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1. Circulating microRNAs associated with prediabetes and geographic location in Latinos

Author

Flowers, Elena, Ramírez-Mares, Juan-Daniel, Velazquez-Villafaña, Marion, Rangel-Salazar, Ruben, Sucher, Anatol, Kanaya, Alka M, Aouizerat, Bradley E, and de la Vega Monroy, Maria Luisa Lazo

Subjects
Epidemiology, Biomedical and Clinical Sciences, Clinical Sciences, Health Sciences, Prevention, Biotechnology, Health Disparities, Minority Health, Diabetes, Women's Health, Clinical Research, Genetics, Nutrition, Metabolic and endocrine, microRNA, Fasting blood glucose, Biomarker, Public Health and Health Services, Endocrinology & Metabolism, Clinical sciences
Abstract

BackgroundGlobally, type 2 diabetes is highly prevalent in individuals of Latino ancestry. The reasons underlying this high prevalence are not well understood, but both genetic and lifestyle factors are contributors. Circulating microRNAs are readily detectable in blood and are promising biomarkers to characterize biological responses (i.e., changes in gene expression) to lifestyle factors. Prior studies identified relationships between circulating microRNAs and risk for type 2 diabetes, but Latinos have largely been under-represented in these study samples.Aims/hypothesisThe aim of this study was to assess for differences in expression levels of three candidate microRNAs (miR-126, miR-146, miR-15) between individuals who had prediabetes compared to normal glycemic status and between individuals who self-identified with Latino ancestry in the United States (US) and native Mexicans living in or near Leon, Mexico.MethodsThis was a cross-sectional study that included 45 Mexicans and 21 Latino participants from the US. Prediabetes was defined as fasting glucose 100-125 mg/dL or 2-h post-glucose challenge between 140 and 199 mg/dL. Expression levels of microRNAs from plasma were measured by qPCR. Linear and logistic regression models were used to assess relationships between individual microRNAs and glycemic status or geographic site.ResultsNone of the three microRNAs was associated with risk for type 2 diabetes. MiR-146a and miR-15 were significantly lower in the study sample from Mexico compared to the US. There was a significant interaction between miR-146a and BMI associated with fasting blood glucose.Conclusions/interpretationThis study did not replicate in Latinos prior observations from other racial groups of associations between miR-126, miR-146a, and miR-15 and risk for type 2 diabetes. Future studies should consider other microRNAs related to different biological pathways as possible biomarkers for type 2 diabetes in Latinos.

Published
2021

2. Intervention Services for Autistic Adults: An ASDEU Study of Autistic Adults, Carers, and Professionals' Experiences

Author

Micai, Martina, Ciaramella, Antonio, Salvitti, Tommaso, Fulceri, Francesca, Fatta, Laura Maria, Poustka, Luise, Diehm, Robert, Iskrov, Georgi, Stefanov, Rumen, Guillon, Quentin, Rogé, Bernadette, Staines, Anthony, Sweeney, Mary Rose, Boilson, Andrew Martin, Leósdóttir, Thora, Saemundsen, Evald, Moilanen, Irma, Ebeling, Hanna, Yliherva, Anneli, Gissler, Mika, Parviainen, Tarja, Tani, Pekka, Kawa, Rafal, Vicente, Astrid, Rasga, Célia, Budisteanu, Magdalena, Dale, Ian, Povey, Carol, Flores, Noelia, Jenaro, Cristina, Monroy, Maria Luisa, Primo, Patricia García, Charman, Tony, Cramer, Susanne, Warberg, Christine Kloster, Canal-Bedia, Ricardo, Posada, Manuel, Scattoni, Maria Luisa, and Schendel, Diana

Abstract

The Autism Spectrum Disorders in the European Union (ASDEU) survey investigated local services' use experiences of autistic adults, carers and professionals with interventions for autistic adults. The majority of the 697 participants experienced recommended considerations prior to deciding on intervention and during the intervention plan and implementation. Psychosocial interventions were the most commonly experienced interventions, while pharmacological interventions NOT recommended for core autistic symptoms were reported by fairly large proportions of participants. Family interventions were experienced slightly more commonly by carers than adults or professionals. Less than the 26% of autistic adult responders who had experienced challenging behaviors reported receiving an intervention to change them. These results provide insights for improving gaps in service provision of interventions among autistic adults.

