Your search keyword '"Martínez de la Piscina Martín, Idoia"' showing total 6 results

1. Rare Germline DICER1 Variants in Pediatric Patients With Cushing's Disease: What Is Their Role?

Author

Pediatría, Pediatria, Martínez de la Piscina Martín, Idoia, Hernández Ramírez, Laura C., Portillo, Nancy, Gómez Gila, Ana L., Urrutia, Inés, Martínez Salazar, Rosa, García Castaño, Alejandro, Aguayo Calcena, Aníbal, Rica, Itxaso, Gaztambide Sáenz, María Sonia, Faucz, Fabio R., Keil, Margaret F., Lodish, Maya B., Quezado, Martha, Pankratz, Nathan, Chittiboina, Prashant, Lane, John, Kay, Denise M., Mills, James L., Castaño González, Luis Antonio, Stratakis, Constantine A., Spanish Corticotroph Adenomas Collaborative, Pediatría, Pediatria, Martínez de la Piscina Martín, Idoia, Hernández Ramírez, Laura C., Portillo, Nancy, Gómez Gila, Ana L., Urrutia, Inés, Martínez Salazar, Rosa, García Castaño, Alejandro, Aguayo Calcena, Aníbal, Rica, Itxaso, Gaztambide Sáenz, María Sonia, Faucz, Fabio R., Keil, Margaret F., Lodish, Maya B., Quezado, Martha, Pankratz, Nathan, Chittiboina, Prashant, Lane, John, Kay, Denise M., Mills, James L., Castaño González, Luis Antonio, Stratakis, Constantine A., and Spanish Corticotroph Adenomas Collaborative

Abstract

Context: The DICER1 syndrome is a multiple neoplasia disorder caused by germline mutations in the DICER1 gene. In DICER1 patients, aggressive congenital pituitary tumors lead to neonatal Cushing's disease (CD). The role of DICER1 in other corticotropinomas, however, remains unknown. Objective: To perform a comprehensive screening for DICER1 variants in a large cohort of CD patients, and to analyze their possible contribution to the phenotype. Design, setting, patients, and interventions: We included 192CD cases: ten young-onset (age <30 years at diagnosis) patients were studied using a next generation sequencing panel, and 182 patients (170 pediatric and 12 adults) were screened via whole-exome sequencing. In seven cases, tumor samples were analyzed by Sanger sequencing. Results: Rare germline DICER1 variants were found in seven pediatric patients with no other known disease-associated germline defects or somatic DICER1 second hits. By immunohistochemistry, DICER1 showed nuclear localization in 5/6 patients. Variant transmission from one of the parents was confirmed in 5/7 cases. One patient had a multinodular goiter; another had a family history of melanoma; no other patients had a history of neoplasms. Conclusions: Our findings suggest that DICER1 gene variants may contribute to the pathogenesis of non-syndromic corticotropinomas. Clarifying whether DICER1 loss-of-function is disease-causative or a mere disease-modifier in this setting, requires further studies.

Published

2020

2. Rare Germline DICER1 Variants in Pediatric Patients With Cushing's Disease: What Is Their Role?

Author

Pediatría, Pediatria, Martínez de la Piscina Martín, Idoia, Hernández Ramírez, Laura C., Portillo, Nancy, Gómez Gila, Ana L., Urrutia, Inés, Martínez Salazar, Rosa, García Castaño, Alejandro, Aguayo Calcena, Aníbal, Rica, Itxaso, Gaztambide Sáenz, María Sonia, Faucz, Fabio R., Keil, Margaret F., Lodish, Maya B., Quezado, Martha, Pankratz, Nathan, Chittiboina, Prashant, Lane, John, Kay, Denise M., Mills, James L., Castaño González, Luis Antonio, Stratakis, Constantine A., Spanish Corticotroph Adenomas Collaborative, Pediatría, Pediatria, Martínez de la Piscina Martín, Idoia, Hernández Ramírez, Laura C., Portillo, Nancy, Gómez Gila, Ana L., Urrutia, Inés, Martínez Salazar, Rosa, García Castaño, Alejandro, Aguayo Calcena, Aníbal, Rica, Itxaso, Gaztambide Sáenz, María Sonia, Faucz, Fabio R., Keil, Margaret F., Lodish, Maya B., Quezado, Martha, Pankratz, Nathan, Chittiboina, Prashant, Lane, John, Kay, Denise M., Mills, James L., Castaño González, Luis Antonio, Stratakis, Constantine A., and Spanish Corticotroph Adenomas Collaborative

