Nitrotyrosine, inducible nitric oxide synthase (iNOS), and endothelial nitric oxide synthase (eNOS) are increased in thyroid tumors from children and adolescents.

Patel A; Fenton C; Terrell RPowers PADinauer CTuttle RMFrancis GL

摘要

Nitric oxide (NO) is a reactive cell signal that controls vascular tone and is generated by inducible (iNOS), endothelial (eNOS) and neuronal (nNOS) NO synthase (NOS). We hypothesized that NO could be important for growth of thyroid tumors and tested this hypothesis, by staining 41 papillary thyroid carcinoma (PTC), 9 follicular thyroid carcinoma (FTC), and 15 benign thyroid lesions for iNOS, eNOS and nitrotyrosine (N-TYR). Staining intensity was determined by 2 blinded, independent examiners, and quantified from grade 1 (absent) to grade 4 (intense). Average N-TYR staining of benign adenomas (2.5+/-0.42, p=0.009), PTC (3.10+/-0.12, p=0.001), FTC (2.44+/-0.30, p=0.001), and autoimmune lesions (3.25+/-0.48, p=0.019) were greater than that of multinodular goiter (1.0 for all 3) and surrounding normal thyroid (1.1+/-0.1). Average iNOS staining of benign adenomas (2.6+/-0.37), PTC (2.7+/-0.16), FTC (2.4+/-0.26) and autoimmune lesions (3.5+/-0.29) were all greater than that of surrounding normal thyroid (1.1+/-0.1, p<0.008), but there were too few multinodular goiters to achieve a significant difference (no.=2, 3.0+/-1.0). Average eNOS staining of benign adenomas (2.9+/-0.40), multinodular goiters (3.5+/-0.5), PTC (3.24+/-0.18), FTC (3.5+/-0.50), and autoimmune lesions (2.8+/-0.6) were also greater than that of surrounding normal thyroid (mean=1.4+/-0.2, p<0.001). N-TYR staining correlated with that of vascular endothelial growth factor (VEGF, r=0.36, p=0.007) and the number of lymphocytes/high power field (r=0.39, p=0.004). Recurrent disease developed only from carcinoma with moderate-intense N-TYR staining, but there were too few recurrent tumors to achieve statistical significance (p=0.08). We conclude that NO is produced by benign adenomas, PTC and FTC suggesting that NO could be important in vascularization of thyroid tumors and autoimmune thyroid diseases.

机译：一氧化氮（NO）是一种控制血管张力的反应性细胞信号，由诱导型（iNOS）、内皮（eNOS）和神经元（nNOS） NO 合酶（NOS）产生。我们假设 NO 可能对甲状腺肿瘤的生长很重要，并通过对 41 个甲状腺状癌（PTC）、9 个滤泡性甲状腺癌（FTC）和 15 个良性甲状腺病变进行 iNOS、eNOS 和硝基酪氨酸（N-TYR）染色来检验这一假设。染色强度由 2 名盲法独立检查员确定，并从 1 级（无）到 4 级（强烈）进行量化。良性腺瘤（2.5+/-0.42，p=0.009）、PTC（3.10+/-0.12，p=0.001）、FTC（2.44+/-0.30，p=0.001）和自身免疫性病变（3.25+/-0.48，p=0.019）的平均N-TYR染色均大于多结节性甲状腺肿（3例均为1.0）和周围正常甲状腺（1.1+/-0.1）。良性腺瘤（2.6+/-0.37）、PTC（2.7+/-0.16）、FTC（2.4+/-0.26）和自身免疫性病变（3.5+/-0.29）的平均iNOS染色均大于周围正常甲状腺（1.1+/-0.1，p<0.008），但多结节性甲状腺肿太少，差异无统计学意义（no.=2,3.0+/-1.0）。良性腺瘤（2.9+/-0.40）、多结节性甲状腺肿（3.5+/-0.5）、PTC（3.24+/-0.18）、FTC（3.5+/-0.50）和自身免疫性病变（2.8+/-0.6）的平均eNOS染色也大于周围正常甲状腺（平均值=1.4+/-0.2，p<0.001）。N-TYR染色与血管内皮生长因子相关（VEGF，r=0.36，p=0。007）和淋巴细胞数/高倍场（r=0.39，p=0.004）。复发性疾病仅由中等强度 N-TYR 染色的癌发展而来，但复发性肿瘤太少，无法达到统计学意义（p=0.08）。我们得出结论，NO 是由良性腺瘤、PTC 和 FTC 产生的，这表明 NO 在甲状腺肿瘤和自身免疫性甲状腺疾病的血管形成中可能很重要。

Nitrotyrosine, inducible nitric oxide synthase (iNOS), and endothelial nitric oxide synthase (eNOS) are increased in thyroid tumors from children and adolescents.

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