Published
2022
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4. Real-World Experiences in Autistic Adult Diagnostic Services and Post-Diagnostic Support and Alignment with Services Guidelines: Results from the ASDEU Study

Author

Scattoni, Maria Luisa, Micai, Martina, Ciaramella, Antonio, Salvitti, Tommaso, Fulceri, Francesca, Fatta, Laura Maria, Poustka, Luise, Diehm, Robert, Iskrov, Georgi, Stefanov, Rumen, Guillon, Quentin, Rogé, Bernadette, Staines, Anthony, Sweeney, Mary Rose, Boilson, Andrew Martin, Leósdóttir, Thora, Saemundsen, Evald, Moilanen, Irma, Ebeling, Hanna, Yliherva, Anneli, Gissler, Mika, Parviainen, Tarja, Tani, Pekka, Kawa, Rafal, Vicente, Astrid, Rasga, Célia, Budisteanu, Magdalena, Dale, Ian, Povey, Carol, Flores, Noelia, Jenaro, Cristina, Monroy, Maria Luisa, Primo, Patricia García, Charman, Tony, Cramer, Susanne, Warberg, Christine Kloster, Canal-Bedia, Ricardo, Posada, Manuel, and Schendel, Diana

Abstract

Research providing an evidence-base for autistic adult services is sparse. The Autism Spectrum Disorders in the European Union (ASDEU) network implemented an on-line survey to determine gaps in autistic adult diagnostic evaluation and post-diagnostic support services. More than 55% in all groups experienced most of the recommended features for diagnostic evaluation for autistic adults. In contrast, < 2% of adults or carers, and < 21% of professionals experienced each of the recommended features for post-diagnostic support. In contrast to 61% of professionals, only about 30% of autistic adults and carers had knowledge of good local services models for autism diagnosis in adulthood. There are major differences between good practice guidelines for diagnostic and post-diagnostic care for autistic adults, and what is actually experienced by services users and professionals.

Published
2021
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11. Autistic Adult Services Availability, Preferences, and User Experiences: Results From the Autism Spectrum Disorder in the European Union Survey

Author

Micai, Martina, primary, Fulceri, Francesca, additional, Salvitti, Tommaso, additional, Romano, Giovanna, additional, Poustka, Luise, additional, Diehm, Robert, additional, Iskrov, Georgi, additional, Stefanov, Rumen, additional, Guillon, Quentin, additional, Rogé, Bernadette, additional, Staines, Anthony, additional, Sweeney, Mary Rose, additional, Boilson, Andrew Martin, additional, Leósdóttir, Thora, additional, Saemundsen, Evald, additional, Moilanen, Irma, additional, Ebeling, Hanna, additional, Yliherva, Anneli, additional, Gissler, Mika, additional, Parviainen, Tarja, additional, Tani, Pekka, additional, Kawa, Rafal, additional, Pisula, Eva, additional, Vicente, Astrid, additional, Rasga, Célia, additional, Budişteanu, Magdalena, additional, Dale, Ian, additional, Povey, Carol, additional, Flores, Noelia, additional, Jenaro, Cristina, additional, Monroy, Maria Luisa, additional, Primo, Patricia García, additional, Charman, Tony, additional, Cramer, Susanne, additional, Warberg, Christine Kloster, additional, Canal-Bedia, Ricardo, additional, Posada, Manuel, additional, Schendel, Diana, additional, and Scattoni, Maria Luisa, additional

Published
2022
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12. Placental Nutrient Transporters and Maternal Fatty Acids in SGA, AGA, and LGA Newborns From Mothers With and Without Obesity

Author

Garcia-Santillan, Juan-Antonio, primary, Lazo-de-la-Vega-Monroy, Maria-Luisa, additional, Rodriguez-Saldaña, Gloria-Celina, additional, Solis-Barbosa, Miguel-Angel, additional, Corona-Figueroa, Maria-Angelica, additional, Gonzalez-Dominguez, Martha-Isabel, additional, Gomez-Zapata, Hector-Manuel, additional, Malacara, Juan-Manuel, additional, and Barbosa-Sabanero, Gloria, additional

Published
2022
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14. Autistic Adult Health and Professional Perceptions of It: Evidence From the ASDEU Project

