Your search keyword '"Kahaly, George J."' showing total 60 results

1. Long-Term Efficacy of Teprotumumab in Thyroid Eye Disease: Follow-Up Outcomes in Three Clinical Trials.

Author

Kahaly, George J., Subramanian, Prem S., Conrad, Elizabeth, Holt, Robert J., and Smith, Terry J.

Subjects

*CLINICAL trials, *THYROID eye disease, *SYMPTOMS, *AUTOIMMUNITY, *EXOPHTHALMOS, *DIPLOPIA

Abstract

Introduction: Thyroid eye disease (TED) is an autoimmune process characterized by extraocular muscle and orbital fat remodeling/expansion resulting in swelling, pain, redness, proptosis, and diplopia. Teprotumumab, an insulin-like growth factor-I receptor inhibitor, demonstrated improvements in TED signs and symptoms in three adequately powered clinical trials of 24 weeks duration. Here we analyze the long-term maintenance of responses with teprotumumab from these trials. Methods: A total of 112 patients who received 7 or 8 infusions of teprotumumab in the Phase 2, Phase 3 (OPTIC study), and OPTIC Extension (OPTIC-X) studies were included in this analysis. Responses, including clinical activity score (CAS ≥2-point improvement), the European Group of Graves' Orbitopathy ophthalmic composite outcome, diplopia (≥1 Gorman grade improvement), proptosis (≥2 mm improvement), Overall (improvement in proptosis + CAS), and disease inactivation (CAS ≤1), were assessed and pooled from study baseline to week 24 (formal study) and up to week 72 (formal follow-up). Graves' Ophthalmopathy quality-of-life (GO-QoL) scores were also assessed. Outcomes included the percentages of observed patient responses from the study baseline. Additional alternative treatments for TED were assessed as a surrogate of persistent benefit from week 24 through week 120 (extended follow-up). Studies differed in the timing of follow-up visits, and data from some visits were unavailable. Results: At week 72, 52/57 (91.2%), 51/57 (89.5%), 35/48 (72.9%), 38/56 (67.9%), and 37/56 (66.1%) of patients were responders for CAS, composite outcome, diplopia, proptosis, and Overall response, respectively. The mean reduction in proptosis was 2.68 mm (SD 1.92, n = 56), mean GO-QoL improvement was 15.22 (SE 2.82, n = 56), and disease inactivation (CAS ≤1) was detected in 40/57 (70.2%). Over 99 weeks following teprotumumab therapy, 19/106 (17.9%) patients reported additional TED therapy during formal and extended follow-up. Conclusion: The long-term response to teprotumumab as observed 51 weeks after therapy was similar to week 24 results in the controlled clinical trials. Inflammatory and ophthalmic composite outcome improvements were seen in 90% of patients with nearly 70% reporting improvement in diplopia and proptosis. Further, 82% of patients in this analysis did not report additional TED treatment (including surgery) over 99 weeks following the final teprotumumab dose. [ABSTRACT FROM AUTHOR]

Published

2024

2. Optimizing levothyroxine treatment for subclinical hypothyroidism during pregnancy.

Author

Gottwald-Hostalek, Ulrike and Kahaly, George J.

Subjects

*MEDICAL personnel, *HYPOTHYROIDISM, *PREGNANCY outcomes, *PREGNANCY, *PREGNANT women

Abstract

The onset of pregnancy places additional stress of the thyroid gland, which must produce additional thyroid hormones to support the developing foetus. Hypothyroidism, including subclinical hypothyroidism (SCH), may appear de novo at this time, or existing thyroid disease may become more severe. Accordingly, SCH is a relatively common complication of up to about 3% of pregnancies, with higher rates in some areas. There is strong evidence from systematic reviews and meta-analyses that uncontrolled SCH is associated with an increased risk of adverse pregnancy outcomes, including miscarriage, preeclampsia, and gestational diabetes. The evidence base also suggests that treatment with levothyroxine (LT4), optimized to control thyrotropin (TSH) to within its pregnancy-specific reference ranges reduces these risks. Current management guidelines provide a clear framework of intervention with LT4 in pregnant women with SCH, especially where TSH is high or where thyroperoxidase autoantibodies are present. Sub-optimal adherence to LT4 is common: it is important that patients take their LT4 correctly and that treating physicians and/or healthcare professionals manage these patients according to the latest management guidelines. The titration of LT4 is likely to occur within a range of LT4 daily doses between 25 µg and 75 µg for the majority of this population. LT4 is a narrow therapeutic index drug and small variations in dosage may produce a clinically significant change in thyroid status. Newer formulations of LT4, engineered to provide more precise and consistent dosing, and with a broad range of tablet strengths, may facilitate the precise titration of the LT4 dose for these patients. [ABSTRACT FROM AUTHOR]

Published

2024

3. Thyrotropin Receptor Antagonism by a Novel Small Molecule: Preclinical In Vitro Observations.

Author

Kahaly, George J., Steiner, Lisa, van der Lee, Miranda M.C., van Achterberg, Tanja A.E., Arends, Roel J., Karstens, Willem F.J., Weirauch, Tobias, Henseling, Jil, Frommer, Lara, Wolf, Jan, and George, Augustine

Subjects

*THYROTROPIN receptors, *SMALL molecules, *CYCLIC adenylic acid, *CHO cell, *MONOCLONAL antibodies, *HYALURONIC acid

Abstract

Background: Treatment of Graves' hyperthyroidism (GH) and Graves' orbitopathy (GO) is far from adequate, and hence, new substances that specifically target the autoantigens in GH/GO are warranted. This study determined the preclinical in vitro efficacy of SYD5115, a novel low-molecular-weight compound that inhibits the thyrotropin receptor (TSH-R). Methods: The TSH-R inhibiting capability of SYD5115 was tested through stimulation of wild-type and chimeric TSH-R expressed in Chinese hamster ovary (CHO) cells using two functional (stimulatory and blocking) cell-based TSH-R-Ab bioassays. TSH-R expressing human orbital fibroblasts, collected from GH+GO patients (GOF), were stimulated with the monoclonal antibody M22 or with stimulatory TSH-R-Ab (TSAb)-positive sera with cyclic adenosine monophosphate (cAMP) or hyaluronic acid (HA) release as readouts. The effect of SYD5115 on the viability of GOF was tested in 4,5-dimethylthiazol-2-yl-2,5-diphenyltetrazolium bromide and scratch cell growth assays. Results: SYD5115 significantly and dose dependently inhibited the TSH-R activation through M22 or TSAb-positive sera in all performed bioassays. Inhibition showed similar levels in the TSAb reporter bioassay and in the cAMP assay with GOF. The % inhibition and compound concentration showed a sigmoidal relationship, with all seven TSAb-positive sera markedly inhibited by SYD5115. An SYD5115 dose-dependent inhibition of M22 (10 ng/mL, 6 hours)-stimulated HA and/or cAMP-release from GOF was observed. Strong SYD5115-induced inhibitions of M22-stimulated cAMP production in GOF were registered with SYD5115 concentrations of 1 (p = 0.0029), 10 (p < 0.0001), 100 (p < 0.0001), 1,000 (p < 0.0001), and 10,000 (p < 0.0001) nM, respectively. SYD5115-induced inhibition of M22-stimulated HA production was noted with SYD5115 concentrations of 100 (p = 0.0392), 1000 (p = 0.0431), and 10,000 (p = 0.0245) nM, respectively. The inhibitory activity of SYD5115 was confirmed in a human osteosarcoma U2OS cell line stably expressing human TSH-R with cAMP as readout. SYD5115 induced 100% inhibition of the M22-induced cAMP levels with a potency of 193 nM. Compared with control, SYD5115 did neither impact the growth nor the migration of cultivated GOF. In addition, SYD5115 did not alter the viability of GOF. Conclusions: SYD5115 blocked M22- and TSAb-induced TSH-R activity with a nanomolar potency in TSH-R-overexpressed CHO cells as well as primary GOF, which demonstrates the ability of this small molecule to block TSH-R overactivity. [ABSTRACT FROM AUTHOR]

Published

2023

4. A novel point-of-care device accurately measures thyrotropin in whole blood, capillary blood and serum.

Author

Kahaly, George J., Lotz, Johannes, Walder, Sara, Hammad, Cara, Krämer, Rebecca, Frommer, Lara, König, Jochem, Wolf, Jan, Gottwald-Hostalek, Ulrike, Urgatz, Bogumila, and Lackner, Karl J.

Subjects

*THYROTROPIN, *THYROID diseases, *POINT-of-care testing, *CAPILLARIES, *RANK correlation (Statistics), *HELLP syndrome

Abstract

Point-of-care (POC) measurement of thyrotropin (TSH) may facilitate prompt diagnosis of thyroid dysfunction. We evaluated the analytical performance of a new POC TSH assay (Wondfo). TSH measurements were made from 730 consecutive, unselected subjects in an outpatient setting, using Wondfo in whole blood, capillary blood and serum or automated reference equipment (serum only). TSH measurements were user-independent. Total intra-and inter-assay variation (CV%) was 12.1 and 16.2%, respectively. Total CV% was 10.6–22.6% and 14.5–21.6% in serum and whole blood, respectively. Linearity was very good. Recovery rate was 97–127%. Prolongation of incubation time increased TSH results of 12% (13%) and 33% (35%) after 2 and 5 additional minutes in serum (blood), respectively. When measured simultaneously in two Wondfo devices, the slope of the regression line was 1.03 (serum) and 1.02 (blood), with Spearman's correlation of 0.99 for both. TSH measurements between Wondfo and reference correlated strongly (r=0.93–0.96), though TSH measurements were lower with Wondfo (slopes of plots of measurements made using the two devices were 0.94 [serum vs. serum]; 0.83 [whole blood vs. serum] and 0.64 [capillary blood vs. serum]). Depending on sample material, TSH in capillary blood was lower vs. whole blood (slope: 0.82) and for whole blood vs. serum (Wondfo and reference method; slope: 0.69 and 0.83). Total haemolysis, but not elevated bilirubin or lipemia, disrupted TSH measurement. The Wondfo system was straightforward to use without need for specialist technicians and demonstrated analytic performance suitable for clinical use for the diagnosis of thyroid dysfunction. [ABSTRACT FROM AUTHOR]

Published

2022

5. Teprotumumab Efficacy, Safety, and Durability in Longer-Duration Thyroid Eye Disease and Re-treatment: OPTIC-X Study.

Author

Douglas, Raymond S., Kahaly, George J., Ugradar, Shoaib, Elflein, Heike, Ponto, Katharina A., Fowler, Brian T., Dailey, Roger, Harris, Gerald J., Schiffman, Jade, Tang, Rosa, Wester, Sara, Jain, Amy Patel, Marcocci, Claudio, Marinò, Michele, Antonelli, Alessandro, Eckstein, Anja, Führer-Sakel, Dagmar, Salvi, Mario, Sile, Saba, and Francis-Sedlak, Megan

Subjects

*THYROID eye disease, *HEARING disorders, *EXOPHTHALMOS, *DISEASE duration, *DISEASE progression

