Archives
4-IPP br Pannexins which form channels connecting cells
Pannexins, which form channels connecting 4-IPP with the extracellular environment, have also been studied in the setting of NASH. When open these channels participate in inflammatory processes. A decrease in lobular inflammation and oxidative stress was observed in mice with pannexin deletion. However, in this study a different gene expression profile was observed in pannexin deficient animals, particularly affecting lipid metabolism and genes involved in the inflammatory and oxidative stress response, suggesting that more experiments focussed on specifically blocking pannexins without modifying gene expression need to be performed. Interestingly, at a cellular level, pannexins contribute to ATP release, which functions as a pro-inflammatory signal for recruitment and activation of inflammatory cells in lipoapoptosis. Overall, these studies suggest that improving GJ permeability, or blocking hemichannels either constituted by Cxs or pannexins may represent relevant therapeutic targets.
Hepatocellular carcinoma
The ability of GJs to regulate cellular proliferation[131], [132] supports the idea that these channels could be involved in cancer pathophysiology. In addition, there is evidence based on experimental studies suggesting a possible role of GJs in liver carcinogenesis. Targeted disruption of the Cx32 gene was associated with an increase in hepatic tumours, possibly because of a reduction in the propagation of apoptotic signals to adjacent cells.[133], [134], [135] In keeping with this and further supporting the idea that Cxs may show tumour suppressive properties, both Cx26 and Cx32 expression are decreased in HCC while a mislocalization (and dysfunction) of the Cxs from the cell membrane to the cytoplasm has also been observed.[136], [137], [138], [139], [140] In HCC tissues, a reduction in the expression of Cx32 was associated with larger more aggressive tumours, vascular invasion, and poorer survival. Thus, experiments exploring the potential benefit of GJ opening drugs should be explored. Concerning this observation, doxorubicin resistant HCC cell lines showed reduced expression of Cx32. By contrast, overexpression of Cx32 resulted in increased sensitivity of HCC cells to the chemotherapy drug, supporting the hypothesis that Cx32 could be also an important target for counteracting drug resistance of HCC.[141], [142] More recently, sorafenib, an oral multikinase inhibitor approved for advanced HCC, was shown to be more efficacious after increasing GJ intercellular communication with all-trans retinoic acid. This effect was abolished after co-incubation with GJ inhibitor 18-alpha glycyrrhetinic acid and oleamide.[42], [142]
In an apparent contradiction, the observation that Cx43 expression is increased in HCC cells suggests that Cx43 may possibly have oncogenic properties instead of suppressing tumorigenesis.[143], [144], [145], [146] In fact, the magnitude of expression of Cx43 and its localization correlated with the malignant potential, migration, invasive capacity and metastatic ability of HCC. However, an alternative explanation could be that the increased expression of Cx43 is a compensatory response to mislocalization of Cx43 as has been postulated to occur in breast cancer. Additional studies are needed to elucidate the exact role of Cx43 in hepatocarcinogenesis.
Conclusions
Financial support
Dr. M. Hernández-Guerra is the recipient of a Grant from Instituto de Salud Carlos III (PI14/01243). This work was supported by a grant for MHG from the Asociación Española para el Estudio del Hígado (AEEH) and Fundación Canaria Doctor Manuel Morales.
Conflict of interest
Authors’ contributions
Acknowledgements
Anatomy and physiology of pain
Nerve injury increases GJ expression in sensory ganglia
Chronic pain can result from a number of distinct types of insult, including diabetes, multiple sclerosis, chronic inflammation and from nerve lesion. Early reports in invertebrates and in rat spinal cord showed that nerve section resulted in transient changes in electrical coupling among the injured motoneurons (e.g., [8], [9]). However, it was a great surprise that astrocytes were similarly affected. Nerve transection upregulated Cx43 in the ipsilateral facial nucleus in rats ([10]; this upregulation was rapid, occurring within 45–90min after lesion) [11].