn S.P., Lund, Lars H., Shah, Sanjiv J., Voors, Adriaan A., Erlinge, David, Saraste, Antti, Pirazzi, Carlo, Grove, Erik L., Barasa, Anders, Schou, Morten, Aziz, Ahmed, Svedlund, Sara, Wijngaarden, Jan Van, Lindstedt, Eva-Lotte, Gustavsson, Andreas, Nelander, Karin, Garkaviy, Pavlo, Gan, Li-Ming, and Gabrielsen, Anders

Abstract

Background Inflammation is a key driver of heart failure with preserved left ventricular ejection fraction. AZD4831 inhibits extracellular myeloperoxidase, decreases inflammation, and improves microvascular function in preclinical disease models. Methods and Results In this double-blind phase 2a study (Safety and Tolerability Study of AZD4831 in Patients With Heart Failure [SATELLITE]; NCT03756285), patients with symptomatic heart failure, left ventricular ejection fraction of ≥40%, and elevated B-type natriuretic peptides were randomized 2:1 to once-daily oral AZD4831 5 mg or placebo for 90 days. We aimed to assess target engagement (primary end point: myeloperoxidase specific activity) and safety of AZD4831. Owing to coronavirus disease 2019, the study was terminated early after randomizing 41 patients (median age 74.0 years, 53.7% male). Myeloperoxidase activity was decreased by more than 50% from baseline to day 30 and day 90 in the AZD4831 group, with a placebo-adjusted decreased of 75% (95% confidence interval, 48, 88, nominal P < .001). No improvements were noted in secondary or exploratory end points, apart from a trend in Kansas City Cardiomyopathy Questionnaire overall summary score. No deaths or treatment-related serious adverse events occurred. AZD4831 treatment-related adverse events were generalized maculopapular rash, pruritus, and diarrhea (all n = 1). Conclusions AZD4831 inhibited myeloperoxidase and was well tolerated in patients with heart failure and left ventricular ejection fraction of 40% or greater. Efficacy findings were exploratory owing to early termination, but warrant further clinical investigation of AZD4831. Lay Summary Few treatments are available for patients with the forms of heart failure known as heart failure with preserved or mildly reduced ejection fraction. Current treatments do not target inflammation, which may play an important role in this condition. We tested a new drug called, Background: Inflammation is a key driver of heart failure with preserved left ventricular ejection fraction. AZD4831 inhibits extracellular myeloperoxidase, decreases inflammation, and improves microvascular function in preclinical disease models. Methods and Results: In this double-blind phase 2a study (Safety and Tolerability Study of AZD4831 in Patients With Heart Failure [SATELLITE]; NCT03756285), patients with symptomatic heart failure, left ventricular ejection fraction of ≥40%, and elevated B-type natriuretic peptides were randomized 2:1 to once-daily oral AZD4831 5 mg or placebo for 90 days. We aimed to assess target engagement (primary end point: myeloperoxidase specific activity) and safety of AZD4831. Owing to coronavirus disease 2019, the study was terminated early after randomizing 41 patients (median age 74.0 years, 53.7% male). Myeloperoxidase activity was decreased by more than 50% from baseline to day 30 and day 90 in the AZD4831 group, with a placebo-adjusted decreased of 75% (95% confidence interval, 48, 88, nominal P <.001). No improvements were noted in secondary or exploratory end points, apart from a trend in Kansas City Cardiomyopathy Questionnaire overall summary score. No deaths or treatment-related serious adverse events occurred. AZD4831 treatment-related adverse events were generalized maculopapular rash, pruritus, and diarrhea (all n = 1). Conclusions: AZD4831 inhibited myeloperoxidase and was well tolerated in patients with heart failure and left ventricular ejection fraction of 40% or greater. Efficacy findings were exploratory owing to early termination, but warrant further clinical investigation of AZD4831. Lay Summary: Few treatments are available for patients with the forms of heart failure known as heart failure with preserved or mildly reduced ejection fraction. Current treatments do not target inflammation, which may play an important role in this condition. We tested a new drug called AZD4831 (mitiperstat), which decreas