Abstract

To evaluate teprotumumab safety/efficacy in patients with thyroid eye disease (TED) who were nonresponsive or who experienced a disease flare. The Treatment of Graves' Orbitopathy to Reduce Proptosis with Teprotumumab Infusions in an Open-Label Clinical Extension Study (OPTIC-X) is a teprotumumab treatment and re-treatment trial following the placebo-controlled teprotumumab Phase 3 Treatment of Graves' Orbitopathy (Thyroid Eye Disease) to Reduce Proptosis with Teprotumumab Infusions in a Randomized, Placebo-Controlled, Clinical Study (OPTIC) trial. Patients who previously received placebo (n = 37) or teprotumumab (n = 14) in OPTIC. OPTIC nonresponders or those who flared (≥2-mm increase in proptosis, ≥2-point increase in clinical activity score [CAS], or both) during follow-up were treated for the first time (previous placebo patients) or re-treated with teprotumumab in OPTIC-X with 8 infusions over 24 weeks. Proptosis response and safety. Secondary outcomes included proptosis, CAS, subjective diplopia, and quality-of-life. Thirty-three of 37 placebo-treated OPTIC patients (89.2%) became proptosis responders (mean ± standard deviation, –3.5 ± 1.7 mm) when treated with teprotumumab in OPTIC-X. The responses were equivalent to the OPTIC study. In these responders, proptosis, CAS of 0 or 1, and diplopia responses were maintained in 29 of 32 patients (90.6%), 20 of 21 patients (95.2%), and 12 of 14 patients (85.7%), respectively, at follow-up week 48. The median TED duration was 12.9 months versus 6.3 months in those treated with teprotumumab in the OPTIC study. Of the 5 OPTIC teprotumumab nonresponders re-treated in OPTIC-X, 2 responded, 1 showed a proptosis reduction of 1.5 mm from OPTIC baseline, and 2 discontinued treatment early. Of the OPTIC teprotumumab responders who experienced flare, 5 of 8 patients (62.5%) responded when re-treated (mean proptosis reduction, 1.9 ± 1.2 mm from OPTIC-X baseline and 3.3 ± 0.7 mm from OPTIC baseline). Compared with published double-masked trials and their integrated follow-up, no new safety signals were identified. Mild hearing impairment was reported; 4 events occurred during the first course of treatment, and 2 events reoccurred after re-treatment. Patients with TED of longer disease duration responded similarly to those treated earlier in the disease course. Patients with an insufficient initial response or flare may benefit from additional teprotumumab therapy. No new safety risk was identified; however additional postmarketing pharmacovigilance is ongoing. [ABSTRACT FROM AUTHOR]

Published

2022

6. Graves' Autoantibodies Exhibit Different Stimulating Activities in Cultures of Thyrocytes and Orbital Fibroblasts Not Reflected by Clinical Assays.

Author

Krieger, Christine C., Kahaly, George J., Azam, Asma, Klubo-Gwiezdzinska, Joanna, Neumann, Susanne, and Gershengorn, Marvin C.

Subjects

*CYCLIC adenylic acid, *AUTOANTIBODIES, *FIBROBLASTS, *THYROTROPIN receptors, *BINDING site assay

Abstract

Background: The pathogenesis of Graves' hyperthyroidism (GH) and associated Graves' orbitopathy (GO) appears to involve stimulatory autoantibodies (thyrotropin receptor [TSHR]-stimulating antibodies [TSAbs]) that bind to and activate TSHRs on thyrocytes and orbital fibroblasts. In general, measurement of circulating TSHR antibodies by clinical assays correlates with the status of GH and GO. However, most clinical measurements of TSHR antibodies use competitive binding assays that do not distinguish between TSAbs and antibodies that bind to but do not activate TSHRs. Moreover, clinical assays for TSAbs measure stimulation of only one signaling pathway, the cyclic adenosine monophosphate (cAMP)-protein kinase A (PKA) pathway, in engineered cells that are not thyrocytes or orbital fibroblasts. We determined whether measuring TSAbs by a cAMP-PKA readout in engineered cells accurately reveals the efficacies of stimulation by these antibodies on thyrocytes and orbital fibroblasts. Methods: We measured TSAb stimulation of normal human thyrocytes and orbital fibroblasts from patients with GO in primary cultures in vitro. In thyrocytes, we measured secretion of thyroglobulin (TG) and in orbital fibroblasts secretion of hyaluronan (hyaluronic acid [HA]). We also measured stimulation of cAMP production in engineered TSHR-expressing cells in an assay similar to clinical assays. Furthermore, we determined whether there were differences in stimulation of thyrocytes and orbital fibroblasts by TSAbs from patients with GH alone versus from patients with GO understanding that patients with GO have accompanying GH. Results: We found a positive correlation between TSAb stimulation of cAMP production in engineered cells and TG secretion by thyrocytes as well as HA secretion by orbital fibroblasts. However, TSAbs from GH patients stimulated thyrocytes more effectively than TSAbs from GO patients, whereas TSAbs from GO patients were more effective in activating orbital fibroblasts than TSAbs from GH patients. Conclusions: Clinical assays of stimulation by TSAbs measuring activation of the cAMP-PKA pathway do correlate with stimulation of thyrocytes and orbital fibroblasts; however, they do not distinguish between TSAbs from GH and GO patients. In vitro, TSAbs exhibit selectivity in activating TSHRs since TSAbs from GO patients were more effective in stimulating orbital fibroblasts and TSAbs from GH patients were more effective in stimulating thyrocytes. [ABSTRACT FROM AUTHOR]

Published

2022

7. Triiodothyronine alongside levothyroxine in the management of hypothyroidism?

Author

Gottwald-Hostalek, Ulrike and Kahaly, George J.

Subjects

*HYPOTHYROIDISM, *TRIIODOTHYRONINE, *LEVOTHYROXINE, *THYROID hormones, *THYROID gland, *INDIVIDUALIZED medicine

Abstract

The current guideline-based management of hypothyroidism recommends monotherapy with levothyroxine (LT4), titrated to maintain the level of thyrotropin within a euthyroid reference range. This has been successful for most people with hypothyroidism, but a substantial minority still report symptoms of hypothyroidism unexplained by a comorbid medical condition. LT4 is essentially a prodrug for triiodothyronine (T3), the thyroid hormone that acts on target tissues in the brain and the periphery. Thyroid hormone replacement with LT4 alone does not restore physiological tissue levels of thyroid hormones, particularly T3. During the last two decades, much interest has focussed on the potential of combinations of LT4 and T3 to provide a superior outcome to LT4 monotherapy for people with hypothyroidism, especially those with residual symptoms despite thyrotropin-optimized LT4. This review seeks to provide an overview of currently available evidence on combination (LT4 + T3) therapy to be used for personalized medicine in patients with hypothyroidism. A number of randomized, controlled trials (RCTs) have failed to demonstrate superiority for the combination therapy approach, largely due to non-physiological T3 doses. However, patients with hypothyroidism are highly heterogeneous in terms of their residual thyroid function, individual set points for optimal thyroid homeostasis and for the presence or absence of polymorphisms in deiodinase enzymes in tissues that activate and deactivate circulating thyroid hormones. Accordingly, these RCTs may have failed to demonstrate benefits of combination therapy in individual hypothyroid phenotypes. The pharmacokinetics of LT4 and T3 also differ, which is a barrier to their co-administration. Future clinical trials using LT4 + T3 tablets better suited for combination therapy will resolve the outstanding research questions relating to the place of LT4 + T3 combination therapy in the management of hypothyroidism. [ABSTRACT FROM AUTHOR]

Published

2021

8. Methodenvergleich und klinischer Nutzen.

Author

Diana, Tanja and Kahaly, George J.

Subjects

*THYROID antagonists, *THYROGLOBULIN, *BIOLOGICAL assay, *THYROID diseases, *IMMUNOGLOBULINS

Abstract

The article reports that autoimmune thyroid disorders are associated with the presence of antibodies to thyroid antigens such as the thyroid peroxidase, the thyroglobulin and the thyroid stimulating hormone receptor. It notes that these antibodies can be obtained using either a competitive binding immunoassay or a cell-based one bioassays. It states that patients with Hashimoto's thyroiditis (HT) can also develop thyroid-associated orbitopathy.

Published

2020

9. Celiac disease and endocrine autoimmunity – the genetic link.

Author

Kahaly, George J., Frommer, Lara, and Schuppan, Detlef

Subjects

*CELIAC disease, *ENTERITIS, *AUTOIMMUNE diseases, *ENDOCRINE system, *AUTOIMMUNE polyendocrinopathies, *HLA histocompatibility antigens

Abstract

Abstract Celiac disease is a small intestinal inflammatory disease with autoimmune features that is triggered and maintained by the ingestion of the storage proteins (gluten) of wheat, barley and rye. The prevalence of celiac disease is increased in patients with monoglandular and/or polyglandular autoimmunity and their relatives. Between 10 and 30% of patients with celiac disease are thyroid and/or type 1 diabetes antibody positive, while around 5 to 7% of patients with autoimmune thyroid disease and/or type 1 diabetes are IgA anti-tissue transglutaminase antibody positive. The close relationship between celiac disease and endocrine autoimmunity is largely explained by sharing a common genetic background. The HLA antigens DQ2 (DQA1*0501-DQB1*0201) and/or DQ8 (DQA1*0301-DQB1*0302), that are tightly linked to DR3 and DR4, respectively, are the major common genetic predisposition. Moreover, functional single nucleotide polymorphisms of various genes that are involved in immune regulation have been identified as "overlap" susceptibility genes for both celiac disease and monoglandular or polyglandular autoimmunity. While plausible, it remains to be established how far a gluten free diet may prevent or ameliorate glandular autoimmunity. In conclusion, all patients with celiac disease should be screened for type 1 diabetes and/or autoimmune thyroid disease. Conversely, patients with the above autoimmune endocrine disorders should be also screened for celiac disease. [ABSTRACT FROM AUTHOR]

Published

2018

10. Autoantibodies against the calcium-sensing receptor and cytokines in autoimmune polyglandular syndromes types 2, 3 and 4.

Author

Kemp, E. Helen, Kahaly, George J., Porter, Julie A., Frommer, Lara, and Weetman, Anthony P.

