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@proceedings{1411821, author = {Gregor, Tomáš and Ryneš, Jan and Trantírková, Silvie and Mayer, Jiří and Krejčí, Pavel and Trantírek, Lukáš}, booktitle = {42nd Congress of the Federation-of-European-Biochemical-Societies (FEBS) on From Molecules to Cells and Back}, keywords = {BCR-ABL; chronic myeloid leukemia}, language = {eng}, title = {Systematic analysis of BCR-ABL interactome in chronic myeloid leukemia}, url = {https://2017.febscongress.org/abstract_preview.aspx?idAbstractEnc=4424170093097092096093424170}, year = {2017} }
TY - CONF ID - 1411821 AU - Gregor, Tomáš - Ryneš, Jan - Trantírková, Silvie - Mayer, Jiří - Krejčí, Pavel - Trantírek, Lukáš PY - 2017 TI - Systematic analysis of BCR-ABL interactome in chronic myeloid leukemia KW - BCR-ABL KW - chronic myeloid leukemia UR - https://2017.febscongress.org/abstract_preview.aspx?idAbstractEnc=4424170093097092096093424170 L2 - https://2017.febscongress.org/abstract_preview.aspx?idAbstractEnc=4424170093097092096093424170 N2 - Chronic myeloid leukemia (CML) is a myeloproliferative cancer that is caused by “Philadelphia chromosome” translocation that results in a formation of fusion protein BCR-ABL. This constitutively active tyrosine kinase is necessary and sufficient to cause CML. Several small molecule tyrosine kinase inhibitors (TKI) targeting BCR-ABL kinase activity had been developed and greatly improved CML prognosis. However, significant number of patients develops resistance to TKIs and relapse. Growing evidence shows the importance of other BCR-ABL interaction partners in CML pathogenesis. Precise elucidation of the interactome can lead to design of conceptually new drug targeting different pathways and overcoming TKI resistance. One of our goals is to elucidate precise binding interface among BCR-ABL and it’s “core complex” interaction partners. Our approach involves use of peptide microarrays, which allow us to map the binding interface with single amino acid resolution. Binding motifs discovered in unstructured parts of BCR-ABL can be used to generate synthetic peptide abolishing particular protein interaction. Furthermore, we created large pallet of BCR-ABL deletion/substitution mutants in order to verify interaction boundaries and co-immunoprecipitation experiments have yielded potential new binding sites for some of the core complex interactors. ER -
GREGOR, Tomáš, Jan RYNEŠ, Silvie TRANTÍRKOVÁ, Jiří MAYER, Pavel KREJČÍ a Lukáš TRANTÍREK. Systematic analysis of BCR-ABL interactome in chronic myeloid leukemia. In \textit{42nd Congress of the Federation-of-European-Biochemical-Societies (FEBS) on From Molecules to Cells and Back}. 2017. ISSN~1742-464X.
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