Distinct 3-O-sulfated heparan sulfate modification patterns are required for kal-1-dependent neurite branching in a context-dependent manner in Caenorhabditis elegans.

[kallmann syndrome]

Heparan sulfate (HS ) is an unbranched glycosaminoglycan exhibiting substantial molecular diversity due to multiple , nonuniformly introduced modifications , including sulfations , epimerization , and acetylation . HS modifications serve specific and instructive roles in neuronal development , leading to the hypothesis of a HS code that regulates nervous system patterning . Although the in vivo roles of many of the HS modifications have been investigated , very little is known about the function of HS 3 -O-sulfation in vivo . By examining patterning of the Caenorhabditis elegans nervous system in loss of function mutants of the two 3 -O-sulfotransferases , hst-3 .1 and hst-3 .2 , we found HS 3 -O-sulfation to be largely dispensable for overall neural development . However , generation of stereotypical neurite branches in hermaphroditic-specific neurons required hst-3 .1 , hst-3 .2 , as well as an extracellular cell adhesion molecule encoded by kal-1 , the homolog of Kallmann Syndrome associated gene 1 /anosmin-1 . In contrast , kal-1 -dependent neurite branching in AIY neurons required catalytic activity of hst-3 .2 but not hst-3 .1 . The context-dependent requirement for hst-3 .2 and hst-3 .1 indicates that both enzymes generate distinct types of HS modification patterns in different cell types , which regulate kal-1 to promote neurite branching . We conclude that HS 3 -O-sulfation does not play a general role in establishing the HS code in C . elegans but rather plays a specialized role in a context-dependent manner to establish defined aspects of neuronal circuits .