Abstract
BackgroundA high prevalence of thyroid papillary cancer was reported in hepatitis-C-virus (HCV) positive patients. However, the mechanistic role of hepatic-fibrosis in thyroid malignancy progressions is still unclear.AimWe aimed to study the immune-modulatory interactions between thyroid papillary carcinoma and hepatic-fibrosis.MethodsHepatic-fibrosis was induced in nude-nu-male mice by intra-peritoneal administration of carbon-tetrachloride. To induce thyroid-tumor, a thyroid papillary carcinoma cell line (NPA) was injected subcutaneously in the backs. Fibrotic profile was estimated by α-smooth-muscle-actin (αSMA) expression in liver tissue extracts using western-blots and RT-PCR. Intra-hepatic NK cells were isolated and stained for NK activity (CD107a) by flow cytometry. Liver histopathology (H&E staining), thyroid tumor mass and serum alanine aminotransferase (ALT), serum vascular endothelial growth factor (VEGF) and free-T4 levels were also assessed.Results Ex-vivo: NPA cells were co-cultured with intra-hepatic NK cells isolated from fibrotic mice with/without the tumor were analyzed for CFSE-proliferations. Both tumor groups (with/without hepatic-fibrosis) excreted higher serum free T4 levels. Hepatic-fibrosis increased tumor weight and size and serum free-T4 levels. In addition, tumor induction increased liver injury (both hepatic-fibrosis, necro-inflammation and serum ALT levels). In addition, tumor-bearing animals with hepatic-fibrosis had increased NK activity. NPA tumor-bearing animals increased fibrosis in spite of increased NK activity; probably due to a direct effect through increased serum free-T4 excretions. Serum VEGF levels were significantly increased in the fibrotic- bearing tumor groups compared to the non-fibrotic groups. In-vitro, NK cells from fibrotic tumor-bearing animals reduced proliferation of NPA cells. This decrease is attributed to increase NK cells activity in the fibrotic animals with the NPA tumors.ConclusionsOur results propose that NK cells although were stimulated in advanced fibrosis with tumor, they lost their anti-tumor and anti-fibrotic activity probably due to secretions of T4 and VEFG and may explain increased risk of thyroid tumors in chronic HCV patients.
Highlights
Thyroid cancer is the most common endocrine malignancy and accounts for the majority of endocrine cancer deaths each year [1, 2]
We aimed to study the immune-modulatory interactions between thyroid papillary carcinoma and hepatic-fibrosis
Our results propose that Natural killer (NK) cells were stimulated in advanced fibrosis with tumor, they lost their anti-tumor and anti-fibrotic activity probably due to secretions of T4 and VEFG and may explain increased risk of thyroid tumors in chronic hepatitis C virus (HCV) patients
Summary
Thyroid cancer is the most common endocrine malignancy and accounts for the majority of endocrine cancer deaths each year [1, 2]. In addition to hepatic-fibrosis, an oncogenic role of hepatitis C virus (HCV) in the pathogenesis of different kinds of extra-hepatic tumors has been suggested; for example, malignant lymphoma and pancreatic cancer [7, 8]. Some studies have reported a high prevalence of thyroid papillary cancer in patients with HCV infection [9,10,11,12,13]. A high prevalence of thyroid papillary cancer was reported in hepatitis-C-virus (HCV) positive patients. The mechanistic role of hepatic-fibrosis in thyroid malignancy progressions is still unclear.
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