Published
2024

5. PNPLA3 has retinyl-palmitate lipase activity in human hepatic stellate cells

Author

Pirazzi, Carlo, Valenti, Luca, Motta, Benedetta Maria, Pingitore, Piero, Hedfalk, Kristina, Mancina, Rosellina Margherita, Burza, Maria Antonella, Indiveri, Cesare, Ferro, Yvelise, Montalcini, Tiziana, Maglio, Cristina, Dongiovanni, Paola, Fargion, Silvia, Rametta, Raffaela, Pujia, Arturo, Andersson, Linda, Ghosal, Saswati, Levin, Malin, Wiklund, Olov, Iacovino, Michelina, Borén, Jan, and Romeo, Stefano

Subjects
Biochemistry and Cell Biology, Biological Sciences, Liver Disease, Digestive Diseases, Rare Diseases, Chronic Liver Disease and Cirrhosis, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Oral and gastrointestinal, Adult, Diterpenes, Female, Gene Expression Regulation, Hep G2 Cells, Hepatic Stellate Cells, Humans, Insulin, Lipase, Lipid Droplets, Male, Membrane Proteins, Middle Aged, Mutation, Non-alcoholic Fatty Liver Disease, Palmitic Acid, Primary Cell Culture, Retinol-Binding Proteins, Plasma, Retinyl Esters, Vitamin A, Medical and Health Sciences, Genetics & Heredity, Genetics
Abstract

Retinoids are micronutrients that are stored as retinyl esters in the retina and hepatic stellate cells (HSCs). HSCs are key players in fibrogenesis in chronic liver diseases. The enzyme responsible for hydrolysis and release of retinyl esters from HSCs is unknown and the relationship between retinoid metabolism and liver disease remains unclear. We hypothesize that the patatin-like phospholipase domain-containing 3 (PNPLA3) protein is involved in retinol metabolism in HSCs. We tested our hypothesis both in primary human HSCs and in a human cohort of subjects with non-alcoholic fatty liver disease (N = 146). Here we show that PNPLA3 is highly expressed in human HSCs. Its expression is regulated by retinol availability and insulin, and increased PNPLA3 expression results in reduced lipid droplet content. PNPLA3 promotes extracellular release of retinol from HSCs in response to insulin. We also show that purified wild-type PNPLA3 hydrolyzes retinyl palmitate into retinol and palmitic acid. Conversely, this enzymatic activity is markedly reduced with purified PNPLA3 148M, a common mutation robustly associated with liver fibrosis and hepatocellular carcinoma development. We also find the PNPLA3 I148M genotype to be an independent (P = 0.009 in a multivariate analysis) determinant of circulating retinol-binding protein 4, a reliable proxy for retinol levels in humans. This study identifies PNPLA3 as a lipase responsible for retinyl-palmitate hydrolysis in HSCs in humans. Importantly, this indicates a potential novel link between HSCs, retinoid metabolism and PNPLA3 in determining the susceptibility to chronic liver disease.

Published
2014

6. Myeloperoxidase Inhibition in Heart Failure With Preserved or Mildly Reduced Ejection Fraction: SATELLITE Trial Results

Author

Lam, Carolyn S P, Lund, Lars H, Shah, Sanjiv J, Voors, Adriaan A, Erlinge, David, Saraste, Antti, Pirazzi, Carlo, Grove, Erik L, Barasa, Anders, Schou, Morten, Aziz, Ahmed, Svedlund, Sara, Wijngaarden, Jan VAN, Lindstedt, Eva-Lotte, Gustavsson, Andreas, Nelander, Karin, Garkaviy, Pavlo, Gan, Li-Ming, and Gabrielsen, Anders