Subjects

*AUTOANTIBODIES, *PHYSIOLOGICAL effects of calcium, *AUTOIMMUNE polyendocrinopathies, *IMMUNOGLOBULINS, *AUTOIMMUNE diseases, *PHYSIOLOGY

Abstract

Objective The frequency of autoimmunity against the parathyroid glands in patients with polyglandular autoimmunity that is not due to autoimmune polyendocrine syndrome type 1 ( APS1) is unclear. To investigate this, this study aimed to determine the prevalence of autoantibodies against parathyroid autoantigens, calcium-sensing receptor (Ca SR) and NACHT leucine-rich-repeat protein 5 ( NALP5), in a large group of patients with non- APS1 polyendocrine autoimmunity. Possible occult APS1 was investigated by cytokine autoantibody measurement and AIRE gene analysis. Design, Subjects and Measurements Subjects were 178 patients with APS2, 3 or 4, and 80 healthy blood donors. Autoantibodies against the Ca SR, NALP5 and cytokines were measured by immunoprecipitation, radioligand binding assays or ELISA, respectively. Results Four patient samples (2.2%), but none of the controls, were positive for Ca SR autoantibodies. NALP5 autoantibodies were not detected in any participant. Eleven patients (6.2%) had cytokine autoantibodies, but none of the control samples was positive. None of the patients with cytokine autoantibodies had any known or novel mutations in the AIRE gene. Conclusions The low prevalence of Ca SR autoantibodies indicate a very low level of subclinical parathyroid autoimmunity in APS types 2, 3 and 4. In addition, autoantibodies against cytokines constitute an uncommon feature of non- APS1 polyglandular autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2018

11. Thyroid Inflammation and Immunity During the COVID-19 Pandemic: A Comprehensive Review and Case Study.

Author

Lampropoulou, Eleni, Benz, Claus, Kahaly, George J., and Führer, Dagmar

Subjects

*SARS-CoV-2, *COVID-19 pandemic, *COVID-19, *THYROTROPIN receptors

Abstract

The coronavirus disease 2019 (COVID-19) pandemic caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has led to the development of various vaccines. Reports have emerged suggesting a possible association between SARS-CoV-2 vaccination and the onset of thyroid diseases. This review explores the clinical aspects of thyroid disorders following SARS-CoV-2 vaccination, including a case report of a patient with concomitant subacute thyroiditis (SAT) and Graves' disease (GD) with blocking thyrotropin receptor autoantibodies (TSH-R-Ab) following SARS-CoV-2 vaccination. SAT, characterized by transient inflammation of the thyroid gland, has been reported after SARS-CoV-2 vaccination. GD, an autoimmune hyperthyroidism, has also been observed post-vaccination, often with stimulating TSH-R-Ab. Graves' orbitopathy (GO) has been associated with SARS-CoV-2 vaccination in patients with a history of immune thyroid disease. The unique case underscores a very rare thyroid condition of functional hypothyroidism in possible relation to SARS-CoV-2 vaccination and the usefulness of functional analysis of TSH-R-Ab that can provide valuable insights into disease pathogenesis and help to guide treatment. This review highlights the need for continued monitoring and awareness of potential thyroid-related complications following SARS-CoV-2 vaccination. [ABSTRACT FROM AUTHOR]

Published

2024

12. Teprotumumab for Thyroid-Associated Ophthalmopathy.

Author

Smith, Terry J., Kahaly, George J., Ezra, Daniel G., Fleming, James C., Dailey, Roger A., Tang, Rosa A., Harris, Gerald J., Antonelli, Alessandro, Salvi, Mario, Goldberg, Robert A., Gigantelli, James W., Couch, Steven M., Shriver, Erin M., Hayek, Brent R., Hink, Eric M., Woodward, Richard M., Gabriel, Kathleen, Magni, Guido, and Douglas, Raymond S.

Subjects

*DIABETES complications, *THERAPEUTIC use of monoclonal antibodies, *CLINICAL trials, *COMPARATIVE studies, *EXOPHTHALMOS, *HYPERGLYCEMIA, *IMMUNOLOGICAL adjuvants, *RESEARCH methodology, *MEDICAL cooperation, *MONOCLONAL antibodies, *QUALITY of life, *QUESTIONNAIRES, *RESEARCH, *RESEARCH funding, *SOMATOMEDIN, *THYROID eye disease, *LOGISTIC regression analysis, *EVALUATION research, *RANDOMIZED controlled trials, *BLIND experiment, *DISEASE complications, *THERAPEUTICS

Abstract

Background: Thyroid-associated ophthalmopathy, a condition commonly associated with Graves' disease, remains inadequately treated. Current medical therapies, which primarily consist of glucocorticoids, have limited efficacy and present safety concerns. Inhibition of the insulin-like growth factor I receptor (IGF-IR) is a new therapeutic strategy to attenuate the underlying autoimmune pathogenesis of ophthalmopathy.Methods: We conducted a multicenter, double-masked, randomized, placebo-controlled trial to determine the efficacy and safety of teprotumumab, a human monoclonal antibody inhibitor of IGF-IR, in patients with active, moderate-to-severe ophthalmopathy. A total of 88 patients were randomly assigned to receive placebo or active drug administered intravenously once every 3 weeks for a total of eight infusions. The primary end point was the response in the study eye. This response was defined as a reduction of 2 points or more in the Clinical Activity Score (scores range from 0 to 7, with a score of ≥3 indicating active thyroid-associated ophthalmopathy) and a reduction of 2 mm or more in proptosis at week 24. Secondary end points, measured as continuous variables, included proptosis, the Clinical Activity Score, and results on the Graves' ophthalmopathy-specific quality-of-life questionnaire. Adverse events were assessed.Results: In the intention-to-treat population, 29 of 42 patients who received teprotumumab (69%), as compared with 9 of 45 patients who received placebo (20%), had a response at week 24 (P<0.001). Therapeutic effects were rapid; at week 6, a total of 18 of 42 patients in the teprotumumab group (43%) and 2 of 45 patients in the placebo group (4%) had a response (P<0.001). Differences between the groups increased at subsequent time points. The only drug-related adverse event was hyperglycemia in patients with diabetes; this event was controlled by adjusting medication for diabetes.Conclusions: In patients with active ophthalmopathy, teprotumumab was more effective than placebo in reducing proptosis and the Clinical Activity Score. (Funded by River Vision Development and others; ClinicalTrials.gov number, NCT01868997 .). [ABSTRACT FROM AUTHOR]

Published

2017

13. Type 1 diabetes associated autoimmunity.

Author

Kahaly, George J. and Hansen, Martin P.

Subjects

*TYPE 1 diabetes, *AUTOIMMUNE diseases, *DISEASE prevalence, *CARDIOVASCULAR diseases, *CELIAC disease, *COMORBIDITY

Abstract

Diabetes mellitus is increasing in prevalence worldwide. The economic costs are considerable given the cardiovascular complications and co-morbidities that it may entail. Type 1 diabetes (T1D) is a chronic autoimmune disease characterized by the loss of insulin-producing pancreatic β-cells. The pathogenesis of T1D is complex and multifactorial and involves a genetic susceptibility that predisposes to abnormal immune responses in the presence of ill-defined environmental insults to the pancreatic islets. Genetic background may affect the risk for autoimmune disease and patients with T1D exhibit an increased risk of other autoimmune disorders such as autoimmune thyroid disease, Addison's disease, autoimmune gastritis, coeliac disease and vitiligo. Approximately 20%–25% of patients with T1D have thyroid antibodies, and up to 50% of such patients progress to clinical autoimmune thyroid disease. Approximately 0.5% of diabetic patients have concomitant Addison's disease and 4% have coeliac disease. The prevalence of autoimmune gastritis and pernicious anemia is 5% to 10% and 2.6% to 4%, respectively. Early detection of antibodies and latent organ-specific dysfunction is advocated to alert physicians to take appropriate action in order to prevent full-blown disease. Patients and family members should be educated to be able to recognize signs and symptoms of underlying disease. [ABSTRACT FROM AUTHOR]

Published

2016

14. Response to comment by Smith on the 2021 EUGOGO guidelines.

Author

Kahaly, George J. and Bartalena, Luigi

Subjects

*PHYSICIANS, *MUSCLE motility

Published

2021

15. Selenium and the Course of Mild Graves' Orbitopathy.

Author

Marcocci, Claudio, Kahaly, George J., Krassas, Gerasimos E., Bartalena, Luigi, Prummel, Mark, Stahl, Matthias, Altea, Maria Antonietta, Nardi, Marco, Pitz, Susanne, Boboridis, Kostas, Sivelli, Paolo, von Arx, George, Mourits, Maarten P., Baldeschi, Lelio, Bencivelli, Walter, and Wiersinga, Wilmar

Subjects

*SELENIUM, *GRAVES' disease, *CYTOKINES, *ANTIOXIDANTS, *QUALITY of life, *THERAPEUTICS

Abstract

Background: Oxygen free radicals and cytokines play a pathogenic role in Graves' orbitopathy. Methods: We carried out a randomized, double-blind, placebo-controlled trial to determine the effect of selenium (an antioxidant agent) or pentoxifylline (an antiinflammatory agent) in 159 patients with mild Graves' orbitopathy. The patients were given selenium (100 μg twice daily), pentoxifylline (600 mg twice daily), or placebo (twice daily) orally for 6 months and were then followed for 6 months after treatment was withdrawn. Primary outcomes at 6 months were evaluated by means of an overall ophthalmic assessment, conducted by an ophthalmologist who was unaware of the treatment assignments, and a Graves' orbitopathy–specific quality-of-life questionnaire, completed by the patient. Secondary outcomes were evaluated with the use of a Clinical Activity Score and a diplopia score. Results: At the 6-month evaluation, treatment with selenium, but not with pentoxifylline, was associated with an improved quality of life (P<0.001) and less eye involvement (P=0.01) and slowed the progression of Graves' orbitopathy (P=0.01), as compared with placebo. The Clinical Activity Score decreased in all groups, but the change was significantly greater in the selenium-treated patients. Exploratory evaluations at 12 months confirmed the results seen at 6 months. Two patients assigned to placebo and one assigned to pentoxifylline required immunosuppressive therapy for deterioration in their condition. No adverse events were evident with selenium, whereas pentoxifylline was associated with frequent gastrointestinal problems. Conclusions: Selenium administration significantly improved quality of life, reduced ocular involvement, and slowed progression of the disease in patients with mild Graves' orbitopathy. (Funded by the University of Pisa and the Italian Ministry for Education, University and Research; EUGOGO Netherlands Trial Register number, NTR524.) N Engl J Med 2011;364:1920-31. [ABSTRACT FROM AUTHOR]

Published

2011

16. Bioassays for TSH-receptor autoantibodies: An update

Author

Lytton, Simon D. and Kahaly, George J.

Subjects

*BIOLOGICAL assay, *AUTOANTIBODIES, *THYROTROPIN, *GRAVES' disease, *IMMUNOGLOBULINS, *BIOMARKERS, *T cells, *AUTOIMMUNE thyroiditis, *PATIENTS

Abstract

Abstract: Immunoglobulins in patients with Graves'' disease (GD) that modulate the thyroid stimulating hormone receptor (TSH-R) do so via stimulating cAMP dependent signals (TSI), blocking TSH or inhibition of TSH-receptor activation (TBI) or inducing apoptotic signals. These functional immunoglobulins represent powerful biomarkers of anti-self reactivity in the thyroid and systemic tissues that harbor TSH-R expressing target cells. TSI on thyrocytes induce hyperthyroidism, and TSI on TSH-R fibroblasts of orbital muscles, skin and heart provoke the release of cytokines and antigen-specific T-cell responses leading to systemic inflammation. Bioassays of anti-TSH-R autoantibodies provide decisive information on GD activity. This review examines the past and present bioassays in GD. The critical goal of cell-based anti-TSH-R autoantibody bioassays, to identify the pathogenic immunoglobulins in GD under robust and standardized conditions suitable for routine clinical laboratory practice, is discussed. [Copyright &y& Elsevier]

Published

2010

17. Cardiovascular involvement in patients with different causes of hyperthyroidism.

Author

Biondi, Bernadette and Kahaly, George J.

