CCZ1 is a modulator of TPC2 activity and melanoma cell migration

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CCZ1 is a modulator of TPC2 activity and melanoma cell migration

Authors

Yang, Z.; Feldmann, C.; Ouologuem, L.; Lin, A.; Fenske, S.; Michalakis, S.; Bartel, K.; Schaenzler, M.; Grimm, C.; Chen, C.-C.; Wahl-Schott, C.; Biel, M.

Abstract

The small GTPase RAB7a is a key regulator of melanoma progression by enhancing the activity of the endolysosomal two-pore cation channel TPC2. In this study, we demonstrate that CCZ1- a core component of the RAB7a guanine nucleotide exchange factor (GEF) complex- is essential for mediating this RAB7a-dependent enhancement of TPC2. Unexpectedly, we find that constitutively active (GTP-locked) RAB7a fails to bind and regulate TPC2 in the absence of CCZ1, indicating that CCZ1 contributes to the RAB7a-TPC2 interaction through mechanisms beyond its GEF activity. Furthermore, the CCZ1 facilitated GTPase-activating function on RAB5 is dispensable for modulating TPC2. Notably, in the absence of CCZ1, TPC2 exhibits increased affinity for its agonist, PI(3,5)P2, along with markedly upregulated channel activity. In melanoma cell lines, this upregulation enhances migratory capacity. Our findings identify CCZ1 as a functional inhibitor of TPC2 and highlight its critical role in regulating cancer cell migration.

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