Subjects
Cardiology and Cardiovascular Medicine
Abstract

BACKGROUND: Inflammation is a key driver of heart failure (HF) with preserved left ventricular ejection fraction (LVEF). AZD4831 inhibits extracellular myeloperoxidase, reduces inflammation and improves microvascular function in preclinical disease models.METHODS: In this double-blind phase 2a study (SATELLITE; NCT03756285), patients with symptomatic HF, LVEF ≥40%, and elevated B-type natriuretic peptides were randomized 2:1 to once-daily oral AZD4831 5 mg or placebo for 90 days. We aimed to assess target engagement (primary endpoint: myeloperoxidase specific activity) and safety of AZD4831.RESULTS: Due to COVID-19, the study was terminated early after randomizing 41 patients (median age, 74.0 years; 53.7% male). Myeloperoxidase activity was reduced by >50% from baseline to day 30 and 90 in the AZD4831 group, with a placebo-adjusted reduction of 75% (95% confidence interval: 48, 88; nominal P CONCLUSIONS: AZD4831 inhibited myeloperoxidase and was well tolerated in patients with HF and LVEF ≥40%. Efficacy findings were exploratory due to early termination but warrant further clinical investigation of AZD4831.LAY SUMMARY: Few treatments are available for patients with the forms of heart failure known as 'heart failure with preserved or mildly reduced ejection fraction'. Current treatments do not target inflammation, which may play an important role in this condition. We tested a new drug called AZD4831 (mitiperstat), which reduces inflammation by inhibiting the enzyme myeloperoxidase. Among the 41 patients in our clinical trial, AZD4831 had a good safety profile and inhibited myeloperoxidase by the expected amount. Results mean we can conduct further trials to see whether AZD4831 reduces the symptoms of heart failure and improves patients' ability to take physical exercise.

Published
2023
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8. Additional file 1 of Effects of Bilberry and Oat intake on lipids, inflammation and exercise capacity after Acute Myocardial Infarction (BIOAMI): study protocol for a randomized, double-blind, placebo-controlled trial

Author

Bergh, Cecilia, Landberg, Rikard, Andersson, Kristina, Heyman-Lindén, Lovisa, Rascón, Ana, Magnuson, Anders, Khalili, Payam, Kåregren, Amra, Nilsson, Johan, Pirazzi, Carlo, Erlinge, David, and Fröbert, Ole

Abstract

Additional file 1. Trial Registration Data Set according to WHO.

Published
2021
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11. High prevalence of genetic determined familial hypercholesterolemia in premature coronary artery disease

Author

Pirazzi,Carlo, HÃ¥kansson,Lina, Gustafsson,Carola, Omerovic,Elmir, Wiklund,Olov, and Mancina,Rosellina M.

Subjects
The Application of Clinical Genetics
Abstract

Carlo Pirazzi,1 Lina Håkansson,1 Carola Gustafsson,1 Elmir Omerovic,1,2 Olov Wiklund,2 Rosellina Margherita Mancina21Department of Cardiology, Sahlgrenska University Hospital, Gothenburg, Sweden; 2Department of Molecular and Clinical Medicine, Institute of Medicine, Sahlgrenska Academy, Wallenberg Laboratory, University of Gothenburg, Gothenburg, SwedenBackground: Premature coronary artery disease (CAD) is a major cause of mortality and morbidity. Increased low-density lipoprotein-cholesterol (LDL-C) level is a major risk factor for CAD and thus the main target for its prevention. Familial Hypercholesterolemia (FH) is a genetic inherited disorder characterized by high LDL-C, and subsequent premature CAD development. Early drug treatment with lipid-lowering medications in FH prevents cardiovascular disease onset. The FH prevalence in the Northern European general population is 0.3%, and it is estimated that it explains 20% of premature CAD cases in individuals with familial clustering. Despite the wide number of papers showing the prevalence of clinical FH in cardiovascular disease, the prevalence of genetic FH in individuals with premature CAD is not yet well known. Here, we examined the prevalence of genetically determined FH in individuals with premature CAD.Patients and methods: 66 patients who underwent coronary angiography with suspected premature acute coronary syndrome (age

