Affiliation:
1. Department of Cellular, Computational and Integrative Biology—CIBIO, University of Trento, 38123 Trento, Italy
Abstract
Neuroblastoma is among the most common childhood cancers. Neuroblastoma in advanced stages is one of the most intractable pediatric cancers, notwithstanding the recent therapeutic advances. ALK mutations are among the leading cause of hereditary neuroblastoma and account for more than 14% of the somatically acquired alterations. ALK kinase activity is currently one of the main targets for pharmacological strategies. However, evidence from ALK fusion-positive lung cancer studies has shown that resistance to ALK inhibition arises during the therapy, causing a relapse within several years. IgLONs are membrane-bound proteins involved in cell-to-cell adhesion. The expression of the IgLON family results altered in different cancers. We found that the IgLON member Negr1 is downregulated in neuroblastoma. The ectopic overexpression of Negr1 impairs neuroblastoma growth in vitro and in vivo. Negr1 exists as a GPI-anchored membrane-bound protein and as a soluble protein released upon metalloprotease cleavage. We generated and characterized a panel of Negr1-derived peptides. The treatment with Negr1 protein and derived peptides induce ALK downregulation and halt neuroblastoma progression in vitro and in vivo.
Reference56 articles.
1. Mahapatra, S., and Challagundla, K.B. (2021). StatPearls, StatPearls Publishing.
2. Sokol, E., and Desai, A.V. (2019). The Evolution of Risk Classification for Neuroblastoma. Children, 6.
3. The Quest to Develop an Effective Therapy for Neuroblastoma;Bhoopathi;J. Cell Physiol.,2021
4. Bartolucci, D., Montemurro, L., Raieli, S., Lampis, S., Pession, A., Hrelia, P., and Tonelli, R. (2022). MYCN Impact on High-Risk Neuroblastoma: From Diagnosis and Prognosis to Targeted Treatment. Cancers, 14.
5. Neuroblastoma: A Tough Nut to Crack;Speleman;Am. Soc. Clin. Oncol. Educ. Book,2016