Author

Micai, Martina, primary, Ciaramella, Antonio, additional, Salvitti, Tommaso, additional, Fulceri, Francesca, additional, Fatta, Laura Maria, additional, Poustka, Luise, additional, Diehm, Robert, additional, Iskrov, Georgi, additional, Stefanov, Rumen, additional, Guillon, Quentin, additional, Rogé, Bernadette, additional, Staines, Anthony, additional, Sweeney, Mary Rose, additional, Boilson, Andrew Martin, additional, Leósdóttir, Thora, additional, Saemundsen, Evald, additional, Moilanen, Irma, additional, Ebeling, Hanna, additional, Yliherva, Anneli, additional, Gissler, Mika, additional, Parviainen, Tarja, additional, Tani, Pekka, additional, Kawa, Rafal, additional, Vicente, Astrid, additional, Rasga, Célia, additional, Budişteanu, Magdalena, additional, Dale, Ian, additional, Povey, Carol, additional, Flores, Noelia, additional, Jenaro, Cristina, additional, Monroy, Maria Luisa, additional, Primo, Patricia García, additional, Charman, Tony, additional, Cramer, Susanne, additional, Warberg, Christine Kloster, additional, Canal-Bedia, Ricardo, additional, Posada, Manuel, additional, Scattoni, Maria Luisa, additional, and Schendel, Diana, additional

Published
2021
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15. Intervention Services for Autistic Adults: An ASDEU Study of Autistic Adults, Carers, and Professionals’ Experiences

Author

Micai, Martina, primary, Ciaramella, Antonio, additional, Salvitti, Tommaso, additional, Fulceri, Francesca, additional, Fatta, Laura Maria, additional, Poustka, Luise, additional, Diehm, Robert, additional, Iskrov, Georgi, additional, Stefanov, Rumen, additional, Guillon, Quentin, additional, Rogé, Bernadette, additional, Staines, Anthony, additional, Sweeney, Mary Rose, additional, Boilson, Andrew Martin, additional, Leósdóttir, Thora, additional, Saemundsen, Evald, additional, Moilanen, Irma, additional, Ebeling, Hanna, additional, Yliherva, Anneli, additional, Gissler, Mika, additional, Parviainen, Tarja, additional, Tani, Pekka, additional, Kawa, Rafal, additional, Vicente, Astrid, additional, Rasga, Célia, additional, Budişteanu, Magdalena, additional, Dale, Ian, additional, Povey, Carol, additional, Flores, Noelia, additional, Jenaro, Cristina, additional, Monroy, Maria Luisa, additional, Primo, Patricia García, additional, Charman, Tony, additional, Cramer, Susanne, additional, Warberg, Christine Kloster, additional, Canal-Bedia, Ricardo, additional, Posada, Manuel, additional, Scattoni, Maria Luisa, additional, and Schendel, Diana, additional

Published
2021
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19. FGF21 and its Relationship with Inflammatory and Metabolic Parameters in HIV Patients after Antiretroviral Treatment

Author

Ruiz-Padilla, Alan Joel, primary, Ruiz-Noa, Yeniley, additional, del Rocio Ibarra-Reynoso, Lorena, additional, Lazo-de-la-Vega-Monroy, Maria-Luisa, additional, Alonso-Castro, Angel Josabad, additional, Sánchez-Barajas, Mauricio, additional, Alvarez-Alvarez, Rosa Margarita, additional, and del Carmen Preciado-Puga, Mónica, additional

Published
2020
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20. Association of placental nutrient sensing pathways with birth weight

Author

Lazo-de-la-Vega-Monroy, Maria-Luisa, primary, Mata-Tapia, Karen-Alejandra, additional, Garcia-Santillan, Juan-Antonio, additional, Corona-Figueroa, Maria-Angelica, additional, Gonzalez-Dominguez, Martha-Isabel, additional, Gomez-Zapata, Hector-Manuel, additional, Malacara, Juan-Manuel, additional, Daza-Benitez, Leonel, additional, and Barbosa-Sabanero, Gloria, additional

Published
2020
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21. SUN-LB131 Association of Receptor for Advanced Glycation End Product (RAGE) Gene Polymorphisms & Serum Levels of Soluble RAGE (sRAGE) With Metabolic Syndrome (MS) in Mexican Population