Published
2019

12. PNPLA 3 I148M genetic variant associates with insulin resistance and baseline viral load in HCV genotype 2 but not in genotype 3 infection

Author

Rembeck Karolina, Maglio Cristina, Lagging Martin, Christensen Peer, Färkkilä Martti, Langeland Nina, Buhl Mads, Pedersen Court, Mørch Kristine, Norkrans Gunnar, Hellstrand Kristoffer, Lindh Magnus, Pirazzi Carlo, Burza Maria, Romeo Stefano, and Westin Johan

Subjects
Hepatitis C, PNPLA 3, Insulin resistance, Viral load, Internal medicine, RC31-1245, Genetics, QH426-470
Abstract

Abstract Background Hepatic steatosis in HCV patients has been postulated as a risk factor associated with a higher frequency of fibrosis and cirrhosis. A single genetic variant, PNPLA3 I148M, has been widely associated with increased hepatic steatosis. Previous studies of the PNPLA3 I148M sequence variant in HCV infected individuals have reported an association between this variant and prevalence of steatosis, fibrosis, and cirrhosis. To evaluate the impact of PNPLA3 I148M variant on metabolic traits and treatment response in HCV genotype 2 and 3 infected patients. Methods Three hundred and eighty-two treatment naïve HCV genotype 2 or 3 infected patients were included in a phase III, open label, randomized, multicenter, investigator-initiated trial (the NORDynamIC study), in which pretreatment liver biopsies were mandatory. PNPLA3I148M genotyping was performed in a total of 359 Caucasian patients. Results In HCV genotype 2 infected patients carrying the PNPLA3 148M allele, there was significantly increased insulin resistance (P = 0.023) and lower viral load (P = 0.005) at baseline as well as the first seven days of antiviral treatment. These results were not observed in HCV genotype 3 infected patients. Conclusions Our results suggest a possible association between the PNPLA3 148M allele and insulin resistance as well as baseline viral load in HCV genotype 2, but not in genotype 3.

Published
2012
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14. Molecular genetics of patatin-like phospholipase domain-containing 3 and chronic liver disease

Author

pirazzi, carlo

Subjects
NAFLD, hepatic stellate cells, VLDL, PNPLA3, retinol
Abstract

Chronic liver disease is a major health burden worldwide. Major determinants of this condition are viral infections, alcohol abuse and obesity. Genetic background modulates the effect of damaging agents on the liver. The genetic variant rs738409 in the patatin-like phospholipase domain-containing 3 (PNPLA3) gene associates with increased susceptibility to the entire spectrum of chronic liver disease, and in particular with non-alcoholic fatty liver disease. The variant results in an isoleucine to methionine substitution at position 148 (I148M) of the amino acidic sequence and was first associated with increased hepatocyte fat content. Despite the strength of the genetic association, the mechanisms causing liver fat accumulation and hepatocyte damage are not yet understood. In this thesis, we tested the following hypotheses: 1) PNPLA3 is involved in hepatic very low density lipoprotein secretion 2) the protein acts as a glycerolipid hydrolase and the 148M mutation is a loss of function 3) PNPLA3 has a specific role in retinol metabolism in hepatic stellate cells. We tested the first hypothesis measuring VLDL secretion in a cohort of 55 individuals genotyped for the I148M variant and we found that carriers of the 148M allele secret less VLDL for a given amount of liver fat. We confirmed this result in vitro by measuring APOB secretion in cell lines stably overexpressing the 148I or the 148M PNPLA3. We tested the second hypothesis performing enzymatic activity assays using purified 148I and 148M recombinant proteins. The wild type protein had glycerolipid hydrolase activity and the 148M mutation induced a loss of function. Finally, we tested the third hypothesis assessing the effect of PNPLA3 up- and down-regulation on hepatic stellate cell retinyl palmitate content and retinol release. We found that PNPLA3 insulin–mediated up-regulation induces retinol release from hepatic stellate cells and that this effect is abolished by PNPLA3 silencing. We confirmed this finding by looking at human circulating levels of RBP4, a reliable marker of retinol plasma levels, in 146 individuals genotyped for the I148M variant. We found carriers of the M allele to have lower RBP4 plasma levels, confirming the role of PNPLA3 in retinol metabolism. In conclusion, we identified two possible mechanisms underlying the susceptibility to chronic liver disease in carriers of the PNPLA3 mutation: 1) reduced intracellular triglyceride mobilization leading to hepatocyte damage 2) impaired hepatic stellate cell retinol metabolism causing abnormal response of hepatocytes to damaging agents.

