Your search keyword '"Ahlf DR"' showing total 4 results

1. Developing top down proteomics to maximize proteome and sequence coverage from cells and tissues.

Author

Ahlf DR, Thomas PM, and Kelleher NL

Subjects

Animals, Chromatography, Liquid, Electrophoresis, Humans, Mass Spectrometry, Molecular Weight, Proteome chemistry, Proteome analysis, Proteomics methods

Abstract

Mass spectrometry based proteomics generally seeks to identify and characterize protein molecules with high accuracy and throughput. Recent speed and quality improvements to the independent steps of integrated platforms have removed many limitations to the robust implementation of top down proteomics (TDP) for proteins below 70 kDa. Improved intact protein separations coupled to high-performance instruments have increased the quality and number of protein and proteoform identifications. To date, TDP applications have shown >1000 protein identifications, expanding to an average of ∼3-4 more proteoforms for each protein detected. In the near future, increased fractionation power, new mass spectrometers and improvements in proteoform scoring will combine to accelerate the application and impact of TDP to this century's biomedical problems., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

2. Evaluation of the compact high-field orbitrap for top-down proteomics of human cells.

Author

Ahlf DR, Compton PD, Tran JC, Early BP, Thomas PM, and Kelleher NL

Subjects

Amino Acid Sequence, Camptothecin pharmacology, Cell Cycle Checkpoints, Cell Line, Tumor, Cellular Senescence, DNA Damage, Humans, Molecular Sequence Data, Peptide Fragments chemistry, Peptide Mapping, Proteome isolation & purification, Proteomics, Reference Standards, Topoisomerase Inhibitors pharmacology, Fourier Analysis, Proteome chemistry, Tandem Mass Spectrometry standards

Abstract

Mass spectrometry based proteomics generally seeks to identify and fully characterize protein species with high accuracy and throughput. Recent improvements in protein separation have greatly expanded the capacity of top-down proteomics (TDP) to identify a large number of intact proteins. To date, TDP has been most tightly associated with Fourier transform ion cyclotron resonance (FT-ICR) mass spectrometry. Here, we couple the improved separations to a Fourier-transform instrument based not on ICR but using the Orbitrap Elite mass analyzer. Application of this platform to H1299 human lung cancer cells resulted in the unambiguous identification of 690 unique proteins and over 2000 proteoforms identified from proteins with intact masses<50 kDa. This is an early demonstration of high throughput TDP (>500 identifications) in an Orbitrap mass spectrometer and exemplifies an accessible platform for whole protein mass spectrometry.

Published

2012

3. Mapping intact protein isoforms in discovery mode using top-down proteomics.

Author

Tran JC, Zamdborg L, Ahlf DR, Lee JE, Catherman AD, Durbin KR, Tipton JD, Vellaichamy A, Kellie JF, Li M, Wu C, Sweet SM, Early BP, Siuti N, LeDuc RD, Compton PD, Thomas PM, and Kelleher NL

Subjects

Alternative Splicing, Cell Line, Cellular Senescence genetics, DNA Damage, Databases, Protein, HMGA1a Protein analysis, HMGA1b Protein analysis, HeLa Cells, Humans, Phenotype, Protein Processing, Post-Translational, Proteolysis, Proteomics instrumentation, Protein Isoforms analysis, Protein Isoforms chemistry, Proteome analysis, Proteome chemistry, Proteomics methods

Abstract

A full description of the human proteome relies on the challenging task of detecting mature and changing forms of protein molecules in the body. Large-scale proteome analysis has routinely involved digesting intact proteins followed by inferred protein identification using mass spectrometry. This 'bottom-up' process affords a high number of identifications (not always unique to a single gene). However, complications arise from incomplete or ambiguous characterization of alternative splice forms, diverse modifications (for example, acetylation and methylation) and endogenous protein cleavages, especially when combinations of these create complex patterns of intact protein isoforms and species. 'Top-down' interrogation of whole proteins can overcome these problems for individual proteins, but has not been achieved on a proteome scale owing to the lack of intact protein fractionation methods that are well integrated with tandem mass spectrometry. Here we show, using a new four-dimensional separation system, identification of 1,043 gene products from human cells that are dispersed into more than 3,000 protein species created by post-translational modification (PTM), RNA splicing and proteolysis. The overall system produced greater than 20-fold increases in both separation power and proteome coverage, enabling the identification of proteins up to 105 kDa and those with up to 11 transmembrane helices. Many previously undetected isoforms of endogenous human proteins were mapped, including changes in multiply modified species in response to accelerated cellular ageing (senescence) induced by DNA damage. Integrated with the latest version of the Swiss-Prot database, the data provide precise correlations to individual genes and proof-of-concept for large-scale interrogation of whole protein molecules. The technology promises to improve the link between proteomics data and complex phenotypes in basic biology and disease research.

Published

2011

4. A robust two-dimensional separation for top-down tandem mass spectrometry of the low-mass proteome.

Author

Lee JE, Kellie JF, Tran JC, Tipton JD, Catherman AD, Thomas HM, Ahlf DR, Durbin KR, Vellaichamy A, Ntai I, Marshall AG, and Kelleher NL

Subjects

HeLa Cells, Humans, Specimen Handling methods, Biomarkers, Tumor analysis, Chemical Fractionation methods, Electrophoresis, Gel, Two-Dimensional methods, Neoplasm Proteins analysis, Proteome analysis, Spectroscopy, Fourier Transform Infrared methods

Abstract

For fractionation of intact proteins by molecular weight (MW), a sharply improved two-dimensional (2D) separation is presented to drive reproducible and robust fractionation before top-down mass spectrometry of complex mixtures. The "GELFrEE" (i.e., gel-eluted liquid fraction entrapment electrophoresis) approach is implemented by use of Tris-glycine and Tris-tricine gel systems applied to human cytosolic and nuclear extracts from HeLa S3 cells, to achieve a MW-based fractionation of proteins from 5 to >100 kDa in 1 h. For top-down tandem mass spectroscopy (MS/MS) of the low-mass proteome (5-25 kDa), between 5 and 8 gel-elution (GE) fractions are sampled by nanocapillary-LC-MS/MS with 12 or 14.5 tesla Fourier transform ion cyclotron resonance (FT-ICR) mass spectrometers. Single injections give about 40 detectable proteins, about half of which yield automated ProSight identifications. Reproducibility metrics of the system are presented, along with comparative analysis of protein targets in mitotic versus asynchronous cells. We forward this basic 2D approach to facilitate wider implementation of top-down mass spectrometry and a variety of other protein separation and/or characterization approaches.

Published

2009