Subjects

*COMORBIDITY, *HYPERTHYROIDISM, *CARDIOVASCULAR diseases, *HEART diseases, *DISEASE complications, *GRAVES' disease, *ADENOMA, *GOITER

Abstract

Various clinical disorders can cause hyperthyroidism, the effects of which vary according to the patient's age, severity of clinical presentation and association with other comorbidities. Hyperthyroidism is associated with increased morbidity and mortality from cardiovascular disease, although whether the risk of specific cardiovascular complications is related to the etiology of hyperthyroidism is unknown. This article will focus on patients with Graves disease, toxic adenoma and toxic multinodular goiter, and will compare the cardiovascular risks associated with these diseases. Patients with toxic multinodular goiter have a higher cardiovascular risk than do patients with Graves disease, although cardiovascular complications in both groups are differentially influenced by the patient's age and the cause of hyperthyroidism. Atrial fibrillation, atrial enlargement and congestive heart failure are important cardiac complications of hyperthyroidism and are prevalent in patients aged > or = 60 years with toxic multinodular goiter, particularly in those with underlying cardiac disease. An increased risk of stroke is common in patients > 65 years of age with atrial fibrillation. Graves disease is linked with autoimmune complications, such as cardiac valve involvement, pulmonary arterial hypertension and specific cardiomyopathy. Consequently, the etiology of hyperthyroidism must be established to enable correct treatment of the disease and the cardiovascular complications. [ABSTRACT FROM AUTHOR]

Published

2010

18. Polyglandular autoimmune syndromes.

Author

Kahaly, George J.

Subjects

*AUTOIMMUNE diseases, *CHROMOSOMES, *ETIOLOGY of diseases, *IMMUNOLOGICAL tolerance, *GENETIC mutation, *T cell receptors, *AUTOANTIBODIES

Abstract

The polyglandular autoimmune syndromes (PAS) comprise a wide spectrum of autoimmune disorders and are divided into a very rare juvenile (PAS type I) and a relatively common adult type with (PAS II) or without adrenal failure (PAS III). First clinical manifestation of PAS I usually occurs in childhood, whereas PAS II mostly occurs during the third and fourth decades. PAS I is caused by mutations in the autoimmune regulatory (AIRE) gene on chromosome 21 and is inherited in an autosomal recessive manner. Mutations in the AIRE gene result in defect proteins which cause autoimmune destruction of target organs by disturbing the immunological tolerance of the patients. Genetic testing may identify patients with PAS I, but not those with PAS II/III. For PAS II/III, susceptibility genes are known which increase the risk for developing autoimmune disorders, but must not be causative. These are certain HLA genes, the cytotoxic T lymphocyte antigen gene, and the protein tyrosine phosphatase nonreceptor type 22 gene on chromosomes 6, 2 and 1 respectively. Actual diagnosis of PAS involves serological measurement of organ-specific autoantibodies and subsequent functional testing. Management of patients with PAS including their family relatives is best performed in centres with special expertise in autoimmune endocrine disorders. [ABSTRACT FROM AUTHOR]

Published

2009

19. Teprotumumab for Active Thyroid Eye Disease: Reply.

Author

Douglas, Raymond S. and Kahaly, George J.

Published

2020

20. Graves’ Disease.

Author

Kahaly, George J., Olivo, Paul D., Smith, Terry J, and Hegedüs, Laszlo

Subjects

*GRAVES' disease, *AUTOANTIBODIES, *THYROTROPIN receptors, *DIAGNOSIS

Abstract

A letter to the editor is presented in response to the article "Graves' Disease," by Terry J. Smith and Laszlo Hegedüzs in the October 20, 2016 issue.

Published

2017

21. Phase 2/3 results show teprotumumab effective treatment option for TED.

Author

Charters, Lynda and Kahaly, George J.

Subjects

*THERAPEUTIC use of monoclonal antibodies, *THYROID diseases, *THYROID eye disease, *CLINICAL trials, *DISEASE complications

Abstract

The article reports on the phase 2 and 3 clinical trials, which showed the effectiveness of teprotumumab-trbw from Horizon Therapeutics in improving the clinical course of active thyroid eye disease (TED) in the long term. The drug is already approved by the U.S. Food and Drug Administration (FDA). In the trials, Doctor George J. Kahaly and colleagues focused on diplopia and proptosis.

Published

2021

22. Author reply

Author

Ponto, Katharina A. and Kahaly, George J.

Published

2013

23. Thyrotropin Receptor Blocking Antibodies.

Author

Diana, Tanja, Olivo, Paul D., and Kahaly, George J.

Subjects

*THYROTROPIN, *BLOCKING antibodies, *AUTOANTIBODIES, *IMMUNOASSAY, *HYPOTHYROIDISM

Abstract

Autoantibodies (Ab) against the thyroid-stimulating hormone receptor (TSHR) are frequently found in autoimmune thyroid disease (AITD). Autoantibodies to the TSHR (anti-TSHR-Ab) may mimic or block the action of TSH or be functionally neutral. Measurement of anti-TSHR-Ab can be done either via competitive- binding immunoassays or with functional cell-based bioassays. Antibody-binding assays do not assess anti-TSHR-Ab functionality, but rather measure the concentration of total anti-TSHR binding activity. In contrast, functional cell-based bioassays indicate whether anti-TSHR-Ab have stimulatory or blocking activity. Historically bioassays for anti-TSHR-Ab were research tools and were used to study the pathophysiology of Graves' disease and Hashimoto's thyroiditis. In the past, bioassays for anti-TSHR-Abs were laborious and time-consuming and varied widely in performance from laboratory to laboratory. Recent advances in the development of cell-based assays, including the application of molecular engineering, have led to significant improvements that have enabled bioassays to be employed routinely in clinical laboratories. The prevalence and functional significance of TSHR blocking autoantibodies (TBAb) in autoimmune hypothyroidism has been less well investigated compared to TSHR stimulating Ab. There is an increasing body of data, however, that demonstrate the clinical utility and relevance of TBAb, and thus the importance of TBAb bioassays, in the diagnosis and management of patients with AITD. In the present review, we summarize the different methods used to measure TBAb, and discuss their prevalence and clinical relevance. [ABSTRACT FROM AUTHOR]

Published

2018

24. Laboratory Testing in Hyperthyroidism

Author

Grebe, Stefan K.G. and Kahaly, George J.

Subjects

*HYPERTHYROIDISM diagnosis, *CLINICAL pathology, *DIAGNOSTIC ultrasonic imaging, *GRAVES' disease, *CLINICAL medicine, *THYROID diseases

Abstract

Abstract: The clinical diagnosis of hypo- or hyperthyroidism is difficult (full text available online: http://education.amjmed.com/pp1/272). Clinical symptoms and signs are often non-specific, and there is incomplete correlation between structural and functional thyroid gland changes. Laboratory testing is therefore indispensible in establishing the diagnosis of thyrotoxicosis. Similar considerations apply to treatment monitoring. Laboratory testing also plays a crucial role in establishing the most likely cause for a patient''s hyperthyroidism. Finally, during pregnancy, when isotopic scanning is relatively contraindicated and ultrasound is more difficult to interpret, laboratory testing becomes even more important. [Copyright &y& Elsevier]

Published

2012

25. Imaging of Thyrotoxicosis

Author

Sipos, Jennifer A. and Kahaly, George J.

Subjects

*GRAVES' disease, *DIAGNOSTIC ultrasonic imaging, *HYPERTHYROIDISM, *RADIOIMMUNOIMAGING, *CORDOCENTESIS, *AUTOANTIBODIES, *DIAGNOSIS

Abstract

Abstract: The diagnostic algorithm for patients with Graves'' disease frequently involves the use of thyroid autoantibody testing and radioisotope scanning (full text available online: http://education.amjmed.com/pp1/248). However, ultrasound has myriad uses in the evaluation of patients with hyperthyroidism. The purpose of this paper is to review the medical literature outlining the important role that ultrasonography (US) can play in the diagnosis and management of patients with hyperthyroidism. We will make a case for the use of ultrasonography in the initial evaluation of all patients with thyrotoxicosis. This review will delineate the advantages of ultrasonography compared to nuclear medicine imaging in determining the etiology of the hyperthyroidism. The role of sonography in predicting remission and relapse of Graves'' disease will also be examined. Finally, this paper will detail the importance of ultrasonography in the workup of hyperthyroidism during pregnancy. We will also outline its utility for predicting fetal thyroid dysfunction in maternal Graves'' disease without the need for cordocentesis and its attendant complications. [Copyright &y& Elsevier]

Published

2012

26. Autoimmune Thyrotoxicosis: Diagnostic Challenges

Author

Ponto, Katharina A. and Kahaly, George J.

Subjects

*GRAVES' disease, *AUTOIMMUNE thyroiditis, *HYPERTHYROIDISM, *THYROTROPIN, *T cell receptors, *DIAGNOSIS

Abstract

Abstract: Autoimmune thyrotoxicosis or Graves'' disease (GD) is the most common cause of hyperthyroidism in the United States (full text available online: http://education.amjmed.com/pp1/249). GD occurs more often in women (ratio 5:1) and has a population prevalence of 1-2%. A genetic determinant to the susceptibility to GD is suspected because of familial clustering of the disease, a high sibling recurrence risk, and the familial occurrence of thyroid autoantibodies. GD is a systemic autoimmune thyroid disorder characterized by the infiltration of immune effector cells and thyroid-antigen-specific T cells into the thyroid and thyroid stimulating hormone receptor (TSHR) expressing tissues, i.e. orbit, skin, with the production of autoantibodies to well-defined thyroidal antigens. Stimulatory autoantibodies in GD activate the TSHR leading to thyroid hyperplasia and unregulated thyroid hormone production and secretion. Diagnosis of GD is straightforward in a patient with a diffusely enlarged, heterogeneous, hypervascular (increased Doppler flow on neck ultrasound) thyroid gland, associated orbitopathy, biochemically confirmed thyrotoxicosis, positive TSHR autoantibodies, and often a family history of autoimmune disorders. [Copyright &y& Elsevier]

Published

2012

27. Reply

Author

Ponto, Katharina A. and Kahaly, George J.

Published

2012

28. Graves' Disease: Diagnostic and Therapeutic Challenges (Multimedia Activity)

Author

Kahaly, George J., Grebe, Stefan K.G., Lupo, Mark A., McDonald, Nicole, and Sipos, Jennifer A.

