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乳铁蛋白在骨和软骨人类肿瘤中是否表现为免疫组织化学的癌胚标志物?

Does lactoferrin behave as an immunohistochemical oncofetal marker in bone and cartilage human neoplasms?

机构信息

Department of Human Pathology, Azienda Ospedaliera Universitaria Policlinico G Martino, Pad D, Via Consolare Valeria, 98125 Messina, Italy.

出版信息

Pathol Oncol Res. 2011 Jun;17(2):287-93. doi: 10.1007/s12253-010-9311-5. Epub 2010 Oct 24.

Abstract

By immunohistochemistry, lactoferrin (LF) has been extensively investigated in human neoplastic tissues; moreover, LF is able to promote bone growth in a murine model. Until now, no systematic studies on human osteocartilagineous fetal samples have been performed in comparison to corresponding neoplastic specimens to verify if LF may represent an oncofetal marker in this field of pathology. By a monoclonal antibody (clone 1A1; Biodesign International; w.d. 1:75) the distribution pattern of LF in bones of 25 human fetal tissues (8-34 gestation weeks), 10 adults (47-82 years) and 30 cartilage as well as 27 bone tumours (9-76 years) was analyzed. LF was encountered in 23/57 cases of osteocartilagineous tumors and namely in 10/10 giant cell tumours, 5/7 osteoid osteomas, 3/3 chondroblastomas, 3/3 chondromyxoid fibromas, 1/1 myeloma, 1/1 adamantinoma. No LF immunoexpression was detected in osteosarcomas, chondrosarcomas, ossifying fibromas, osteochondroma and enchondromas. In embryo-fetal tissues, LF immunoreactivity was localized in mesenchymal cells as well as in chondroblasts at the 8th gestational week and in immature osteocytes and osteoblasts up to the 18th gestation week, with a considerable decrease by the 24th week. No LF expression was found in any bone district since the 30th and up to the 34th week of gestation as well as in corresponding adult samples. Our findings indicate a role for LF as a bone growth regulator in the early phases of the human endochondral ossification, although the hypothesis of LF as oncofetal marker appears questionable in bone tumours.

摘要

通过免疫组织化学方法,乳铁蛋白 (LF) 在人类肿瘤组织中得到了广泛研究;此外,LF 能够在小鼠模型中促进骨骼生长。到目前为止,尚未与相应的肿瘤标本进行比较,对人类骨软骨胎儿样本进行系统研究,以验证 LF 是否可以作为该病理学领域的癌胚标志物。通过单克隆抗体(克隆 1A1;Biodesign International;w.d. 1:75),分析了 25 个人类胎儿组织(8-34 孕周)、10 个成人(47-82 岁)和 30 个软骨以及 27 个骨肿瘤(9-76 岁)中 LF 的分布模式。在 57 例骨软骨肿瘤中有 23 例(10/10 巨细胞瘤、5/7 骨样骨瘤、3/3 软骨母细胞瘤、3/3 软骨粘液样纤维瘤、1/1 骨髓瘤、1/1 造釉细胞瘤)中发现 LF。在骨肉瘤、软骨肉瘤、骨化性纤维瘤、骨软骨瘤和内生软骨瘤中未检测到 LF 免疫反应。在胚胎胎儿组织中,LF 免疫反应性定位于第 8 孕周的间充质细胞和软骨细胞,以及第 18 孕周的未成熟成骨细胞和成骨细胞,到第 24 孕周时明显减少。在妊娠第 30 周至第 34 周以及相应的成人样本中,在任何骨区均未发现 LF 表达。我们的研究结果表明 LF 作为人类软骨内骨化早期阶段的骨生长调节剂的作用,尽管 LF 作为癌胚标志物的假说在骨肿瘤中似乎值得怀疑。

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