Retrograde trafficking of VMAT2 and its role in protein stability
in non-neuronal cells
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Graphical Abstract
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Abstract
Increasing evidence suggests that the impaired neuroprotection of vesicular monoamine transporter 2 (VMAT2)
contributes to the pathogenesis of Parkinson's disease. That has been linked to aberrant subcellular retrograde
trafficking as strongly indicated by recent genomic studies on familial Parkinson's diseases. However, whether
VMAT2 function is regulated by retrograde trafficking is unknown. By using biochemistry and cell biology
approaches, we have shown that VMAT2 was stringently localized to the trans-Golgi network and underwent
retrograde trafficking in non-neuronal cells. The transporter also interacted with the key component of retromer,
Vps35, biochemically and subcellularly. Using specific siRNA, we further showed that Vps35 depletion altered
subcellular localization of VMAT2. Moreover, siRNA-mediated Vps35 knockdown also decreased the stability of
VMAT2 as demonstrated by the reduced half-life. Thus, our work suggested that altered vesicular trafficking of
VMAT2 may play a vital role in neuroprotection of the transporter as well as in the pathogenesis of Parkinson's
disease.
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