Subjects

*GRAVES' disease, *AUTOIMMUNE disease diagnosis, *GENETICS of disease susceptibility, *HYPERTHYROIDISM, *AUTOIMMUNE thyroiditis, *THYROID gland

Abstract

Graves'' disease is the most common cause of hyperthyroidism in the United States. Graves'' disease occurs more often in women with a female:male ratio of 5:1 and a population prevalence of 1% to 2%. A genetic determinant to the susceptibility to Graves'' disease is suspected because of familial clustering of the disease, a high sibling recurrence risk, the familial occurrence of thyroid autoantibodies, and the 30% concordance in disease status between identical twins. Graves'' disease is an autoimmune thyroid disorder characterized by the infiltration of immune effector cells and thyroid antigen–specific T cells into the thyroid and thyroid-stimulating hormone receptor expressing tissues, with the production of autoantibodies to well-defined thyroidal antigens, such as thyroid peroxidase, thyroglobulin, and the thyroid-stimulating hormone receptor. The thyroid-stimulating hormone receptor is central to the regulation of thyroid growth and function. Stimulatory autoantibodies in Graves'' disease activate the thyroid-stimulating hormone receptor leading to thyroid hyperplasia and unregulated thyroid hormone production and secretion. Below-normal levels of baseline serum thyroid-stimulating hormone receptor, normal to elevated serum levels of T4, elevated serum levels of T3 and thyroid-stimulating hormone receptor autoantibodies, and a diffusely enlarged, heterogeneous, hypervascular (increased Doppler flow) thyroid gland confirm diagnosis of Graves'' disease (available at: http://supplements.amjmed.com/2010/hyperthyroid/faculty.php). This Resource Center is also available through the website of The American Journal of Medicine (www.amjmed.com). Click on the “Thyroid/Graves'' Disease” link in the “Resource Centers” section, found on the right side of the Journal homepage. [Copyright &y& Elsevier]

Published

2011

29. A Multicenter, Single-Blind, Case-Control, Immunohistochemical Study of Orbital Tissue in Thyroid Eye Disease.

Author

Hai, Yuan-Ping, Saeed, Mohamed E.M., Ponto, Katharina A., Elflein, Heike M., Lee, Alan Chun Hong, Fang, Sijie, Zhou, Huifang, Frommer, Lara, Längericht, Jan, Efferth, Thomas, and Kahaly, George J.

Subjects

*INSULIN-like growth factor receptors, *SOMATOMEDIN C, *THYROTROPIN receptors, *IMMUNOSTAINING, *CONNECTIVE tissues, *THYROID eye disease

Abstract

Background: Thyroid eye disease (TED) involves several pathogenic pathways and a battery of infiltrating mononuclear cells, cytokines, and chemokines in the orbit. Revealing the main molecules, which play a major role in the pathogenesis of TED, will help developing novel treatment strategies. Methods: In a multicenter, single-blind, case-control study, 60 tissue samples were collected during orbital decompression (44 TED patients) or non-TED related oculoplastic (16 controls) surgeries. Formalin-fixation and paraffin embedding preserved orbital tissue. Tissue sections were immunostained with 18 antibodies by the micro-polymer labeling technique. Immunostaining slides were scanned by Panoramic Desk and blindly evaluated by a user-independent viewer software. Results: Marked lymphocyte infiltration was observed in orbital tissue specimens of patients with clinically active TED (n = 22) and to a much lesser extent in inactive cases (n = 22), while it was absent in controls. Increased vascularity was noted in all samples, with orbital congestion in specimens of clinically active TED. Tissue fibrosis was present in TED samples but not in controls. Immunohistochemistry of orbital tissue clearly differentiated between TED and controls, as well as between active and inactive TED. In contrast to controls and with the exception of cluster of differentiation 20 (CD20), 17 out of 18 antibodies were highly expressed in orbital connective tissue of TED patients. Especially, thyrotropin receptor (TSH-R), insulin-like growth factor 1 receptor (IGF-1R), CD40, cluster of differentiation 40 ligand (CD40L), CD3, CD68, interleukin-17A (IL-17A), IL-23A, IL-1β, IL-4, regulated on activation, normal T cell expressed and secreted (RANTES), macrophage chemoattractant protein 1 (MCP-1), IL-16, and B cell activating factor (BAFF) were overexpressed in clinically active TED (all p < 0.001). Also, the expression of CD40L, IL-17A, IL-23A, IL-6, IL-1β, RANTES, and BAFF was very high (TED/control ratio >3), moderate (ratio >2), and low in active (p < 0.001), inactive TED and controls, respectively. The expression of TSH-R, IGF-1R, CD40, CD40L, CD3, CD68, CD20, IL-17A, IL-23A, RANTES, MCP-1, and BAFF positively and significantly correlated with both serum TSH-R stimulatory antibody concentrations and clinical activity scores while it negatively correlated with TED duration. Orbital irradiation decreased TSH-R (p < 0.001) and IGF-1R expression (p = 0.012); in contrast, neither smoking, age, nor gender did impact immunohistochemical staining. Conclusions: Adaptive and cell-mediated immunity, overexpression of TSH-R/IGF-1R and CD40/CD40L are the relevant pathomechanisms in TED. Targeting these key players in the active phase of the disease offers specific and novel treatment approaches. [ABSTRACT FROM AUTHOR]

Published

2022

30. Imaging of the medial rectus muscle predicts the development of optic neuropathy in thyroid eye disease.

Author

Berger, Marcel, Matlach, Juliane, Pitz, Susanne, Berres, Manfred, Axmacher, Franz, Kahaly, George J., Brockmann, Marc A., and Müller-Eschner, Matthias

Subjects

*THYROID eye disease, *MUSCLE growth, *OPTIC neuritis, *NEUROPATHY, *COMPUTED tomography, *MULTIVARIATE analysis

Abstract

Goal of the study was to evaluate bony orbit remodeling and extraocular muscle (EOM) volume in thyroid eye disease (TED) and their role as predicting factors for development of dysthyroid optic neuropathy (DON). Orbital computed tomography of 92 patients with TED with (76 orbits) or without DON (98 orbits) were retrospectively evaluated. Orbits (n = 40) of subjects without TED served as controls. Measurements of the bony orbit as well as EOM volume were incorporated into a generalized linear mixed model to predict DON. The angle of the medial orbital wall was significantly smaller (p < 0.001) in patients with TED (− 2.3 ± 3.6°) compared to patients with TED + DON (1.0 ± 4.1°). Both groups differed significantly from controls (− 4.2 ± 2.7°). Bowing of the medial orbital wall correlated positively with muscle volume (r = 0.564; p < 0.001). Total EOM volume was significantly larger in TED + DON (7.6 ± 2.5cm3) compared to TED only (5.6 ± 3.0cm3; p < 0.001) or controls (2.6 ± 0.5cm3). Multivariate analysis revealed the medial rectus muscle volume (TED: 1.06 ± 0.48cm3 vs. TED + DON: 2.16 ± 0.84cm3) as the strongest predictor, achieving a specifity of 86.7% and a sensitivity of 73.7% in diagnosing DON in univariate analysis. Though characterized by a wide range of variability, increased medial rectus muscle volume is the strongest predictor for DON in our patient cohort with TED when analyzing a single muscle. [ABSTRACT FROM AUTHOR]

Published

2022

31. SENSITIVITY OF THREE THYROTROPIN RECEPTOR ANTIBODY ASSAYS IN THYROID-ASSOCIATED ORBITOPATHY.

Author

Matutinović, Marija Sarić, Diana, Tanja, Beleslin, Biljana Nedeljković, Ćirić, Jasmina, Žarković, Miloš, Blagojević, Iva Perović, Kahaly, George J., and Ignjatović, Svetlana

Subjects

*THYROTROPIN receptors, *RECEPTOR antibodies, *BINDING site assay, *AUTOANTIBODIES, *BIOLOGICAL assay, *IMMUNOASSAY

Abstract

Background: Thyrotropin receptor autoantibodies (TSH-R-Ab) are indispensable biomarkers in the laboratory assessment of thyroid-associated orbitopathy (TAO). Clinical sensitivity of three different assays for TSH-R-Ab determination was evaluated in patients with TAO. Methods: 87 consecutive TAO patients were enrolled and their serum samples analyzed in parallel with three assays. An ECLIA competitive binding and a chemiluminescent bridge immunoassay were used to measure total and binding TSH-R-Ab concentration, while their functional activity was determined using a stimulatory TSH-R-Ab (TSAb) cellbased bioassay. Results: Compared to the two binding assays (ECLIA p<0.001, bridge p=0.003), the TSAb bioassay was more sensitive pertaining to the positive detection of TSH-R-Ab in TAO patients. No difference (p=0.057) was noted between the ECLIA and bridge assays regarding sensitivity rate. All patients with active and/or moderate-to-severe TAO tested positive in the TSAb bioassay (100% and 100%, respectively), while the positivity rates for bridge and ECLIA binding assays were 89.7% and 82.1% for active TAO, and 90.2% and 86.3% for severe TAO, respectively. Negative predictive values of the bioassay, bridge, and ECLIA assays were 100%, 75%, and 71%, respectively for active TAO, and 100%, 86%, and 71%, respectively for moderate-to-severe TAO. The superiority of the bioassay was most prominent in euthyroid (ET) TAO. Positivity rates of the TSAb bioassay, bridge and ECLIA binding assays were 89.6%, 75%, and 64.6%, respectively for inactive TAO; 86.1%, 69.4%, and 52.8%, respectively for mild TAO; 87.5%, 62.5%, and 12.5%, respectively for euthyroid TAO. The bridge assay correlated better with the ECLIA binding assay (p =0.893, p<0.001), compared to the bioassay (p=0.669, p<0.001). Conclusions: In patients with TAO of various activity and severity, the TSAb bioassay demonstrates a superior clinical performa nce compared to both ECLIA and bridge binding assays. [ABSTRACT FROM AUTHOR]

Published

2022

32. Grave's Orbitopathy A Multidisciplinary Approach - Questions and Answers.

Author

Wiersinga, Wilmar M. and Kahaly, George J.

Subjects

*TISSUES, *NONFICTION, *DISEASES

Published

2017

33. Graves' Orbitopathy: A Multidisciplinary Approach -- Questions and Answers.

Author

Wiersinga, Wilmar M. and Kahaly, George J.

