Junctional Adhesion Molecule-C expression specifies a CD138low/neg multiple myeloma cell population in mice and humans.
Andreas BrandlAntonio SolimandoZeinab MokhtariPaula TabaresJuliane MedlerHannah ManzMatteo Claudio Da ViaGiorgio Alberto CrociMiriam KurzwartSina ThusekTheresa SchneiderRegina EbertFranz JakobHermann EinseleAndreas BeilhackPublished in: Blood advances (2021)
Deregulation such as overexpression of adhesion molecules influences cancer progression and survival. Metastasis of malignant cells from their primary tumor site to distant organs is the most common reason for cancer-related deaths. Junctional adhesion molecule (JAM)-C, a member of the Ig-like JAM family, can homodimerize and aid cancer cell migration and metastasis. Here we show that this molecule is dynamically expressed on multiple myeloma (MM) cells in the marrow and co-localizes with blood vessels within the bone marrow of mice and humans. Additionally, JAM-C upregulation inversely correlates with the downregulation of the canonical plasma cell marker CD138 (syndecan-1), whose surface expression has recently been found to dynamically regulate a switch between MM growth in situ and MM dissemination. Moreover, targeting JAM-C in a syngeneic in vivo MM model ameliorates MM progression and improves outcome. Overall, our data demonstrate that JAM-C might serve not only as an additional novel diagnostic biomarker but also as a therapeutic target in MM disease.
Keyphrases
- cell migration
- multiple myeloma
- poor prognosis
- bone marrow
- papillary thyroid
- cell proliferation
- single cell
- signaling pathway
- biofilm formation
- cell therapy
- induced apoptosis
- cell cycle arrest
- mesenchymal stem cells
- squamous cell
- young adults
- squamous cell carcinoma
- escherichia coli
- oxidative stress
- cell death
- childhood cancer
- cancer therapy
- staphylococcus aureus
- candida albicans
- drug delivery
- artificial intelligence
- cell adhesion
- cystic fibrosis