Published
2014

15. The androgen receptor confers protection against diet-induced atherosclerosis, obesity, and dyslipidemia in female mice

Author

Fagman, Johan B., Wilhelmson, Anna S., Motta, Benedetta M., Pirazzi, Carlo, Alexanderson, Camilla, De Gendt, Karel, Verhoeven, Guido, Holmäng, Agneta, Anesten, Fredrik, Jansson, John-Olov, Levin, Malin, Borén, Jan, Ohlsson, Claes, Krettek, Alexandra, Romeo, Stefano, Tivesten, Åsa, Fagman, Johan B., Wilhelmson, Anna S., Motta, Benedetta M., Pirazzi, Carlo, Alexanderson, Camilla, De Gendt, Karel, Verhoeven, Guido, Holmäng, Agneta, Anesten, Fredrik, Jansson, John-Olov, Levin, Malin, Borén, Jan, Ohlsson, Claes, Krettek, Alexandra, Romeo, Stefano, and Tivesten, Åsa

Abstract

Androgens have important cardiometabolic actions in males, but their metabolic role in females is unclear. To determine the physiologic androgen receptor (AR)-dependent actions of androgens on atherogenesis in female mice, we generated female AR-knockout (ARKO) mice on an atherosclerosis-prone apolipoprotein E (apoE)-deficient background. After 8 weeks on a high-fat diet, but not on a normal chow diet, atherosclerosis in aorta was increased in ARKO females (+59% vs. control apoE-deficient mice with intact AR gene). They also displayed increased body weight (+18%), body fat percentage (+62%), and hepatic triglyceride levels, reduced insulin sensitivity, and a marked atherogenic dyslipidemia (serum cholesterol, +52%). Differences in atherosclerosis, body weight, and lipid levels between ARKO and control mice were abolished in mice that were ovariectomized before puberty, consistent with a protective action of ovarian androgens mediated via the AR. Furthermore, the AR agonist dihydrotestosterone reduced atherosclerosis (-41%; thoracic aorta), subcutaneous fat mass (-44%), and cholesterol levels (-35%) in ovariectomized mice, reduced hepatocyte lipid accumulation in hepatoma cells in vitro, and regulated mRNA expression of hepatic genes pivotal for lipid homeostasis. In conclusion, we demonstrate that the AR protects against diet-induced atherosclerosis in female mice and propose that this is mediated by modulation of body composition and lipid metabolism.-Fagman, J. B., Wilhelmson, A. S., Motta, B. M., Pirazzi, C., Alexanderson, C., De Gendt, K., Verhoeven, G., Holmäng, A., Anesten, F., Jansson, J. -O., Levin, M., Borén, J., Ohlsson, C., Krettek, A., Romeo, S., Tivesten, A. The androgen receptor confers protection against diet-induced atherosclerosis, obesity, and dyslipidemia in female mice.

Published
2015
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17. The IRS1 rs2943641 Variant and Risk of Future Cancer Among Morbidly Obese Individuals.