Subjects

*THYROID eye disease, *NONFICTION

Published

2017

34. Redox mechanisms in autoimmune thyroid eye disease.

Author

Buonfiglio, Francesco, Ponto, Katharina A., Pfeiffer, Norbert, Kahaly, George J., and Gericke, Adrian

Subjects

*THYROID eye disease, *TRANSFORMING growth factors, *OXIDATION-reduction reaction, *EYE-sockets, *OXIDATIVE stress, *TOBACCO smoke

Abstract

Thyroid eye disease (TED) is an autoimmune condition affecting the orbit and the eye with its adnexa, often occurring as an extrathyroidal complication of Graves' disease (GD). Orbital inflammatory infiltration and the stimulation of orbital fibroblasts, triggering de novo adipogenesis, an overproduction of hyaluronan, myofibroblast differentiation, and eventual tissue fibrosis are hallmarks of the disease. Notably, several redox signaling pathways have been shown to intensify inflammation and to promote adipogenesis, myofibroblast differentiation, and fibrogenesis by upregulating potent cytokines, such as interleukin (IL)-1β, IL-6, and transforming growth factor (TGF)-β. While existing treatment options can manage symptoms and potentially halt disease progression, they come with drawbacks such as relapses, side effects, and chronic adverse effects on the optic nerve. Currently, several studies shed light on the pathogenetic contributions of emerging factors within immunological cascades and chronic oxidative stress. This review article provides an overview on the latest advancements in understanding the pathophysiology of TED, with a special focus of the interplay between oxidative stress, immunological mechanisms and environmental factors. Furthermore, cutting-edge therapeutic approaches targeting redox mechanisms will be presented and discussed. [Display omitted] • Thyroid Eye Disease is an autoimmune condition that poses a threat to vision and can result in disfigurement. • The disease's pathophysiology is rooted in a complex interplay of autoimmune cascade and redox signaling networks. • Tobacco smoke is a significant risk factor for thyroid eye disease, promoting hypoxia, oxidative stress, and inflammation. • Antioxidants, such as selenium, may have beneficial effects on TED by reducing oxidative stress and inflammation. [ABSTRACT FROM AUTHOR]

Published

2024

35. New insights into the pathogenesis and nonsurgical management of Graves orbitopathy.

Author

Taylor, Peter N., Zhang, Lei, Lee, Richard W. J., Muller, Ilaria, Ezra, Daniel G., Dayan, Colin M., Kahaly, George J., and Ludgate, Marian

Subjects

*THYROID eye disease, *PEOPLE with visual disabilities, *CLINICAL trials, *GLUCOCORTICOIDS, *COMBINATION drug therapy, *MONOCLONAL antibodies, *DISEASE management

Abstract

Graves orbitopathy, also known as thyroid eye disease or thyroid-associated orbitopathy, is visually disabling, cosmetically disfiguring and has a substantial negative impact on a patient's quality of life. There is increasing awareness of the need for early diagnosis and rapid specialist input from endocrinologists and ophthalmologists. Glucocorticoids are the mainstay of treatment; however, recurrence occurs frequently once these are withdrawn. Furthermore, in >60% of cases, normal orbital anatomy is not restored, and skilled rehabilitative surgery is required. Clinical trials have shown that considerable benefit can be derived from the addition of antiproliferative agents (such as mycophenolate or azathioprine) in preventing deterioration after steroid cessation. In addition, targeted biologic therapies have shown promise, including teprotumumab, which reduces proptosis, rituximab (anti-CD20), which reduces inflammation, and tocilizumab, which potentially benefits both of these parameters. Other strategies such as orbital radiotherapy have had their widespread role in combination therapy called into question. The pathophysiology of Graves orbitopathy has also been revised with identification of new potential therapeutic targets. In this Review we provide an up-to-date overview of the field, outline the optimal management of Graves orbitopathy and summarize the research developments in this area to highlight future research questions and direct future clinical trials. [ABSTRACT FROM AUTHOR]

Published

2020

36. Antigen-Specific Immunotherapy with Thyrotropin Receptor Peptides in Graves' Hyperthyroidism: A Phase I Study.

Author

Pearce, Simon H.S., Dayan, Colin, Wraith, David C., Barrell, Kevin, Olive, Natalie, Jansson, Lotta, Walker-Smith, Terrie, Carnegie, Christina, Martin, Keith F., Boelaert, Kristien, Gilbert, Jackie, Higham, Claire E., Muller, Ilaria, Murray, Robert D., Perros, Petros, Razvi, Salman, Vaidya, Bijay, Wernig, Florian, and Kahaly, George J.

Subjects

*THYROTROPIN receptors, *THYROTROPIN, *HYPERTHYROIDISM, *PEPTIDES, *THERAPEUTICS, *IMMUNOTHERAPY, *THYROID hormones

Abstract

Background: Graves' disease is one of the most common autoimmune conditions, but treatment remains imperfect. This study explores the first-in-human use of antigen-specific immunotherapy with a combination of two thyrotropin receptor (TSHR) peptides (termed ATX-GD-59) in Graves' hyperthyroidism. Methods: Twelve participants (11 female) with previously untreated mild to moderate Graves' hyperthyroidism were enrolled in a Phase I open label trial to receive 10 doses of ATX-GD-59 administered intradermally over an 18-week period. Adverse events, tolerability, changes in serum free thyroid hormones, and TSHR autoantibodies were measured. Results: Ten subjects received all 10 doses of ATX-GD-59, five (50%) of whom had free triiodothyronine within the reference interval by the 18-week visit. Two further subjects had improved free thyroid hormones by the end of the study (7/10 responders), whereas three subjects showed worsening thyrotoxicosis during the study. Serum TSHR autoantibody concentrations reduced during the study and correlated with changes in free thyroid hormones (r = 0.85, p = 0.002 for TSHR autoantibody vs. free triiodothyronine). Mild injection-site swelling and pain were the most common adverse events. Conclusions: These preliminary data suggest that ATX-GD-59 is a safe and well-tolerated treatment. The improvement in free thyroid hormones in 70% of subjects receiving the medication suggests potential efficacy as a novel treatment for Graves' hyperthyroidism. [ABSTRACT FROM AUTHOR]

Published

2019

37. Comparison of a Bridge Immunoassay with Two Bioassays for Thyrotropin Receptor Antibody Detection and Differentiation.

Author

Allelein, Stephanie, Diana, Tanja, Ehlers, Margret, Kanitz, Michael, Hermsen, Derik, Schott, Matthias, and Kahaly, George J.

Subjects

*THYROTROPIN receptors, *BIOLOGICAL assay, *IMMUNOASSAY, *RECEPTOR antibodies, *AUTOIMMUNE thyroiditis, *THYROID cancer

Abstract

A rapid and fully automated chemiluminescent immunoassay for the detection of thyrotropin receptor autoantibodies (TSHR-Ab) based on a bridge technology was compared with two bioassays that measure either stimulating (TSAb) or blocking (TBAb) antibodies for the detection and differentiation of TSHR-Ab. A total of 229 patients with various thyroid disorders [151 with Graves' disease (GD), 35 with Hashimoto's thyroiditis (HT), 32 with nodular goiter, and 11 with thyroid cancer] were included. The bridge immunoassay was performed according to the manufacturer's instructions (cut-off>0.55 IU/l). TSAb and TBAb were measured with reporter bioassays. Blocking activity was defined as percent inhibition of luciferase expression relative to induction with bovine TSH alone (cut-off>34% inhibition). TSAb was reported as percentage of specimen-to-reference ratio (> 140 SRR%). The 3 TSHR-Ab assays were negative in all patients with benign euthyroid nodular goiter and differentiated thyroid cancer. In contrast, in all patients with GD, irrespective of the disease duration, TSHR-Ab positivity was present in 127 of 151 (84%) and 140 (93%) for the bridge assay and TSAb bioassay, respectively (p<0.001). Fifteen of 151 (10%) GD samples were positive in the TSAb bioassay but negative in the bridge assay. The bridge assay and the TSAb bioassay correlated positively (r=0.39, p<0.0001) in patients with GD. Both assays detected TSHR-Ab in all ten untreated hyperthyroid patients with GD. In GD patients with a duration of less than six months, 27/29 (93%) and 28 (97%) were TSHR-Ab positive with the bridge and TSAb bioassay, respectively. In comparison, TSHR-Ab were present in two of 35 (6%) and five (14%) HT patients with the bridge and TSAb bio-assay, respectively. TSHR blocking antibodies were present in one (3%) patient with HT and in two (1%) patients with GD; these two GD patients were also bridge assay positive but TSAb bioassay negative. In conclusion, the bridge immunoassay and both bioassays are highly sensitive for the detection of TSHR-Ab. The bridge assay is, however, also positive in the presence of TSHR blocking antibodies detected in a TBAb bioassay. [ABSTRACT FROM AUTHOR]

Published

2019

38. Graves Disease With Thyroid-Stimulating Hormone Receptor-Blocking Autoantibodies During Pregnancy.

Author

Decallonne, Brigitte, Martens, Pieter-Jan, Van den Bruel, Annick, Vanhole, Christine, and Kahaly, George J.

Abstract

I Background: i Graves disease is an autoimmune disease caused by thyroid-stimulating hormone receptor antibodies (TSH-R-Ab), which can be stimulating (TSAb), neutral, or blocking (TBAb). Overview of Neonatal Laboratory Variables and Treatment I Discussion: i Graves disease dominated by TBAbs is rare in the spectrum of autoimmune thyroid diseases. For this reason, we believe that clinicians should consider screening for functional TSH-R-Abs before pregnancy when there is a history of autoimmune thyroid disease or a history of radioactive iodine treatment or thyroidectomy ([4]). [Extracted from the article]

Published

2020

39. Graves Disease With Thyroid-Stimulating Hormone Receptor–Blocking Autoantibodies During Pregnancy.

Author

Decallonne, Brigitte, Martens, Pieter-Jan, Van den Bruel, Annick, Vanhole, Christine, and Kahaly, George J.

Subjects

*AUTOANTIBODIES, *PREGNANCY, *DISEASES, *THYROID diseases, *CONGENITAL hypothyroidism, *GRAVES' disease

Abstract

I Background: i Graves disease is an autoimmune disease caused by thyroid-stimulating hormone receptor antibodies (TSH-R-Ab), which can be stimulating (TSAb), neutral, or blocking (TBAb). Overview of Neonatal Laboratory Variables and Treatment I Discussion: i Graves disease dominated by TBAbs is rare in the spectrum of autoimmune thyroid diseases. For this reason, we believe that clinicians should consider screening for functional TSH-R-Abs before pregnancy when there is a history of autoimmune thyroid disease or a history of radioactive iodine treatment or thyroidectomy ([4]). [Extracted from the article]

Published

2020

40. Evidence That Graves' Ophthalmopathy Immunoglobulins Do Not Directly Activate IGF-1 Receptors.

Author

Marcus-Samuels, Bernice, Krieger, Christine C., Boutin, Alisa, Kahaly, George J., Neumann, Susanne, and Gershengorn, Marvin C.