Abstract

Context: The DICER1 syndrome is a multiple neoplasia disorder caused by germline mutations in the DICER1 gene. In DICER1 patients, aggressive congenital pituitary tumors lead to neonatal Cushing's disease (CD). The role of DICER1 in other corticotropinomas, however, remains unknown. Objective: To perform a comprehensive screening for DICER1 variants in a large cohort of CD patients, and to analyze their possible contribution to the phenotype. Design, setting, patients, and interventions: We included 192CD cases: ten young-onset (age <30 years at diagnosis) patients were studied using a next generation sequencing panel, and 182 patients (170 pediatric and 12 adults) were screened via whole-exome sequencing. In seven cases, tumor samples were analyzed by Sanger sequencing. Results: Rare germline DICER1 variants were found in seven pediatric patients with no other known disease-associated germline defects or somatic DICER1 second hits. By immunohistochemistry, DICER1 showed nuclear localization in 5/6 patients. Variant transmission from one of the parents was confirmed in 5/7 cases. One patient had a multinodular goiter; another had a family history of melanoma; no other patients had a history of neoplasms. Conclusions: Our findings suggest that DICER1 gene variants may contribute to the pathogenesis of non-syndromic corticotropinomas. Clarifying whether DICER1 loss-of-function is disease-causative or a mere disease-modifier in this setting, requires further studies.

Published

2020

3. Rare Germline DICER1 Variants in Pediatric Patients With Cushing's Disease: What Is Their Role?

Author

Pediatría, Pediatria, Martínez de la Piscina Martín, Idoia, Hernández Ramírez, Laura C., Portillo, Nancy, Gómez Gila, Ana L., Urrutia, Inés, Martínez Salazar, Rosa, García Castaño, Alejandro, Aguayo Calcena, Aníbal, Rica, Itxaso, Gaztambide Sáenz, María Sonia, Faucz, Fabio R., Keil, Margaret F., Lodish, Maya B., Quezado, Martha, Pankratz, Nathan, Chittiboina, Prashant, Lane, John, Kay, Denise M., Mills, James L., Castaño González, Luis Antonio, Stratakis, Constantine A., Spanish Corticotroph Adenomas Collaborative, Pediatría, Pediatria, Martínez de la Piscina Martín, Idoia, Hernández Ramírez, Laura C., Portillo, Nancy, Gómez Gila, Ana L., Urrutia, Inés, Martínez Salazar, Rosa, García Castaño, Alejandro, Aguayo Calcena, Aníbal, Rica, Itxaso, Gaztambide Sáenz, María Sonia, Faucz, Fabio R., Keil, Margaret F., Lodish, Maya B., Quezado, Martha, Pankratz, Nathan, Chittiboina, Prashant, Lane, John, Kay, Denise M., Mills, James L., Castaño González, Luis Antonio, Stratakis, Constantine A., and Spanish Corticotroph Adenomas Collaborative

