Optogenetic clustering and membrane translocation of the BcLOV4 photoreceptor

Optogenetic clustering is a versatile method to control protein activity in living cells, tissues, and organisms. Here we show that the BcLOV4 photoreceptor both clusters and translocates to the plasma membrane in response to blue light, representing a new class of light-dependent behavior. We demonstrate that dual translocation and clustering can be harnessed for novel single-component optogenetic tools, including for activation of the entire family of epidermal growth factor receptor (ErbB1-4) tyrosine kinases. We further find that clustering and membrane translocation are causally linked. Stronger clustering increased the magnitude of translocation and downstream signaling, increased sensitivity to light by ~3-4-fold, and decreased the expression levels needed for strong signal activation. Thus light-induced clustering of BcLOV4 provides a strategy to generate a new class of optogenetic tools and to enhance existing ones.