Your search keyword '"Peeters, R.P."' showing total 243 results

1. Balancing the benefits and harms of thyroid cancer surveillance in survivors of Childhood, adolescent and young adult cancer: Recommendations from the international Late Effects of Childhood Cancer Guideline Harmonization Group in collaboration with the PanCareSurFup Consortium

Author

Clement, S.C., Kremer, L.C.M., Verburg, F.A., Simmons, J.H., Goldfarb, M., Peeters, R.P., Alexander, E.K., Bardi, E., Brignardello, E., Constine, L.S., Dinauer, C.A., Drozd, V.M., Felicetti, F., Frey, E., Heinzel, A., van den Heuvel-Eibrink, M.M., Huang, S.A., Links, T.P., Lorenz, K., Mulder, R.L., Neggers, S.J., Nieveen van Dijkum, E.J.M., Oeffinger, K.C., van Rijn, R.R., Rivkees, S.A., Ronckers, C.M., Schneider, A.B., Skinner, R., Wasserman, J.D., Wynn, T., Hudson, M.M., Nathan, P.C., and van Santen, H.M.

Published

2018

2. Identifying barriers to vaccination intention at walk-in vaccination facilities in deprived neighbourhoods: A cross-sectional survey

Author

Sana, S., primary, Merkelbach, I., additional, Magnée, T., additional, Kollmann, J., additional, Peeters, R.P., additional, Kocken, P.L., additional, and Denktaş, S., additional

Published

2023

3. Development of a pediatric differentiated thyroid carcinoma registry within the EuRRECa project: rationale and protocol

Author

Clement, S.C. Visser, W.E. Lebbink, C.A. Albano, D. Claahsen-Van der Grinten, H.L. Czarniecka, A. Dias, R.P. Dierselhuis, M.P. Dzivite-Krisane, I. Elisei, R. Garcia-Burillo, A. Izatt, L. Kanaka-Gantenbein, C. Krude, H. Lamartina, L. Lorenz, K. Luster, M. Navardauskaitė, R. Negre Busó, M. Newbold, K. Peeters, R.P. Pellegriti, G. Piccardo, A. Priego, A.L. Redlich, A. de Sanctis, L. Sobrinho-Simões, M. van Trotsenburg, A.S.P. Verburg, F.A. Vriens, M. Links, T.P. Ahmed, S.F. van Santen, H.M. and Clement, S.C. Visser, W.E. Lebbink, C.A. Albano, D. Claahsen-Van der Grinten, H.L. Czarniecka, A. Dias, R.P. Dierselhuis, M.P. Dzivite-Krisane, I. Elisei, R. Garcia-Burillo, A. Izatt, L. Kanaka-Gantenbein, C. Krude, H. Lamartina, L. Lorenz, K. Luster, M. Navardauskaitė, R. Negre Busó, M. Newbold, K. Peeters, R.P. Pellegriti, G. Piccardo, A. Priego, A.L. Redlich, A. de Sanctis, L. Sobrinho-Simões, M. van Trotsenburg, A.S.P. Verburg, F.A. Vriens, M. Links, T.P. Ahmed, S.F. van Santen, H.M.

Abstract

Background: Although differentiated thyroid carcinoma (DTC) is the most frequent endocrine pediatric cancer, it is rare in childhood and adolescence. While tumor persistence and recurrence are not uncommon, mortality remains extremely low. Complications of treatment are however reported in up to 48% of the survivors. Due to the rarity of the disease, current treatment guidelines are predominantly based on the results of small observational retrospective studies and extrapolations from results in adult patients. In order to develop more personalized treatment and follow-up strategies (aiming to reduce complication rates), there is an unmet need for uniform international prospective data collection and clinical trials. Methods and analysis: The European pediatric thyroid carcinoma registry aims to collect clinical data for all patients ≤18 years of age with a confirmed diagnosis of DTC who have been diagnosed, assessed, or treated at a participating site. This registry will be a component of the wider European Registries for Rare Endocrine Conditions project which has close links to Endo-ERN, the European Reference Network for Rare Endocrine Conditions. A multidisciplinary expert working group was formed to develop a minimal dataset comprising information regarding demographic data, diagnosis, treatment, and outcome. We constructed an umbrella-type registry, with a detailed basic dataset. In the future, this may provide the opportunity for research teams to integrate clinical research questions. Ethics and dissemination: Written informed consent will be obtained from all participants and/or their parents/guardians. Summaries and descriptive analyses of the registry will be disseminated via conference presentations and peer-reviewed publications. © 2023 The authors Published by Bioscientifica Ltd.

Published

2023

4. Novel (sulfated) thyroid hormone transporters in the solute carrier 22 family.

Author

Chen, Z., Peeters, R.P., Flach, W., Rooij, L.J. de, Yildiz, S., Teumer, A., Nauck, M., Sterenborg, R.B.T.M., Rutten, J.H.W., Medici, M., Visser, W.E., Meima, M.E., Chen, Z., Peeters, R.P., Flach, W., Rooij, L.J. de, Yildiz, S., Teumer, A., Nauck, M., Sterenborg, R.B.T.M., Rutten, J.H.W., Medici, M., Visser, W.E., and Meima, M.E.

Abstract

Item does not contain fulltext, OBJECTIVE: Thyroid hormone (TH) transport represents a critical first step in governing intracellular TH regulation. It is still unknown whether the full repertoire of TH transporters has been identified. Members of the solute carrier (SLC) 22 family have substrates in common with the known TH transporters of the organic anion-transporting peptide family. Therefore, we screened the SLC22 family for TH transporters. METHODS: Uptake of 1 nM of iodothyronines or sulfated iodothyronines in COS1 cells expressing SLC22 proteins was performed. RESULTS: We first tested 25 mouse (m) SLC22 proteins for TH uptake and found that the majority of the organic anion transporter (OAT) clade were capable of 3,3',5-triiodothyronine and/or thyroxine (T4) transport. Based on phylogenetic tree analysis of the mouse and human (h) SLC22 family, we selected eight hSLC22s that grouped with the newly identified mouse TH transporters. Of these, four tested positive for uptake of one or more substrates, particularly hSLC22A11 showed robust (3-fold over control) uptake of T4. Uptake of sulfated iodothyronines was strongly (up to 17-fold) induced by some SLC22s, most notably SLC22A8, hSLC22A9, mSLC22A27 and mSLC22A29. Finally, the zebrafish orthologues of SLC22A6/8 drOatx and drSlc22a6l also transported almost all (sulfated) iodothyronines tested. The OAT inhibitors lesinurad and probenecid inhibited most SLC22 proteins. CONCLUSIONS: Our results demonstrated that members of the OAT clade of the SLC22 family constitute a novel, evolutionary conserved group of transporters for (sulfated) iodothyronines. Future studies should reveal the relevance of these transporters in TH homeostasis and physiology.

Published

2023

5. European experience with the Afirma Gene Expression Classifier for indeterminate thyroid nodules: A clinical utility study in the Netherlands.

Author

Lončar, I., Velsen, E.F.S. van, Massolt, E.T., Kemenade, F.J. van, Engen-van Grunsven, A.C.H. van, Hemel, B.M. van, Nederveen, F.H. Van, Netea-Maier, R.T., Links, T.P., Peeters, R.P., Ginhoven, T.M. van, Lončar, I., Velsen, E.F.S. van, Massolt, E.T., Kemenade, F.J. van, Engen-van Grunsven, A.C.H. van, Hemel, B.M. van, Nederveen, F.H. Van, Netea-Maier, R.T., Links, T.P., Peeters, R.P., and Ginhoven, T.M. van

Abstract

01 september 2023, Contains fulltext : 296005.pdf (Publisher’s version ) (Open Access), BACKGROUND: The Gene Expression Classifier (GEC) and Genomic Sequencing Classifier (GSC) were developed to improve risk stratification of indeterminate nodules. Our aim was to assess the clinical utility in a European population with restrictive diagnostic workup. METHODS: Clinical utility of the GEC was assessed in a prospective multicenter cohort of 68 indeterminate nodules. Diagnostic surgical rates for Bethesda III and IV nodules were compared to a historical cohort of 171 indeterminate nodules. Samples were post hoc tested with the GSC. RESULTS: The GEC classified 26% as benign. Surgical rates between the prospective and historical cohort did not differ (72.1% vs. 76.6%). The GSC classified 59% as benign, but misclassified six malignant lesions as benign. CONCLUSION: Implementation of GEC in management of indeterminate nodules in a European country with restrictive diagnostic workup is currently not supported, especially in oncocytic nodules. Prospective studies with the GSC in European countries are needed to determine the clinical utility.

Published

2023

6. The optimal healthy ranges of thyroid function defined by the risk of cardiovascular disease and mortality: systematic review and individual participant data meta-analysis

Author

Xu, Y.F., Derakhshan, A., Hysaj, O., Wildisen, L., Ittermann, T., Pingitore, A., Abolhassani, N., Medici, M., Kiemeney, L.A., Riksen, N.P., Dullaart, R.P.F., Trompet, S., Dörr, M., Brown, S.J., Schmidt, Börge, Führer-Sakel, D., Vanderpump, M.P.J., Muendlein, A., Drexel, H., Fink, H.A., Ikram, M.K., Kavousi, M., Rhee, C.M., Bensenor, I.M., Azizi, F., Hankey, G.J., Iacoviello, M., Imaizumi, M., Ceresini, G., Ferrucci, L., Sgarbi, J.A., Bauer, D.C., Wareham, N., Boelaert, K., Bakker, S.J.L., Jukema, J.W., Vaes, B., Iervasi, G., Yeap, B.B., Westendorp, R.G.J., Korevaar, T.I.M., Völzke, H., Razvi, S., Gussekloo, J., Walsh, J.P., Cappola, A.R., Rodondi, N., Peeters, R.P., Chaker, L., Xu, Y.F., Derakhshan, A., Hysaj, O., Wildisen, L., Ittermann, T., Pingitore, A., Abolhassani, N., Medici, M., Kiemeney, L.A., Riksen, N.P., Dullaart, R.P.F., Trompet, S., Dörr, M., Brown, S.J., Schmidt, Börge, Führer-Sakel, D., Vanderpump, M.P.J., Muendlein, A., Drexel, H., Fink, H.A., Ikram, M.K., Kavousi, M., Rhee, C.M., Bensenor, I.M., Azizi, F., Hankey, G.J., Iacoviello, M., Imaizumi, M., Ceresini, G., Ferrucci, L., Sgarbi, J.A., Bauer, D.C., Wareham, N., Boelaert, K., Bakker, S.J.L., Jukema, J.W., Vaes, B., Iervasi, G., Yeap, B.B., Westendorp, R.G.J., Korevaar, T.I.M., Völzke, H., Razvi, S., Gussekloo, J., Walsh, J.P., Cappola, A.R., Rodondi, N., Peeters, R.P., and Chaker, L.

Abstract

Contains fulltext : 297328.pdf (Publisher’s version ) (Closed access), BACKGROUND: Reference intervals of thyroid-stimulating hormone (TSH) and free thyroxine (FT(4)) are statistically defined by the 2·5-97·5th percentiles, without accounting for potential risk of clinical outcomes. We aimed to define the optimal healthy ranges of TSH and FT(4) based on the risk of cardiovascular disease and mortality. METHODS: This systematic review and individual participant data (IPD) meta-analysis identified eligible prospective cohorts through the Thyroid Studies Collaboration, supplemented with a systematic search via Embase, MEDLINE (Ovid), Web of science, the Cochrane Central Register of Controlled Trials, and Google Scholar from Jan 1, 2011, to Feb 12, 2017 with an updated search to Oct 13, 2022 (cohorts found in the second search were not included in the IPD). We included cohorts that collected TSH or FT(4), and cardiovascular outcomes or mortality for adults (aged ≥18 years). We excluded cohorts that included solely pregnant women, individuals with overt thyroid diseases, and individuals with cardiovascular disease. We contacted the study investigators of eligible cohorts to provide IPD on demographics, TSH, FT(4), thyroid peroxidase antibodies, history of cardiovascular disease and risk factors, medication use, cardiovascular disease events, cardiovascular disease mortality, and all-cause mortality. The primary outcome was a composite outcome including cardiovascular disease events (coronary heart disease, stroke, and heart failure) and all-cause mortality. Secondary outcomes were the separate assessment of cardiovascular disease events, all-cause mortality, and cardiovascular disease mortality. We performed one-step (cohort-stratified Cox models) and two-step (random-effects models) meta-analyses adjusting for age, sex, smoking, systolic blood pressure, diabetes, and total cholesterol. The study was registered with PROSPERO, CRD42017057576. FINDINGS: We identified 3935 studies, of which 53 cohorts fulfilled the inclusion criteria and 26 co

Published

2023

7. Intermediate and long-term adverse effects of radioiodine therapy for differentiated thyroid carcinoma – A systematic review

Author

Clement, S.C., Peeters, R.P., Ronckers, C.M., Links, T.P., van den Heuvel-Eibrink, M.M., Nieveen van Dijkum, E.J.M., van Rijn, R.R., van der Pal, H.J.H., Neggers, S.J., Kremer, L.C.M., van Eck-Smit, B.L.F., and van Santen, H.M.