Author

Gonzalez-Guerrero, Diana Elizabeth, primary, Rojas-Rubio, Armando, primary, Lazo-de-la-Vega-Monroy, Maria-Luisa, primary, Gomez-Ojeda, Armando, primary, Luevano-Contreras, Claudia, primary, Macias-Cervantes, Maciste, primary, Fajardo-Araujo, Martha Eugenia, primary, and Garay-Sevilla, Ma Eugenia, primary

Published
2020
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23. Glucose transporters in human placenta and its relation to birth weight

Author

Juan Manuel Malacara, Hector Manuel Gomez-Zapata, Gloria Barbosa-Sabanero, Juan Antonio García-Santillán, Martha I. González-Domínguez, and la Vega-Monroy Maria Luisa Lazo de

Subjects
medicine.medical_specialty, Endocrinology, Birth weight, Internal medicine, Glucose transporter, medicine, Human placenta, Biology
Published
2018

25. Association of the 3′UTR polymorphism (rs11665896) in the FGF21 gene with metabolic status and nutrient intake in children with obesity

Author

Ruiz-Padilla, Alan Joel, primary, Morales-Hernandez, Gerardo, additional, Ruiz-Noa, Yeniley, additional, Alonso-Castro, Angel Josabad, additional, Lazo-de-la-Vega-Monroy, Maria Luisa, additional, Preciado-Puga, Monica del Carmen, additional, Rangel-Salazar, Ruben, additional, and Ibarra-Reynoso, Lorena del Rocio, additional

Published
2019
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27. Differential activation of placental nutrient sensor pathways AMPK, insulin/IGF-1, and mTOR in SGA, AGA and LGA newborns from healthy mothers

Author

Lazo-de-la-Vega-Monroy, Maria-Luisa, primary, Mata-Tapia, Karen-Alejandra, additional, Gonzalez-Domínguez, Martha-Isabel, additional, García-Santillán, Juan-Antonio, additional, Corona-Figueroa, Angélica, additional, Gomez-Zapata, Hector-Manuel, additional, Malacara, Juan-Manuel, additional, Daza-Benítez, Leonel, additional, and Barbosa-Sabanero, Gloria, additional

Published
2019
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31. Specificity of mathematical indexes versus histopathological findings in the diagnosis of nonalcoholic fatty liver disease in mexican population

Author

del, Carmen Preciado-Puga Monica, primary, Garcia-Ramirez, Juana-Rosalba, additional, del, Rocio Ibarra-Reynoso Lorena, additional, Gutierrez-Aguirre, Karen-Ivette, additional, Velazquez-Villafana, Marion, additional, Lazo-de-la-Vega-Monroy, Maria-Luisa, additional, Ruiz-Noa, Yeniley, additional, Jordan-Perez, Benjamin, additional, and Garnelo-Cabanas, Serafin, additional

Published
2018
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32. Association of diabetes-related variants in ADCY5and CDKAL1with neonatal insulin, C-peptide, and birth weight

Author

Aguilera-Venegas, Ivette-Guadalupe, Mora-Peña, Julia-del-Socorro, Velazquez-Villafaña, Marion, Gonzalez-Dominguez, Martha-Isabel, Barbosa-Sabanero, Gloria, Gomez-Zapata, Hector-Manuel, and Lazo-de-la-Vega-Monroy, Maria-Luisa

Abstract

Background and purpose: Neonates at the highest and lowest percentiles of birth weight present an increased risk of developing metabolic diseases in adult life. While environmental events in utero may play an important role in this association, some genetic variants are associated both with birth weight and type 2 diabetes mellitus (T2DM), suggesting a genetic link between intrauterine growth and metabolism in adult life. Variants rs11708067 in ADCY5and rs7754840 in CDKAL1are associated with low birth weight, risk of T2DM, and lower insulin secretion in adults. We aimed to investigate whether, besides birth weight, these polymorphisms were related to insulin secretion at birth. Methods: A cohort of 218 healthy term newborns from uncomplicated pregnancies were evaluated for anthropometric and biochemical variables. Cord blood insulin and C-peptide were analyzed by ELISA. Genotyping of rs11708067 in ADCY5and rs7754840 in CDKAL1was performed. Results: Newborns carrying the A allele of ADCY5rs11708067 had lower cord blood insulin and C-peptide, even after adjusting by maternal glycemia, HbA1c, and pregestational BMI. Lower birth weight was found for AA-AG genotypes compared to GG, but no differences were seen in adjusted birth weight or z-score. Variant rs7754840 in CDKAL1was not associated with birth weight, neonatal insulin, or C-peptide for any genotype or genetic model. Conclusions: The variant rs11708067 in ADCY5is associated with lower neonatal insulin and C-peptide concentrations. Our results suggest that the genetic influence on insulin secretion may be evident from birth, even in healthy newborns, independently of maternal glycemia and BMI.

