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Data from Specific Activation of the CD271 Intracellular Domain in Combination with Chemotherapy or Targeted Therapy Inhibits Melanoma Progression

Posted on 2023-04-05 - 17:20
Abstract

CD271 (NGFR) is a neurotrophin receptor that belongs to the tumor necrosis receptor (TNFR) family. Upon ligand binding, CD271 can mediate either survival or cell death. Although the role of CD271 as a marker of tumor-initiating cells is still a matter of debate, its role in melanoma progression has been well documented. Moreover, CD271 has been shown to be upregulated after exposure to both chemotherapy and targeted therapy. In this study, we demonstrate that activation of CD271 by a short β-amyloid–derived peptide (Aβ(25–35)) in combination with either chemotherapy or MAPK inhibitors induces apoptosis in 2D and 3D cultures of eight melanoma cell lines. This combinatorial treatment significantly reduced metastasis in a zebrafish xenograft model and led to significantly decreased tumor volume in mice. Administration of Aβ(25–35) in ex vivo tumors from immunotherapy- and targeted therapy–resistant patients significantly reduced proliferation of melanoma cells, showing that activation of CD271 can overcome drug resistance. Aβ(25–35) was specific to CD271-expressing cells and induced CD271 cleavage and phosphorylation of JNK (pJNK). The direct protein–protein interaction of pJNK with CD271 led to PARP1 cleavage, p53 and caspase activation, and pJNK-dependent cell death. Aβ(25–35) also mediated mitochondrial reactive oxygen species (mROS) accumulation, which induced CD271 overexpression. Finally, CD271 upregulation inhibited mROS production, revealing the presence of a negative feedback loop in mROS regulation. These results indicate that targeting CD271 can activate cell death pathways to inhibit melanoma progression and potentially overcome resistance to targeted therapy.

Significance:

The discovery of a means to specifically activate the CD271 death domain reveals unknown pathways mediated by the receptor and highlights new treatment possibilities for melanoma.

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FUNDING

Associazione Italiana per la Ricerca sul Cancro (AIRC)

Fondazione Umberto Veronesi (Umberto Veronesi Foundation)

Fondazione Telethon (Telethon Foundation)

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AUTHORS (18)

  • Annalisa Saltari
    Andreas Dzung
    Marika Quadri
    Natascia Tiso
    Nicola Facchinello
    Alberto Hernández-Barranco
    Susana Garcia-Silva
    Laura Nogués
    Corinne Isabelle Stoffel
    Phil F. Cheng
    Patrick Turko
    Ossia M. Eichhoff
    Francesca Truzzi
    Alessandra Marconi
    Carlo Pincelli
    Héctor Peinado
    Reinhard Dummer
    Mitchell P. Levesque

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