- 作者: Neeraj Jain, Jun Hou Tan, Shijin Feng, Bhawana George and Thirumaran Thanabalu
- 作者服務機構: School of Biological Sciences, Nanyang Technological University, Singapore
- 中文摘要: --
- 英文摘要:
Background:
Mutation in the Wiskott-Aldrich syndrome Protein (WASP) causes Wiskott-Aldrich syndrome (WAS), X-linked thrombocytopenia (XLT) and X-linked congenital neutropenia (XLN). The majority of missense mutations causing WAS and XLT are found in the WH1 (WASP Homology) domain of WASP, known to mediate interaction with WIP (WASP Interacting Protein) and CIB1 (Calcium and Integrin Binding).
Results:
We analyzed two WASP missense mutants (L46P and A47D) causing XLT for their effects on T cell chemotaxis. Both mutants, WASPR L46P and WASPR A47D (S1-WASP shRNA resistant) expressed well in JurkatWASP-KD T cells (WASP knockdown), however expression of these two mutants did not rescue the chemotaxis defect of JurkatWASP-KD T cells towards SDF-1α. In addition JurkatWASP-KD T cells expressing these two WASP mutants were found to
be defective in T cell polarization when stimulated with SDF-1α. WASP exists in a closed conformation in the presence of WIP, however both the mutants (WASPR L46P and WASPR A47D) were found to be in an open conformation as determined in the bi-molecular complementation assay. WASP protein undergoes proteolysis upon phosphorylation and this turnover of WASP is critical for T cell migration. Both the WASP mutants were found to be stable and have reduced tyrosine phosphorylation after stimulation with SDF-1α.
Conclusion:
Thus our data suggest that missense mutations WASPR L46P or WASPR
A47D affect the activity of WASP in T cell chemotaxis probably by affecting the turnover of the protein. - 中文關鍵字: --
- 英文關鍵字: Cell migration, Actin cytoskeleton, Proteosome, Cell polarity, Hematopoietic cell kinase