Abstract

Context: The DICER1 syndrome is a multiple neoplasia disorder caused by germline mutations in the DICER1 gene. In DICER1 patients, aggressive congenital pituitary tumors lead to neonatal Cushing's disease (CD). The role of DICER1 in other corticotropinomas, however, remains unknown. Objective: To perform a comprehensive screening for DICER1 variants in a large cohort of CD patients, and to analyze their possible contribution to the phenotype. Design, setting, patients, and interventions: We included 192CD cases: ten young-onset (age <30 years at diagnosis) patients were studied using a next generation sequencing panel, and 182 patients (170 pediatric and 12 adults) were screened via whole-exome sequencing. In seven cases, tumor samples were analyzed by Sanger sequencing. Results: Rare germline DICER1 variants were found in seven pediatric patients with no other known disease-associated germline defects or somatic DICER1 second hits. By immunohistochemistry, DICER1 showed nuclear localization in 5/6 patients. Variant transmission from one of the parents was confirmed in 5/7 cases. One patient had a multinodular goiter; another had a family history of melanoma; no other patients had a history of neoplasms. Conclusions: Our findings suggest that DICER1 gene variants may contribute to the pathogenesis of non-syndromic corticotropinomas. Clarifying whether DICER1 loss-of-function is disease-causative or a mere disease-modifier in this setting, requires further studies.

Published

2020

4. Broad Phenotypes of Disorders/Differences of Sex Development in MAMLD1 Patients Through Oligogenic Disease

Author

Medicina, Medikuntza, Flueck, Christa E., Audi, Laura, Fernández Cancio, Mónica, Sauter, Kay Sara, Martínez de la Piscina Martín, Idoia, Castaño González, Luis Antonio, Esteva, Isabel, Camats, Nuria, Medicina, Medikuntza, Flueck, Christa E., Audi, Laura, Fernández Cancio, Mónica, Sauter, Kay Sara, Martínez de la Piscina Martín, Idoia, Castaño González, Luis Antonio, Esteva, Isabel, and Camats, Nuria

Abstract

Disorders/differences of sex development (DSD) are the result of a discordance between chromosomal, gonadal, and genital sex. DSD may be due to mutations in any of the genes involved in sex determination and development in general, as well as gonadal and/or genital development specifically. MAMLD1 is one of the recognized DSD genes. However, its role is controversial as some MAMLD1 variants are present in normal individuals, several MAMLD1 mutations have wild-type activity in functional studies, and the Mamld1-knockout male mouse presents with normal genitalia and reproduction. We previously tested nine MAMLD1 variants detected in nine 46, XY DSD patients with broad phenotypes for their functional activity, but none of the mutants, except truncated L210X, had diminished transcriptional activity on known target promoters CYP17A1 and HES3. In addition, protein expression of MAMLD1 variants was similar to wild-type, except for the truncated L210X. We hypothesized that MAMLD1 variants may not be sufficient to explain the phenotype in 46, XY DSD individuals, and that further genetic studies should be performed to search for additional hits explaining the broad phenotypes. We therefore performed whole exome sequencing (WES) in seven of these 46, XY patients with DSD and in one 46, XX patient with ovarian insufficiency, who all carried MAMLD1 variants. WES data were filtered by an algorithm including disease-tailored lists of MAMLD1-related and DSD-related genes. Fifty-five potentially deleterious variants in 41 genes were identified; 16/55 variants were reported in genes in association with hypospadias, 8/55 with cryptorchidism, 5/55 with micropenis, and 13/55 were described in relation with female sex development. Patients carried 1-16 variants in 1-16 genes together with their MAMLD1 variation. Network analysis of the identified genes revealed that 23 genes presented gene/protein interactions with MAMLD1. Thus, our study shows that the broad phenotypes of individual DSD

Published

2019

5. Broad Phenotypes of Disorders/Differences of Sex Development in MAMLD1 Patients Through Oligogenic Disease

Author

Medicina, Medikuntza, Flueck, Christa E., Audi, Laura, Fernández Cancio, Mónica, Sauter, Kay Sara, Martínez de la Piscina Martín, Idoia, Castaño González, Luis Antonio, Esteva, Isabel, Camats, Nuria, Medicina, Medikuntza, Flueck, Christa E., Audi, Laura, Fernández Cancio, Mónica, Sauter, Kay Sara, Martínez de la Piscina Martín, Idoia, Castaño González, Luis Antonio, Esteva, Isabel, and Camats, Nuria

