Your search keyword '"Iňigo Landa"' showing total 12 results

1. The prognostic power of gene mutations in thyroid cancer

Author

Sara Ahmadi and Iñigo Landa

Subjects

thyroid cancer, genomic, prognosis, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

The introduction and generalization of next-generation sequencing techniques have significantly increased the identification of mutations in thyroid tumors from multiple patient cohorts. The understanding of the association between specific mutations and clinical outcomes is gradually leading to individualizing the care of patients with thyroid cancer. BRAFV600 is the most common mutation seen in thyroid cancer patients and unequivocally predicts malignancy, but when considered in isolation, it is not recommended to be used as an independent prognostic factor. Mutations in RAS are the second most common alterations in thyroid cancer but can be found in benign and malignant lesions. Rearrangements involving receptor tyrosine kinases, primarily RET, are found in a subset of thyroid tumors without mutations in either BRAF or RAS. The assessment of additional mutations is increasingly employed in thyroid cancer prognostication. The coexistence of BRAF with alterations in genes such as PIK3CA, TERT promoter, or TP53 is associated with less favorable outcomes. Similar studies have also shown that additional oncogenic mutations in RAS-mutant thyroid carcinoma, such as those affecting the EIF1AX gene, likely predict a more aggressive clinicopathologic behavior. Overall, emerging evidence suggests that the co-occurrence of specific alterations in defined genes with BRAF or RAS mutations can become prognostic tools and useful predictors of thyroid tumor aggressiveness.

Published

2024

2. Clinical experience following implementation of routine SPECT-CT imaging following 131-iodine administration for thyroid cancer

Author

Sara Ahmadi, Alexandra Coleman, Nathalie Silva de Morais, Iñigo Landa, Theodora Pappa, Alex Kang, Matthew I Kim, Ellen Marqusee, and Erik K Alexander

Subjects

spect-ct imaging, 131-iodine treatment, planar scintigraphy, thyroid cancer, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Background: Planar scintigraphy has long been indicated in patients receiving I-131 therapy for thyroid cancer to determine the anatomic location of metastases. We studied our experience upon implementing additional single-photon emission (SPECT)-CT scanning in these patients. Method: We performed a retrospective study of consecutive adult patients with newly diagnosed thyroid cancer treated with I-131 between 2011 and 20 17. Radiologic findings detected with planar scintigraphy alone vs those identified with SPECT-CT scanning were primary endpoints. Result: In this study, 212 consecutive patients with thyroid cancer were analyzed in two separate cohorts (107 planar scintigraphy alone and 105 planar scintigraphy with SPECT-CT). The addition of SPECT-CT resulted in more findings, b oth thyroid-related and incidental. However, we identified only 3 of 21 cases in whi ch SPECT-CT provided an unequivocal additional benefit by changing clinical managemen t beyond planar scintigraphy alone. No difference in the detection of distant me tastatic disease or outcome was identified between cohorts. Conclusion: Synergistic SPECT-CT imaging in addition to planar nuclear scintigraphy adds limited clinical value to thyroid cancer patients harboring a low risk of distant metastases, while frequently identifying clinically insignificant findings. These data from a typical cohort of patients receiving standard thyroid cancer care provide insight into the routine use of SPECT-CT in such patients.

Published

2022

3. Point of Care Measurement of Body Mass Index and Thyroid Nodule Malignancy Risk Assessment

Author

Sara Ahmadi, Theodora Pappa, Alex S. Kang, Alexandra K. Coleman, Iñigo Landa, Ellen Marqusee, Matthew Kim, Trevor E. Angell, and Erik K. Alexander

Subjects

BMI, obesity, thyroid nodule, thyroid cancer, nodule size, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

BackgroundLarge scale epidemiology studies have suggested obesity may increase the risk of thyroid cancer, though no prospective analyses using real-world measurement of BMI at a time proximate to initial thyroid nodule evaluation have been performed.MethodsWe performed a prospective, cohort analysis over 3 years of consecutive patients presenting for thyroid nodule evaluation. We measured BMI proximate to the time of initial evaluation and correlated this with the final diagnosis of benign or malignant disease. We further correlated patient BMI with aggressivity of thyroid cancer, if detected.ResultsAmong 1,259 consecutive patients with clinically relevant nodules, 199(15%) were malignant. BMI averaged 28.6 kg/m2 (SD: 6.35, range:16.46-59.26). There was no correlation between the measurement of BMI and risk of thyroid cancer (p=0.58) as mean BMI was 28.9 kg/m2 and 28.6 kg/m2 in cancerous and benign cohorts, respectively. Similarly, BMI did not predict aggressive thyroid cancer (p=0.15). While overall nodule size was associated with increased BMI (p

