EXPRESSION OF INTERCELLULAR-ADHESION MOLECULE-1 ON HUMAN THYROID-CELLS FROM PATIENTS WITH AUTOIMMUNE THYROID-DISEASE - STUDY OF THYROID XENOGRAFTS IN NUDE AND SEVERE COMBINED IMMUNODEFICIENT MICE AND TREATMENTWITH FK-506

Authors
ARREAZA G YOSHIKAWA N MUKUTA T RESETKOVA E BARSUK A NISHIKAWA M MUALLIM C MILLER N JAMIESON C VOLPE R
Citation
G. Arreaza et al., EXPRESSION OF INTERCELLULAR-ADHESION MOLECULE-1 ON HUMAN THYROID-CELLS FROM PATIENTS WITH AUTOIMMUNE THYROID-DISEASE - STUDY OF THYROID XENOGRAFTS IN NUDE AND SEVERE COMBINED IMMUNODEFICIENT MICE AND TREATMENTWITH FK-506, The Journal of clinical endocrinology and metabolism, 80(12), 1995, pp. 3724-3731
Citations number
57
Categorie Soggetti
Endocrynology & Metabolism
Journal title
The Journal of clinical endocrinology and metabolismACNP
ISSN journal
0021972X
Volume
80
Issue
12
Year of publication
1995
Pages
3724 - 3731
Database
ISI
SICI code
0021-972X(1995)80:12<3724:EOIMOH>2.0.ZU;2-1
Abstract
It has been suggested that intercellular adhesion molecule-1 (ICAM-1) may play an important role in the initiation, localization, and perpet uation of autoimmune thyroid diseases (AITD). In an effort to clarify its role, we have investigated the expression of ICAM-1 on thyroid epi thelial cells (TEC) of patients with AITD, patients with nontoxic goit er (NTG), and normal subjects (PN) by flow cytometric analysis under b asal conditions and after modulation with cytokines, before and after 8 weeks of thyroid tissue xenotransplantation in nude athymic mice (wh ich lyses all passenger lymphocytes), and in severe combined immunodef icient (SCID) mice where these cells survive. Before xenografting, ICA M-1 was expressed on 56% of TEC from Hashimoto's thyroiditis (n = 5), 54% of Graves' disease (n = 6), 15% of NTG (n = 5), and 12% of PN TEC. After the xenografts had been 8 weeks in nude mice, ICAM-1 expression decreased markedly in AITD TEC [from 56% to 10% in Hashimoto's thyroi ditis (P < 0.001) and from 54% to 8% in Graves' disease (P < 0.01)], b ut did not change significantly in NTG or PN. After the xenografts had been 8 weeks in SCID mice, the expression of ICAM-1 was significantly higher on TEC of AITD compared with the same tissue in nude mice. Whe n the SCID mice engrafted with AITD tissue were treated with the anti- CD4(+) T (helper) cell agent FK-506, the expression of ICAM-1 was redu ced significantly compared with that in the original tissue or that in nontreated mice engrafted with the same tissue. The proportion of TEC that were ICAM-1 positive was up-regulated in all cases by certain cy tokines (e.g. interferon-gamma and tumor necrosis factor-alpha applied alone or in combination). We also detected the presence of ICAM-1 in AITD frozen tissues using an immunohistochemical technique. These data suggest a role for ICAM-1 in human AITD. How ever, the expression of ICAM-1 appears to be a secondary phenomenon in response to the immune assault, rather than a primary event. Our results support the idea tha t TEC may act as passive captives to immunological events in human AIT D.