Abstract

Disorders/differences of sex development (DSD) are the result of a discordance between chromosomal, gonadal, and genital sex. DSD may be due to mutations in any of the genes involved in sex determination and development in general, as well as gonadal and/or genital development specifically. MAMLD1 is one of the recognized DSD genes. However, its role is controversial as some MAMLD1 variants are present in normal individuals, several MAMLD1 mutations have wild-type activity in functional studies, and the Mamld1-knockout male mouse presents with normal genitalia and reproduction. We previously tested nine MAMLD1 variants detected in nine 46, XY DSD patients with broad phenotypes for their functional activity, but none of the mutants, except truncated L210X, had diminished transcriptional activity on known target promoters CYP17A1 and HES3. In addition, protein expression of MAMLD1 variants was similar to wild-type, except for the truncated L210X. We hypothesized that MAMLD1 variants may not be sufficient to explain the phenotype in 46, XY DSD individuals, and that further genetic studies should be performed to search for additional hits explaining the broad phenotypes. We therefore performed whole exome sequencing (WES) in seven of these 46, XY patients with DSD and in one 46, XX patient with ovarian insufficiency, who all carried MAMLD1 variants. WES data were filtered by an algorithm including disease-tailored lists of MAMLD1-related and DSD-related genes. Fifty-five potentially deleterious variants in 41 genes were identified; 16/55 variants were reported in genes in association with hypospadias, 8/55 with cryptorchidism, 5/55 with micropenis, and 13/55 were described in relation with female sex development. Patients carried 1-16 variants in 1-16 genes together with their MAMLD1 variation. Network analysis of the identified genes revealed that 23 genes presented gene/protein interactions with MAMLD1. Thus, our study shows that the broad phenotypes of individual DSD

Published

2019

6. Broad Phenotypes of Disorders/Differences of Sex Development in MAMLD1 Patients Through Oligogenic Disease

Author

Medicina, Medikuntza, Flueck, Christa E., Audi, Laura, Fernández Cancio, Mónica, Sauter, Kay Sara, Martínez de la Piscina Martín, Idoia, Castaño González, Luis Antonio, Esteva, Isabel, Camats, Nuria, Medicina, Medikuntza, Flueck, Christa E., Audi, Laura, Fernández Cancio, Mónica, Sauter, Kay Sara, Martínez de la Piscina Martín, Idoia, Castaño González, Luis Antonio, Esteva, Isabel, and Camats, Nuria

Abstract

Disorders/differences of sex development (DSD) are the result of a discordance between chromosomal, gonadal, and genital sex. DSD may be due to mutations in any of the genes involved in sex determination and development in general, as well as gonadal and/or genital development specifically. MAMLD1 is one of the recognized DSD genes. However, its role is controversial as some MAMLD1 variants are present in normal individuals, several MAMLD1 mutations have wild-type activity in functional studies, and the Mamld1-knockout male mouse presents with normal genitalia and reproduction. We previously tested nine MAMLD1 variants detected in nine 46, XY DSD patients with broad phenotypes for their functional activity, but none of the mutants, except truncated L210X, had diminished transcriptional activity on known target promoters CYP17A1 and HES3. In addition, protein expression of MAMLD1 variants was similar to wild-type, except for the truncated L210X. We hypothesized that MAMLD1 variants may not be sufficient to explain the phenotype in 46, XY DSD individuals, and that further genetic studies should be performed to search for additional hits explaining the broad phenotypes. We therefore performed whole exome sequencing (WES) in seven of these 46, XY patients with DSD and in one 46, XX patient with ovarian insufficiency, who all carried MAMLD1 variants. WES data were filtered by an algorithm including disease-tailored lists of MAMLD1-related and DSD-related genes. Fifty-five potentially deleterious variants in 41 genes were identified; 16/55 variants were reported in genes in association with hypospadias, 8/55 with cryptorchidism, 5/55 with micropenis, and 13/55 were described in relation with female sex development. Patients carried 1-16 variants in 1-16 genes together with their MAMLD1 variation. Network analysis of the identified genes revealed that 23 genes presented gene/protein interactions with MAMLD1. Thus, our study shows that the broad phenotypes of individual DSD

Published

2019