Projektdaten

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Development of parallel accumulation – serial fragmentation (PASEF) acquisition modes on a trapped ion mobility (TIMS) mass spectrometer

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Most targeted therapeutics aim to alter the activity of proteins. To better understand how leukemia cells react to these drugs, we aim to develop a scalable and sensitive mass spectrometry-based phosphoproteomics platform that enables time- and dose-dependent drug response profiling. Quantifying drug-dependent signalling pathway engagement on a proteome-wide scale could help elucidating molecular response and resistance mechanisms.