Author

Maglio, Cristina, Ericson, Ulrika, Burza, Maria Antonella, Mancina, Rosellina Margherita, Pirazzi, Carlo, Assarsson, Johanna Andersson, Sjöholm, Kajsa, Baroni, Marco Giorgio, Svensson, Per-Arne, Montalcini, Tiziana, Pujia, Arturo, Sjöström, Lars, Wiklund, Olov, Carlsson, Lena, Borén, Jan, Orho-Melander, Marju, Romeo, Stefano, Maglio, Cristina, Ericson, Ulrika, Burza, Maria Antonella, Mancina, Rosellina Margherita, Pirazzi, Carlo, Assarsson, Johanna Andersson, Sjöholm, Kajsa, Baroni, Marco Giorgio, Svensson, Per-Arne, Montalcini, Tiziana, Pujia, Arturo, Sjöström, Lars, Wiklund, Olov, Carlsson, Lena, Borén, Jan, Orho-Melander, Marju, and Romeo, Stefano

Abstract

Context:Obesity and insulin resistance are risk factors for cancer development. The IRS1 rs2943641 genetic variant has been widely associated with insulin resistance.Objective:The aim of the study was to examine whether the IRS1 rs2943641 associates with cancer incidence in obese individuals.Design, Setting and Patients:The IRS1 rs2943641 was genotyped in participants from the Swedish Obese Subjects (SOS) study, an intervention trial on the effect of bariatric surgery on mortality and morbidity compared with usual care and in the population-based Malmö Diet and Cancer (MDC) cohort. In both studies, the median follow-up for cancer incidence was about 15 years.Intervention and Main Outcome Measure:Cancer incidence was assessed in both the SOS and the MDC cohorts through national and local registers.Results:The IRS1 T allele was associated with lower insulin resistance in both the SOS and the MDC studies. A lower cancer incidence was found in T allele carriers from the SOS control group (hazard ratio [HR] 0.77, 95% confidence interval [CI] 0.62-0.96; P = .021) and was restricted to morbidly obese individuals (HR 0.67, 95% CI 0.50-0.91; P = .011). No evidence of such association was detected in the surgery group (interaction P = .005). In the MDC cohort, a nonsignificant tendency for lower cancer incidence in T allele carriers was observed only in morbidly obese individuals. A meta-analysis of morbidly obese individuals (body mass index > 40 kg/m(2)) from the two cohorts strengthened the evidence for the association (HR 0.66, 95% CI 0.50-0.87; P = .004).Conclusions:Our results suggest that the T allele of rs2943641 near IRS1 may associate with lower cancer incidence in morbidly obese individuals.

Published
2013

18. Bariatric Surgery and Prevention of Type 2 Diabetes in Swedish Obese Subjects

Author

Carlsson, Lena M. S., Peltonen, Markku, Ahlin, Sofie, Anveden, Åsa, Bouchard, Claude, Carlsson, Björn, Jacobson, Peter, Lönroth, Hans, Maglio, Cristina, Näslund, Ingmar, Pirazzi, Carlo, Romeo, Stefano, Sjöholm, Kajsa, Sjöström, Elisabeth, Wedel, Hans, Svensson, Per-Arne, Sjöström, Lars, Carlsson, Lena M. S., Peltonen, Markku, Ahlin, Sofie, Anveden, Åsa, Bouchard, Claude, Carlsson, Björn, Jacobson, Peter, Lönroth, Hans, Maglio, Cristina, Näslund, Ingmar, Pirazzi, Carlo, Romeo, Stefano, Sjöholm, Kajsa, Sjöström, Elisabeth, Wedel, Hans, Svensson, Per-Arne, and Sjöström, Lars

