The small GTPase ARF family member ARL15 gene locus is associated in population studies with increased risk of type 2 diabetes, lower adiponectin and higher fasting insulin levels. Previously, loss of ARL15 was shown to reduce insulin secretion in a human β-cell line and loss of function mutations are found in some lipodystrophy patients. We set out to understand the role of ARL15 in adipogenesis and showed that endogenous ARL15 palmitoylated and localised in the Golgi of mouse liver. Adipocyte overexpression of palmitoylation-deficient ARL15 resulted in redistribution to the cytoplasm and a mild reduction in expression of some adipogenesis-related genes. Further investigation of the localisation of ARL15 during differentiation of a human white adipocyte cell line showed that ARL15 was predominantly co-localised with a marker of the cis face of Golgi at the preadipocyte stage and then translocated to other Golgi compartments after differentiation was induced. Finally, co-immunoprecipitation and mass spectrometry identified potential interacting partners of ARL15, including the ER-localised protein ARL6IP5. Together, these results suggest a palmitoylation dependent trafficking-related role of ARL15 as a regulator of adipocyte differentiation via ARL6IP5 interaction.
Palmitoylated small GTPase ARL15 is translocated within Golgi network during adipogenesis
These authors contributed equally to the work
- Award Group:
- Funder(s): Medical Research Council
- Award Id(s): MC_U142661184
- Funder(s):
- Award Group:
- Funder(s): Tenovus Scotland Grant
- Award Id(s): T16/44
- Funder(s):
- Award Group:
- Funder(s): Wellcome Trust Seed Award
- Award Id(s): 202061/Z/16/Z
- Funder(s):
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- Accepted Manuscript 15 November 2021
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Yixing Wu, Ying Bai, David G. McEwan, Liz Bentley, Dimitra Aravani, Roger D. Cox; Palmitoylated small GTPase ARL15 is translocated within Golgi network during adipogenesis. Biol Open 2021; bio.058420. doi: https://doi.org/10.1242/bio.058420
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