Published

2015

8. The timecourse of apoptotic cell death during postnatal remodeling of the mouse cochlea and its premature onset by triiodothyronine (T3)

Author

Peeters, R.P., Ng, L., Ma, M., and Forrest, D.

Published

2015

9. Is outcome of differentiated thyroid carcinoma influenced by tumor stage at diagnosis?

Author

Clement, S.C., Kremer, L.C.M., Links, T.P., Mulder, R.L., Ronckers, C.M., van Eck-Smit, B.L.F., van Rijn, R.R., van der Pal, H.J.H., Tissing, W.J.E., Janssens, G.O., van den Heuvel-Eibrink, M.M., Neggers, S.J.C.M.M., van Dijkum, E.J.M. Nieveen, Peeters, R.P., and van Santen, H.M.

Published

2015

10. P17-08 Innovative animal-free assessment of thyroid-mediated developmental neurotoxicity based on human biology

Author

Dierichs, N.T.O.M., primary, Piersma, A.H., additional, van Oostrom, C.T.M., additional, de Leeuw, V.C., additional, Visser, W.E., additional, Gunhanlar, N., additional, Peeters, R.P., additional, and Hessel, E.V.S., additional

Published

2022

11. S24-01 Building an IATA-based testing strategy for thyroid hormone disruption resulting in developmental neurotoxicity

Author

Dierichs, N.T., Heikamp, K., van den Brand, A., Meima, M.E., Visser, E.W., Piersma, A.H., Peeters, R.P., van Duursen, M., Hamers, T., and Hessel, E.V.

Published

2024

12. The association of maternal thyroid function with placental hemodynamics

Author

Barjaktarovic, M., Korevaar, T.I.M., Chaker, L., Jaddoe, V.W.V., de Rijke, Y.B., Visser, T.J., Steegers, E.A.P., and Peeters, R.P.

Published

2017

13. Multikinase Inhibitors for the Treatment of Asymptomatic Radioactive Iodine-Refractory Differentiated Thyroid Cancer: Global Noninterventional Study (RIFTOS MKI)

Author

Brose, M.S. Smit, J.W.A. Lin, C.-C. Tori, M. Bowles, D.W. Worden, F. Shen, D.H.-Y. Huang, S.-M. Tsai, H.-J. Alevizaki, M. Peeters, R.P. Takahashi, S. Rumyantsev, P. Guan, R. Babajanyan, S. Ozgurdal, K. Sugitani, I. Pitoia, F. Lamartina, L. and Brose, M.S. Smit, J.W.A. Lin, C.-C. Tori, M. Bowles, D.W. Worden, F. Shen, D.H.-Y. Huang, S.-M. Tsai, H.-J. Alevizaki, M. Peeters, R.P. Takahashi, S. Rumyantsev, P. Guan, R. Babajanyan, S. Ozgurdal, K. Sugitani, I. Pitoia, F. Lamartina, L.

Abstract

Background: Sorafenib and lenvatinib are multikinase inhibitors (MKIs) approved for patients with radioactive iodine-refractory (RAI-R) differentiated thyroid cancer (DTC). There is no consensus on when to initiate MKI treatment. The objective of this study was to evaluate time to symptomatic progression (TTSP) in patients with RAI-R DTC for whom the decision to treat with an MKI was made at study entry. Methods: International, prospective, open-label, noninterventional cohort study (NCT02303444). Eligible patients had asymptomatic progressive RAI-R DTC, with ‡1 lesion ‡1 cm in diameter and life expectancy ‡6 months. The decision to treat with an MKI was at the treating physician’s discretion. Primary endpoint was TTSP from study entry. Two cohorts were evaluated: patients for whom a decision to initiate an MKI was made at study entry (Cohort 1) and patients for whom there was a decision not to initiate an MKI at study entry (Cohort 2). Cohorts were compared descriptively. Results: The full analysis set (FAS) comprised 647 patients. The median duration of observation was 35.5 months (range <1–59.4). Of 344 MKI-treated patients, 209 received sorafenib, 191 received lenvatinib, and 19 received another MKI at some point. Median TTSP was 55.4 months (interquartile range [IQR] 18.6–not estimable [NE]) overall, 55.4 months (IQR 15.2–NE) in Cohort 1 (n = 169), and 51.4 months (IQR 20.0–NE) in Cohort 2 (n = 478). TTSP ‡36 months was achieved in 64.5% of patients overall, 59.5% of patients in Cohort 1, and 66.4% of patients in Cohort 2. Median overall survival from classification as RAI-R was 167 months and median progression-free survival from start of MKI therapy was 19.2 months and from start of sorafenib therapy 16.7 months. Among sorafenib-treated patients, 70% had dose modifications, 35% had a dose reduction, 89% experienced ‡1 treatment-emergent adverse event (TEAE), and 82% experienced ‡1 drug-related TEAE. Conclusions: This real-world study provides valuable insi

Published

2022

14. Thyroid Status and Brain Circulation: The Rotterdam Study.

Author

Fani, L., Roa Dueñas, O., Bos, D., Vernooij, M.W., Klaver, C.C.W., Ikram, M.K., Peeters, R.P., Ikram, M.Arfan, Chaker, L., Fani, L., Roa Dueñas, O., Bos, D., Vernooij, M.W., Klaver, C.C.W., Ikram, M.K., Peeters, R.P., Ikram, M.Arfan, and Chaker, L.

Abstract

Item does not contain fulltext, CONTEXT: Whether thyroid dysfunction is related to altered brain circulation in the general population remains unknown. OBJECTIVE: We determined the association of thyroid hormones with different markers of brain circulation within community-dwelling elderly people. METHODS: This was a population-based study of 3 subcohorts of the Rotterdam Study, starting in 1989, 2000, and 2006. A total of 5142 participants (mean age, 63.8 years; 55.4% women), underwent venipuncture to measure serum thyroid-stimulating hormone (TSH) and free thyroxine (FT4). Between 2005 and 2015, all participants underwent phase-contrast brain magnetic resonance imaging to assess global brain perfusion (mL of blood flow/100 mL of brain/minute). Arteriolar retinal calibers were assessed using digitized images of stereoscopic fundus color transparencies in 3105 participants as markers of microcirculation. We investigated associations of TSH, FT4 with brain circulation measures using (non)linear regression models. RESULTS: FT4 (in pmol/L) levels had an inverse U-shaped association with global brain perfusion, such that high and low levels of FT4 were associated with lower global brain perfusion than middle levels of FT4. The difference in global brain perfusion between high FT4 levels (25 pmol/L) and middle FT4 levels (FT4 = 15 pmol/L; P nonlinearity = .002) was up to -2.44 mL (95% CI -4.31; -0.56). Higher and lower levels of FT4, compared with middle FT4 levels, were associated with arteriolar retinal vessels (mean difference up to -2.46 µm, 95% CI -4.98; 0.05 for lower FT4). CONCLUSION: These results suggest that thyroid dysfunction could lead to brain diseases such as stroke or dementia through suboptimal brain circulation that is potentially modifiable.

Published

2022

15. Functional Characterization of the Novel and Specific Thyroid Hormone Transporter SLC17A4

Author

Groeneweg, S., Geest, F.S. van, Chen, Z., Farina, S., Heerebeek, R.E.A. van, Meima, M.E., Peeters, R.P., Heuer, H., Medici, M., Visser, Wesley J., Groeneweg, S., Geest, F.S. van, Chen, Z., Farina, S., Heerebeek, R.E.A. van, Meima, M.E., Peeters, R.P., Heuer, H., Medici, M., and Visser, Wesley J.

Abstract

Item does not contain fulltext, Background: A recent genome-wide association study identified the SLC17A4 locus associated with circulating free thyroxine (T4) concentrations. Human SLC17A4, being widely expressed in the gastrointestinal tract, was characterized as a novel triiodothyronine (T3) and T4 transporter. However, apart from the cellular uptake of T3 and T4, transporter characteristics are currently unknown. In this study, we delineated basic transporter characteristics of this novel thyroid hormone (TH) transporter. Methods: We performed a broad range of well-established TH transport studies in COS-1 cells transiently overexpressing SLC17A4. We studied cellular TH uptake in various incubation buffers, TH efflux, and the inhibitory effects of different TH metabolites and known inhibitors of other TH transporters on SLC17A4-mediated TH transport. Finally, we determined the effect of tunicamycin, a pharmacological inhibitor of N-linked glycosylation, and targeted mutations in Asn residues on SLC17A4 function. Results: SLC17A4 induced the cellular uptake of T3 and T4 by ∼4 times, and of reverse (r)T3 by 1.5 times over control cells. The uptake of T4 by SLC17A4 was Na(+) and Cl(-) independent, stimulated by low extracellular pH, and reduced by various iodothyronines and metabolites thereof, particularly those that contain at least three iodine moieties irrespective of the presence of modification at the alanine side chain. None of the classical TH transporter inhibitors studied attenuated SLC17A4-mediated TH transport. SLC17A4 also facilitates the efflux of T3 and T4, and to a lesser extent of 3,3'-diiodothyronine (T2). Immunoblot studies on lysates of transfected cells cultured in absence or presence of tunicamycin indicated that SLC17A4 is subject to N-linked glycosylation. Complementary mutational studies identified Asn66, Asn75, and Asn90, which are located in extracellular loop 1, as primary targets. Conclusions: Our studies show that SLC17A4 facilitates the transport of T3 and T4, and l

Published

2022

16. The Effects of Common Genetic Variation in 96 Genes Involved in Thyroid Hormone Regulation on TSH and FT4 Concentrations

Author

Sterenborg, R.B.T.M., Galesloot, T.E., Teumer, A., Netea-Maier, R.T., Speed, D., Meima, M.E., Visser, Wesley J., Smit, J.W.A., Peeters, R.P., Medici, M., Sterenborg, R.B.T.M., Galesloot, T.E., Teumer, A., Netea-Maier, R.T., Speed, D., Meima, M.E., Visser, Wesley J., Smit, J.W.A., Peeters, R.P., and Medici, M.

Abstract

Contains fulltext : 251756.pdf (Publisher’s version ) (Open Access), OBJECTIVE: While most of the variation in thyroid function is determined by genetic factors, single nucleotide polymorphisms (SNPs) identified via genome-wide association analyses have only explained ~5% to 9% of this variance so far. Most SNPs were in or nearby genes with no known role in thyroid hormone (TH) regulation. Therefore, we performed a large-scale candidate gene study investigating the effect of common genetic variation in established TH regulating genes on serum thyrotropin [thyroid-stimulating hormone (TSH)] and thyroxine (FT4) concentrations. METHODS: SNPs in or within 10 kb of 96 TH regulating genes were included (30 031 TSH SNPs, and 29 962 FT4 SNPs). Associations were studied in 54 288 individuals from the ThyroidOmics Consortium. Linkage disequilibrium-based clumping was used to identify independently associated SNPs. SNP-based explained variances were calculated using SumHer software. RESULTS: We identified 23 novel TSH-associated SNPs in predominantly hypothalamic-pituitary-thyroid axis genes and 25 novel FT4-associated SNPs in mainly peripheral metabolism and transport genes. Genome-wide SNP variation explained ~21% (SD 1.7) of the total variation in both TSH and FT4 concentrations, whereas SNPs in the 96 TH regulating genes explained 1.9% to 2.6% (SD 0.4). CONCLUSION: Here we report the largest candidate gene analysis on thyroid function, resulting in a substantial increase in the number of genetic variants determining TSH and FT4 concentrations. Interestingly, these candidate gene SNPs explain only a minor part of the variation in TSH and FT4 concentrations, which substantiates the need for large genetic studies including common and rare variants to unravel novel, yet unknown, pathways in TH regulation.