Abstract

BACKGROUND: Weight loss protects against type 2 diabetes but is hard to maintain with behavioral modification alone. In an analysis of data from a nonrandomized, prospective, controlled study, we examined the effects of bariatric surgery on the prevention of type 2 diabetes. METHODS: In this analysis, we included 1658 patients who underwent bariatric surgery and 1771 obese matched controls (with matching performed on a group, rather than individual, level). None of the participants had diabetes at baseline. Patients in the bariatric-surgery cohort underwent banding (19%), vertical banded gastroplasty (69%), or gastric bypass (12%); nonrandomized, matched, prospective controls received usual care. Participants were 37 to 60 years of age, and the body-mass index (BMI; the weight in kilograms divided by the square of the height in meters) was 34 or more in men and 38 or more in women. This analysis focused on the rate of incident type 2 diabetes, which was a prespecified secondary end point in the main study. At the time of this analysis (January 1, 2012), participants had been followed for up to 15 years. Despite matching, some baseline characteristics differed significantly between the groups; the baseline body weight was higher and risk factors were more pronounced in the bariatric-surgery group than in the control group. At 15 years, 36.2% of the original participants had dropped out of the study, and 30.9% had not yet reached the time for their 15-year follow-up examination. RESULTS: During the follow-up period, type 2 diabetes developed in 392 participants in the control group and in 110 in the bariatric-surgery group, corresponding to incidence rates of 28.4 cases per 1000 person-years and 6.8 cases per 1000 person-years, respectively (adjusted hazard ratio with bariatric surgery, 0.17; 95% confidence interval, 0.13 to 0.21; P< 0.001). The effect of bariatric surgery was influenced by the presence or absence of impaired fasting glucose (P = 0.002 for the inte, Funding Agencies:AstraZeneca New York Obesity Nutrition Research Center Pathway Genomics Weight Watchers Nike Human Kinetics and Informa Healthcare Pfizer Roche Novartis Johnson Johnson Swedish federal government under the LUA/ALF VINNOVA-VINNMER program Wenner-Gren Foundations Hoffmann-La Roche Cederroth Sanofi-Aventis

Published
2012
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19. Paradoxical Lower Serum Triglyceride Levels and Higher Type 2 Diabetes Mellitus Susceptibility in Obese Individuals with the PNPLA3 148M Variant

Author

Palmer, Colin N. A., primary, Maglio, Cristina, additional, Pirazzi, Carlo, additional, Burza, Maria Antonella, additional, Adiels, Martin, additional, Burch, Lindsay, additional, Donnelly, Louise A., additional, Colhoun, Helen, additional, Doney, Alexander S., additional, Dillon, John F., additional, Pearson, Ewan R., additional, McCarthy, Mark, additional, Hattersley, Andrew T., additional, Frayling, Tim, additional, Morris, Andrew D., additional, Peltonen, Markku, additional, Svensson, Per-Arne, additional, Jacobson, Peter, additional, Borén, Jan, additional, Sjöström, Lars, additional, Carlsson, Lena M. S., additional, and Romeo, Stefano, additional

Published
2012
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20. Identification and characterization of two novel mutations in the LPL gene causing type I hyperlipoproteinemia

Author

Pingitore, Piero, Lepore, Saverio Massimo, Pirazzi, Carlo, Mancina, Rosellina Margherita, Motta, Benedetta Maria, Valenti, Luca, Berge, Knut Erik, Retterstøl, Kjetil, Leren, Trond P., Wiklund, Olov, and Romeo, Stefano

Subjects
Hypertriglyceridemia, Nutrition and Dietetics, Endocrinology, Diabetes and Metabolism, Hyperchylomicronemia, Internal Medicine, nutritional and metabolic diseases, lipids (amino acids, peptides, and proteins), Missense and frameshift mutations, Cardiology and Cardiovascular Medicine, Familial lipoprotein lipase deficiency (FLD), Type 1 hyperlipoproteinemia
Abstract