Subjects

*THYROID eye disease, *IMMUNOGLOBULINS, *THYROTROPIN receptors, *AUTOANTIBODIES, *SOMATOMEDIN C, *PATIENTS

Abstract

Background: Graves' ophthalmopathy (GO) pathogenesis involves thyrotropin (TSH) receptor (TSHR)-stimulating autoantibodies. Whether there are autoantibodies that directly stimulate insulin-like growth factor 1 receptors (IGF-1Rs), stimulating insulin-like growth factor receptor antibodies (IGFRAbs), remains controversial. This study attempted to determine whether there are stimulating IGFRAbs in patients with GO. Methods: Immunoglobulins (Igs) were purified from normal volunteers (NV-Igs) and patients with GO (GO-Igs). The effects of TSH, IGF-1, NV-Igs, and GO-Igs on pAKT and pERK1/2, members of pathways used by IGF-1R and TSHR, were compared in orbital fibroblasts from GO patients (GOFs) and U2OS-TSHR cells overexpressing TSHRs, and U2OS cells that express TSHRs at very low endogenous levels. U2OS-TSHR and U2OS cells were used because GOFs are not easily manipulated using molecular techniques such as transfection, and U2OS cells because they express TSHRs at levels that do not measurably stimulate signaling. Thus, comparing U2OS-TSHR and U2OS cells permits specifically distinguishing signaling mediated by the TSHR and IGF-1R. Results: In GOFs, all GO-Igs stimulated pERK1/2 formation and 69% stimulated pAKT. In U2OS-TSHR cells, 15% of NV-IGs and 83% of GO-Igs stimulated increases in pERK1/2, whereas all NV-Igs and GO-Igs stimulated increases in pAKT. In U2OS cells, 70% of GO-Igs stimulated small increases in pAKT. Knockdown of IGF-1R caused a 65 ± 6.3% decrease in IGF-1-stimulated pAKT but had no effect on GO-Igs stimulation of pAKT. Thus, GO-Igs contain factor(s) that stimulate pAKT formation. However, this factor(s) does not directly activate IGF-1R. Conclusions: Based on the findings analyzing these two signaling pathways, it is concluded there is no evidence of stimulating IGFRAbs in GO patients. [ABSTRACT FROM AUTHOR]

Published

2018

41. Functional TSH receptor antibodies in children with autoimmune thyroid diseases.

Author

Stożek, Karolina, Bossowski, Artur, Ziora, Katarzyna, Bossowska, Anna, Mrugacz, Małgorzata, Noczyńska, Anna, Walczak, Mieczysław, Petriczko, Elżbieta, Pyrżak, Beata, Kucharska, Anna, Szalecki, Mieczysław, Diana, Tanja, and Kahaly, George J.

Subjects

*IMMUNOGLOBULINS, *AUTOIMMUNE diseases, *THYROID diseases, *DISEASE prevalence, *JUVENILE idiopathic arthritis

Abstract

Introduction: The diagnostic value of the level of TSH receptor antibodies (TSHR-Ab) in the population of children with autoimmune thyroid diseases (AITDs) is still unknown. The aim of this cross-sectional study was to investigate the prevalence of TSHR-Ab in a paediatric cohort with AITD and healthy controls.Materials and methods: A total of 240 serum samples were obtained from 205 patients with AITD, type 1 diabetes (T1D), juvenile arthritis (JA), and healthy controls (C). TSHR stimulating (TSI) and -blocking (TBI) immunoglobulins were measured in cell-based bioassays using CHO cells expressing a chimeric TSHR and a c-AMP response-element-dependent luciferase. TSI was reported as percentage of specimen-to-reference ratio (cutoff 140SRR%). Blocking activity was defined as percent inhibition of luciferase expression relative to induction with bovine TSH alone (40% inhibition).Results: C as well as children with JA and T1D were both TSI and TBI negative. In contrast, children with Graves’ disease (GD) were positive for TSI in 47/53 samples (88.7%) while those with thyroidal and orbital GD showed TSI positivity in 95.8% (23/24 samples). Serum TSI levels were SRR% 320 ± 157 and 417 ± 135 in GD and GD + orbitopathy, respectively (p = .02). Children with Hashimoto’s thyroiditis (HT) were TSI positive in 4/83 (4.8%) samples, including two with orbital involvement. TSI levels were increased in HT children with vs. those without eye disease (SRR% 177 vs. 51, p < .01). In comparison, TBI were negative in all tested samples of children with GD but positive in one HT sample.Conclusions: In conclusion, TSI is prevalent in children with GD while the highest serum TSI levels were noted in children with AITD and orbitopathy. [ABSTRACT FROM AUTHOR]

Published

2018

42. Graves’ Orbitopathy.

Author

Hiromatsu, Yuji, Wall, Jack R., Kahaly, George J., and Kakizaki, Hirohiko

Subjects

*GRAVES' disease, *AUTOIMMUNE diseases, *AUTOANTIGENS, *INSULIN-like growth factor receptors, *IODIDE peroxidase

Published

2015

43. Graves’ Orbitopathy.

Author

Hiromatsu, Yuji, Wall, Jack R., Kahaly, George J., and Kakizaki, Hirohiko

Subjects

*GRAVES' disease, *AUTOIMMUNE diseases, *AUTOANTIGENS, *INSULIN-like growth factor receptors, *AUTOANTIBODIES, *BIOMARKERS

Published

2015

44. New levothyroxine formulation meeting 95-105% specification over the whole shelf-life: results from two pharmacokinetic trials.

Author

Gottwald-Hostalek, Ulrike, Uhl, Wolfgang, Wolna, Peter, and Kahaly, George J.

Subjects

*LEVOTHYROXINE, *EXCIPIENTS, *PHARMACOKINETICS, *COMPARATIVE studies, *CROSSOVER trials, *RESEARCH methodology, *MEDICAL cooperation, *PHARMACEUTICAL chemistry, *RESEARCH, *STATISTICAL sampling, *DRUG tablets, *THYROXINE, *EVALUATION research, *RANDOMIZED controlled trials

Abstract

Objective: Small levothyroxine (L-T4) dose changes can lead to significant clinical effects. To ensure thyroid hormone levels are safely maintained, authorities are increasingly adopting stricter potency specifications for L-T4, the most stringent of these being 95-105% of the labeled dose over the whole shelf-life. Levothyroxine sodium (Euthyrox, Eutirox, Lévothyrox ) has been reformulated, and two studies performed, to ensure bioequivalence to the currently marketed formulation and dosage form proportionality of the new formulation.Methods: The bioequivalence study was an open-label, randomized, single-dose, two-period, two-sequence crossover comparing the highest dosage strengths of the currently marketed and the new L-T4 formulation at a total dose of 600 μg. The dosage form proportionality study was an open-label, randomized, three-period, six-sequence crossover, comparing 50 μg, 100 μg, and 200 μg L-T4 tablets, at a total dose of 600 μg. Blood samples were taken at predefined time intervals. Primary outcomes were area under the curve (AUC) and maximum concentration (Cmax) of thyroxine (T4) in plasma.Results: In the bioequivalence study, comparing the T4 profiles for the new and current formulation of L-T4, the geometric least square mean ratio of the baseline-adjusted AUC0-72,adj was 99.3% (90% confidence interval [CI]: 95.6-103.2) and the Cmax,adj was 101.7% (90% CI: 98.8-104.6). Bioequivalence was established if the 90% CI lay within the predefined 0.9-1.11 limits. In the dosage form proportionality study, pairwise comparisons ranged from 99.3% to 104.8%, and all 95% CIs were within the predefined CI range (0.8-1.25): the three dose strengths were dosage form proportional.Conclusions: The new formulation of L-T4 meets the most stringent potency specification guidelines, and has been demonstrated to be bioequivalent to the current formulation and to show dosage form proportionality. The new formulation will enable patients to receive a dose fine tuned to their medical needs, contributing to improved safety in the use of L-T4. [ABSTRACT FROM AUTHOR]

Published

2017

45. Decreased proportions of CD4 + IL17+/CD4 + CD25 + CD127− and CD4 + IL17+/CD4 + CD25 + CD127 − FoxP3+ T cells in children with autoimmune thyroid diseases

Author

Bossowski, Artur, Moniuszko, Marcin, Idźkowska, Ewelina, Grubczak, Kamil, Singh, Paulina, Bossowska, Anna, Diana, Tanja, and Kahaly, George J.

Subjects

*CD40 antigen, *INTERLEUKIN-17, *CD25 antigen, *AUTOIMMUNE thyroiditis, *TH1 cells, *TH2 cells, *THYROID antagonists, *LYMPHOCYTES, *PATIENTS

Abstract

Until now, altered balance of Th1 and Th2 immune cells has been postulated to play an important role in the pathogenesis of autoimmune thyroid diseases (AITD). However, recent studies on thyroid diseases have suggested a new role for Th17 cells that have been classified as a new lineage, distinct from Th1, Th2 and Treg cells. Despite wide interest, the role of Th17 cells in the pathogenesis of inflammatory and autoimmune diseases is still debated. The aim of the study was to estimate the proportions of Th17/Treg T cells in peripheral blood from patients with Graves’ disease (GD;n = 29, mean age 15.4 ± 5.1 years), Hashimoto’s thyroiditis (HT;n = 39, mean age 15.2 ± 4.1 years) and in healthy controls (n = 49, mean age 14.8 ± 3 years). Polychromatic flow cytometry and several fluorochrome-conjugated monoclonal antibodies were applied to delineate Th17 and Treg cells. The analysis of Th17/Treg T cell proportions in peripheral blood from patients with Graves’ disease revealed significantly lower ratios of CD4 + IL17+/CD4 + CD25 + CD127 − (p < 0.0021) and CD4 + IL17+/CD4 + CD25 + CD127 − FoxP3 + (p < 0.0031) than in the control group. In addition, in the case of HT, we observed a significant decrease in the ratios of CD4 + IL17+/CD4 + CD25 + CD127 − (p < 0.0001) and CD4 + IL17+/CD4 + CD25 + CD127 − FoxP3 + (p < 0.0001) T cells in comparison to healthy children. In patients with untreated GD, a statistically significant positive correlation was found between the proportions of CD4 + IL17+/CD4 + CD25 + CD127−, CD4 + IL17+/CD4 + CD25 + CD127 − FoxP3+ T cells and the TRAbs (R = 0.71,p < 0.029;R = 0.72,p < 0.026, respectively) and a positive correlation was noted between the percentage of CD4 + CD − IL − 17 + T cells and the level of TSAbs (R = 0.66,p < 0.037). We conclude that the changes in the proportion of Th17/Treg T cells in peripheral blood and their significant relationship with the level of anti-thyroid antibodies indicate an involvement of these cells in the pathogenesis of AITD. [ABSTRACT FROM PUBLISHER]

Published

2016

46. Analytical Performance and Validation of a Bioassay for Thyroid-Blocking Antibodies.

Author

Diana, Tanja, Yunsheng Li, Olivo, Paul D., Lackner, Karl J., Hannah Kim, Kanitz, Michael, and Kahaly, George J.

