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间隙连接蛋白 43 的异常表达与胃癌的腹膜转移相关,并且 Cx43 介导的间隙连接增强了胃癌细胞从腹膜间皮的穿出。

Aberrant expression of Cx43 is associated with the peritoneal metastasis of gastric cancer and Cx43-mediated gap junction enhances gastric cancer cell diapedesis from peritoneal mesothelium.

机构信息

General Surgery Center of PLA, Southwest Hospital, the Third Military Medical University, Chongqing, China.

出版信息

PLoS One. 2013 Sep 11;8(9):e74527. doi: 10.1371/journal.pone.0074527. eCollection 2013.

Abstract

The process of peritoneal metastasis involves the diapedesis of intra-abdominal exfoliated gastric cancer cells through the mesothelial cell monolayers; however, the related molecular mechanisms for this process are still unclear. Heterocellular gap-junctional intercellular communication (GJIC) between gastric cancer cells and mesothelial cells may play an active role during diapedesis. In this study we detected the expression of connexin 43 (Cx43) in primary gastric cancer tissues, intra-abdominal exfoliated cancer cells, and matched metastatic peritoneal tissues. We found that the expression of Cx43 in primary gastric cancer tissues was significantly decreased; the intra-abdominal exfoliated cancer cells and matched metastatic peritoneal tissues exhibited increasing expression compared with primary gastric cancer tissues. BGC-823 and SGC-7901 human gastric cancer cells were engineered to express Cx43 or Cx43T154A (a mutant protein that only couples gap junctions but provides no intercellular communication) and were co-cultured with human peritoneal mesothelial cells (HPMCs). Heterocellular GJIC and diapedesis through HPMC monolayers on matrigel-coated coverslips were investigated. We found that BGC-823 and SGC-7901 gastric cancer cells expressing Cx43 formed functional heterocellular gap junctions with HPMC monolayers within one hour. A significant increase in diapedesis was observed in engineered Cx43-expressing cells compared with Cx43T154A and control group cells, which suggested that the observed upregulation of diapedesis in Cx43-expressing cells required heterocellular GJIC. Further study revealed that the gastric cancer cells transmigrated through the intercellular space between the mesothelial cells via a paracellular route. Our results suggest that the abnormal expression of Cx43 plays an essential role in peritoneal metastasis and that Cx43-mediated heterocellular GJIC between gastric cancer cells and mesothelial cells may be an important regulatory step during metastasis. Finally, we observed that the diapedesis of exfoliated gastric cancer cells through mesothelial barriers is a viable route of paracellular migration.

摘要

腹膜转移的过程涉及腹腔内脱落的胃癌细胞通过间皮细胞单层的穿胞作用;然而,这个过程的相关分子机制尚不清楚。胃癌细胞与间皮细胞之间的异质细胞缝隙连接细胞间通讯(GJIC)在穿胞作用中可能发挥积极作用。在这项研究中,我们检测了原发胃癌组织、腹腔内脱落癌细胞和匹配的转移性腹膜组织中连接蛋白 43(Cx43)的表达。我们发现,原发胃癌组织中 Cx43 的表达明显降低;与原发胃癌组织相比,腹腔内脱落的癌细胞和匹配的转移性腹膜组织表现出表达增加。我们构建了 BGC-823 和 SGC-7901 人胃癌细胞表达 Cx43 或 Cx43T154A(一种仅连接缝隙但不提供细胞间通讯的突变蛋白),并与人腹膜间皮细胞(HPMCs)共培养。研究了 BGC-823 和 SGC-7901 胃癌细胞与 HPMC 单层在 Matrigel 包被盖玻片上的异质细胞 GJIC 和穿胞作用。我们发现,表达 Cx43 的 BGC-823 和 SGC-7901 胃癌细胞在一个小时内与 HPMC 单层形成功能性异质细胞缝隙连接。与 Cx43T154A 和对照组细胞相比,工程化表达 Cx43 的细胞的穿胞作用明显增加,这表明观察到的 Cx43 表达细胞的穿胞作用上调需要异质细胞 GJIC。进一步的研究表明,胃癌细胞通过细胞间间隙穿过间皮细胞,通过细胞旁途径迁移。我们的研究结果表明,Cx43 的异常表达在腹膜转移中起着重要作用,Cx43 介导的胃癌细胞与间皮细胞之间的异质细胞 GJIC 可能是转移过程中的一个重要调节步骤。最后,我们观察到脱落的胃癌细胞通过间皮屏障的穿胞作用是一种可行的细胞旁迁移途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2f9d/3770585/e408c76fb346/pone.0074527.g001.jpg

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