BackgroundType 1 hyperlipoproteinemia is a rare autosomal recessive disorder most often caused by mutations in the lipoprotein lipase (LPL) gene resulting in severe hypertriglyceridemia and pancreatitis.ObjectivesThe aim of this study was to identify novel mutations in the LPL gene causing type 1 hyperlipoproteinemia and to understand the molecular mechanisms underlying the severe hypertriglyceridemia.MethodsThree patients presenting classical features of type 1 hyperlipoproteinemia were recruited for DNA sequencing of the LPL gene. Pre-heparin and post-heparin plasma of patients were used for protein detection analysis and functional test. Furthermore, in vitro experiments were performed in HEK293 cells. Protein synthesis and secretion were analyzed in lysate and medium fraction, respectively, whereas medium fraction was used for functional assay.ResultsWe identified two novel mutations in the LPL gene causing type 1 hyperlipoproteinemia: a two base pair deletion (c.765_766delAG) resulting in a frameshift at position 256 of the protein (p.G256TfsX26) and a nucleotide substitution (c.1211 T > G) resulting in a methionine to arginine substitution (p.M404 R). LPL protein and activity were not detected in pre-heparin or post-heparin plasma of the patient with p.G256TfsX26 mutation or in the medium of HEK293 cells over-expressing recombinant p.G256TfsX26 LPL. A relatively small amount of LPL p.M404 R was detected in both pre-heparin and post-heparin plasma and in the medium of the cells, whereas no LPL activity was detected.ConclusionsWe conclude that these two novel mutations cause type 1 hyperlipoproteinemia by inducing a loss or reduction in LPL secretion accompanied by a loss of LPL enzymatic activity.

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21. End-to-end deep-learning model for the detection of coronary artery stenosis on coronary CT images.

Author

Gupta V, Petursson P, Rawshani A, Boren J, Ramunddal T, Bhatt DL, Omerovic E, Angerås O, Smith G, Sattar N, Andersson E, Redfors B, Hilgendorf L, Bergström G, Pirazzi C, Skoglund K, and Rawshani A

Subjects
Humans, Male, Female, Middle Aged, Aged, Severity of Illness Index, Predictive Value of Tests, Retrospective Studies, Reproducibility of Results, Radiographic Image Interpretation, Computer-Assisted methods, Deep Learning, Coronary Stenosis diagnostic imaging, Computed Tomography Angiography methods, Coronary Angiography methods, Coronary Vessels diagnostic imaging
Abstract

Purpose: We examined whether end-to-end deep-learning models could detect moderate (≥50%) or severe (≥70%) stenosis in the left anterior descending artery (LAD), right coronary artery (RCA) or left circumflex artery (LCX) in iodine contrast-enhanced ECG-gated coronary CT angiography (CCTA) scans., Methods: From a database of 6293 CCTA scans, we used pre-existing curved multiplanar reformations (CMR) images of the LAD, RCA and LCX arteries to create end-to-end deep-learning models for the detection of moderate or severe stenoses. We preprocessed the images by exploiting domain knowledge and employed a transfer learning approach using EfficientNet, ResNet, DenseNet and Inception-ResNet, with a class-weighted strategy optimised through cross-validation. Heatmaps were generated to indicate critical areas identified by the models, aiding clinicians in understanding the model's decision-making process., Results: Among the 900 CMR cases, 279 involved the LAD artery, 259 the RCA artery and 253 the LCX artery. EfficientNet models outperformed others, with EfficientNetB3 and EfficientNetB0 demonstrating the highest accuracy for LAD, EfficientNetB2 for RCA and EfficientNetB0 for LCX. The area under the curve for receiver operating characteristic (AUROC) reached 0.95 for moderate and 0.94 for severe stenosis in the LAD. For the RCA, the AUROC was 0.92 for both moderate and severe stenosis detection. The LCX achieved an AUROC of 0.88 for the detection of moderate stenoses, though the calibration curve exhibited significant overestimation. Calibration curves matched probabilities for the LAD but showed discrepancies for the RCA. Heatmap visualisations confirmed the models' precision in delineating stenotic lesions. Decision curve analysis and net reclassification index assessments reinforced the efficacy of EfficientNet models, confirming their superior diagnostic capabilities., Conclusion: Our end-to-end deep-learning model demonstrates, for the LAD artery, excellent discriminatory ability and calibration during internal validation, despite a small dataset used to train the network. The model reliably produces precise, highly interpretable images., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2025. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ Group.)

Published
2025
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