Published
2021
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33. 11 beta-hydroxysteroid dehydrogenase 2 promoter methylation is associated with placental protein expression in small for gestational age newborns

Author

Lazo-de-la-Vega-Monroy, Maria-Luisa, primary, Solís-Martínez, Martha-Olivia, additional, Romero-Gutiérrez, Gustavo, additional, Aguirre-Arzola, Victor E., additional, Wrobel, Katarzyna, additional, Wrobel, Kazimierz, additional, Zaina, Silvio, additional, and Barbosa-Sabanero, Gloria, additional

Published
2017
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34. Comparison between mathematical indexes and histopathological findings in the diagnosis of nonalcoholic fatty liver disease in mexican population

Author

Gutierrez-Aguirre, Karen-Ivette, primary, Lazo-de-la-Vega-Monroy, Maria-Luisa, additional, Ruiz-Noa, Yeniley, additional, Ibarra-Reynoso, Lorena-del-Rocio, additional, Garcia-Ramirez, Juana-Rosalba, additional, Jordan-Perez, Benjamin, additional, Garnelo-Cabanas, Serafin, additional, and Preciado-Puga, Monica-del-Carmen, additional

Published
2017
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36. EVALUACIÓN DEL PERFIL METABOLÓMICO DE PLACENTA DE RECIÉN NACIDOS CON ALTERACIONES IDIOPÁTICAS DEL PESO AL NACIMIENTO Y OBESIDAD MATERNA.

Author

Monreal Lucero, Salazar, José Juan, Ordaz Ortiz, Sabanero Gloria, Barbosa, Monroy Maria Luisa, Lazo de la Vega, and Francisco Javier, Bolaños Jiménez

Abstract

Copyright of Revista Mexicana de Endocrinología, Metabolismo y Nutrición is the property of Publicidad Permanyer SLU and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2023

39. Efectos de la suplementación con biotina sobre el islote pancreático

Author

Lazo De La Vega Monroy, Maria Luisa and Fernández Mejía, María Cristina

Subjects
Ciencias Biológicas, Químicas y de la Salud, Biología, Biotina, Fisiología
Abstract

tesis que para obtener el grado de Doctorado en Ciencias Biomédicas, presenta Maria Luisa Lazo de la Vega Monroy ; asesor María Cristina Fernández Mejía96 páginas : ilustracionesDoctorado en Ciencias Biomédicas UNAM, Instituto de Investigaciones Biomédicas, 2012

Published
2012

45. Polymorphisms -374 T/A and -429 T/C of the Receptor for Advanced Glycation End-Products (RAGE) and Serum Levels of RAGE (sRAGE) Are Not Associated with Metabolic Syndrome.

Author

González-Guerrero DE, Lazo-de-la-Vega-Monroy ML, Gómez-Ojeda A, Luévano-Contreras C, Rojas-Rubio A, and Garay-Sevilla ME

Abstract

RAGE is a multi-ligand transmembrane glycoprotein that promotes biological signals associated with inflammatory responses and degenerative diseases. sRAGE is a soluble variant, proposed as an inhibitor of RAGE activity. -374 T/A and -429 T/C polymorphisms of the advanced glycation end products receptor AGER gene are associated with the development of some diseases, such as type of cancer, cardiovascular disease, and micro and macrovascular disease in diabetes among others but their role in metabolic syndrome (MS) is still unknown. We studied 80 healthy men without MS, and 80 men with MS according to the harmonized criteria. -374 T/A and -429 T/C polymorphisms were genotyped by RT-PCR, and sRAGE was measured by ELISA. Allelic and genotypic frequencies did not differ between Non-MS and MS groups (-374 T/A p = 0.48, p = 0.57 and -429 T/C p = 0.36, p = 0.59). Significant differences were found in fasting glucose levels and diastolic blood pressure among the genotypes of the -374 T/A polymorphism in the Non-MS group ( p < 0.01 and p = 0.008). Glucose levels were different between -429 T/C genotypes in the MS group ( p = 0.02). sRAGE levels were similar in both groups, but in the Non-MS group showed a significant difference between individuals with only 1 or 2 components of the metabolic syndrome ( p = 0.047). However, no associations of any SNP with MS were found (recessive model p = 0.48, dominant model p = 0.82 for -374 T/A; recessive model p = 0.48, dominant model p = 0.42 for -429 T/C). -374 T/A and -429 T/C polymorphisms are not associated with MS in Mexican population and have no influence on serum sRAGE levels.

