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Identification of SUMO-2/3-modified proteins associated with mitotic chromosomes. | LitMetric

AI Article Synopsis

  • - Sumoylation is crucial for mitosis, but many protein targets and their functions are still unclear; this study focuses on understanding SUMO-2/3 localization in mitotic chromosomes.
  • - The researchers identified 149 substrates associated with SUMO-2/3 using advanced purification methods, with about one-third linked to mitosis, including proteins related to centromeres and kinetochores.
  • - Their findings highlight sumoylation's role in regulating chromatin structure and identified over 30 proteins involved in chromatin modification, while also presenting new methodologies for studying sumoylated proteins.

Article Abstract

Sumoylation is essential for progression through mitosis, but the specific protein targets and functions remain poorly understood. In this study, we used chromosome spreads to more precisely define the localization of SUMO-2/3 (small ubiquitin-related modifier) to the inner centromere and protein scaffold of mitotic chromosomes. We also developed methods to immunopurify proteins modified by endogenous, untagged SUMO-2/3 from mitotic chromosomes. Using these methods, we identified 149 chromosome-associated SUMO-2/3 substrates by nLC-ESI-MS/MS. Approximately one-third of the identified proteins have reported functions in mitosis. Consistent with SUMO-2/3 immunolocalization, we identified known centromere- and kinetochore-associated proteins, as well as chromosome scaffold associated proteins. Notably, >30 proteins involved in chromatin modification or remodeling were identified. Our results provide insights into the roles of sumoylation as a regulator of chromatin structure and other diverse processes in mitosis. Furthermore, our purification and fractionation methodologies represent an important compliment to existing approaches to identify sumoylated proteins using exogenously expressed and tagged SUMOs.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4445636PMC
http://dx.doi.org/10.1002/pmic.201400400DOI Listing

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