Autores: Gabriela Souza Chmieleski, Laura Sterian Ward, Natássia Elena Búfalo.

Instituição: Universidade Estadual de Campinas (UNICAMP), Campinas - SP.

DOI: https://doi.org/10.25248/anais.e8232.2021.

Referências

BOISSAN M, et al. The NDPK/NME superfamily: state of the art. Laboratory Investigation, 2018; 98: 164-174.

KHAN I, et al. The relationship of NM23 (NME) metastasis suppressor histidine phosphorylation to its nucleoside diphosphate kinase, histidine protein kinase and motility suppression activities. Oncotarget, 2018; 9: 10185-10202.

LIU L, et al. Prognostic value and clinicopathologic significance of nm23 in various cancers: a systematic review and meta-analysis. International Journal of Surgery, 2018; 60: 257-265.

MÁTYÁSI B, et al. The Function of NM23-H1/NME1 and Its Homologs in Major Processes Linked to Metastasis. Pathology & Oncology Research, 2020; 26: 49-61.

WANG Y, et al. NME1 Drives Expansion of Melanoma Cells with Enhanced Tumor Growth and Metastatic Properties. Mol Cancer Res, 2019; 17:1665-1674.

YU L, et al.The Multiple Regulation of Metastasis Suppressor NM23-H1 in Cancer. Life Sciences, 2021; 268: e118995