Published
2023
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46. Nutritional, pharmacological, and environmental programming of NAFLD in early life.

Author

Galvan-Martinez DH, Bosquez-Mendoza VM, Ruiz-Noa Y, Ibarra-Reynoso LDR, Barbosa-Sabanero G, and Lazo-de-la-Vega-Monroy ML

Subjects
Pregnancy, Child, Female, Adolescent, Humans, Obesity metabolism, Overweight, Fetal Development, Fetal Growth Retardation, Non-alcoholic Fatty Liver Disease epidemiology, Non-alcoholic Fatty Liver Disease etiology, Non-alcoholic Fatty Liver Disease metabolism, Prenatal Exposure Delayed Effects epidemiology, Prenatal Exposure Delayed Effects metabolism
Abstract

Nonalcoholic fatty liver disease (NAFLD) is the main liver disease worldwide, and its prevalence in children and adolescents has been increasing in the past years. It has been demonstrated that parental exposure to different conditions, both preconceptionally and during pregnancy, can lead to fetal programming of several metabolic diseases, including NAFLD. In this article, we review some of the maternal and paternal conditions that may be involved in early-life programing of adult NAFLD. First, we describe the maternal nutritional factors that have been suggested to increase the risk of NAFLD in the offspring, such as an obesogenic diet, overweight/obesity, and altered lipogenesis. Second, we review the association of certain vitamin supplementation and the use of some drugs during pregnancy, for instance, glucocorticoids, with a higher risk of NAFLD. Furthermore, we discuss the evidence showing that maternal-fetal pathologies, including gestational diabetes mellitus (GDM), insulin resistance (IR), and intrauterine growth restriction (IUGR), as well as the exposure to environmental contaminants, and the impact of microbiome changes, are important factors in early-life programming of NAFLD. Finally, we review how paternal preconceptional conditions, such as exercise and diet (particularly obesogenic diets), may impact fetal growth and liver function. Altogether, the presented evidence supports the hypothesis that both in utero exposure and parental conditions may influence fetal outcomes, including the development of NAFLD in early life and adulthood. The study of these conditions is crucial to better understand the diverse mechanisms involved in NAFLD, as well as for defining new preventive strategies for this disease.

Published
2023
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47. [Transcription factors in the adult beta cell].

Author

Lazo-de-la-Vega-Monroy ML and Fernández-Mejía C

Subjects
Animals, Basic Helix-Loop-Helix Transcription Factors physiology, Forkhead Box Protein O1, Forkhead Transcription Factors physiology, Hepatocyte Nuclear Factor 3-beta physiology, Homeodomain Proteins physiology, Humans, Maf Transcription Factors, Large physiology, Mice, Trans-Activators physiology, Insulin-Secreting Cells physiology, Transcription Factors physiology
Abstract

Insulin secretion by the pancreatic beta cell is critical to maintain glucose homeostasis. This secretion is impaired in type 1 diabetes, by beta cell autoimmune destruction, in type 2 diabetes, by multifactorial failures still not well determined, and in monogenic diabetes (MODY), by mutations in specific genes. During the last few years, several beta cell-specific transcription factors that regulate insulin synthesis and secretion in response to glucose have been discovered. Knockout mice studies for these genes and MODY diabetes demonstrate their importance for normal development and function of the beta cell. These factors are regulated not only in their expression by other genes, but also in their activity by other proteins and by post-translational modifications, therefore participating in physiologically important signaling pathways of the beta cell. The study of transcription factors is crucial for understanding the normal function of the beta cell, essential knowledge in developing new strategies for fighting diabetes.

Published
2009

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