Published

2022

17. FDG-PET/CT in indeterminate thyroid nodules: cost-utility analysis alongside a randomised controlled trial

Author

Koster, E.J. de, Vriens, D., Aken, M.O. van, Dijkhorst-Oei, L.T., Oyen, W.J.G., Peeters, R.P., Schepers, A., Geus-Oei, L.F. de, Hout, W.B. Van den, Koster, E.J. de, Vriens, D., Aken, M.O. van, Dijkhorst-Oei, L.T., Oyen, W.J.G., Peeters, R.P., Schepers, A., Geus-Oei, L.F. de, and Hout, W.B. Van den

Abstract

Item does not contain fulltext, PURPOSE: To evaluate cost-effectiveness of an [(18)F]FDG-PET/CT-driven diagnostic workup as compared to diagnostic surgery, for thyroid nodules with Bethesda III/IV cytology. [(18)F]FDG-PET/CT avoids 40% of futile diagnostic surgeries for benign Bethesda III/IV nodules. METHODS: Lifelong societal costs and quality-adjusted life years (QALYs) were assessed for 132 patients participating in a randomised controlled multicentre trial comparing [(18)F]FDG-PET/CT to diagnostic surgery. The observed 1-year trial results were extrapolated using a Markov model. The probability of cost-effectiveness was estimated using cost-effectiveness acceptability curves, taking uncertainty about sampling, imputation, and parameters into account. RESULTS: The observed 1-year cost difference of [(18)F]FDG-PET/CT as compared to diagnostic surgery was - euro1000 (95% CI: - euro2100 to euro0) for thyroid nodule-related care (p = 0.06). From the broader societal perspective, the 1-year difference in total societal costs was - euro4500 (- euro9200 to euro150) (p = 0.06). Over the modelled lifelong period, the cost difference was - euro9900 (- euro23,100 to euro3200) (p = 0.14). The difference in QALYs was 0.019 (- 0.045 to 0.083) at 1 year (p = 0.57) and 0.402 (- 0.581 to 1.385) over the lifelong period (p = 0.42). For a willingness to pay of euro50,000 per QALY, an [(18)F]FDG-PET/CT-driven work-up was the cost-effective strategy with 84% certainty. CONCLUSION: Following the observed reduction in diagnostic surgery, an [(18)F]FDG-PET/CT-driven diagnostic workup reduced the 1-year thyroid nodule-related and societal costs while sustaining quality of life. It is very likely cost-effective as compared to diagnostic surgery for Bethesda III/IV nodules. TRIAL REGISTRATION NUMBER: This trial is registered with ClinicalTrials.gov: NCT02208544 (5 August 2014), https://clinicaltrials.gov/ct2/show/NCT02208544 .

Published

2022

18. Incorporating Baseline Outcome Data in Individual Participant Data Meta-Analysis of Non-randomized Studies

Author

Syrogiannouli, L., Wildisen, L., Meuwese, C., Bauer, D.C., Cappola, A.R., Gussekloo, J., Elzen, W.P.J. den, Trompet, S., Westendorp, R.G.J., Jukema, J.W., Ferrucci, L., Ceresini, G., Asvold, B.O., Chaker, L., Peeters, R.P., Imaizumi, M., Ohishi, W., Vaes, B., Volzke, H., Sgarbi, J.A., Walsh, J.P., Dullaart, R.P.F., Bakker, S.J.L., Iacoviello, M., Rodondi, N., Giovane, C. del, Thyroid Studies Collaboration, Epidemiology, Internal Medicine, Laboratory for Endocrinology, APH - Personalized Medicine, APH - Aging & Later Life, Groningen Institute for Organ Transplantation (GIOT), and Groningen Kidney Center (GKC)

Subjects

baseline imbalance, cohorts, continuous outcome, individual participant data, non-randomized studies, Prevention, Clinical Sciences, 360 Soziale Probleme, Sozialdienste, 610 Medicine & health, Psychiatry and Mental health, SDG 3 - Good Health and Well-being, 360 Social problems & social services, Public Health and Health Services, Psychology, 610 Medizin und Gesundheit

Abstract

BackgroundIn non-randomized studies (NRSs) where a continuous outcome variable (e.g., depressive symptoms) is assessed at baseline and follow-up, it is common to observe imbalance of the baseline values between the treatment/exposure group and control group. This may bias the study and consequently a meta-analysis (MA) estimate. These estimates may differ across statistical methods used to deal with this issue. Analysis of individual participant data (IPD) allows standardization of methods across studies. We aimed to identify methods used in published IPD-MAs of NRSs for continuous outcomes, and to compare different methods to account for baseline values of outcome variables in IPD-MA of NRSs using two empirical examples from the Thyroid Studies Collaboration (TSC).MethodsFor the first aim we systematically searched in MEDLINE, EMBASE, and Cochrane from inception to February 2021 to identify published IPD-MAs of NRSs that adjusted for baseline outcome measures in the analysis of continuous outcomes. For the second aim, we applied analysis of covariance (ANCOVA), change score, propensity score and the naïve approach (ignores the baseline outcome data) in IPD-MA from NRSs on the association between subclinical hyperthyroidism and depressive symptoms and renal function. We estimated the study and meta-analytic mean difference (MD) and relative standard error (SE). We used both fixed- and random-effects MA.ResultsTen of 18 (56%) of the included studies used the change score method, seven (39%) studies used ANCOVA and one the propensity score (5%). The study estimates were similar across the methods in studies in which groups were balanced at baseline with regard to outcome variables but differed in studies with baseline imbalance. In our empirical examples, ANCOVA and change score showed study results on the same direction, not the propensity score. In our applications, ANCOVA provided more precise estimates, both at study and meta-analytical level, in comparison to other methods. Heterogeneity was higher when change score was used as outcome, moderate for ANCOVA and null with the propensity score.ConclusionANCOVA provided the most precise estimates at both study and meta-analytic level and thus seems preferable in the meta-analysis of IPD from non-randomized studies. For the studies that were well-balanced between groups, change score, and ANCOVA performed similarly.

Published

2022

19. Subclinical thyroid dysfunction and incident diabetes: a systematic review and an individual participant data analysis of prospective cohort studies

Author

Alwan, H., Villoz, F., Feller, M., Dullaart, R.P.F., Bakker, S.J.L., Peeters, R.P., Kavousi, M., Bauer, D.C., Cappola, A.R., Yeap, B.B., Walsh, J.P., Brown, S.J., Ceresini, G., Ferrucci, L., Gussekloo, J., Trompet, S., Iacoviello, M., Moon, J.H., Razvi, S., Bensenor, I.M., Azizi, F., Amouzegar, A., Valdes, S., Colomo, N., Wareham, N.J., Jukema, J.W., Westendorp, R.G.J., Kim, K.W., Rodondi, N., Giovane, C. del, Thyroid Studies Collaboration, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Internal Medicine, Epidemiology, Alwan, Heba [0000-0001-5516-6022], Bakker, Stephan JL [0000-0003-3356-6791], Peeters, Robin P [0000-0001-7732-9371], Yeap, Bu B [0000-0002-7612-5892], Razvi, Salman [0000-0002-9047-1556], Amouzegar, Atieh [0000-0001-9433-9408], and Apollo - University of Cambridge Repository

Subjects

Adult, Data Analysis, Male, Endocrinology, Diabetes and Metabolism, Clinical Sciences, Thyrotropin, 610 Medicine & health, Hyperthyroidism, Paediatrics and Reproductive Medicine, Cohort Studies, Endocrinology & Metabolism, Endocrinology, SDG 3 - Good Health and Well-being, Hypothyroidism, 360 Social problems & social services, Clinical Research, Diabetes Mellitus, Humans, Prospective Studies, Metabolic and endocrine, screening and diagnosis, Prevention, Diabetes, General Medicine, Middle Aged, Thyroid Diseases, Detection, Female, 4.2 Evaluation of markers and technologies

Abstract

ObjectiveFew prospective studies have assessed whether individuals with subclinical thyroid dysfunction are more likely to develop diabetes, with conflicting results. In this study, we conducted a systematic review of the literature and an individual participant data analysis of multiple prospective cohorts to investigate the association between subclinical thyroid dysfunction and incident diabetes.MethodsWe performed a systematic review of the literature in Medline, Embase, and the Cochrane Library from inception to February 11, 2022. A two-stage individual participant data analysis was conducted to compare participants with subclinical hypothyroidism and subclinical hyperthyroidism vs euthyroidism at baseline and the adjusted risk of developing diabetes at follow-up.ResultsAmong 61 178 adults from 18 studies, 49% were females, mean age was 58 years, and mean follow-up time was 8.2 years. At the last available follow-up, there was no association between subclinical hypothyroidism and incidence of diabetes (odds ratio (OR) = 1.02, 95% CI: 0.88–1.17, I2 = 0%) or subclinical hyperthyroidism and incidence of diabetes (OR = 1.03, 95% CI: 0.82–1.30, I2 = 0%), in age- and sex-adjusted analyses. Time-to-event analysis showed similar results (hazard ratio for subclinical hypothyroidism: 0.98, 95% CI: 0.87–1.11; hazard ratio for subclinical hyperthyroidism: 1.07, 95% CI: 0.88–1.29). The results were robust in all sub-group and sensitivity analyses.ConclusionsThis is the largest systematic review and individual participant data analysis to date investigating the prospective association between subclinical thyroid dysfunction and diabetes. We did not find an association between subclinical thyroid dysfunction and incident diabetes. Our results do not support screening patients with subclinical thyroid dysfunction for diabetes.Significance statementEvidence is conflicting regarding whether an association exists between subclinical thyroid dysfunction and incident diabetes. We therefore aimed to investigate whether individuals with subclinical thyroid dysfunction are more prone to develop diabetes in the long run as compared to euthyroid individuals. We included data from 18 international cohort studies with 61 178 adults and a mean follow-up time of 8.2 years. We did not find an association between subclinical hypothyroidism or subclinical hyperthyroidism at baseline and incident diabetes at follow-up. Our results have clinical implications as they neither support screening patients with subclinical thyroid dysfunction for diabetes nor treating them in the hope of preventing diabetes in the future. Objective: Few prospective studies have assessed whether individuals with subclinical thyroid dysfunction are more likely to develop diabetes, with conflicting results. In this study, we conducted a systematic review of the literature and an individual participant data analysis of multiple prospective cohorts to investigate the association between subclinical thyroid dysfunction and incident diabetes. Methods: We performed a systematic review of the literature in Medline, Embase, and the Cochrane Library from inception to February 11, 2022. A two-stage individual participant data analysis was conducted to compare participants with subclinical hypothyroidism and subclinical hyperthyroidism vs euthyroidism at baseline and the adjusted risk of developing diabetes at follow-up. Results: Among 61 178 adults from 18 studies, 49% were females, mean age was 58 years, and mean follow-up time was 8.2 years. At the last available follow-up, there was no association between subclinical hypothyroidism and incidence of diabetes (odds ratio (OR) = 1.02, 95% CI: 0.88-1.17, I2 = 0%) or subclinical hyperthyroidism and incidence of diabetes (OR = 1.03, 95% CI: 0.82-1.30, I2 = 0%), in age- and sex-adjusted analyses. Time-to-event analysis showed similar results (hazard ratio for subclinical hypothyroidism: 0.98, 95% CI: 0.87-1.11; hazard ratio for subclinical hyperthyroidism: 1.07, 95% CI: 0.88-1.29). The results were robust in all sub-group and sensitivity analyses. Conclusions: This is the largest systematic review and individual participant data analysis to date investigating the prospective association between subclinical thyroid dysfunction and diabetes. We did not find an association between subclinical thyroid dysfunction and incident diabetes. Our results do not support screening patients with subclinical thyroid dysfunction for diabetes. Significance statement: Evidence is conflicting regarding whether an association exists between subclinical thyroid dysfunction and incident diabetes. We therefore aimed to investigate whether individuals with subclinical thyroid dysfunction are more prone to develop diabetes in the long run as compared to euthyroid individuals. We included data from 18 international cohort studies with 61 178 adults and a mean follow-up time of 8.2 years. We did not find an association between subclinical hypothyroidism or subclinical hyperthyroidism at baseline and incident diabetes at follow-up. Our results have clinical implications as they neither support screening patients with subclinical thyroid dysfunction for diabetes nor treating them in the hope of preventing diabetes in the future.