Published

2022

4. Mouse Models as a Tool for Understanding Progression in Braf-Driven Thyroid Cancers

Author

Iñigo Landa and Jeffrey A. Knauf

Subjects

Proto-oncogene proteins B-raf, Thyroid neoplasms, Mice, transgenic, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

The development of next generation sequencing (NGS) has led to marked advancement of our understanding of genetic events mediating the initiation and progression of thyroid cancers. The NGS studies have confirmed the previously reported high frequency of mutually-exclusive oncogenic alterations affecting BRAF and RAS proto-oncogenes in all stages of thyroid cancer. Initially identified by traditional sequencing approaches, the NGS studies also confirmed the acquisition of alterations that inactivate tumor protein p53 (TP53) and activate phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit alpha (PIK3CA) in advanced thyroid cancers. Novel alterations, such as those in telomerase reverse transcriptase (TERT) promoter and mating-type switching/sucrose non-fermenting (SWI/SNF) complex, are also likely to promote progression of the BRAFV600E-driven thyroid cancers. A number of genetically engineered mouse models (GEMM) of BRAFV600E-driven thyroid cancer have been developed to investigate thyroid tumorigenesis mediated by oncogenic BRAF and to explore the role of genetic alterations identified in the genomic analyses of advanced thyroid cancer to promote tumor progression. This review will discuss the various GEMMs that have been developed to investigate oncogenic BRAFV600E-driven thyroid cancers.

Published

2019

5. Methodological Factors Involved in the Study of Temporal Binding Using the Open Source Software Labclock Web

Author

Carmelo P. Cubillas, Íñigo Landáburu, and Helena Matute

Subjects

temporal binding, intentional binding, Libet’s clock, Labclock Web, online experiments, Psychology, BF1-990

Abstract

Temporal binding occurs when an action and an outcome that follows it after a short period of time are judged as occurring closer to each other in time than they actually are. This effect has often been studied using Libet’s clock methodology. Garaizar et al. (2016) presented Labclock Web, a free HTML5 open source software that allows researchers to conduct temporal binding and other experiments using Libet’s clock through the Internet. The purpose of the three experiments presented here was to test how certain methodological modifications in the Labclock Web task could impact the temporal binding effect. In comparison with the original study, we aimed to: (a) reduce the interval between action and outcome in the delayed condition to 100 ms, instead of 500, (b) present the two types of trials, immediate and delayed, in two separate consecutive blocks, instead of intermixed, (c) use a visual, rather than auditory, outcome following the action, and (d) reduce the number of trials. In addition to its potential theoretical implications, the results confirm that Labclock Web is a useful and reliable tool for conducting temporal binding experiments and that it is well suited to measure temporal binding effects in a broad range of situations.

Published

2020

6. An epistatic interaction between the PAX8 and STK17B genes in papillary thyroid cancer susceptibility.

Author

Iñigo Landa, Cesar Boullosa, Lucía Inglada-Pérez, Ana Sastre-Perona, Susana Pastor, Antonia Velázquez, Veronika Mancikova, Sergio Ruiz-Llorente, Francesca Schiavi, Ricard Marcos, Nuria Malats, Giuseppe Opocher, Ramon Diaz-Uriarte, Pilar Santisteban, Alfonso Valencia, and Mercedes Robledo

Subjects

Medicine, Science

Abstract

Papillary Thyroid Cancer (PTC) is a heterogeneous and complex disease; susceptibility to PTC is influenced by the joint effects of multiple common, low-penetrance genes, although relatively few have been identified to date. Here we applied a rigorous combined approach to assess both the individual and epistatic contributions of genetic factors to PTC susceptibility, based on one of the largest series of thyroid cancer cases described to date. In addition to identifying the involvement of TSHR variation in classic PTC, our pioneer study of epistasis revealed a significant interaction between variants in STK17B and PAX8. The interaction was detected by MD-MBR (p = 0.00010) and confirmed by other methods, and then replicated in a second independent series of patients (MD-MBR p = 0.017). Furthermore, we demonstrated an inverse correlation between expression of PAX8 and STK17B in a set of cell lines derived from human thyroid carcinomas. Overall, our work sheds additional light on the genetic basis of thyroid cancer susceptibility, and suggests a new direction for the exploration of the inherited genetic contribution to disease using association studies.

