| Literature DB >> 32001092 |
Annelies Bogaert1, Esperanza Fernandez1, Kris Gevaert2.
Abstract
The collection of chemically different protein variants, or proteoforms, by far exceeds the number of protein-coding genes in the human genome. Major contributors are alternative splicing and protein modifications. In this review, we focus on those proteoforms that differ at their N termini with a molecular link to disease. We describe the main underlying mechanisms that give rise to such N-terminal proteoforms, these being splicing, initiation of protein translation, and protein modifications. Given their role in several human diseases, it is becoming increasingly clear that several of these N-terminal proteoforms may have potential as therapeutic interventions and/or for diagnosing and prognosing their associated disease.Entities:
Keywords: N-terminal modifications; N-terminal proteoforms; alternative splicing; alternative translation initiation; protein N termini
Year: 2020 PMID: 32001092 DOI: 10.1016/j.tibs.2019.12.009
Source DB: PubMed Journal: Trends Biochem Sci ISSN: 0968-0004 Impact factor: 13.807