Immunohistochemical Markers of Soft Tissue Tumors: Pathologic Diagnosis, Genetic Contributions, and Therapeutic Options

D. Parham
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引用次数: 12

Abstract

After ~30 years of widespread usage, immunohistochemistry (IHC) has become a standard method of diagnosis for surgical pathology. Because of the plethora of diagnoses and often subtle nature of diagnostic criteria, IHC finds particular utility in soft tissue tumors. The use of progressively small amounts of tissue for diagnosis highlights the importance of this method. The sensitivity and crispness of IHC stains have progressively improved with the advent of new techniques. Traditionally, IHC detects cell-typic markers that characterize cell phenotypes, such as chromogranin for neuroectodermal tissue, myogenin for skeletal muscle, and cytokeratin for epithelium. However, the advent of genetic discoveries have led to IHC testing for detection of fusion gene products or overexpressed oncogenes associated with deletions and mutations. Proliferation-based markers such as Ki-67 can also be used for prognosis and grading, but more standardization is needed. Development of monoclonal antibody-based pharmaceuticals, such as imatinib or crizotinib, holds the promise of tailored anticancer therapy. IHC thus has assumed importance not only for diagnosis but also for guidance of personalized medicine.
软组织肿瘤的免疫组织化学标记物:病理诊断、遗传贡献和治疗选择
经过近30年的广泛应用,免疫组织化学(IHC)已成为外科病理诊断的标准方法。由于诊断的过多和诊断标准的微妙性质,免疫结构在软组织肿瘤中发现了特别的效用。使用逐渐少量的组织进行诊断,突出了这种方法的重要性。随着新技术的出现,IHC染色的灵敏度和脆度逐渐提高。传统上,免疫组化检测表征细胞表型的细胞型标记物,如神经外胚层组织的铬粒蛋白,骨骼肌的肌原蛋白和上皮的细胞角蛋白。然而,基因发现的出现导致了IHC检测,用于检测融合基因产物或与缺失和突变相关的过表达癌基因。基于增殖的标志物如Ki-67也可用于预后和分级,但需要更多的标准化。以单克隆抗体为基础的药物,如伊马替尼或克里唑替尼,有望实现量身定制的抗癌治疗。因此,免疫健康不仅对诊断很重要,而且对个性化医疗的指导也很重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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