Published

2022

20. Higher thyroid stimulating hormone leads to cardiovascular disease and an unfavorable lipid profile: EVidence from multi-cohort Mendelian randomization and metabolomic profiling

Author

Van Vliet, N.A., primary, Bos, M.M., additional, Thesing, C.S., additional, Chaker, L., additional, Pietzner, M., additional, Houtman, E., additional, Neville, M.J., additional, Li-Gao, R., additional, Trompet, S., additional, Mustafa, R., additional, Ahmadizar, F., additional, Beekman, M., additional, Bot, M., additional, Budde, K., additional, Christodoulides, C., additional, Dehghan, A., additional, Delles, C., additional, Elliott, P., additional, Evangelou, M., additional, Gao, H., additional, Ghanbari, M., additional, Van Herwaarden, A.E., additional, Ikram, M.A., additional, Jaeger, M., additional, Jukema, J.W., additional, Karaman, I., additional, Karpe, F., additional, Kloppenburg, M., additional, Meessen, J.M.T.A., additional, Meulenbelt, I., additional, Milaneschi, Y., additional, Mooijaart, S.P., additional, Mook-Kanamori, D.O., additional, Netea, M.G., additional, Netea-Maier, R.T., additional, Peeters, R.P., additional, Penninx, B.W.J.H., additional, Sattar, N., additional, Slagboom, P.E., additional, Suchiman, H.E.D., additional, Völzke, H., additional, Van Dijk, K. Willems, additional, and Noordam, R., additional

Published

2021

21. Effects of Thyroid Status on Regional Brain Volumes: A Diagnostic and Genetic Imaging Study in UK Biobank

Author

Chambers, T., Anney, R J L, Taylor, P.N., Teumer, A., Peeters, R.P., Medici, M., Caseras, X., Rees, D.A., Chambers, T., Anney, R J L, Taylor, P.N., Teumer, A., Peeters, R.P., Medici, M., Caseras, X., and Rees, D.A.

Abstract

Contains fulltext : 232420.pdf (Publisher’s version ) (Open Access), BACKGROUND: Thyroid hormone is essential for optimal human neurodevelopment and may modify the risk of attention-deficit/hyperactivity disorder (ADHD). However, the brain structures involved are unknown and it is unclear if the adult brain is also susceptible to changes in thyroid status. METHODS: We used International Classification of Disease-10 codes, polygenic thyroid scores at different thresholds of association with thyroid traits (PT-values), and image-derived phenotypes in UK Biobank (n = 18 825) to investigate the effects of a recorded diagnosis of thyroid disease and genetic risk for thyroid status on cerebellar and subcortical gray matter volume. Regional genetic pleiotropy between thyroid status and ADHD was explored using the GWAS-pairwise method. RESULTS: A recorded diagnosis of hypothyroidism (n = 419) was associated with significant reductions in total cerebellar and pallidum gray matter volumes (β [95% CI] = -0.14[-0.23, -0.06], P = 0.0005 and β [95%CI] = -0.12 [-0.20, -0.04], P = 0.0042, respectively), mediated in part by increases in body mass index. While we found no evidence for total cerebellar volume alterations with increased polygenic scores for any thyroid trait, opposing influences of increased polygenic scores for hypo- and hyperthyroidism were found in the pallidum (PT < 1e-3: β [95% CI] = -0.02 [-0.03, -0.01], P = 0.0003 and PT < 1e-7: β [95% CI] = 0.02 [0.01, 0.03], P = 0.0003, respectively). Neither hypo- nor hyperthyroidism showed evidence of regional genetic pleiotropy with ADHD. CONCLUSIONS: Thyroid status affects gray matter volume in adults, particularly at the level of the cerebellum and pallidum, with potential implications for the regulation of motor, cognitive, and affective function.

Published

2021

22. Variation in Normal Range Thyroid Function Affects Serum Cholesterol Levels, Blood Pressure, and Type 2 Diabetes Risk: A Mendelian Randomization Study

Author

Kuś, A., Marouli, E., Greco, M.F. Del, Chaker, L., Bednarczuk, T., Peeters, R.P., Teumer, A., Medici, M., Deloukas, P., Kuś, A., Marouli, E., Greco, M.F. Del, Chaker, L., Bednarczuk, T., Peeters, R.P., Teumer, A., Medici, M., and Deloukas, P.

Abstract

Item does not contain fulltext, Background: Observational studies have demonstrated that variation in normal range thyroid function is associated with major cardiovascular risk factors, including dyslipidemia, hypertension, type 2 diabetes (T2D), and obesity. As observational studies are prone to residual confounding, reverse causality, and selection bias, we used a Mendelian randomization (MR) approach to investigate whether these associations are causal or not. Methods: Two-sample MR analysis using data from the largest available genome-wide association studies on normal range thyrotropin (TSH) and free thyroxine (fT4) levels, serum lipid levels, blood pressure measurements, T2D, and obesity traits (body mass index [BMI] and waist/hip ratio). Results: A one standard deviation (SD) increase in genetically predicted TSH levels was associated with a 0.037 SD increase in total cholesterol levels (p = 3.0 × 10(-4)). After excluding pleiotropic instruments, we also observed significant associations between TSH levels and low-density lipoprotein levels (β = 0.026 SD, p = 1.9 × 10(-3)), pulse pressure (β = -0.477 mmHg, p = 7.5 × 10(-10)), and T2D risk (odds ratio = 0.95, p = 2.5 × 10(-3)). While we found no evidence of causal associations between TSH or fT4 levels and obesity traits, we found that a one SD increase in genetically predicted BMI was associated with a 0.075 SD decrease in fT4 levels (p = 3.6 × 10(-4)). Conclusions: Variation in normal range thyroid function affects serum cholesterol levels, blood pressure, and T2D risk.

Published

2021

23. Higher thyrotropin leads to unfavorable lipid profile and somewhat higher cardiovascular disease risk: evidence from multi-cohort Mendelian randomization and metabolomic profiling

Author

Vliet, N.A. van, Bos, M.M., Thesing, C.S., Chaker, L., Pietzner, M., Houtman, E., Neville, M.J., Li-Gao, R., Trompet, S., Mustafa, R., Ahmadizar, F., Beekman, M., Bot, M., Budde, K., Christodoulides, C., Dehghan, A., Delles, C., Elliott, P., Evangelou, M., Gao, H., Ghanbari, M., Herwaarden, A.E. van, Ikram, M.Arfan, Jaeger, M., Jukema, J.W., Karaman, I., Karpe, F., Kloppenburg, M., Meessen, J., Meulenbelt, I., Milaneschi, Y., Mooijaart, S.P., Mook-Kanamori, D.O., Netea, M.G., Netea, R.T., Peeters, R.P., Penninx, B., Sattar, N., Slagboom, P.Eline, Suchiman, H. Eka D., Völzke, H., Dijk, K.W van, Noordam, R., Heemst, D. van, Vliet, N.A. van, Bos, M.M., Thesing, C.S., Chaker, L., Pietzner, M., Houtman, E., Neville, M.J., Li-Gao, R., Trompet, S., Mustafa, R., Ahmadizar, F., Beekman, M., Bot, M., Budde, K., Christodoulides, C., Dehghan, A., Delles, C., Elliott, P., Evangelou, M., Gao, H., Ghanbari, M., Herwaarden, A.E. van, Ikram, M.Arfan, Jaeger, M., Jukema, J.W., Karaman, I., Karpe, F., Kloppenburg, M., Meessen, J., Meulenbelt, I., Milaneschi, Y., Mooijaart, S.P., Mook-Kanamori, D.O., Netea, M.G., Netea, R.T., Peeters, R.P., Penninx, B., Sattar, N., Slagboom, P.Eline, Suchiman, H. Eka D., Völzke, H., Dijk, K.W van, Noordam, R., and Heemst, D. van

Abstract

Contains fulltext : 245686.pdf (Publisher’s version ) (Open Access), BACKGROUND: Observational studies suggest interconnections between thyroid status, metabolism, and risk of coronary artery disease (CAD), but causality remains to be proven. The present study aimed to investigate the potential causal relationship between thyroid status and cardiovascular disease and to characterize the metabolomic profile associated with thyroid status. METHODS: Multi-cohort two-sample Mendelian randomization (MR) was performed utilizing genome-wide significant variants as instruments for standardized thyrotropin (TSH) and free thyroxine (fT4) within the reference range. Associations between TSH and fT4 and metabolic profile were investigated in a two-stage manner: associations between TSH and fT4 and the full panel of 161 metabolomic markers were first assessed hypothesis-free, then directional consistency was assessed through Mendelian randomization, another metabolic profile platform, and in individuals with biochemically defined thyroid dysfunction. RESULTS: Circulating TSH was associated with 52/161 metabolomic markers, and fT4 levels were associated with 21/161 metabolomic markers among 9432 euthyroid individuals (median age varied from 23.0 to 75.4 years, 54.5% women). Positive associations between circulating TSH levels and concentrations of very low-density lipoprotein subclasses and components, triglycerides, and triglyceride content of lipoproteins were directionally consistent across the multivariable regression, MR, metabolomic platforms, and for individuals with hypo- and hyperthyroidism. Associations with fT4 levels inversely reflected those observed with TSH. Among 91,810 CAD cases and 656,091 controls of European ancestry, per 1-SD increase of genetically determined TSH concentration risk of CAD increased slightly, but not significantly, with an OR of 1.03 (95% CI 0.99-1.07; p value 0.16), whereas higher genetically determined fT4 levels were not associated with CAD risk (OR 1.00 per SD increase of fT4; 95% CI 0.96-1.04; p value 0.5

Published

2021

24. Thyroid Function and Mood Disorders: A Mendelian Randomization Study

Author

Kuś, A., Kjaergaard, A.D., Marouli, E., Greco, M.F. Del, Sterenborg, R.B.T.M., Chaker, L., Peeters, R.P., Bednarczuk, T., Åsvold, B.O., Burgess, S., Deloukas, P., Teumer, A., Ellervik, C., Medici, M., Kuś, A., Kjaergaard, A.D., Marouli, E., Greco, M.F. Del, Sterenborg, R.B.T.M., Chaker, L., Peeters, R.P., Bednarczuk, T., Åsvold, B.O., Burgess, S., Deloukas, P., Teumer, A., Ellervik, C., and Medici, M.

Abstract

Item does not contain fulltext, Background: Observational studies suggest that even minor variations in thyroid function are associated with the risk of mood disorders, including major depressive disorder (MDD) and bipolar disorder (BD). However, it is unknown whether these associations are causal or not. We used a Mendelian randomization (MR) approach to investigate causal effects of minor variations in thyrotropin (TSH) and free thyroxine (fT4) levels on MDD and BD risk. Materials and Methods: We performed two-sample MR analyses using data from the largest publicly available genome-wide association studies on normal-range TSH (n = 54,288) and fT4 (n = 49,269) levels, MDD (170,756 cases, 329,443 controls) and BD (20,352 cases, 31,358 controls). Secondary MR analyses investigated the effects of TSH and fT4 levels on specific MDD and BD subtypes. Reverse MR was also performed to assess the effects of MDD and BD on TSH and fT4 levels. Results: There were no associations between genetically predicted TSH and fT4 levels and MDD risk, nor MDD subtypes and minor depressive symptoms. A one standard deviation increase in fT4 levels was nominally associated with an 11% decrease in the overall BD risk (odds ratio [OR] = 0.89, 95% confidence interval [CI] = 0.80-0.98, p = 0.022) and a 13% decrease in the BD type 1 risk (OR = 0.87, CI = 0.75-1.00, p = 0.047). In the reverse direction, genetic predisposition to MDD and BD was not associated with TSH nor fT4 levels. Conclusions: Variations in normal-range TSH and fT4 levels have no effects on the risk of MDD and its subtypes, and neither on minor depressive symptoms. This indicates that depressive symptoms should not be attributed to minor variations in thyroid function. Borderline associations with BD and BD type 1 risks suggest that further clinical studies should investigate the effect of thyroid hormone treatment in BD.

