Abstract
The receptor tyrosine kinase KIT plays an important role in development of germ cells, hematopoietic cells, and interstitial pacemaker cells. Oncogenic KIT mutations play an important "driver" role in gastrointestinal stromal tumors, acute myeloid leukemias, and melanoma, among other cancers. Here we describe the crystal structure of a recurring somatic oncogenic mutation located in the C-terminal Ig-like domain (D5) of the ectodomain, rendering KIT tyrosine kinase activity constitutively activated. The structural analysis, together with biochemical and biophysical experiments and detailed analyses of the activities of a variety of oncogenic KIT mutations, reveals that the strength of homotypic contacts and the cooperativity in the action of D4D5 regions determines whether KIT is normally regulated or constitutively activated in cancers. We propose that cooperative interactions mediated by multiple weak homotypic contacts between receptor molecules are responsible for regulating normal ligand-dependent or oncogenic RTK activation via a "zipper-like" mechanism for receptor activation.
| Original language | English |
|---|---|
| Pages (from-to) | 191-201 |
| Number of pages | 11 |
| Journal | Molecular Cell |
| Volume | 57 |
| Issue number | 1 |
| DOIs | |
| State | Published - 8 Jan 2015 |
Bibliographical note
Publisher Copyright:© 2015 Elsevier Inc.
Funding
This work was supported by a grant from Kolltan (to I.L.). The SEC-MALS instrumentation was supported by NIH Award Number 1S10RR023748-01 (to E.F.-S.). We thank the members of the Schlessinger laboratory for valuable discussions and critical comments and Nathan Kucera for his help with manuscript preparation. We also thank the staff of NSLS of X25, X29A, and X6A beamlines.
| Funders | Funder number |
|---|---|
| National Institutes of Health | |
| National Center for Research Resources | S10RR023748 |
