2020
DOI: 10.1016/j.tibs.2019.12.009
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N-Terminal Proteoforms in Human Disease

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Cited by 43 publications
(48 citation statements)
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“…Besides full-length detection, the top-down method has an advantage in detecting PTMs of peptides. The removal of the initiator methionine and N-terminal acetylation is a highly conserved and widespread phenomenon for most proteins that mainly occurs co-translationally [ 25 ]. For example, Ac-GDVEKGKKIFVQK, an N-terminal peptide of IP_571906, was first detected ( Figure 2 c).…”
Section: Resultsmentioning
confidence: 99%
“…Besides full-length detection, the top-down method has an advantage in detecting PTMs of peptides. The removal of the initiator methionine and N-terminal acetylation is a highly conserved and widespread phenomenon for most proteins that mainly occurs co-translationally [ 25 ]. For example, Ac-GDVEKGKKIFVQK, an N-terminal peptide of IP_571906, was first detected ( Figure 2 c).…”
Section: Resultsmentioning
confidence: 99%
“…33,35 The N-term truncation of ERG was proposed as the major mechanism leading to the conformational change and reduced binding of SPOP to the ERG degron. The fact that the N-terminal post-translational modifications could define ERG stability 34,59 encourage us to characterize the N-terminal composition of the endogenous TMPRSS2-ERG fusin protein in VCaP cells. Our SRM measurements of the N-term peptide N-acetyl-TASSSSDYGQTSK revealed that Thr1 and Ser4 were not phosphorylated.…”
Section: Discussionmentioning
confidence: 99%
“…We thus assumed that the N-terminus of ERG could be further modified through acetylation, methionine cleavage, and threonine or serine phosphorylation. Our motivation to reveal the N-terminal identity of ERG stemmed not only from the challenge of detecting a unique fusion peptide, but also from the fact the knowledge on the N-term structure of ERG protein could be useful to elucidate the increased stability of TMPRSS2-ERG fusion protein, 33 and facilitate development of the targeted therapeutic strategies for inhibition or degradation 34 of oncogenic, but not the wild-type ERG forms.…”
Section: Identification Of the N-terminal Peptide Of T1/e4 Tmprss2-ermentioning
confidence: 99%
“…Each individual molecular form of an expressed protein has been called a proteoform. This term captures the disparate sources of biological variation that alter primary sequence and composition at the whole-protein level [ 138 , 139 , 140 ]. The process of identifying aberrantly expressed proteins and disease-associated proteoforms has led to a better understanding of the underlying mechanisms of diseases, particularly tumorigenesis [ 141 ].…”
Section: Immunoaffinity Capillary Electrophoresis Applicationsmentioning
confidence: 99%