Published

2021

25. Clinical and Functional Consequences of C-Terminal Variants in MCT8: A Case Series

Author

Geest, F.S. van, Meima, M.E., Stuurman, K.E., Wolf, N.I., Knaap, M.S. van der, Lorea, C.F., Poswar, F.O., Vairo, F., Brunetti-Pierri, N., Cappuccio, G., Bakhtiani, P., Munnik, S.A. de, Peeters, R.P., Visser, W.E., Groeneweg, S., Geest, F.S. van, Meima, M.E., Stuurman, K.E., Wolf, N.I., Knaap, M.S. van der, Lorea, C.F., Poswar, F.O., Vairo, F., Brunetti-Pierri, N., Cappuccio, G., Bakhtiani, P., Munnik, S.A. de, Peeters, R.P., Visser, W.E., and Groeneweg, S.

Abstract

Contains fulltext : 231654.pdf (Publisher’s version ) (Open Access)

Published

2021

26. Urinary Iodine Concentrations in Pregnant Women and Offspring Brain Morphology

Author

Mulder, T.A., Korevaar, Tim I.M., Peeters, R.P., Herwaarden, A.E. van, Rijke, Y.B. de, White, T., Tiemeier, H., Mulder, T.A., Korevaar, Tim I.M., Peeters, R.P., Herwaarden, A.E. van, Rijke, Y.B. de, White, T., and Tiemeier, H.

Abstract

Item does not contain fulltext

Published

2021

27. Supplementary material to: Long-term efficacy of T3 analogue Triac in children and adults with MCT8 deficiency: a real-life retrospective cohort study

Author

Geest, F.S. (Ferdy) van, Groeneweg, S. (Stefan), Akker, E.L.T. (Erica) van den, Bacos, I. (Iuliu), Barca, D. (Diana), Berg, S.A.A. (Sjoerd) van den, Bertini, E. (Enrico), Brunner, D. (Doris), Brunetti-Pierri, N. (Nicola), Cappa, M. (Marco), Cappuccio, G. (Gerarda), Chatterjee, K. (Krishna), Chesover, A.D. (Alexander), Christian, P. (Peter), Coutant, R. (Régis), Craiu, D. (Dana), Crock, P. (Patricia), Dewey, C. (Cheyenne), Dica, A. (Alice), Dimitri, P. (Paul), Dubey, R. (Rachana), Enderli, A. (Anina), Fairchild, J. (Jan), Gallichan, J. (Jonathan), Garibaldi, L.R. (Luigi), George, B. (Belinda), Hackenberg, A. (Annette), Heinrich, B. (Bianka), Huynh, Tony (T.), Klosowska, A. (Anna), Lawson-Yuen, A. (Amy), Linder-Lucht, M. (Michaela), Lyons, G. (Greta), Monti Lora, F. (Felipe), Moran, C. (Carla), Müller, K. (Katalin), Paone, L. (Laura), Paul, P.G. (Praveen), Polak, M. (Michel), Porta, F. (Francesco), Reinauer, C. (Christina), Rijke, Y.B. (Yolanda) de, Seckold, R. (Rowen), Seven Menevse, T. (Tuba), Simm, P. (Peter), Simon, A. (Anna), Spada, M. (Marco), Stoupa, A. (Athanasia), Szeifert, L. (Lilla), Tonduti, D. (Davide), Toor, H. (Hans) van, Turan, S. (Serap), Vanderniet, J. (Joel), Waart, M. (Monique) de, Wal, R. (Ronald) van der, Walt, A. (Adri) van der, Wermeskerken, A-M. (Anne-Marie) van, Wierzba, J. (Jolanta), Zibordi, F. (Federica), Zung, A. (Amnon), Peeters, R.P. (Robin), Visser, W.E. (Edward), Geest, F.S. (Ferdy) van, Groeneweg, S. (Stefan), Akker, E.L.T. (Erica) van den, Bacos, I. (Iuliu), Barca, D. (Diana), Berg, S.A.A. (Sjoerd) van den, Bertini, E. (Enrico), Brunner, D. (Doris), Brunetti-Pierri, N. (Nicola), Cappa, M. (Marco), Cappuccio, G. (Gerarda), Chatterjee, K. (Krishna), Chesover, A.D. (Alexander), Christian, P. (Peter), Coutant, R. (Régis), Craiu, D. (Dana), Crock, P. (Patricia), Dewey, C. (Cheyenne), Dica, A. (Alice), Dimitri, P. (Paul), Dubey, R. (Rachana), Enderli, A. (Anina), Fairchild, J. (Jan), Gallichan, J. (Jonathan), Garibaldi, L.R. (Luigi), George, B. (Belinda), Hackenberg, A. (Annette), Heinrich, B. (Bianka), Huynh, Tony (T.), Klosowska, A. (Anna), Lawson-Yuen, A. (Amy), Linder-Lucht, M. (Michaela), Lyons, G. (Greta), Monti Lora, F. (Felipe), Moran, C. (Carla), Müller, K. (Katalin), Paone, L. (Laura), Paul, P.G. (Praveen), Polak, M. (Michel), Porta, F. (Francesco), Reinauer, C. (Christina), Rijke, Y.B. (Yolanda) de, Seckold, R. (Rowen), Seven Menevse, T. (Tuba), Simm, P. (Peter), Simon, A. (Anna), Spada, M. (Marco), Stoupa, A. (Athanasia), Szeifert, L. (Lilla), Tonduti, D. (Davide), Toor, H. (Hans) van, Turan, S. (Serap), Vanderniet, J. (Joel), Waart, M. (Monique) de, Wal, R. (Ronald) van der, Walt, A. (Adri) van der, Wermeskerken, A-M. (Anne-Marie) van, Wierzba, J. (Jolanta), Zibordi, F. (Federica), Zung, A. (Amnon), Peeters, R.P. (Robin), and Visser, W.E. (Edward)

Published

2021

28. Clinical and Functional Consequences of C-Terminal Variants in MCT8: A Case Series

Author

Geest, F.S. (Ferdy) van, Meima, M.E. (Marcel), Stuurman, K.E. (Kyra), Wolf, N.I. (Nicole I.), van der Knaap, M.S. (Marjo S.), Lorea, C.F. (Cláudia F), Poswar, F.O. (Fabiano O.), Vairo, F. (Filippo), Brunetti-Pierri, N. (Nicola), Cappuccio, G. (Gerarda), Bakhtiani, P. (Priyanka), Munnik, S.A. (Sonja) de, Peeters, R.P. (Robin), Visser, W.E. (Edward), Groeneweg, S. (Stefan), Geest, F.S. (Ferdy) van, Meima, M.E. (Marcel), Stuurman, K.E. (Kyra), Wolf, N.I. (Nicole I.), van der Knaap, M.S. (Marjo S.), Lorea, C.F. (Cláudia F), Poswar, F.O. (Fabiano O.), Vairo, F. (Filippo), Brunetti-Pierri, N. (Nicola), Cappuccio, G. (Gerarda), Bakhtiani, P. (Priyanka), Munnik, S.A. (Sonja) de, Peeters, R.P. (Robin), Visser, W.E. (Edward), and Groeneweg, S. (Stefan)

Abstract

CONTEXT: Genetic variants in SLC16A2, encoding the thyroid hormone transporter MCT8, can cause intellectual and motor disability and abnormal serum thyroid function tests, known as MCT8 deficiency. The C-terminal domain of MCT8 is poorly conserved, which complicates prediction of the deleteriousness of variants in this region. We studied the functional consequences of 5 novel variants within this domain and their relation to the clinical phenotypes. METHODS: We enrolled male subjects with intellectual disability in whom genetic variants were identified in exon 6 of SLC16A2. The impact of identified variants was evaluated in transiently transfected cell lines and patient-derived fibroblasts. RESULTS: Seven individuals from 5 families harbored potentially deleterious variants affecting the C-terminal domain of MCT8. Two boys with clinical features considered atypical for MCT8 deficiency had a missense variant [c.1724A>G;p.(His575Arg) or c.1796A>G;p.(Asn599Ser)] that did not affect MCT8 function in transfected cells or patient-derived fibroblasts, challenging a causal relationship. Two brothers with classical MCT8 deficiency had a truncating c.1695delT;p.(Val566*) variant that completely inactivated MCT8 in vitro. The 3 other boys had relatively less-severe clinical features and harbored frameshift variants that elongate the MCT8 protein [c.1805delT;p.(Leu602HisfsTer680) and c.del1826-1835;p.(Pro609GlnfsTer676)] and retained ~50% residual activity. Additional truncating variants within transmembrane domain 12 were fully inactivating, whereas those within the intracellular C-terminal tail were tolerated. CONCLUSIONS: Variants affecting the intracellular C-terminal tail of MCT8 are likely benign unless they cause frameshifts that elongate the MCT8 protein. These findings provide clinical guidance in the assessment of the pathogenicity of variants within the C-terminal domain of MCT8.

Published

2021

29. Long-Term Effects of Radioiodine Treatment on Salivary Gland Function in Adult Survivors of Pediatric Differentiated Thyroid Carcinoma

Author

Selvakumar, T., Nies, M., Hesselink, M.S.K., Brouwers, A.H., Horst-Schrivers, A.N.A. van der, Hesselink, E.N.K., Tissing, W.J.E., Vissink, A., Links, T.P., Bocca, G., Burgerhof, J.G.M., Dam, E.W.C.M. van, Havekes, B., Heuvel-Eibrink, M.M. van den, Corssmit, E.P.M., Kremer, L.C.M., Netea-Maier, R.T., Pal, H.J.H. van der, Peeters, R.P., Smit, J.W.A., Plukker, J.T.M., Ronckers, C.M., Santen, H.M. van, Dutch Pediat Thyroid Canc Study Co, Guided Treatment in Optimal Selected Cancer Patients (GUTS), Personalized Healthcare Technology (PHT), Translational Immunology Groningen (TRIGR), Damage and Repair in Cancer Development and Cancer Treatment (DARE), ​Basic and Translational Research and Imaging Methodology Development in Groningen (BRIDGE), Internal medicine, CCA - Cancer Treatment and quality of life, Amsterdam Reproduction & Development (AR&D), Internal Medicine, RS: NUTRIM - R1 - Obesity, diabetes and cardiovascular health, MUMC+: MA Endocrinologie (9), and Interne Geneeskunde

Subjects

salivary gland dysfunction, medicine.medical_specialty, Saliva, FLOW, 030209 endocrinology & metabolism, XEROSTOMIA, Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], Gastroenterology, Healthcare improvement science Radboud Institute for Health Sciences [Radboudumc 18], Thyroid carcinoma, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, 0302 clinical medicine, stomatognathic system, QUALITY-OF-LIFE, Internal medicine, medicine, FERTILITY, Endocrine system, Radiology, Nuclear Medicine and imaging, I-131 THERAPY, Thyroid cancer, RISK, radioiodine treatment, Salivary gland, business.industry, Cancer, pediatric differentiated thyroid carcinoma, RADIOACTIVE IODINE THERAPY, medicine.disease, CANCER, Sialadenitis, INTERMEDIATE, medicine.anatomical_structure, SIALADENITIS, Radiology Nuclear Medicine and imaging, 030220 oncology & carcinogenesis, business, Rare disease

Abstract

Pediatric differentiated thyroid cancer (DTC) is a rare disease. Initial treatment of DTC consists of a total or near-total thyroidectomy and 131 I therapy. Previous studies on adults showed that 131 I treatment may reduce salivary gland function (SGF). Studies regarding SGF in children treated for DTC are sparse. Our aim was to assess the long-term effects of 131 I treatment on SGF in survivors of pediatric DTC. Methods: In a nationwide cross-sectional study, SGF in patients treated for pediatric DTC between 1970 and 2013 (.5 y after diagnosis, $18 y old at the time of evaluation) was studied. SGF was assessed by sialometry, sialochemistry, and a xerostomia inventory. Salivary gland dysfunction (SGD) was defined as an unstimulated whole saliva flow of no more than 0.2 mL/min or a stimulated whole saliva flow of no more than 0.7 mL/min. Results: Sixty-five patients underwent 131 I treatment (median age at evaluation, 33 y, with an interquartile range [IQR] of 25–40 y; 86.2% female; median follow-up period, 11 y, with an IQR of 6–22 y). Median cumulative 131 I activity was 5.88 GBq, with an IQR of 2.92–12.95 GBq, and 47.7% underwent multiple 131 I administrations. SGD was present in 30 (47.6%) patients. Levels of amylase and total protein in saliva were reduced. Moderate to severe xerostomia was present in 22 (35.5%) patients. Stimulated salivary secretion was lower and the severity of xerostomia complaints higher in patients treated with higher cumulative 131 I activity. Conclusion: In survivors of pediatric DTC, clinically significant SGD was found in 35.5% and was related to the cumulative 131 I activity of the treatment.