Published

2013

7. Correction: An Epistatic Interaction between the and Genes in Papillary Thyroid Cancer Susceptibility.

Author

Iñigo Landa, Cesar Boullosa, Lucía Inglada-Pérez, Ana Sastre-Perona, Susana Pastor, Antonia Velázquez, Veronika Mancikova, Sergio Ruiz-Llorente, Francesca Schiavi, Ricard Marcos, Nuria Malats, Giuseppe Opocher, Ramon Diaz-Uriarte, Pilar Santisteban, Alfonso Valencia, and Mercedes Robledo

Subjects

Medicine, Science

Published

2013

8. The variant rs1867277 in FOXE1 gene confers thyroid cancer susceptibility through the recruitment of USF1/USF2 transcription factors.

Author

Iñigo Landa, Sergio Ruiz-Llorente, Cristina Montero-Conde, Lucía Inglada-Pérez, Francesca Schiavi, Susanna Leskelä, Guillermo Pita, Roger Milne, Javier Maravall, Ignacio Ramos, Víctor Andía, Paloma Rodríguez-Poyo, Antonino Jara-Albarrán, Amparo Meoro, Cristina del Peso, Luis Arribas, Pedro Iglesias, Javier Caballero, Joaquín Serrano, Antonio Picó, Francisco Pomares, Gabriel Giménez, Pedro López-Mondéjar, Roberto Castello, Isabella Merante-Boschin, Maria-Rosa Pelizzo, Didac Mauricio, Giuseppe Opocher, Cristina Rodríguez-Antona, Anna González-Neira, Xavier Matías-Guiu, Pilar Santisteban, and Mercedes Robledo

Subjects

Genetics, QH426-470

Abstract

In order to identify genetic factors related to thyroid cancer susceptibility, we adopted a candidate gene approach. We studied tag- and putative functional SNPs in genes involved in thyroid cell differentiation and proliferation, and in genes found to be differentially expressed in thyroid carcinoma. A total of 768 SNPs in 97 genes were genotyped in a Spanish series of 615 cases and 525 controls, the former comprising the largest collection of patients with this pathology from a single population studied to date. SNPs in an LD block spanning the entire FOXE1 gene showed the strongest evidence of association with papillary thyroid carcinoma susceptibility. This association was validated in a second stage of the study that included an independent Italian series of 482 patients and 532 controls. The strongest association results were observed for rs1867277 (OR[per-allele] = 1.49; 95%CI = 1.30-1.70; P = 5.9x10(-9)). Functional assays of rs1867277 (NM_004473.3:c.-283G>A) within the FOXE1 5' UTR suggested that this variant affects FOXE1 transcription. DNA-binding assays demonstrated that, exclusively, the sequence containing the A allele recruited the USF1/USF2 transcription factors, while both alleles formed a complex in which DREAM/CREB/alphaCREM participated. Transfection studies showed an allele-dependent transcriptional regulation of FOXE1. We propose a FOXE1 regulation model dependent on the rs1867277 genotype, indicating that this SNP is a causal variant in thyroid cancer susceptibility. Our results constitute the first functional explanation for an association identified by a GWAS and thereby elucidate a mechanism of thyroid cancer susceptibility. They also attest to the efficacy of candidate gene approaches in the GWAS era.

Published

2009

9. Supplementary Table S3 from EIF1AX and RAS Mutations Cooperate to Drive Thyroid Tumorigenesis through ATF4 and c-MYC

Author

James A. Fagin, Gunnar Rätsch, Jeffrey A. Knauf, Ronald A. Ghossein, John Blenis, Prasanna P. Tamarapu, Snjezana Dogan, Hans-Guido Wendel, Kamini Singh, Mahesh Saqcena, James Nagarajah, Iňigo Landa, Gina Lee, Scott W. Lowe, Zhen Zhao, Steven D. Leach, Natalie R. Davidson, and Gnana P. Krishnamoorthy

Abstract

Positively enriched gene signatures by GSEA using MsigDB-HALLMARKS and CANONICAL PATHWAYS genesets in CAL62-splice vs CAL62 cells.

