癌细胞核中的连接蛋白46：作为转录调节因子的潜在作用。

Connexin46 in the nucleus of cancer cells: a possible role as transcription modulator.

作者信息

Fernández-Olivares Ainoa, Orellana Viviana P, Llanquinao Jesús, Nuñez Gonzalo, Pérez-Moreno Pablo, Contreras-Riquelme Sebastián, Martin Alberto Jm, Mammano Fabio, Alfaro Ivan E, Calderón Juan F, Stehberg Jimmy, Sáez Mauricio A, Retamal Mauricio A

机构信息

Programa de Comunicación Celular en Cáncer, Instituto de Ciencias e Innovación en Medicina, Facultad de Medicina, Clínica Alemana Universidad del Desarrollo, Santiago, Chile.

Translational Medicine Laboratory, Instituto Oncológico Fundación Arturo López Pérez, Santiago 7500691, Chile.

出版信息

Cell Commun Signal. 2025 Mar 27;23(1):153. doi: 10.1186/s12964-025-02151-w.

DOI:10.1186/s12964-025-02151-w

PMID:40148950

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11948717/

Abstract

BACKGROUND

Oncogenes drive cancer progression, but few are active exclusively in tumor cells. Connexins (Cxs), traditionally recognized as ion channel proteins, can localize to the nucleus and regulate gene expression, playing key roles in both physiological and pathological processes. Cx46, once thought to be restricted to the eye lens, has been implicated in tumor growth, though its underlying mechanisms remain unclear. This study investigates the nuclear presence of Cx46 in cancer cells and its potential role as a transcriptional modulator.

METHODS

We employed ChIP-Seq, confocal immunofluorescence, and nuclear protein purification to assess Cx46 localization and DNA interactions. Functional assays were conducted to evaluate its effects on invasion, division, spheroid formation, and mesenchymal marker expression. Single-point mutations and molecular dynamics simulations were used to explore potential Cx46-DNA interactions.

RESULTS

Cx46 mRNA upregulation was found in a variety of tumors compared to adjacent healthy tissue. In HeLa cells, which do not express Cx46, its transfection promoted proliferation, invasion and self-renewal capacity, cancer stem cell traits and mesenchymal features. Consistently, in Sk-Mel-2, which naturally express Cx46, reduced Cx46 expression led to a decrease in the similar parameters. In HeLa cells, nuclear Cx46 was detected in two forms, full length 46 kDa and a 30 kDa fragment (GJA3-30 k), ChIP-Seq experiments revealed that Cx46 binds to the DNA at intergenic and promoter regions, leading to the activation of oncogenic pathways. Molecular dynamics simulations suggest that GJA3-30 k dimerizes in a RAD50-like structure, forming stable DNA complexes. Cx46 and in some cases GJA3-30 k were detected in the nuclei of multiple cancer cell lines, including prostate, breast and skin cancers.

CONCLUSIONS

Our findings reveal a novel nuclear role for Cx46 in cancer, demonstrating its function as a transcriptional regulator and its potential as a therapeutic target.

摘要

背景

癌基因驱动癌症进展，但很少有癌基因仅在肿瘤细胞中活跃。连接蛋白（Cxs）传统上被认为是离子通道蛋白，可定位于细胞核并调节基因表达，在生理和病理过程中均起关键作用。Cx46曾被认为仅限于晶状体，但其与肿瘤生长有关，尽管其潜在机制尚不清楚。本研究调查了癌细胞中Cx46的核内存在情况及其作为转录调节因子的潜在作用。

方法

我们采用染色质免疫沉淀测序（ChIP-Seq）、共聚焦免疫荧光和核蛋白纯化来评估Cx46的定位和与DNA的相互作用。进行功能测定以评估其对侵袭、分裂、球体形成和间充质标志物表达的影响。使用单点突变和分子动力学模拟来探索潜在的Cx46-DNA相互作用。

结果

与相邻健康组织相比，在多种肿瘤中发现Cx46 mRNA上调。在不表达Cx46的HeLa细胞中，转染Cx46可促进增殖、侵袭和自我更新能力、癌症干细胞特性和间充质特征。同样，在天然表达Cx46的Sk-Mel-2细胞中，Cx46表达降低导致类似参数下降。在HeLa细胞中，检测到两种形式的核内Cx46，全长46 kDa和30 kDa片段（GJA3-30 k），ChIP-Seq实验表明Cx46在基因间区域和启动子区域与DNA结合，导致致癌途径激活。分子动力学模拟表明，GJA3-30 k以类似RAD50的结构二聚化，形成稳定的DNA复合物。在包括前列腺癌、乳腺癌和皮肤癌在内的多种癌细胞系的细胞核中检测到Cx46，在某些情况下还检测到GJA3-30 k。