Published

2018

30. Non thyroidal illness: to treat or not to treat?

Author

Peeters, R.P.

Published

2007

31. Nonthyroidal illness

Author

Peeters, R.P., primary

Published

2011

32. 1918P Final analysis of RIFTOS MKI, a global, non-interventional study assessing the use of multikinase inhibitors (MKIs) for the treatment of patients with asymptomatic radioactive iodine-refractory differentiated thyroid cancer (RAI-R DTC)

Author

Brose, M.S., primary, Smit, J.W.A., additional, Lin, C-C., additional, Tori, M., additional, Bowles, D.W., additional, Worden, F., additional, Shen, D.H-Y., additional, Huang, S-M., additional, Alevizaki, M., additional, Peeters, R.P., additional, Takahashi, S., additional, Rumyantsev, P., additional, Guan, R., additional, Babajanyan, S., additional, Ozgurdal, K., additional, Sugitani, I., additional, Pitoia, F., additional, and Lamartina, L., additional

Published

2020

33. High-normal thyroid function and risk of atrial fibrillation: The Rotterdam Study

Author

Heeringa, Jan, Hoogendoorn, E.H., van der Deure, W.M., Hofman, Albert, Peeters, R.P., Hop, W.C.J., den Heijer, M., Visser, Theo J., and Witteman, Jacqueline C.M.

Subjects

Atrial fibrillation -- Risk factors, Atrial fibrillation -- Research, Hyperthyroidism -- Research, Health

Published

2008

34. Long-Term Effects of Radioiodine Treatment on Female Fertility in Survivors of Childhood Differentiated Thyroid Carcinoma

Author

Nies, M., Cantineau, A.E.P., Arts, E., Berg, M.H. van den, Leeuwen, F.E. van, Kobold, A.C., Hesselink, M.S. Klein, Burgerhof, J.G., Brouwers, A.H., Dam, E. van, Havekes, B., Heuvel-Eibrink, M.M. van den, Corssmit, E.P.M., Kremer, L.C., Netea-Maier, R.T., Pal, H.J. van der, Peeters, R.P., Plukker, J.T., Ronckers, C.M., Santen, H.M. van, Horst-Schrivers, Anouk N. van de, Tissing, W.J., Bocca, G., Dulmen-den Broeder, E. van, Links, T.P., Nies, M., Cantineau, A.E.P., Arts, E., Berg, M.H. van den, Leeuwen, F.E. van, Kobold, A.C., Hesselink, M.S. Klein, Burgerhof, J.G., Brouwers, A.H., Dam, E. van, Havekes, B., Heuvel-Eibrink, M.M. van den, Corssmit, E.P.M., Kremer, L.C., Netea-Maier, R.T., Pal, H.J. van der, Peeters, R.P., Plukker, J.T., Ronckers, C.M., Santen, H.M. van, Horst-Schrivers, Anouk N. van de, Tissing, W.J., Bocca, G., Dulmen-den Broeder, E. van, and Links, T.P.

Abstract

Item does not contain fulltext, Background: Differentiated thyroid carcinoma (DTC) during childhood is a rare disease. Its excellent survival rate requires a focus on possible long-term adverse effects. This study aimed to evaluate fertility in female survivors of childhood DTC by assessing various reproductive characteristics combined with anti-Müllerian hormone (AMH) levels (a marker of ovarian reserve). Methods: Female survivors of childhood DTC, diagnosed at ≤18 years of age between 1970 and 2013, were included. Survivors were excluded when follow-up time was less than five years or if they developed other malignancies before or after diagnosis of DTC. Survivors filled out a questionnaire regarding reproductive characteristics (e.g., age at menarche and menopause, pregnancies, pregnancy outcomes, need for assisted reproductive therapy). Survivors aged <18 years during evaluation received an altered questionnaire without questions regarding pregnancy and pregnancy outcomes. These data were combined with information from medical records. AMH levels were measured in serum samples and were compared with AMH levels from 420 women not treated for cancer. Results: Fifty-six survivors with a median age of 31.0 (interquartile range, IQR, 25.1-39.6) years were evaluated after a median follow-up of 15.4 (IQR 8.3-24.7) years. The median cumulative dose of (131)I administered was 7.4 (IQR 3.7-13.0) GBq/200.0 (IQR 100.0-350.0) mCi. Twenty-five of the 55 survivors aged 18 years or older during evaluation reported 64 pregnancies, 45 of which resulted in live birth. Of these 55, 10.9% visited a fertility clinic. None of the survivors reported premature menopause. Age at AMH evaluation did not differ between DTC survivors and the comparison group (p = 0.268). Median AMH levels did not differ between DTC survivors and the comparison group [2.0 (IQR 1.0-3.7) μg/L vs. 1.6 (IQR 0.6-3.1) μg/L, respectively, p = 0.244]. The cumulative dose of (131)I was not associated with AMH levels in DTC survivors (r(s) = 0.210, p

Published

2020

35. The Genetic Basis of Thyroid Function: Novel Findings and New Approaches

Author

Kus, A., Chaker, L., Teumer, A., Peeters, R.P., Medici, M., Kus, A., Chaker, L., Teumer, A., Peeters, R.P., and Medici, M.

Abstract

Contains fulltext : 220563.pdf (publisher's version ) (Closed access), CONTEXT: Genetic factors are major determinants of thyroid function. Over the last two decades, multiple genetic variants have been associated with variations in normal range thyroid function tests. Most recently, a large-scale genome-wide association study (GWAS) doubled the number of known variants associated with normal range thyrotropin (TSH) and free thyroxine (FT4) levels. EVIDENCE ACQUISITION: This review summarizes the results of genetic association studies on normal range thyroid function and explores how these genetic variants can be used in future studies to improve our understanding of thyroid hormone regulation and disease. EVIDENCE SYNTHESIS: Serum TSH and FT4 levels are determined by multiple genetic variants on virtually all levels of the hypothalamus-pituitary-thyroid (HPT) axis. Functional follow-up studies on top of GWAS hits has the potential to discover new key players in thyroid hormone regulation, as exemplified by the identification of the thyroid hormone transporter SLC17A4 and the metabolizing enzyme AADAT. Translational studies may use these genetic variants to investigate causal associations between thyroid function and various outcomes in Mendelian Randomization (MR) studies, to identify individuals with an increased risk of thyroid dysfunction, and to predict the individual HPT axis setpoint. CONCLUSIONS: Recent genetic studies have greatly improved our understanding of the genetic basis of thyroid function, and have revealed novel pathways involved in its regulation. In addition, these findings have paved the way for various lines of research that can improve our understanding of thyroid hormone regulation and thyroid diseases, as well as the potential use of these markers in future clinical practice.

Published

2020

36. Overt Thyroid Dysfunction and Anti-Thyroid Antibodies Predict Response to Anti-PD-1 Immunotherapy in Cancer Patients

Author

Basak, E.A., Meer, J.W.M. van der, Hurkmans, D.P., Schreurs, M.W., Hoop, E. de, Veldt, A.A.M. van der, Bins, S., Joosse, A., Koolen, S.L., Debets, R., Peeters, R.P., Aerts, J., Mathijssen, R.H., Medici, M., Basak, E.A., Meer, J.W.M. van der, Hurkmans, D.P., Schreurs, M.W., Hoop, E. de, Veldt, A.A.M. van der, Bins, S., Joosse, A., Koolen, S.L., Debets, R., Peeters, R.P., Aerts, J., Mathijssen, R.H., and Medici, M.

Abstract

Contains fulltext : 225902.pdf (publisher's version ) (Closed access), Background: Thyroid dysfunction is among the most common adverse effects during anti-programmed cell death 1 (PD-1) immunotherapy, and alongside correlations with elevated anti-thyroid antibodies (ATAb), studies have found correlations with survival. However, the exact relations remain to be clarified. We, therefore, aimed at clarifying the relationship between thyroid dysfunction, ATAbs, and survival in anti-PD-1 treated cancer patients. Methods: We included 168 patients with nonsmall-cell lung carcinoma, renal cell carcinoma, and metastatic melanoma treated with nivolumab or pembrolizumab. Thyrotropin and free T4 (fT4) levels were measured before each anti-PD-1 infusion. ATAb levels (anti-thyroid peroxidase [TPO] and anti-thyroglobulin [Tg]) were measured at baseline and after two months of treatment. Although the vast majority of patients had detectable levels of ATABs, only a few patients had positive ATAbs when using conventional cut-offs. To study the consequences of detectable ATABs, the cut-off levels were a priori set at the median concentrations at baseline in the study population. Tumor progression was classified according to RECIST v1.1. Results: Patients who acquired overt thyroid dysfunction during treatment had significantly higher overall survival (OS) (hazard ratio [HR] = 0.18 confidence interval [CI: 0.04-0.76]; p = 0.020) and progression-free survival (PFS) (HR = 0.39 [0.15-0.998]; p = 0.050) than patients without thyroid dysfunction with 1-year OS rates of 94% vs. 59% and 1-year PFS rates of 64% vs. 34%. During treatment, patients with ATAb levels above the median had a higher OS (HR = 0.39 [0.21-0.72]; p = 0.003) and PFS (HR = 0.52 [0.33-0.81]; p = 0.004) than patients with ATAb levels below the median, with 1-year OS rates of 83% vs. 49% and PFS rates of 54% vs. 20%, respectively. When analyzing ATAb levels over time, patients with a persistent ATAb level above the median had a higher OS (HR = 0.41 [0.19-0.89], p = 0.025) and PFS (HR = 0.54 [0.

Published

2020

37. The synthesis of 13C6-labeled L-thyronine, 3,5-diiodothyronine, 3,3′,5-triiodothyroacetic acid and 3,3′,5,5′-tetraiodothyroacetic acid

Author

Pilzak, G.S. (Gregor S.), Jongejan, R.M.S. (Rutchanna M.S.), van den Bergh, T. (Toine), Peeters, R.P. (Robin), Meulemans, T. (Tommi), Rijke, Y.B. (Yolanda) de, Pilzak, G.S. (Gregor S.), Jongejan, R.M.S. (Rutchanna M.S.), van den Bergh, T. (Toine), Peeters, R.P. (Robin), Meulemans, T. (Tommi), and Rijke, Y.B. (Yolanda) de

Abstract

The effects of thyroid hormone metabolites (THMs) other than T3, rT3 and T4 are largely unknown, partially due to the lack of adequate methods. For adequate analysis, internal standards for all THMs are essential, but unfortunately not commercially available. Reported approaches for the synthesis of T0, 3,5-T2, TA3 and TA4 lack sensitivity and/or are not adaptable for 13C6-labeled analogues. In this paper, we describe the synthesis of four 13C6-labeled THMs, T0-13C6, 3,5-T2-13C6, TA3-13C6, TA4-13C6. Starting with 13C6-bromo-benzene, a short and versatile synthesis route was developed in which the formation of the diphenyl ether by a Chan-Lam coupling reaction was fundamental.