Subjects

*BIOLOGICAL assay, *IMMUNOGLOBULINS, *THYROID cancer treatment, *THYROTROPIN receptors, *IMMUNOGLOBULIN G, *AUTOIMMUNE diseases

Abstract

Background and Objective: A cell-based bioassay for the measurement of thyroid blocking autoantibodies (TBAb) has been recently reported. The analytical performance and validation of this bioassay is assessed and described. Methods: Chinese hamster ovary cells expressing a chimeric thyrotropin receptor were treated with bovine (b) TSH and different concentrations of an immunoglobulin G (IgG) monoclonal human TBAb (K1-70). TBAb was measured as a function of luciferase activity relative to bTSH alone and expressed as percent inhibition. Results obtained in the chimeric cell line were compared with those of a wild-type cell line. Analytical performance studies were subsequently performed with the chimeric cell line only. Results: Immunodepletion of K1-70 IgG by using a protein G-Sepharose column showed that positive percent inhibition in the TBAb bioassay was detectable from K1-70 IgG only. The limit of blank was determined to be 12.2%. The limit of detection was 14% inhibition, equivalent to 0.4 ng/mL K1-70, while the limit of quantitation was 22% (coefficient of variation [CV] 12%) equivalent to 0.625 ng/mL K1-70. The dynamic range was between 14 ± 3.7 (mean % inhibition ± standard deviation) and 101 ± 2.6, equivalent to 0.4â€"10 ng/mL K1-70. The linear range was between 22 ± 2.6 and 93 ± 0.6 inhibition, equivalent to 0.625â€"5 ng/mL K1-70. The upper limit of the 99th percent reference range was 34% inhibition. In two laboratories, CV values for the intra- and inter-assay precisions for K1-70 ranged from 2% to 12% and from 1.7% to 14.5%, respectively. For patient sera, the CV values for the intra- and inter-assay precisions ranged from 3% to 9% and from 3% to 11%, respectively. No interference was found when follicle-stimulating hormone, luteinizing hormone, and human chorionic gonadotrophin were tested in the TBAb bioassay. The median of % inhibition values in 40 TBAb positive sera from patients with autoimmune thyroid disease were 93.5 (range 25â€"103) and 92 (range 64â€"107) for the wild type and chimeric cell lines, respectively. Further, all 40 samples of patients with various non-thyroidal autoimmune diseases were TBAb negative. Conclusions: This TBAb bioassay exhibits excellent analytical performance and high level of reproducibility. [ABSTRACT FROM AUTHOR]

Published

2016

47. PREGO (presentation of Graves' orbitopathy) study: changes in referral patterns to European Group On Graves' Orbitopathy (EUGOGO) centres over the period from 2000 to 2012.

Author

Perros, Petros, Žarković, Miloš, Azzolini, Claudio, Ayvaz, Göksun, Baldeschi, Lelio, Bartalena, Luigi, Boschi, Antonella, Bournaud, Claire, Brix, Thomas Heiberg, Covelli, Danila, Ćirić, Slavica, Daumerie, Chantal, Eckstein, Anja, Fichter, Nicole, Führer, Dagmar, Hegedüs, Laszlo, Kahaly, George J., Konuk, Onur, Lareida, Jürg, and Lazarus, John

Subjects

*THYROID eye disease, *DISEASE incidence, *SEVERITY of illness index, *EYE diseases, *OPHTHALMOLOGY

Abstract

Background/aims The epidemiology of Graves' orbitopathy (GO) may be changing. The aim of the study was to identify trends in presentation of GO to tertiary centres and initial management over time. Methods Prospective observational study of European Group On Graves' Orbitopathy (EUGOGO) centres. All new referrals with a diagnosis of GO over a 4-month period in 2012 were included. Clinical and demographic characteristics, referral timelines and initial decisions about management were recorded. The data were compared with a similar EUGOGO survey performed in 2000. Results The demographic characteristics of 269 patients studied in 2012 were similar to those collected in the year 2000, including smoking rates (40.0% vs 40.2%). Mild (60.5% vs 41.2%, p<0.01) and inactive GO (63.2% vs 39.9%, p<0.01) were more prevalent in 2012. The times from diagnosis of thyroid disease to being seen in EUGOGO centres (6 vs 16 months) and from first symptoms of GO (9 vs 16 months) or from diagnosis of GO (6 vs 12 months) to first consultation in EUGOGO centres were shorter in 2012 ( p<0.01). The initial management plans for GO were no different except surgical treatments for patients with mild inactive disease were more frequently offered in the 2012 cohort than in 2000 (27.3% vs 17%, p<0.05), and selenium supplements were offered only in the 2012 cohort (21.2% vs 0%, p<0.01). Conclusions These findings suggest that the clinical manifestations of patients with GO may be changing over time in Europe. [ABSTRACT FROM AUTHOR]

Published

2015

48. Prevalence, Phenotype, and Psychosocial Well-Being in Euthyroid/Hypothyroid Thyroid-Associated Orbitopathy.

Author

Ponto, Katharina A., Binder, Harald, Diana, Tanja, Matheis, Nina, Otto, Anna F., Pitz, Susanne, Pfeiffer, Norbert, and Kahaly, George J.

Subjects

*THYROID eye disease, *HYPOTHYROIDISM, *DISEASE prevalence, *PSYCHOLOGICAL well-being, *QUALITY of life measurement

Abstract

Background: At the onset of thyroid-associated orbitopathy (TAO), most patients are hyperthyroid, while scarce data are available on euthyroid/hypothyroid TAO. The aim of this study was to assess the prevalence, phenotype, and psychosocial burden of patients with initially euthyroid/hypothyroid TAO. Methods: The medical records of 461 consecutive and unselected patients with TAO followed at a specialized joint thyroid-eye clinic were analyzed within this retrospective cross-sectional study. Main outcome measures were the prevalence of initially eu- or hypothyroid TAO as well as ophthalmic signs and symptoms, disease-specific quality of life (QoL), work impairment, and rate of psychotherapy in initially eu-/hypothyroid versus hyperthyroid TAO. Results: The prevalences of eu-/hypothyroid and hyperthyroid TAO were 4.3% ( n=20; [confidence interval, CI, 2.6-6.3]) and 95.7% ( n=441; [9.37-9.74]), respectively. In 12 patients (2.6% [CI 1.3-4.3]), Hashimoto's thyroiditis was present and in 8 (1.7% [CI 0.7-3.0]) no thyroid disease was noted at the time of inclusion. One (0.05%) patient with eu-/hypothyroid TAO and 172 (39%) with hyperthyroid TAO had clinically active TAO ( p=0.001). In eu-/hypothyroid versus hyperthyroid patients, 14 (70%) versus 135 (30.6%) had a mild TAO, 6 (30%) versus 183 (64.2%) a moderate-to-severe TAO, and 0 versus 23 (5.4%) had a sight-threatening TAO ( p<0.001). TAO was asymmetric in 4 (20%) eu-/hypothyroid and in 27 (6.1%) hyperthyroid patients ( p=0.038). Only 5.3% versus 30.2% and 10.5% versus 44.1% of patients with eu-/hypothyroid and hyperthyroid TAO, respectively, were on sick leave ( p=0.003) or work disabled ( p=0.018). QoL was less impaired in eu-/hypothyroid versus hyperthyroid TAO (median visual functioning and appearance scores: 100 versus 75; p<0.001 and 81.25 versus 75; p=0.315). Of patients with eu-/hypothyroid and hyperthyroid TAO, 15% and 20.2% had psychotherapy respectively ( p=0.409). Eu-/hypothyroid TAO was positively (odds ratio 7.05, p=0.060) and negatively (odds ratio: 0.09, p=0.026) associated with a unilateral involvement and thyrotropin-receptor autoantibodies respectively. Conclusions: Compared with hyperthyroid TAO, QoL and working ability are less impaired in eu-/hypothyroid TAO with an often asymmetric and less severe clinical phenotype. [ABSTRACT FROM AUTHOR]

Published

2015

49. Standardization of a Bioassay for Thyrotropin Receptor Stimulating Autoantibodies.

Author

Diana, Tanja, Kanitz, Michael, Lehmann, Markus, Li, Yunsheng, Olivo, Paul D., and Kahaly, George J.

Subjects

*BIOLOGICAL assay, *AUTOANTIBODIES, *THYROTROPIN receptors, *DOSE-response relationship in biochemistry, GREAT Britain. National Institute for Biological Standards & Control

Abstract

Background: Cell-based bioassays for functional thyroid stimulating autoantibodies (TSAb) are sensitive diagnostic tools. However, there is no bioassay available that is standardized with international reference material. We aimed to promote the standardization of the test results among laboratories that perform TSAb bioassays and calibrate TSAb levels against the second international standard (IS) 08/204 from the National Institute for Biological Standards and Control (NIBSC). Methods: Serum TSAb activity was measured with a FDA-cleared bioassay that utilizes CHO cells expressing a chimeric thyrotropin receptor (TSHR) and a c-AMP response-element-dependent luciferase. The IS was applied for calibration. TSAb results were reported as percentage of specimen-to-reference ratio (SRR%) and converted into mIU/L. Results: The IS dose-response curve was obtained using concentrations from 0.3125 to 200 mIU/L. Mean TSAb SRR%±standard deviation ( SD) values for the IS concentrations 0.3125, 0.625, 1.25, 2.5, 5, 10, 20, 40, 60, 80, 100, 120, 160, and 200 mIU/L were 63±4 (CV 6.3%), 63±4 (6.3), 67±2 (3.0), 76±6 (7.9), 91±8 (8), 134±8 (5.9), 201±13 (6.5), 294±12 (4.1), 336±10 (3.0), 348±8 (2.3), 360±14 (3.8), 371±15 (4.0), 381±9 (2.4), and 389±10 (2.6), respectively. A total of 127 dilution experiments were performed using 12 high TSAb-positive sera from patients with Graves' disease. When diluting TSAb-positive sera, IS concentrations within the linear range 5, 10, 20, 40, and 80 mIU/L were used for the calibration curve. All standard curves had R2 values >0.95. Low coefficient of variation (CV %) values for the IS calibration curve (4-6%) were obtained. Compared to bovine TSH, no significant differences were noted using either a pool of healthy donors or a normal serum as reference controls. The average IU measured value for the assay cutoff (SRR 140%) corresponded to 9.54±1.68 mIU/L, and clinical application was shown in 60 Graves' patients. Conclusions: The TSAb bioassay demonstrated excellent performance in terms of linear range, limit of quantitation, and imprecision. The dilution experiments showed a high correlation coefficient and excellent reproducibility. Thus, TSAb levels can be reliably converted from SRR% to IU/L. These results offer the perspective of standardizing TSAb levels among laboratories and enable more accurate comparison of TSAb studies. [ABSTRACT FROM AUTHOR]

Published

2015

50. Analytical Performance and Clinical Utility of a Bioassay for Thyroid-Stimulating Immunoglobulins.

Author

Leschik, Johannes J., Diana, Tanja, Olivo, Paul D., König, Jochem, Krahn, Ulrike, Yunsheng Li, Kanitz, Michael, and Kahaly, George J.

Subjects

*THYROTROPIN, *IMMUNOGLOBULINS, *GRAVES' disease, *AUTOANTIBODIES, *PROTEIN binding

Abstract

The analytical performance and the clinical utility of a thyrotropin receptor (TSHR)-stimulating immunoglobulin (TSI) bioassay were compared with those of a TSHR-binding inhibitory immunoglobulin (TBII) assay. Limits of detection (LoD) and quantitation (LoQ), assay cutoff, and the half-maximal effective concentration (EC50) were measured. Dilution analysis was performed in sera of hyperthyroid patients with Graves disease (GD) during antithyroid treatment (ATD). Titer was defined as the first dilution step at which measurement of TSI or TBII fell below the assay cutoff. The LoD, LoQ, cutoff, and EC of the bioassay 50 were 251-, 298-, 814-, and 827-fold lower than for the TBII assay. There were 22%, 42%, 23%, and 14% more positive samples in the TSI bioassay at dilutions of 1:3, 1:9, 1:27, and 1:81 (P < .0001), respectively. Responders to ATD demonstrated marked differences in titers compared with nonresponders. The bioassay detected lower levels of TSHR autoantibodies, and the dilution analysis provided similar predictive values of both assays in GD. [ABSTRACT FROM AUTHOR]

Published

2013