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首页> 外文期刊>Applied immunohistochemistry and molecular morphology: AIMM >Assessment of T-cell Clonality via T-cell Receptor-gamma Rearrangements in Cutaneous T-cell-Dominant Infiltrates Using Polymerase Chain Reaction and Single-stranded DNA Conformational Polymorphism Assay.
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Assessment of T-cell Clonality via T-cell Receptor-gamma Rearrangements in Cutaneous T-cell-Dominant Infiltrates Using Polymerase Chain Reaction and Single-stranded DNA Conformational Polymorphism Assay.

机译:使用聚合酶链反应和单链DNA构象多态性分析通过皮肤T细胞优势浸润物中T细胞受体-γ重排评估T细胞克隆性。

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摘要

Discerning the pathologic significance of cutaneous T-cell infiltrates can pose a diagnostic challenge for dermatopathologists. Reactive conditions such as drug-associated lymphomatoid hypersensitivity and lymphomatoid lupus erythematosus can demonstrate lymphoid atypia and a phenotype resembling cutaneous T-cell lymphoma (CTCL). Further, lymphoid dyscrasias such as pityriasis lichenoides chronica, large plaque parapsoriasis, and atypical pigmentary purpura confuse the picture because they not only mimic CTCL but also represent prelymphomatous states with inherent malignant potential. Although the emergence of a dominant clone has been considered a clue indicative of a T-cell dyscrasia, there are reports concerning the identification of monoclonality in biopsies of reactive lymphoid infiltrates. We have conducted a modified single-stranded DNA conformational polymorphism (SSCP) assay using paraffin-embedded, formalin-fixed tissue on 92 T-cell-rich biopsies to determine the relative specificity and sensitivity of this methodology. In addition, laser capture microdissection (LCM) was performed on 22 of the 92 samples to isolate the area of interest and to compare its specificity and sensitivity with those SSCP assays performed without LCM. We found that monoclonality or oligoclonality is 86% specific for preneoplastic and neoplastic states, whereas the finding of polyclonality appears to be relatively specific for a reactive process. Some cases of reversible T-cell dyscrasia produced a molecular profile mimicking lymphoma or prelymphomatous states by virtue of monoclonality or oligoclonality. Although LCM appears to improve the sensitivity for detecting preneoplastic conditions, the relative specificity appears to be the same as that encountered with routine SSCP.
机译:认识到皮肤T细胞浸润的病理学意义可能对皮肤病理学家提出诊断挑战。诸如药物相关性淋巴瘤样超敏反应和红细胞淋巴瘤样红斑狼疮等反应性疾病可表现出淋巴样异型和类似于皮肤T细胞淋巴瘤(CTCL)的表型。此外,淋巴发育不良,例如慢性糠疹,斑块状银屑病和非典型性色素性紫癜,使图片混乱,因为它们不仅模仿CTCL,而且代表具有固有恶性潜能的淋巴瘤前状态。尽管已经认为显性克隆的出现提示了T细胞发育异常,但是有报道涉及在活体淋巴浸润活检中鉴定单克隆抗体。我们对富含T细胞的92个T细胞活检组织使用石蜡包埋,福尔马林固定的组织进行了改良的单链DNA构象多态性(SSCP)分析,以确定该方法的相对特异性和敏感性。此外,对92个样本中的22个样本进行了激光捕获显微切割(LCM),以分离出感兴趣的区域,并将其特异性和敏感性与没有LCM的SSCP分析进行比较。我们发现单克隆或寡克隆性对于肿瘤前和赘生状态具有86%的特异性,而多克隆性的发现似乎对反应过程具有相对特异性。某些可逆性T细胞发育异常的病例由于单克隆或寡克隆性而产生了模仿淋巴瘤或淋巴瘤前状态的分子图谱。尽管LCM似乎可以提高检测肿瘤前状况的灵敏度,但相对特异性似乎与常规SSCP相同。

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