Published

2023

10. Supplementary Figures S1 - S10, Tables S1 - S3 from NF2 Loss Promotes Oncogenic RAS-Induced Thyroid Cancers via YAP-Dependent Transactivation of RAS Proteins and Sensitizes Them to MEK Inhibition

Author

James A. Fagin, Ronald Ghossein, Filippo Giancotti, Kety H. Huberman, Adriana Heguy, Agnes Viale, Suresh C. Jhanwar, Yuqiang Fang, Gisele Oler, Yogindra Persaud, Barry S. Taylor, Ian Ganly, Vicki E. Smith, Francesca Voza, Jeffrey A. Knauf, Iňigo Landa, Brian R. Untch, Julio C. Ricarte-Filho, and Maria E.R. Garcia-Rendueles

Abstract

Supplementary Figure S1. Loss of heterozygosity of Ch22q genes in poorly differentiated (PDTC) and anaplastic thyroid cancers (ATC). Supplementary Figure S2. Focal NF2-exon 4 homozygous deletion in KHM-5M anaplastic thyroid cancer cells. Supplementary Figure S3. FISH for NF2 in anaplastic thyroid cancers. Supplementary Figure S4. NF2/Merlin defects in thyroid cancer cell lines. Supplementary Figure S5. Merlin inhibits RAC1-PAK activity. Supplementary Figure S6. Merlin effects on EGFR signaling and growth of RAS mutant thyroid cancer cell lines. Supplementary Figure S7. PCR of genomic DNA from mouse thyroid tissues of the indicated genotypes with primers that distinguish wild-type from mutant Hras alleles. Supplementary Figure S8. TEAD1 is the most abundant TEAD isoform in thyroid cancer cells. Supplementary Figure S9. A) Left, Concentration-dependent growth inhibitory effects of the MEK inhibitor selumetinib (AZD6244) in RAS mutant thyroid cancer cell lines cells. Black, null/low NF2. Red, wt NF2. The IC50 of each cell line is shown in the boxed legend. Right, Western blots for merlin, pMEK and pERK in the cell lines studied. B) C643 cells expressing scrambled (pLKO.1) or shNF2 were treated with FRAX, AZD or their combination at the indicated concentrations (nM) in 1 percent of serum. Cells were counted at 6 days (*p

Published

2023

11. EIF1AX and RAS mutations cooperate to drive thyroid tumorigenesis through ATF4 and c-MYC

Author

Snjezana Dogan, Iňigo Landa, Ronald Ghossein, Prasanna P. Tamarapu, John Blenis, Natalie R. Davidson, Gunnar Rätsch, Kamini Singh, Hans-Guido Wendel, Steven D. Leach, Zhen Zhao, Jeffrey A. Knauf, Gina Lee, James A. Fagin, Gnana P. Krishnamoorthy, Scott W. Lowe, Mahesh Saqcena, and James Nagarajah

Subjects

0301 basic medicine, Carcinogenesis, Eukaryotic Initiation Factor-1, Apoptosis, medicine.disease_cause, Mice, 0302 clinical medicine, Eukaryotic initiation factor, 2.1 Biological and endogenous factors, Phosphorylation, Aetiology, Thyroid cancer, Cancer, Mutation, Cultured, Kinase, TOR Serine-Threonine Kinases, Translation (biology), Tumor Cells, Oncology, 030220 oncology & carcinogenesis, Female, BRD4, endocrine system, Oncology and Carcinogenesis, Biology, SCID, Article, 03 medical and health sciences, Rare Diseases, medicine, Genetics, Animals, Humans, Thyroid Neoplasms, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Cell Proliferation, Neoplastic, medicine.disease, Xenograft Model Antitumor Assays, Activating Transcription Factor 4, Alternative Splicing, 030104 developmental biology, Gene Expression Regulation, Protein Biosynthesis, Cancer research, ras Proteins, Inbred NOD

