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NKX3.1 免疫反应在间叶性软骨肉瘤中无法识别:25 例病例队列研究。

NKX3.1 immunoreactivity is not identified in mesenchymal chondrosarcoma: a 25-case cohort study.

机构信息

Department of Pathology, Brigham and Women's Hospital and Harvard Medical School, Boston, MA, USA.

出版信息

Histopathology. 2021 Jan;78(2):334-337. doi: 10.1111/his.14231. Epub 2020 Oct 19.

Abstract

AIMS

Mesenchymal chondrosarcoma (MC) is characterised typically by a bimorphic microscopic appearance of islands of a well-differentiated cartilaginous component, admixed with a primitive small cell component, which commonly expresses CD99 and NKX2.2. Given the variable relative abundance of each component and histological overlap with other small round cell tumours, the diagnosis can be challenging, especially in a limited sample. A distinctive gene fusion between HEY1 (located in 8q21) and NCOA2 (located in 8q13) was identified in MC, but the downstream molecular events are unknown. NKX3.1 (coding gene located in 8p21.1) was recently reported to be expressed in a small number of MC cases. The purpose of this study was to evaluate the potential diagnostic utility of NKX3.1 immunohistochemistry in MC.

METHODS AND RESULTS

We evaluated sections from 25 cases of MC, including 20 extraskeletal and five osseous. The tumour affected nine females and 16 males, with a median age of 34 years (age range = 7-82 years). Two different rabbit antibodies against NKX3.1 (monoclonal and polyclonal) were used for immunohistochemistry. However, no immunoreactivity was observed with either of the antibodies in all 25 (100%) MC.

CONCLUSIONS

NKX3.1 immunoreactivity was not identified in our cohort. Clonality of the antibody could not explain the negativity.

摘要

目的

间叶性软骨肉瘤(MC)的特征通常是具有良好分化的软骨成分的岛屿和原始小细胞成分的二相微观外观,其中常见 CD99 和 NKX2.2 的表达。鉴于每种成分的相对含量不同,以及与其他小圆细胞肿瘤的组织学重叠,诊断具有挑战性,尤其是在有限的样本中。在 MC 中鉴定出 HEY1(位于 8q21)和 NCOA2(位于 8q13)之间的独特基因融合,但下游分子事件尚不清楚。NKX3.1(位于 8p21.1 的编码基因)最近报道在少数 MC 病例中表达。本研究的目的是评估 NKX3.1 免疫组化在 MC 中的潜在诊断效用。

方法和结果

我们评估了 25 例 MC 病例的切片,包括 20 例骨外和 5 例骨。肿瘤影响了 9 名女性和 16 名男性,中位年龄为 34 岁(年龄范围为 7-82 岁)。使用针对 NKX3.1 的两种不同兔抗体(单克隆和多克隆)进行免疫组化。然而,在用两种抗体对所有 25 例(100%)MC 进行免疫组化时,均未观察到任何免疫反应性。

结论

在我们的队列中未发现 NKX3.1 免疫反应性。抗体的克隆性不能解释其阴性。

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