CGC Bibliography Paper 5014

UNC-16, a JNK-signaling scaffold protein, regulates vesicle transport in C. elegans.

Byrd DT, Kawasaki M, Walcoff M, Hisamoto N, Matsumoto K, Jin Y

Medline:
11738026
Citation:
Neuron 32: 787-800 2001
Type:
ARTICLE
Genes:
jkk-1 jnk-1 klc-1 klc-2 sek-1 unc-16 unc-104 unc-116 nDf40 qDf2 sDf110 sDf127
Abstract:
Transport of synaptic components is a regulated process. Loss-of-function mutations in the C. elegans unc-16 gene result in the mislocalization of synaptic vesicle and glutamate receptor markers. unc-16 encodes a homolog of mouse JSAP1/JIP3 and Drosophila Sunday Driver. Like JSAP1/JIP3, UNC-16 physically interacts with JNK. and JNK kinases. Deletion mutations in Caenorhabditis elegans JNK and JNK kinases result in similar mislocalization of synaptic vesicle markers and enhance weak unc-16 mutant phenotypes. unc-116 kinesin heavy chain mutants also mislocalize synaptic vesicle markers, as well as a functional UNC16::GFP. Intriguingly, unc-16 mutations partially suppress the vesicle retention defect in unc-104 KIF1A kinesin mutants. Cur results suggest that UNC-16 may regulate the localization of vesicular cargo by integrating JNK signaling and kinesin-1 transport.