# Gap Junction–Mediated Communication in Melanoma: From Tumor Progression to Treatment Response

**Authors:** Juliana Massoud, Sarah Ibrahim, Madison Jensen, Michael C. Beary, Ben Nafchi, Michael Springer, Shoshanna N. Zucker

PMC · DOI: 10.3390/ijms27062705 · International Journal of Molecular Sciences · 2026-03-16

## TL;DR

This review explores how gap junction proteins, called connexins, play a dual role in melanoma progression and could be potential targets for new treatments.

## Contribution

The paper provides a comprehensive overview of how connexins function differently at various stages of melanoma, suggesting their potential as biomarkers and therapeutic targets.

## Key findings

- Connexins act as tumor suppressors in early-stage melanoma but promote metastasis in late-stage disease.
- Cx43 and Cx26 are key connexin isoforms involved in skin function and melanoma progression.
- Stage-related changes in connexin expression could lead to new therapeutic strategies with reduced toxicity.

## Abstract

Melanoma is a highly malignant neoplasm of the skin with early metastatic spread and increasing incidence worldwide. Although there are significant therapeutic advances in immunotherapy, especially with the checkpoint inhibitors targeting PD-1 and CTLA-4, challenges such as treatment-related toxicities, a heterogeneous response to therapy, and drug resistance continue to exist. There are unmet needs for novel therapeutic strategies and/or approaches to complement the existing treatment options. Potential targets for future melanoma treatment are the gap junction proteins, connexins, which show an altered pattern of regulation during melanoma progression. In this review, we highlight the regulation of gap junctions during melanoma progression and the characterization of gap junctions as tumor suppressors during early-stage tumor development and then the reversion to enhancers of tumor metastasis during late-stage melanoma progression. We provide a comprehensive overview of gap junctions in the skin and how the connexin proteins, which comprise gap junctions, are alternatively regulated in melanoma progression. Connexins are protein channels in the human body that consist of 21 isoforms. These isoforms form gap junctions that provide important intercellular signaling and permeability channels. Each connexin protein consists of four transmembrane domains and a C-terminal tail, which is an important part of its function and regulation. Permeants of gap junctions include signaling molecules such as cyclic AMP and inositol triphosphate which are linked to key cellular behaviors such as proliferation and migration, making them essential for several tumor-related processes. At least ten connexin isoforms are found in normal skin. Connexin 43 (Cx43) is classified as the most prevalent isoform while Connexin 26 (Cx26) has been reported to be more specialized with restricted expression patterns. Cx43 and Cx26 regulate the growth, differentiation, and repair of the epidermis after injury. Evidence suggests that connexins have a stage-related function in melanoma. Loss of connexin expression and gap junctional intercellular communication is linked to tumor suppression and loss of differentiation in early-stage melanoma, while re-expression or overexpression of specific connexins, notably Cx43, may promote metastasis through enhanced tumor–stromal interactions and increased motility in late-stage melanoma. Such opposing actions of connexins support their candidacy as biomarkers and therapeutic targets. Understanding the dual-stage related functions of connexins in melanoma development and progression may lead to less cytotoxic and more efficient future therapeutic approaches.

## Linked entities

- **Genes:** GJA1 (gap junction protein alpha 1) [NCBI Gene 2697], GJB2 (gap junction protein beta 2) [NCBI Gene 2706]
- **Proteins:** GJA1 (gap junction protein alpha 1), GJB2 (gap junction protein beta 2)
- **Chemicals:** cyclic AMP (PubChem CID 6076), inositol triphosphate (PubChem CID 55310)
- **Diseases:** melanoma (MONDO:0005105)

## Full-text entities

- **Genes:** GJB2 (gap junction protein beta 2) [NCBI Gene 2706] {aka BAPS, CX26, DFNA3, DFNA3A, DFNB1, DFNB1A}, PDCD1 (programmed cell death 1) [NCBI Gene 5133] {aka ADMIO4, AIMTBS, CD279, PD-1, PD1, SLEB2}, GJA1 (gap junction protein alpha 1) [NCBI Gene 2697] {aka AVSD3, CMDR, CX43, EKVP, EKVP3, GJAL}, CTLA4 (cytotoxic T-lymphocyte associated protein 4) [NCBI Gene 1493] {aka ALPS5, CD, CD152, CELIAC3, CTLA-4, GRD4}
- **Diseases:** metastasis (MESH:D009362), toxicities (MESH:D064420), Tumor (MESH:D009369), Melanoma (MESH:D008545), skin (MESH:D012871)
- **Chemicals:** cyclic AMP (MESH:D000242), inositol triphosphate (-)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Full text

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## Figures

2 figures with captions in the complete paper: https://tomesphere.com/paper/PMC13026816/full.md

## References

69 references — full list in the complete paper: https://tomesphere.com/paper/PMC13026816/full.md

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Source: https://tomesphere.com/paper/PMC13026816