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Faster, quantitative, and accurate precursor acquisition independent from ion count.


ABSTRACT: Data-dependent precursor ion selection is widely used in shotgun proteomics to profile the protein components of complex samples. Although very popular, this bottom-up method presents major drawbacks in terms of detectable dynamic range. Recently, we demonstrated the superior performance of a data-independent method we termed precursor acquisition independent from ion count (PAcIFIC). Here, we report a faster, accurate, multiplexed, and quantitative PAcIFIC method. Our results show that the time needed to perform such analysis can be decreased by 33% to 66% using modern ion trap instruments and that high mass accuracy can be applied to such a strategy. Quantification capability is demonstrated on protein standards and a whole bacterial cell lysate using isobaric tagging. Finally, we confirm in yeast the dynamic range capabilities of such a method where proteins down to less than 50 copies per cell can be monitored without sample prefractionation.

SUBMITTER: Panchaud A 

PROVIDER: S-EPMC3217585 | biostudies-literature | 2011 Mar

REPOSITORIES: biostudies-literature

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Faster, quantitative, and accurate precursor acquisition independent from ion count.

Panchaud Alexandre A   Jung Sunhee S   Shaffer Scott A SA   Aitchison John D JD   Goodlett David R DR  

Analytical chemistry 20110222 6


Data-dependent precursor ion selection is widely used in shotgun proteomics to profile the protein components of complex samples. Although very popular, this bottom-up method presents major drawbacks in terms of detectable dynamic range. Recently, we demonstrated the superior performance of a data-independent method we termed precursor acquisition independent from ion count (PAcIFIC). Here, we report a faster, accurate, multiplexed, and quantitative PAcIFIC method. Our results show that the time  ...[more]

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