Published

2020

38. Thyroid Hormone Transporters

Author

Groeneweg, S. (Stefan), Geest, F.S. (Ferdy) van, Peeters, R.P. (Robin), Heuer, H. (Heike), Visser, W.E. (Edward), Groeneweg, S. (Stefan), Geest, F.S. (Ferdy) van, Peeters, R.P. (Robin), Heuer, H. (Heike), and Visser, W.E. (Edward)

Abstract

Thyroid hormone transporters at the plasma membrane govern intracellular bioavailability of thyroid hormone. Monocarboxylate transporter (MCT) 8 and MCT10, organic anion transporting polypeptide (OATP) 1C1, and SLC17A4 are currently known as transporters displaying the highest specificity toward thyroid hormones. Structure-function studies using homology modeling and mutational screens have led to better understanding of the molecular basis of thyroid hormone transport. Mutations in MCT8 and in OATP1C1 have been associated with clinical disorders. Different animal models have provided insight into the functional role of thyroid hormone transporters, in particular MCT8. Different treatment strategies for MCT8 deficiency have been explored, of which thyroid hormone analogue therapy is currently applied in patients. Future studies may reveal the identity of as-yet-undiscovered thyroid hormone transporters. Complementary studies employing animal and human models will provide further insight into the role of transporters in health and disease. (En

Published

2020

39. Objectives, design and main findings until 2020 from the Rotterdam Study

Author

Ikram, M.Arfan, Brusselle, G., Ghanbari, M., Goedegebure, A., Ikram, M.K., Kavousi, M., Kieboom, B.C., Klaver, C.C.W., Knegt, R.J. de, Luik, A.I., Nijsten, T.E., Peeters, R.P., Rooij, F.J. van, Stricker, B.H., Uitterlinden, A.G., Vernooij, M.W., Voortman, T., Ikram, M.Arfan, Brusselle, G., Ghanbari, M., Goedegebure, A., Ikram, M.K., Kavousi, M., Kieboom, B.C., Klaver, C.C.W., Knegt, R.J. de, Luik, A.I., Nijsten, T.E., Peeters, R.P., Rooij, F.J. van, Stricker, B.H., Uitterlinden, A.G., Vernooij, M.W., and Voortman, T.

Abstract

Contains fulltext : 220949.pdf (Publisher’s version ) (Open Access), The Rotterdam Study is an ongoing prospective cohort study that started in 1990 in the city of Rotterdam, The Netherlands. The study aims to unravel etiology, preclinical course, natural history and potential targets for intervention for chronic diseases in mid-life and late-life. The study focuses on cardiovascular, endocrine, hepatic, neurological, ophthalmic, psychiatric, dermatological, otolaryngological, locomotor, and respiratory diseases. As of 2008, 14,926 subjects aged 45 years or over comprise the Rotterdam Study cohort. Since 2016, the cohort is being expanded by persons aged 40 years and over. The findings of the Rotterdam Study have been presented in over 1700 research articles and reports. This article provides an update on the rationale and design of the study. It also presents a summary of the major findings from the preceding 3 years and outlines developments for the coming period.

Published

2020

40. Response to Letter to the Editor: Association of Maternal Iodine Status With Child IQ: A Meta-Analysis of Individual Participant Data

Author

Levie, D. (Deborah), Bath, S.C. (Sarah C.), Dineva, M. (Mariana), Tiemeier, H.W. (Henning), Rayman, M.P. (Margaret), Guxens Junyent, M. (Mònica), Peeters, R.P. (Robin), Korevaar, T.I.M. (Tim), Levie, D. (Deborah), Bath, S.C. (Sarah C.), Dineva, M. (Mariana), Tiemeier, H.W. (Henning), Rayman, M.P. (Margaret), Guxens Junyent, M. (Mònica), Peeters, R.P. (Robin), and Korevaar, T.I.M. (Tim)

Published

2020

41. Thyroid Function Affects the Risk of Stroke via Atrial Fibrillation: A Mendelian Randomization Study

Author

Marouli, E. (Eirini), Kus̈, A. (Aleksander), Del Greco M, F. (Fabiola), Chaker, L. (Layal), Peeters, R.P. (Robin), Teumer, A. (Alexander), Deloukas, P. (Panos), Medici, M. (Marco), Marouli, E. (Eirini), Kus̈, A. (Aleksander), Del Greco M, F. (Fabiola), Chaker, L. (Layal), Peeters, R.P. (Robin), Teumer, A. (Alexander), Deloukas, P. (Panos), and Medici, M. (Marco)

Abstract

CONTEXT: Observational studies suggest that variations in normal range thyroid function are associated with cardiovascular diseases. However, it remains to be determined whether these associations are causal or not. OBJECTIVE: To test whether genetically determined variation in normal range thyroid function is causally associated with the risk of stroke and coronary artery disease (CAD) and investigate via which pathways these relations may be mediated. DESIGN, SETTING, AND PARTICIPANTS: Mendelian randomization analyses for stroke and CAD using genetic instruments associated with normal range thyrotropin (TSH) and free thyroxine levels or Hashimoto's thyroiditis and Graves' disease. The potential mediating role of known stroke and CAD risk factors was examined. Publicly available summary statistics data were used. MAIN OUTCOME MEASURES: Stroke or CAD risk per genetically predicted increase in TSH or FT4 levels. RESULTS: A 1 standard deviation increase in TSH was associated with a 5% decrease in the risk of stroke (odds ratio [OR], 0.95; 95% confidence interval [CI], 0.91-0.99; P = 0.008). Multivariable MR analyses indicated that this effect is mainly mediated via atrial fibrillation. MR analyses did not show a causal association between normal range thyroid function and CAD. Secondary analyses showed a causal relationship between Hashimoto's thyroiditis and a 7% increased risk of CAD (OR, 1.07; 95% CI, 1.01-1.13; P = 0.026), which was mainly mediated via body mass index. CONCLUSION: These results provide important new insights into the causal relationships and mediating pathways between thyroid function, stroke, and CAD. We identify variation in normal range thyroid function and Hashimoto's thyroiditis as risk factors for stroke and CAD, respectively.

Published

2020

42. The genetic basis of thyroid function: Novel findings and new approaches

Author

Kus̈, A. (Aleksander), Chaker, L. (Layal), Teumer, A. (Alexander), Peeters, R.P. (Robin), Medici, M. (Marco), Kus̈, A. (Aleksander), Chaker, L. (Layal), Teumer, A. (Alexander), Peeters, R.P. (Robin), and Medici, M. (Marco)

Abstract

Context: Genetic factors are major determinants of thyroid function. Over the last two decades,multiple genetic variants have been associated with variations in normal range thyroid functiontests. Most recently, a large-scale genome-wide association study (GWAS) doubled the number ofknown variants associated with normal range thyrotropin (TSH) and free thyroxine (FT4) levels.Evidence Acquisition: This review summarizes the results of genetic association studies onnormal range thyroid function and explores how these genetic variants can be used in futurestudies to improve our understanding of thyroid hormone regulation and disease.Evidence Synthesis: Serum TSH and FT4 levels are determined by multiple genetic variantson virtually all levels of the hypothalamus-pituitary-thyroid (HPT) axis. Functional followup studies on top of GWAS hits has the potential to discover new key players in thyroidhormone regulation, as exemplified by the identification of the thyroid hormone transporterSLC17A4 and the metabolizing enzyme AADAT. Translational studies may use these geneticvariants to investigate causal associations between thyroid function and various outcomes inMendelian Randomization (MR) studies, to identify individuals with an increased risk of thyroiddysfunction, and to predict the individual HPT axis setpoint.Conclusions: Recent genetic studies have greatly

Published

2020

43. Insights into the mechanism of MCT8 oligomerization

Author

Groeneweg, S. (Stefan), van den Berge, A.P.J., Lima De Souza, E.C. (Elaine), Meima, M.E. (Marcel), Peeters, R.P. (Robin), Visser, W.E. (Edward), Groeneweg, S. (Stefan), van den Berge, A.P.J., Lima De Souza, E.C. (Elaine), Meima, M.E. (Marcel), Peeters, R.P. (Robin), and Visser, W.E. (Edward)

Abstract

Mutations in the thyroid hormone transporter monocarboxylate transporter 8 (MCT8) result in MCT8 deficiency, characterized by severe intellectual and motor disability. The MCT8 protein is predicted to have 12 transmembrane domains (TMDs) and is expressed as monomers, homodimers, and homo-oligomers. This study aimed to delineate the mechanism of

Published

2020

44. An overview of clinical activities in Endo-ERN: the need for alignment of future network criteria

Author

de Vries, F. (Friso), Bruin, M. (Mees), Cersosimo, A. (Angelica), van Beuzekom, C.N. (Charlotte N.), Ahmed, S.F. (Sayed), Peeters, R.P. (Robin), Biermasz, N.R., Hiort, O. (Olaf), Pereira, A.M. (Alberto), de Vries, F. (Friso), Bruin, M. (Mees), Cersosimo, A. (Angelica), van Beuzekom, C.N. (Charlotte N.), Ahmed, S.F. (Sayed), Peeters, R.P. (Robin), Biermasz, N.R., Hiort, O. (Olaf), and Pereira, A.M. (Alberto)

Abstract

Objective: Given that volumes of patients and interventions are important criteria to qualify as a reference centre (RC) for the European Reference Network on Rare Endocrine Conditions (Endo-ERN), the present study aimed to evaluate the data that were reported in the original application against subsequent assessments of activity and review the criteria that may define RCs using two main thematic groups (MTGs): Pituitary and Thyroid, as examples. Methods: Review of content in application forms and continuous monitoring data and of a survey distributed to RCs. A list of 'key procedures' for the assessment of performance of RCs was composed with the help of the Pituitary and Thyroid MTG chairs. Results: In the original application, the number of undefined procedures ranged from 20 to 5500/year (Pituitary) and from 10 to 2700/year (phyroid) between applicants. In the survey, the number of key procedures per centre ranged from 18 to 150/year (Pituitary) and from 20 to 1376/year (Thyroid). The median numbers of new patients reported in the continuous monitoring program were comparable with the application and survey; however, some centres reported large variations. Conclusions: Monitoring of clinical activity in an ERN requires clear definitions that are optimally aligned with clinical practice, diagnosis registration, and hospital IT systems. This is a particular challenge in the rare disease field where the centre may also provide expert input in collaboration with local hospitals. Application of uniform definitions, in addition to condition-specific clinical benchmarks, which can include patient-reported- as well as clinician-reported outcome measures, is urgently needed to allow benchmarking of care across Endo-ERN.

Published

2020

45. A Mass Spectrometry-Based Panel of Nine Thyroid Hormone Metabolites in Human Serum

Author

Jongejan, R.M.S., Klein, T. (Theo), Meima, M.E. (Marcel), Visser, W.E. (Edward), Heerebeek, R. (Ramona) van, Luider, T.M. (Theo), Peeters, R.P. (Robin), Rijke, Y.B. (Yolanda) de, Jongejan, R.M.S., Klein, T. (Theo), Meima, M.E. (Marcel), Visser, W.E. (Edward), Heerebeek, R. (Ramona) van, Luider, T.M. (Theo), Peeters, R.P. (Robin), and Rijke, Y.B. (Yolanda) de

Abstract

BACKGROUND: While thyroxine (T4), 3,3’,5-triiodothyronine (T3), and 3,3’,5’-triiodothyronine (rT3) have routine methods available for evaluating patients with suspected thyroid disease, appropriate methods for the measurement of other thyroid hormone metabolites (THMs) are lacking. The effects of other iodothyronines or iodothyroacetic acids are therefore less explored. To better understand the (patho)physiological role of THMs, a robust method to measure iodothyronines and iodothyroacetic acids in serum in a single analysis is needed, including associated reference intervals. METHODS: Clinical and Laboratory Standards Institute guidelines, European Medicines Agency guidelines, and the National Institute of Standards and Technology protocol were used for the method validation and reference intervals. Reference intervals were determined in 132 healthy males and 121 healthy females. Serum samples were deproteinized with acetonitrile, followed by anion-exchange solid phase extraction and analysis with LC-MS/MS, using eight 13C6-internal standards RESULTS: The analytical method validation was performed for all nine THMs. Reference intervals (2.5th to 97.5th percentile) were determined for L-thyronine (4.9–11.3 ng/dL), 3-monoiodothyronine (0.06 –0.41 ng/ dL), 3,5-diiodothyronine (<0.13 ng/dL), 3,3’-diiodothyronine (0.25–0.77 ng/dL), T3 (66.4–129.9 ng/dL), rT3 (15.0–64

Published

2020

46. Removing critical gaps in chemical test methods by developing new assays for the identification of thyroid hormone system-disrupting chemicals—the athena project

