1. Academic Validation
  2. SorLA regulates the activity of lipoprotein lipase by intracellular trafficking

SorLA regulates the activity of lipoprotein lipase by intracellular trafficking

  • J Cell Sci. 2011 Apr 1;124(Pt 7):1095-105. doi: 10.1242/jcs.072538.
Stine C Klinger 1 Simon Glerup Merete K Raarup Muriel C Mari Mette Nyegaard Gerbrand Koster Thaneas Prabakaran Stefan K Nilsson Maj M Kjaergaard Oddmund Bakke Anders Nykjær Gunilla Olivecrona Claus Munck Petersen Morten S Nielsen
Affiliations

Affiliation

  • 1 The MIND-Center, Department of Medical Biochemistry, University of Aarhus, Ole Worms Allé 1170, DK 8000 Aarhus C, Denmark.
Abstract

Many different tissues and cell types exhibit regulated secretion of lipoprotein Lipase (LPL). However, the sorting of LPL in the trans Golgi network has not, hitherto, been understood in detail. Here, we characterize the role of SorLA (officially known as SorLA-1 or sortilin-related receptor) in the intracellular trafficking of LPL. We found that LPL bound to SorLA under neutral and acidic conditions, and in cells this binding mainly occurred in vesicular structures. SorLA expression changed the subcellular distribution of LPL so it became more concentrated in endosomes. From the endosomes, LPL was further routed to the lysosomes, which resulted in a degradation of newly synthesized LPL. Consequently, an 80% reduction of LPL activity was observed in cells that expressed SorLA. By analogy, SorLA regulated the vesicle-like localization of LPL in primary neuronal cells. Thus, LPL binds to SorLA in the biosynthetic pathway and is subsequently transported to endosomes. As a result of this SorLA mediated-transport, newly synthesized LPL can be routed into specialized vesicles and eventually sent to degradation, and its activity thereby regulated.

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