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Sequence analysis of phosphoserine-containing peptides. Modification for picomolar sensitivity.

作者信息

Meyer H E, Hoffmann-Posorske E, Korte H, Heilmeyer L M

出版信息

FEBS Lett. 1986 Aug 11;204(1):61-6. doi: 10.1016/0014-5793(86)81388-6.

Abstract

Sequencing of phosphoserine-containing peptides yields normally no identifiable PTH-derivatives at those positions where phosphoserine is located. Here a new method is described which allows identification of the position of phosphoserine by chemical modification just before sequence analysis. In a one-step microbatch reaction, phosphoserine present in the intact peptide can be transformed quantitatively into stable derivatives such as beta-methylaminoalanine (MAA), S-ethanolcysteine or S-ethylcysteine. These derivatives are detectable during microsequencing with less than 100 pmol peptide using an Applied Biosystems gas-phase sequencer equipped with an on-line PTH amino acid analyzer.

摘要

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