Pathology Department, Assuit University Hospitals, Sohag University, Egypt.
Exp Mol Pathol. 2010 Apr;88(2):316-23. doi: 10.1016/j.yexmp.2009.12.006. Epub 2010 Jan 4.
Cholesteatoma consists of keratinizing squamous epithelium, granulation tissue and keratin plugs. The pathogenesis of cholesteatoma may be related to alterations in the stromal immune cell infiltrate.
To examine the immunophenotypic characteristics of the immune cell infiltrate in invasive cholesteatomas.
This study included 12 patients with invasive cholesteatomas causing wide bone erosion of the mastoid, middle ear structures, and the bony plates of middle ear cleft. Diagnosis of invasiveness was based on the clinical, radiological and intraoperative findings. Canal wall-down surgical approach was done in all cases to control the disease process. We used the cholesteatomatous tissue specimens to perform immunohistochemical stains for B cells (CD20), T cells (CD3), histiocytes (CD68) and Langerhans' cells (CD1a). Mouse monoclonal antibodies and immunoperoxidase staining methods were used. The results of immunohistology were scored as mean values of positively stained immune cells. The data were compared with findings in 10 specimens of external ear skin (control group).
Immunohistochemistry showed highly significant (p<0.00) counts of immune cells in invasive cholesteatomas (CD3: 4.7+/-0.4, CD68:4.6+/-0.5, CD20: 0.8+/-0.1 and CD1a: 0.8 +/-0.1) compared to those in external canal skin (control group: CD3:0.8+/-0.3, CD68: 1.0+/-0.4, CD20: 0.2+/-0.1 and CD1a: 0.1+/-0.1). In cholesteatomas, the predominant of CD3(+) T lymphocytes and CD68(+) cells (histiocytes). Rare CD20(+) cells and CD1a(+) cells (Langerhans' cells) were also observed.
This preliminary study describes the profile of the immune cell infiltrate in invasive cholesteatomas. The numeric dominance of CD3(+) cells and CD68(+) cells suggests that cell-mediated immunity has important role in the development of cholesteatoma and in its autodestructive properties. Further studies are recommended to categorize the T cell subsets in different stages of cholesteatomas.
胆脂瘤由角化的鳞状上皮、肉芽组织和角化栓组成。胆脂瘤的发病机制可能与基质免疫细胞浸润的改变有关。
研究侵袭性胆脂瘤中免疫细胞浸润的免疫表型特征。
本研究纳入了 12 例因广泛乳突、中耳结构和中耳裂隙骨板骨质侵蚀而导致侵袭性胆脂瘤的患者。侵袭性的诊断基于临床、影像学和术中发现。所有病例均采用经耳道后壁入路手术以控制疾病进程。我们使用胆脂瘤组织标本进行 B 细胞(CD20)、T 细胞(CD3)、组织细胞(CD68)和朗格汉斯细胞(CD1a)的免疫组织化学染色。使用鼠单克隆抗体和免疫过氧化物酶染色方法。免疫组织化学结果评分作为阳性染色免疫细胞的平均值。将数据与 10 例外耳皮肤标本(对照组)的结果进行比较。
免疫组织化学显示,侵袭性胆脂瘤中免疫细胞计数显著升高(p<0.00)(CD3:4.7+/-0.4,CD68:4.6+/-0.5,CD20:0.8+/-0.1,CD1a:0.8 +/-0.1),与外耳道皮肤(对照组:CD3:0.8+/-0.3,CD68:1.0+/-0.4,CD20:0.2+/-0.1,CD1a:0.1+/-0.1)相比。在胆脂瘤中,CD3(+)T 淋巴细胞和 CD68(+)细胞(组织细胞)占优势。也观察到罕见的 CD20(+)细胞和 CD1a(+)细胞(朗格汉斯细胞)。
本初步研究描述了侵袭性胆脂瘤中免疫细胞浸润的特征。CD3(+)细胞和 CD68(+)细胞的数量优势表明,细胞介导的免疫在胆脂瘤的发展及其自毁特性中具有重要作用。建议进一步研究以对不同阶段胆脂瘤中的 T 细胞亚群进行分类。