Abstract

Translation initiation is orchestrated by the cap binding and 43S preinitiation complexes (PIC). Eukaryotic initiation factor 1A (EIF1A) is essential for recruitment of the ternary complex and for assembling the 43S PIC. Recurrent EIF1AX mutations in papillary thyroid cancers are mutually exclusive with other drivers, including RAS. EIF1AX mutations are enriched in advanced thyroid cancers, where they display a striking co-occurrence with RAS, which cooperates to induce tumorigenesis in mice and isogenic cell lines. The C-terminal EIF1AX-A113splice mutation is the most prevalent in advanced thyroid cancer. EIF1AX-A113splice variants stabilize the PIC and induce ATF4, a sensor of cellular stress, which is co-opted to suppress EIF2α phosphorylation, enabling a general increase in protein synthesis. RAS stabilizes c-MYC, an effect augmented by EIF1AX-A113splice. ATF4 and c-MYC induce expression of amino acid transporters and enhance sensitivity of mTOR to amino acid supply. These mutually reinforcing events generate therapeutic vulnerabilities to MEK, BRD4, and mTOR kinase inhibitors. Significance: Mutations of EIF1AX, a component of the translation PIC, co-occur with RAS in advanced thyroid cancers and promote tumorigenesis. EIF1AX-A113splice drives an ATF4-induced dephosphorylation of EIF2α, resulting in increased protein synthesis. ATF4 also cooperates with c-MYC to sensitize mTOR to amino acid supply, thus generating vulnerability to mTOR kinase inhibitors. This article is highlighted in the In This Issue feature, p. 151

Published

2018

12. NF2 Loss Promotes Oncogenic RAS-Induced Thyroid Cancers via YAP-Dependent Transactivation of RAS Proteins and Sensitizes Them to MEK Inhibition

Author

Yogindra Persaud, Jeffrey A. Knauf, Maria E.R. Garcia-Rendueles, Ronald Ghossein, Vicki Smith, Agnes Viale, Adriana Heguy, Kety Huberman, Julio C. Ricarte-Filho, Yuqiang Fang, Barry S. Taylor, Suresh C. Jhanwar, Iňigo Landa, Brian R. Untch, Gisele Oler, Ian Ganly, Francesca Voza, Filippo G. Giancotti, and James A. Fagin

Subjects

Transcriptional Activation, MAPK/ERK pathway, DNA Copy Number Variations, Chromosomes, Human, Pair 22, Cell Cycle Proteins, Mice, Transgenic, Biology, Bioinformatics, medicine.disease_cause, Models, Biological, Mice, Transactivation, Cell Line, Tumor, Anti-apoptotic Ras signalling cascade, Gene Order, medicine, Animals, Humans, Position-Specific Scoring Matrices, Thyroid Neoplasms, HRAS, Nucleotide Motifs, Promoter Regions, Genetic, Protein Kinase Inhibitors, Transcription factor, Neoplasm Staging, Neurofibromin 2, Binding Sites, Nuclear Proteins, Gene Expression Regulation, Neoplastic, Merlin (protein), Disease Models, Animal, Cell Transformation, Neoplastic, Genes, ras, Oncology, Drug Resistance, Neoplasm, Gene Targeting, Cancer research, Chromosome Deletion, Mitogen-Activated Protein Kinases, Signal transduction, Carcinogenesis, Gene Deletion, Protein Binding, Signal Transduction, Transcription Factors

Abstract

Ch22q LOH is preferentially associated with RAS mutations in papillary and in poorly differentiated thyroid cancer (PDTC). The 22q tumor suppressor NF2, encoding merlin, is implicated in this interaction because of its frequent loss of function in human thyroid cancer cell lines. Nf2 deletion or Hras mutation is insufficient for transformation, whereas their combined disruption leads to murine PDTC with increased MAPK signaling. Merlin loss induces RAS signaling in part through inactivation of Hippo, which activates a YAP–TEAD transcriptional program. We find that the three RAS genes are themselves YAP–TEAD1 transcriptional targets, providing a novel mechanism of promotion of RAS-induced tumorigenesis. Moreover, pharmacologic disruption of YAP–TEAD with verteporfin blocks RAS transcription and signaling and inhibits cell growth. The increased MAPK output generated by NF2 loss in RAS-mutant cancers may inform therapeutic strategies, as it generates greater dependency on the MAPK pathway for viability. Significance: Intensification of mutant RAS signaling through copy-number imbalances is commonly associated with transformation. We show that NF2/merlin inactivation augments mutant RAS signaling by promoting YAP/TEAD-driven transcription of oncogenic and wild-type RAS, resulting in greater MAPK output and increased sensitivity to MEK inhibitors. Cancer Discov; 5(11); 1178–93. ©2015 AACR. This article is highlighted in the In This Issue feature, p. 1111

Published

2015