Author

Kortenkamp, A. (Andreas), Axelstad, M. (M.), Baig, A.H. (Asma H.), Bergman, A. (Åke), Bornehag, C.-G. (Carl-Gustaf), Cenijn, P. (Peter), Christiansen, S. (S.), Demeneix, B.A. (Barbara), Derakhshan, A. (Arash), Fini, J.-B. (Jean-Baptiste), Frädrich, C. (Caroline), Hamers, T. (Timo), Hellwig, L. (Lina), Köhrle, J. (Josef), Korevaar, T.I.M. (Tim), Lindberg, J. (Johan), Martin, O. (Olwenn), Meima, M.E. (Marcel), Mergenthaler, P. (Philipp), Nikolov, N. (Nikolai), Pasquier, D.D. (David Du), Peeters, R.P. (Robin), Platzack, B. (Bjorn), Ramhøj, L. (Louise), Remaud, S. (Sylvie), Renko, K. (Kostja), Scholze, M. (M.), Stachelscheid, H. (Harald), Svingen, T. (Terje), Wagenaars, F. (Fabian), Wedebye, E.B. (Eva Bay), Zoeller, R.T. (R. Thomas), Kortenkamp, A. (Andreas), Axelstad, M. (M.), Baig, A.H. (Asma H.), Bergman, A. (Åke), Bornehag, C.-G. (Carl-Gustaf), Cenijn, P. (Peter), Christiansen, S. (S.), Demeneix, B.A. (Barbara), Derakhshan, A. (Arash), Fini, J.-B. (Jean-Baptiste), Frädrich, C. (Caroline), Hamers, T. (Timo), Hellwig, L. (Lina), Köhrle, J. (Josef), Korevaar, T.I.M. (Tim), Lindberg, J. (Johan), Martin, O. (Olwenn), Meima, M.E. (Marcel), Mergenthaler, P. (Philipp), Nikolov, N. (Nikolai), Pasquier, D.D. (David Du), Peeters, R.P. (Robin), Platzack, B. (Bjorn), Ramhøj, L. (Louise), Remaud, S. (Sylvie), Renko, K. (Kostja), Scholze, M. (M.), Stachelscheid, H. (Harald), Svingen, T. (Terje), Wagenaars, F. (Fabian), Wedebye, E.B. (Eva Bay), and Zoeller, R.T. (R. Thomas)

Abstract

The test methods that currently exist for the identification of thyroid hormone system-disrupting chemicals are woefully inadequate. There are currently no internationally validated in vitro assays, and test methods that can capture the consequences of diminished or enhanced thyroid hormone action on the developing brain are missing entirely. These gaps put the public at risk and risk assessors in a difficult position. Decisions about the status of chemicals as thyroid hormone system disruptors currently are based on inadequate toxicity data. The ATHENA project (Assays for the identification of Thyroid Hormone axis-disrupting chemicals: Elaborating Novel Assessment strategies) has been conceived to address these gaps. The project will develop new test methods for the disruption of thyroid hormone transport across biological barriers such as the blood–brain and blood–placenta barriers. It will also devise methods for the disruption of the downstream effects on the brain. ATHENA will deliver a testing strategy based on those elements of the thyroid hormone system that, when disrupted, could have the greatest impact on diminished or enhanced thyroid hormone action and therefore should be targeted through effective testing. To further enhance the impact of the ATHENA test method developments, the project will develop concepts for better international collaboration and development in the area of thyroid hormone system disruptor identification and regulation.

Published

2020

47. Objectives, design and main findings until 2020 from the Rotterdam Study

Author

Ikram, M.A. (Arfan), Brusselle, G.G. (Guy), Ghanbari, M. (Mohsen), Goedegebure, A. (Andre), Ikram, M.K. (Kamran), Kavousi, M. (Maryam), Kieboom, B.C.T. (Brenda), Klaver, C.C.W. (Caroline), Knegt, R.J. (Robert) de, Luik, A.I. (Annemarie), Nijsten, T.E.C. (Tamar), Peeters, R.P. (Robin), Rooij, F.J.A. (Frank) van, Stricker, B.H.Ch. (Bruno), Uitterlinden, A.G. (André), Vernooij, M.W. (Meike), Voortman, R.G. (Trudy), Ikram, M.A. (Arfan), Brusselle, G.G. (Guy), Ghanbari, M. (Mohsen), Goedegebure, A. (Andre), Ikram, M.K. (Kamran), Kavousi, M. (Maryam), Kieboom, B.C.T. (Brenda), Klaver, C.C.W. (Caroline), Knegt, R.J. (Robert) de, Luik, A.I. (Annemarie), Nijsten, T.E.C. (Tamar), Peeters, R.P. (Robin), Rooij, F.J.A. (Frank) van, Stricker, B.H.Ch. (Bruno), Uitterlinden, A.G. (André), Vernooij, M.W. (Meike), and Voortman, R.G. (Trudy)

Abstract

The Rotterdam Study is an ongoing prospective cohort study that started in 1990 in the city of Rotterdam, The Netherlands. The study aims to unravel etiology, preclinical course, natural history and potential targets for intervention for chronic diseases in mid-life and late-life. The study focuses on cardiovascular, endocrine, hepatic, neurological, ophthalmic, psychiatric, dermatological, otolaryngological, locomotor, and respiratory diseases.As of 2008, 14,926 subjects aged 45 years or over comprise the Rotterdam Study cohort. Since 2016, the cohort is being expanded by persons aged 40 years and over. The findings of the Rotterdam Study have been presented in over 1700 research articles and reports. This article provides an update on the rationale and design of the study. It also presents a summary of the major findings from the preceding 3 years and outlines developments for the coming period.

Published

2020

48. Clinical and functional consequences of C-terminal variants in MCT8

Author

Geest, F.S. (Ferdy) van, Meima, M.E. (Marcel), Stuurman, K.E. (Kyra), Wolf, N.I. (Nicole), Knaap, M.S. (Marjo) van der, C.F. (Cláudia) Lorea, F.O. (Fabiano) Poswar, F. (Filippo) Vairo, Brunetti-Pierri, N. (Nicola), G. (Gerarda) Cappuccio, P. (Priyanka) Bakhtiani, Munnik, S.A. (Sonja) de, Peeters, R.P. (Robin), Visser, W.E. (Edward), Groeneweg, S. (Stefan), Geest, F.S. (Ferdy) van, Meima, M.E. (Marcel), Stuurman, K.E. (Kyra), Wolf, N.I. (Nicole), Knaap, M.S. (Marjo) van der, C.F. (Cláudia) Lorea, F.O. (Fabiano) Poswar, F. (Filippo) Vairo, Brunetti-Pierri, N. (Nicola), G. (Gerarda) Cappuccio, P. (Priyanka) Bakhtiani, Munnik, S.A. (Sonja) de, Peeters, R.P. (Robin), Visser, W.E. (Edward), and Groeneweg, S. (Stefan)

Published

2020

49. Evaluation of the 2015 ATA Guidelines in Patients With Distant Metastatic Differentiated Thyroid Cancer

Author

Velsen, E.F.S. (Evert) van, Stegenga, M.T. (Merel), Kemenade, F.J. (Folkert) van, Kam, B.L.R. (Boen), Ginhoven, T.M. (Tessa) van, Visser, W.E. (Edward), Peeters, R.P. (Robin), Velsen, E.F.S. (Evert) van, Stegenga, M.T. (Merel), Kemenade, F.J. (Folkert) van, Kam, B.L.R. (Boen), Ginhoven, T.M. (Tessa) van, Visser, W.E. (Edward), and Peeters, R.P. (Robin)

Abstract

CONTEXT: Current American Thyroid Association (ATA) Management Guidelines for the treatment of differentiated thyroid cancer (DTC) stratify patients to decide on additional radioiodine (RAI) therapy after surgery, and to predict recurring/persisting disease. However, studies evaluating the detection of distant metastases and how these guidelines perform in patients with distant metastases are scarce. OBJECTIVE: To evaluate the 2015 ATA Guidelines in DTC patients with respect to 1) the detection of distant metastases, and 2) the accuracy of its Risk Stratification System in patients with distant metastases. PATIENTS AND MAIN OUTCOME MEASURES: We retrospectively included 83 DTC patients who were diagnosed with distant metastases around the time of initial therapy, and a control population of 472 patients (312 low-risk, 160 intermediate-risk) who did not have a routine indication for RAI therapy. We used the control group to assess the percentage of distant metastases that would have been missed if no RAI therapy was given. RESULTS: Two hundred forty-six patients had no routine indication for RAI therapy of which 4 (1.6%) had distant metastases. Furthermore, among the 83 patients with distant metastases, 14 patients (17%) had excellent response, while 55 (67%) had structural disease after a median follow-up of 62 months. None of the 14 patients that achieved an excellent response had a recurrence. CONCLUSIONS: In patients without a routine indication for RAI therapy according to the 2015 ATA Guidelines, distant metastases would initially have been missed in 1.6% of the patients. Furthermore, in patients with distant metastases upon diagnosis, the 2015 ATA Guidelines are an excellent predictor of both persistent disease and recurrence.

Published

2020

50. Association of Exposure to Ambient Air Pollution with Thyroid Function during Pregnancy

Author

Ghassabian, A. Pierotti, L. Basterrechea, M. Chatzi, L. Estarlich, M. Fernández-Somoano, A. Fleisch, A.F. Gold, D.R. Julvez, J. Karakosta, P. Lertxundi, A. Lopez-Espinosa, M.-J. Mulder, T.A. Korevaar, T.I.M. Oken, E. Peeters, R.P. Rifas-Shiman, S. Stephanou, E. Tardón, A. Tiemeier, H. Vrijheid, M. Vrijkotte, T.G.M. Sunyer, J. Guxens, M.

Subjects

endocrine system

Abstract

Importance: Air pollutants interact with estrogen nuclear receptors, but their effect on thyroid signaling is less clear. Thyroid function is of particular importance for pregnant women because of the thyroid's role in fetal brain development. Objective: To determine the short-term association of exposure to air pollution in the first trimester with thyroid function throughout pregnancy. Design, Setting, and Participants: In this cohort study, 9931 pregnant women from 4 European cohorts (the Amsterdam Born Children and Their Development Study, the Generation R Study, Infancia y Medio Ambiente, and Rhea) and 1 US cohort (Project Viva) with data on air pollution exposure and thyroid function during pregnancy were included. The recruitment period for the Amsterdam Born Children and Their Development Study was January 2003 to March 2004; for Generation R, April 2002 to January 2006; for Infancia y Medio Ambiente, November 2003 to January 2008; for Rhea, February 2007 to February 2008; and for Project Viva, April 1999 to November 2002. Statistical analyses were conducted from January 2018 to April 2019. Main Outcomes and Measures: Residential air pollution concentrations (ie, nitrogen oxide and particulate matter [PM]) during the first trimester of pregnancy were estimated using land-use regression and satellite-derived aerosol optical depth models. Free thyroxine, thyrotropin, and thyroid peroxidase antibody levels were measured across gestation. Hypothyroxinemia was defined as free thyroxine below the fifth percentile of the cohort distribution with normal thyrotropin levels, following the American Thyroid Association guidelines. Results: Among 9931 participants, the mean (SD) age was 31.2 (4.8) years, 4853 (48.9%) had more than secondary educational levels, 5616 (56.6%) were nulliparous, 404 (4.2%) had hypothyroxinemia, and 506 (6.7%) tested positive for thyroid peroxidase antibodies. Concentrations of nitrogen dioxide and PM with an aerodynamic diameter of 2.5 μm or less (PM2.5) were lower and had less variation in women in the US cohort than those in European cohorts. No associations of nitrogen oxide with thyroid function were found. Higher exposures to PM2.5 were associated with higher odds of hypothyroxinemia in pregnant women (odds ratio per 5-μg/m3change, 1.21; 95% CI, 1.00-1.47). Although exposure to PM with an aerodynamic diameter of 10 μm or less was not significantly associated with hypothyroxinemia, the coefficient was similar to that for the association of PM2.5 with hypothyroxinemia (odds ratio per 10-μg/m3change, 1.18; 95% CI, 0.93-1.48). Absorbances of PM2.5 and PM with aerodynamic diameter from 2.5 to 10 μg and were not associated with hypothyroxinemia. There was substantial heterogeneity among cohorts with respect to thyroid peroxidase antibodies (P for heterogeneity

Published

2019