Prospective study on thyroid autoimmunity and dysfunction related to chronic hepatitis C and interferon therapy.

6533b850fe1ef96bd12a8546

RESEARCH PRODUCT

Prospective study on thyroid autoimmunity and dysfunction related to chronic hepatitis C and interferon therapy.

Giuseppe Montalto S. Gallo Maurizio Soresi S. Tripi Alberto Notarbartolo V. Scafidi N Custro

subject

Adult Male endocrine system medicine.medical_specialty endocrine system diseases Endocrinology Diabetes and Metabolism Thyroid Gland Thyrotropin Interferon alpha-2 Thyroid function tests Gastroenterology Iodide Peroxidase Thyroiditis Autoimmune Diseases Autoimmune thyroiditis Endocrinology Internal medicine medicine Humans Prospective Studies Autoantibodies Autoimmune disease medicine.diagnostic_test business.industry Thyroid Interferon-alpha Middle Aged medicine.disease Hepatitis C Thyroid Diseases Anti-thyroid autoantibodies Recombinant Proteins Discontinuation Thyroxine medicine.anatomical_structure Immunology Triiodothyronine Female Thyroid function business

description

This study was designed to assess patients with chronic hepatitis C (CHC) for the presence of thyroid autoimmunity and dysfunction, to evaluate the risk of thyroid disorders associated with interferon (IFN) therapy, and to survey the outcome of possible treatment-related thyroid injury. Out of 104 consecutive untreated patients (30 women and 74 men; mean age, 52.7 years), 8 (7.7%) were found seropositive for thyroid autoantibodies (ThyAb), whereas seropositivity in healthy controls was 1/98 (1.3%). The relative increase in risk of developing thyroid autoimmunity associated with CHC was 760% (95% Cl, 220–1300%). No patients had abnormalities of thyroid function tests, but on IFN treatment, 3/3 patients showed a rapid over-range rise in circulating thyrotropin, which returned to normal after therapy discontinuation. In the other 5 seropositive patients who refused treatment, thyroid function remained normal. Out of the 58 initially seronegative patients who consented to IFN treatment, 9 (15.5%) developed thyroid autoimmunity. Seven of them (77,7%) had thyroid dysfunction: hypothyroidism in 4 cases, transient thyrotoxicosis in 2 cases. The last patient developed TSH-receptor antibodies and Graves’ disease, requiring methimazole therapy. Thyroid function recovered in the former 6 cases following IFN discontinuation. In the 28 initially seronegative patients who refused IFN and participated in a preliminary tauroursodeoxycholic acid trial, antithyroglobulin antibodies alone appeared in one case, but no thyroid dysfunction was observed. The relative risk of thyroid autoimmune disorder associated with IFN therapy was 342% (28–636%). The patients with CHC were unlikely to develop thyroid dysfunction in the absence of IFN therapy, in spite of being ThyAb seropositive. Moreover, a considerable proportion of seronegative patients, when IFN-treated, developed thyroid autoimmunity and then thyroid dysfunction. Both in seropositive and seronegative patients immediate IFN discontinuation normalized thyroid function and hormone replacement therapy was not necessary.

year	journal	country	edition	language
1997-07-01

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