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牙源性囊肿和肿瘤中破骨细胞生成因子的差异蛋白表达。

Differential protein expression of osteoclastogenic factors in odontogenic cysts and tumors.

机构信息

Universidade Federal da Bahia - UFBA, Graduate Program in Dentistry and Health, Salvador, BA, Brazil.

Universidade Federal do Pernambuco - UFPE, Department of Dentistry, Graduate Program in Oral Pathology, Recife, PE, Brazil.

出版信息

Braz Oral Res. 2022 May 2;36:e072. doi: 10.1590/1807-3107bor-2022.vol36.0072. eCollection 2022.

Abstract

The osteolytic activity of odontogenic cysts and tumors is directly associated with their growth and aggressiveness. The influence of proteins expressed by epithelial and mesenchymal cells on this biological event differs between indolent cystic lesions, aggressive cystic lesions, and odontogenic tumors. The objective of this study was to compare the immunohistochemical expression of factors that stimulate (receptor activator of nuclear factor kappa-Β ligand - RANKL, cathepsin K - CatK and matrix metallopeptidase 8 - MMP-8) and inhibit (osteoprotegerin - OPG) osteoclastogenesis between dentigerous cyst (DC), glandular odontogenic cyst (GOC), odontogenic keratocyst (OKC), and ameloblastoma (AB). Paraffin-embedded sections of nine DCs, nine GOCs, 20 OKCs, 21 ABs, and four dental follicles (DFs) were subjected to immunohistochemistry. Immunoreactivity was analyzed semiquantitatively and quantitatively in epithelium and connective tissue, respectively. The proteins were immunoexpressed in epithelial and mesenchymal cells of all lesions studied. The expression of RANKL and CatK was higher in OKC, AB, and GOC (p<0.005). Higher expression of OPG was found in DF and DC compared to the other markers (p<0.005). MMP-8 expression was high in GOC and OKC. This study demonstrated the differential expression of factors that inhibit and stimulate bone resorption during the development of DC, GOC, OKC, and AB. Higher expression of RANKL and CatK was observed in more aggressive lesions. OPG appears to be one of the molecules responsible for the slower growth of DC.

摘要

牙源性囊肿和肿瘤的溶骨性活性与其生长和侵袭性直接相关。上皮细胞和间充质细胞表达的蛋白对这一生物学事件的影响在良性囊性病变、侵袭性囊性病变和牙源性肿瘤之间有所不同。本研究旨在比较牙源性囊(DC)、腺牙源性囊(GOC)、牙源性角化囊肿(OKC)和造釉细胞瘤(AB)中刺激(核因子κB 受体激活剂配体-RANKL、组织蛋白酶 K-CatK 和基质金属蛋白酶 8-MMP-8)和抑制(骨保护素-OPG)破骨细胞形成的因子的免疫组织化学表达。对 9 例 DC、9 例 GOC、20 例 OKC、21 例 AB 和 4 例牙滤泡(DF)的石蜡包埋切片进行免疫组织化学染色。分别对上皮组织和结缔组织进行半定量和定量的免疫反应性分析。所有研究病变的上皮和间充质细胞均有免疫表达。RANKL 和 CatK 的表达在 OKC、AB 和 GOC 中较高(p<0.005)。与其他标志物相比,DF 和 DC 中 OPG 的表达较高(p<0.005)。MMP-8 在 GOC 和 OKC 中表达较高。本研究表明,在 DC、GOC、OKC 和 AB 的发展过程中,抑制和刺激骨吸收的因子表达存在差异。在侵袭性更强的病变中观察到 RANKL 和 CatK 的表达更高。OPG 似乎是导致 DC 生长较慢的分子之一。

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