The Cytoplasmic and Transmembrane Domains of the p75 and Trk A Receptors Regulate High Affinity Binding to NGF

Ligand-induced receptor oligomerization is an established mechanism for receptor tyrosine kinase activation. However, numerous receptor tyrosine kinases are expressed in multicomponent complexes with other receptors that may signal independently or alter the binding characteristics of the receptor tyrosine kinase. NGF interacts with two structurally unrelated receptors, the Trk A receptor tyrosine kinase and p75, a TNF receptor family member. Each receptor binds independently to NGF with predominantly low affinity (Kd=10-9M), but produce high affinity binding sites (Kd=10-11M) upon receptor co-expression. Here we provide evidence that the number of high affinity sites is regulated by the ratio of the two receptors, and by specific domains of Trk A and p75. Co-expression of Trk A containing mutant transmembrane or cytoplasmic domains with p75 yielded reduced numbers of high affinity binding sites. Similarly, co-expression of mutant p75 containing altered transmembrane and cytoplasmic domains with Trk A also resulted in predominantly low affinity binding sites. Surprisingly, extracellular domain mutations of p75 that abolished NGF binding still generated high affinity binding with Trk A. These results indicate that the transmembrane and cytoplasmic domains of Trk A and p75 are responsible for high affinity site formation and suggest that p75 alters the conformation of Trk A to generate high affinity NGF binding. by gest on Sptem er 1, 2017 hp://w w w .jb.org/ D ow nladed from