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ACTN4 基因扩增和肌动蛋白-4 蛋白过表达驱动卵巢透明细胞腺癌中高级别亚组的肿瘤发生和组织学进展。

ACTN4 gene amplification and actinin-4 protein overexpression drive tumour development and histological progression in a high-grade subset of ovarian clear-cell adenocarcinomas.

机构信息

Department of Basic Pathology, National Defense Medical College, Saitama, Japan.

出版信息

Histopathology. 2012 Jun;60(7):1073-83. doi: 10.1111/j.1365-2559.2011.04163.x. Epub 2012 Feb 20.

DOI:10.1111/j.1365-2559.2011.04163.x
PMID:22348389
Abstract

AIMS

Actinin-4, encoded by the ACTN4 gene located on chromosome 19q13.2, enhances cell motility by bundling the actin cytoskeleton. We assessed how ACTN4/actinin-4 alterations contribute to the tumorigenesis of ovarian clear-cell adenocarcinomas (CCAs).

METHODS AND RESULTS

Fluorescence in-situ hybridization analysis demonstrated that ACTN4 amplification (≥4 ACTN4 copies in ≥40% of cells) occurred in 27 (33%) of 81 CCAs and genomic gains of ACTN4 were associated strongly with immunohistochemical actinin-4 overexpression, poorly differentiated tumour histology and shorter patient survival (all P < 0.05). From the 27 ACTN4-amplified CCAs, 23 tumours with adjacent putative precursor lesions were selected and examined for ACTN4/actinin-4 alterations with respect to their intratumoral heterogeneity. In this selected cohort, none of the precursors lacking cytological atypia exhibited gains of ACTN4 or actinin-4 overexpression; 50% of the atypical endometrioses and 75% of the borderline CCAFs showed low-level gains of ACTN4 and actinin-4 overexpression, respectively. In 12 of 23 ACTN4-amplified CCAs, intratumoral heterogeneity for ACTN4 alterations was documented in carcinomatous components; the better differentiated carcinoma components exhibited fewer alterations than those with poorly differentiated histology.

CONCLUSION

Accumulative genomic gains of ACTN4, causing actinin-4 protein overexpression, drive the development and progression of ovarian CCAs with high-grade histology.

摘要

目的

肌动蛋白 4(actinin-4)由位于 19q13.2 染色体上的 ACTN4 基因编码,通过束状排列肌动蛋白细胞骨架增强细胞迁移能力。我们评估了 ACTN4/肌动蛋白 4 改变如何促进卵巢透明细胞腺癌(CCAs)的肿瘤发生。

方法和结果

荧光原位杂交分析显示,81 例 CCAs 中有 27 例(33%)存在 ACTN4 扩增(≥40%的细胞中≥4 个 ACTN4 拷贝),ACTN4 的基因组增益与免疫组织化学肌动蛋白-4 过表达、肿瘤组织学分化差和患者生存时间缩短密切相关(均 P < 0.05)。在 27 例 ACTN4 扩增的 CCAs 中,选择了 23 例具有相邻假定前体病变的肿瘤,并对 ACTN4/肌动蛋白-4 改变进行了研究,以评估其肿瘤内异质性。在这个选定的队列中,没有一个缺乏细胞学异型性的前体显示 ACTN4 或肌动蛋白-4 过表达的增益;50%的非典型子宫内膜异位症和 75%的交界性 CCAFs 分别显示出低水平的 ACTN4 增益和肌动蛋白-4 过表达。在 23 例 ACTN4 扩增的 CCAs 中有 12 例,癌性成分存在 ACTN4 改变的肿瘤内异质性;分化较好的癌性成分的改变比组织学分化差的癌性成分少。

结论

ACTN4 的累积性基因组增益导致肌动蛋白-4 蛋白过表达,从而促进具有高级别组织学特征的卵巢 CCAs 的发展和进展。

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